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Livro Cirurgia Blumgarts Surgery of The Liver Biliary Tract and Pancreas William R Jarnagin Et Al Eds 6th Ed 2017
Livro Cirurgia Blumgarts Surgery of The Liver Biliary Tract and Pancreas William R Jarnagin Et Al Eds 6th Ed 2017
ASSOCIATE EDITORS
Peter J. Allen, MD
William C. Chapman, MD, FACS
Michael I. D’Angelica, MD, FACS
Ronald P. DeMatteo, MD, FACS
Richard Kinh Gian Do, MD, PhD
Jean-Nicolas Vauthey, MD, FACS
EDITOR EMERITUS
Leslie H. Blumgart, BDS, MD, DSc(Hon), FACS, FRCS(Eng, Edin), FRCPS(Glas)
VOLUME 1
1600 John F. Kennedy Blvd.
Ste 1800
Philadelphia, PA 19103-2899
Blumgart’s Surgery of the Liver, Biliary Tract, and Pancreas ISBN: 978-0-323-34062-5
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vii
CONTRIBUTORS
viii
CONTRIBUTORS ix
Theresa Pluth Yeo, PhD, MPH, ACNP-BC George Zogopoulos, MD, PhD, FRCS(C), FACS
Co-Director, Jefferson Pancreas Tumor Registry Assistant Professor of Surgery, McGill University
Department of Surgery Hepato-Pancreato-Biliary and Abdominal Organ Transplant
Thomas Jefferson University Hospital; Surgery
Adjunct Associate Professor McGill University Health Centre
Jefferson College of Nursing Montreal, Quebec, Canada
Philadelphia, Pennsylvania
PREFACE
The sixth edition of Blumgart’s Surgery of the Liver, Biliary Tract, to discuss specific topics based not only on the published litera-
and Pancreas is the largest and most ambitious effort in the long ture but on their own views. To that effect, overlap between
history of this textbook and maintains the tradition of embrac- chapters and discussion of controversy was encouraged in order
ing change in order to keep the book relevant to what Dr. Leslie to allow for conflicting points of view.
H. Blumgart established long ago. The initial section of the book remains dedicated to HPB
The sixth edition continues the tradition of using associate anatomy and physiology, with Chapter 2, “Surgical and Radio-
editors to comprehensively cover the extraordinary growth of logic Anatomy of the Liver, Biliary Tract, and Pancreas,” forming
knowledge and advances over the past four years.The associate the backbone of this section. Chapter 2 is one of the most
editors are all world-class experts in the field and bring great important chapters in the entire book and forms the foundation
insight to the book based on personal experience. Dr. Jean- for understanding much of the discussion in the subsequent
Nicolas Vauthey of University of Texas MD Anderson Cancer sections on physiology, molecular biology and immunology,
Center joins Dr. William Chapman of Washington University imaging, and perioperative management. Technical advances
in St. Louis in taking primary oversight of sections dealing in liver, biliary and pancreatic resection, transplantation, and
largely with hepatic resection and transplantation, reflecting the minimally invasive surgery are covered in detail, particularly in
substantial contributions they have made in these areas. My the new chapters “Advances in the Molecular Characterization
colleagues at Memorial Sloan Kettering Cancer are owed a of Liver Tumors” and “Stones in the Bile Duct: Minimally
great debt of gratitude for their great efforts. Drs. Ronald Invasive Surgical Approaches.” Recent advances in the imaging
DeMatteo and Michael D’Angelica once again brought their field are highlighted in Chapter 14, “Emerging Techniques in
expertise to bear in the sections on basic science/physiology and Diagnostic Imaging,” which should be an invaluable resource
biliary tract disease, respectively. Drs. Peter Allen and Richard to those in the field of radiology. We have again included a great
Kinh Gian Do joined the editorship with this edition and made deal of technical detail, which can be viewed with the expanded
substantive improvements in the sections on pancreatic disease list of videos on the Expert Consult website.
and radiology, respectively. In summary, the sixth edition attempts to include all aspects
The current edition reflects the ongoing and major changes of the anatomy, pathology diagnosis, and surgical and non-
in the field of hepatopancreatobiliary (HPB) surgery, including surgical treatments related to HPB disorders. We hope the work
minimally invasive resection techniques, molecular biology of is of value to a wide range of readers, from seasoned HPB
HPB malignancy, and advances in systemic and ablative thera- practitioners to surgical trainees and physicians in related dis-
pies. The organization of the book remains similar to the fifth ciplines. We have expanded our list of contributors in order to
edition; several new chapters have been added while others have ensure the broadest and most contemporary viewpoints possible.
been expanded. We have maintained the general format by I would like to again express sincere thanks to the co-editors
covering all surgical aspects of the management of HPB disor- who have collaborated with me in this project. We hope that the
ders, while the radiologic, endoscopic and other nonsurgical readers find this text to be a valuable resource for many years
approaches are presented in detail and highlighted when they to come.
represent the preferred therapy. As with past editions, contribu- W.R. Jarnagin, MD
tors were chosen largely based on their expertise and were asked New York, 2016
xxv
ACKNOWLEDGMENTS
The Editors are very grateful to our colleagues in surgery and other disciplines who have
contributed to the current edition. Without their enthusiastic support and insightful contri-
butions, often highlighting areas of controversy and differing opinion, this project would
never have been possible. Special thanks to our respective staffs in New York, St. Louis, and
Houston who have assisted in the preparation of this work. Finally, thanks and appreciation
are due to Dee Simpson, Michael Houston, and all of the staff of our esteemed publisher,
Elsevier, for their great support throughout the project.
xxvi
VIDEO CONTENTS
T. Peter Kingham, MD/Video Editor
CHAPTER 2 Surgical and Radiologic Anatomy of the Liver, Biliary • Pedicle Ligation, Right Pedicle
Tract, and Pancreas • Pedicle Ligation, Left Pedicle
• Basic Hepatic Anatomy: Three-Dimensional Model Outflow Control
• Right Hepatic Vein
CHAPTER 6 Liver Regeneration: Mechanisms and Clinical • Left and Middle Hepatic Veins
Relevance • Left Hepatic Vein
• Atrophy/Hyperthrophy Complex of the Liver Parenchymal Transection
• Clamp Crushing
CHAPTER 31 Bile Duct Exploration and Biliary-Enteric • Stapler
Anastomosis • Water Jet
• Exploration of Common Bile Duct Major Hepatic Resections
• Biliary Entreric Anastomosis—Running, Interrupted • Right Hemihepatectomy
• Extended Right Hepatectomy
CHAPTER 33 Cholecystitis • Left Hemihepatectomy
• Mirizzi Syndrome • Extended Left Hepatectomy
Hepatic Tumors
CHAPTER 49 Tumors of the Gallbladder • Enucleation of Benign Hepatic Tumors
• General Principles for Gallbladder and Hilar Cholangiocarcinoma Resection for Biliary Malignancy
• Biliary and Liver Resection for Gallbladder and Hilar Cancer • Left Hepatectomy with En Bloc Resection of the Bile Duct and
Caudate Lobe
CHAPTER 66 Techniques of Pancreatic Resection: • Right Hepatectomy with En Bloc Resection of the Bile Duct
Pancreaticoduodenectomy, Distal Pancreatectomy, Segmental Gallbladder Cancer
Pancreatectomy, Total Pancreatectomy, and Transduodenal • Porta Hepatitis Lymphadenectomy with Bile Duct Preservation for
Resection of the Papilla of Vater Incidental Gallbladder Cancer
• Pylorus-Preserving Pancreaticoduodenectomy for Adenocarinoma • Segmentectomy IVb/V for Gallbladder Cancer
of the Pancreas CHAPTER 104 Resection Technique for Live-Donor Transplantation
• Central Pancreatectomy and Pancreatiocogastrostomy for
Endocrine Tumor • Resection for Living Donor Transplantation: Donor Right
• Distal Pancreatectomy and Splenectomy Hepatectomy Including the MHV
• Ampullectomy for Ampullary Tumors CHAPTER 105 Minimally Invasive Techniques in Hepatic
CHAPTER 67 Minimally Invasive Pancreatic Resectional Resection
Techniques • Laparoscopic Right Hepatectomy
• Laparoscopic Distal Pancreatectomy • Laparoscopic Left Lateral Sectionectomy
• Laparoscopic Pancreaticoduodenectomy CHAPTER 107 Vascular Reconstruction Techniques
CHAPTER 74 Hydatid Disease of the Liver • Reconstruction During Hepatectomy
• Right Hepatectomy and Pericystectomy for Hydatid Disease CHAPTER 108B Segment-Oriented Anatomic Liver Resections
CHAPTER 99 Regional Chemotherapy for Liver Tumors Segmental Resections
• Robotic Hepatic Artery Pump Placement • Left Lateral Sectionectomy, Segments 2 and 3
• Right Posterior Sectionectomy, Segments 6 and 7
CHAPTER 103B Hepatic Resection for Benign Disease and for • Central Hepatectomy, Segments 4, 5, and 8
Liver and Biliary Tumors • Resection of Segment 3
TECHNIQUES OF HEPATIC RESECTION • Caudate Hepatectomy, Segment 1
Inflow Control CHAPTER 116 Orthotopic Liver Transplantation
• Extrahepatic Approach, Right Hepatic Artery and Portal Vein
• Extrahepatic Approach, Left Hepatic Artery and Portal Vein • Orthotopic Liver Transplantation
xxxii
INTRODUCTION
Hepatobiliary and pancreatic surgery:
historical perspective
Leslie H. Blumgart
A cursory examination of the Table of Contents of this book (Celsus, 1935). Celsus lived in the first century and described
reveals how some of the extraordinary achievements of modern symptoms attributable to liver disease. Gallstones were recog-
medical science and clinical practice have been applied to the nized in the embalming of mummies in ancient Egypt. In 1909
management of liver, biliary, and pancreatic disease. The near- a mummy with a preserved liver and a gallbladder containing
miraculous developments in our understanding of the molecu- 30 gallstones was presented to the Museum of the Royal College
lar nature of disease, combined with the wonders of modern of Surgeons in London. This mummy came from Deir-el-Bahn
imaging technology, advances in anesthesiology, and refine- at Thebes and was that of a priestess of the 21st dynasty around
ments in surgical technique, can be so absorbing as to blind a 1500 BCE. Elliot-Smith, an outstanding English anatomist and
contemporary physician to the rich history that lies behind Egyptologist, described the gallbladder as being large and con-
today’s practice. This introductory essay examines the key taining “many spherical calculi.” The specimen was destroyed
achievements of the past, on which the modern practice of liver, by German bombs during World War II, but the description of
biliary, and pancreatic surgery depends. it was accepted as evidence that the gallstones contained therein
were the earliest specimen of such calculi to have survived from
antiquity (1971). Gordon-Taylor, a noted surgical historian in
ANCIENT HISTORY UNTIL THE England, had likewise called attention to the terminal illness of
EIGHTEENTH CENTURY Alexander the Great at the age of 34 (323 BCE) as an example
of fatal biliary tract disease. The description of Alexander’s
“For the King of Babylon stood at the parting of the way, at illness, as recounted by Weigall (1933), suggests that Alexander
the head of the two ways, to use divination: he made his died of complications culminating in peritonitis.
arrows bright, he consulted with images, he looked in the Rhazes (850–923) and Avicenna (980–1037), two Persians,
liver.” wrote on general surgical topics and the nature of disease and
appreciated the gallbladder but lacked knowledge of the
EZEKIEL 21:21
common bile duct. Biliary fistulae were known to have formed
In ancient societies, the priest had the simultaneous duties of after the drainage of an abdominal wall abscess, and it was
divination, protection, and treatment of the ill. For individuals known that individuals with fistulae had a better prognosis than
with the responsibility of divining the future, the liver was of those who had an external communication with the intestines
central importance. As exposed by wounds sustained in combat, (Glenn, 1971).
at sacrificial offerings, and at incisions after death, the liver is Greek academic achievements surpassed that of all other
the most obvious organ in the abdomen and was observed to civilizations until the fifth century BCE. Hippocrates, widely
contain the most blood; because life and blood were perceived acclaimed in medicine then and since that time, recognized the
to be synonymous, the liver was considered the seat of the soul. seriousness of biliary tract disease as evident in the following
A tablet believed to be from the time of Hammurabi (about passage from The Genuine Works of Hippocrates (translated by
2000 BCE), now in the British Museum, names the various parts Adams in 1939): “[I]n a bilious fever, jaundice coming on with
of the liver and indicates the prognostic significance of each rigor before the seventh day carries off the fever, but if it occurs
(Jastrow, 1908). The liver was divided into about 50 portions without the fever, and not at the proper time, it is a fatal
for individual inspection in an effort to overlook as little as symptom.” He also noted that in the case of jaundice, “[I]f the
possible. Such hepatoscopy was widely in vogue over the fol- liver hardens it is a bad sign.”
lowing centuries and was practiced by the Etruscans, as evi- A few centuries after Aristotle recognized jaundice as an
denced by a bronze tablet in a museum at Piacenza depicting element of disease, Galen viewed biliary tract disease as a rec-
the liver, this being strikingly similar to the Babylonian clay ognized clinical entity to be treated successfully in part by diet.
tablet in the British Museum. Although Celsus had drawn attention to the gallbladder and
The Roman Celsus in his text De Medicina, translated by liver in the first century CE, in the second century, Galen was
W.G. Spencer in 1935, mentioned the liver and described its the most noted author of the Greco-Roman age. Galen named
anatomic location: “[T]he liver, which starts from the actual three main organs that govern the body: the heart, the source
partition under the praecordia on the right side, is concave of heat and the principal organ; the brain, the source of sensitiv-
within (that is on the inferior surface) and convex without; its ity for all parts; and the liver, as a principal part of the nutritive
projecting part rests lightly on the stomach and it is divided into organs (Green, 1951). Galen considered jaundice to be due to
four lobes. Outside its lower part, the gallbladder adheres to it” yellow bile flowing into the skin and recognized that although
1
2 Introduction Hepatobiliary and pancreatic surgery: historical perspective
veins traversing the capillaries into the vena cava at a time when
no microscopic studies of the liver had been done (Walker,
1966). Some of his illustrations are remarkably similar to those
of Couinaud (1954, 1957, 1981) and to the images displayed
today in three-dimensionally constructed computed tomogra-
phy (CT) scans. Glisson was one of the great clinical physicians
of all time, yet his name is related to an anatomic structure of
FIGURE 0.3 Giovanni Battista Morgagni (1682–1771), physician.
limited importance.
In the century that followed the time of Harvey, great activ-
ity in publication among individuals engaged in medicine tumor, having arisen in the epigastrium, and being opened,
occurred. As today, senior professors often held opposing opin- either by art or spontaneously discharged cystic calculi at its
ions and expressed their feelings based on fact or fancy with aperture … the first was cured; the second had a fistula left,
equal fervor. In an attempt to select the factual, Morgagni (Fig. by which a thin and chylous kind of liquor, but of a yellow
0.3), senior professor of anatomy and president of the Univer- color, distilled; and the third had an ulcer remain, which with
sity of Padua, published in 1761 an analysis of disease (trans- its sanies discharged bilious calculi at times.
lated by Benjamin Alexander in 1960) under the title Seats and
Causes of Disease, among which are those of the liver and biliary Morgagni, as is evident in his text, presented the matter of
tract. In referring to gallstones, Morgagni analyzed the distribu- biliary tract disease in logical sequence. He considered the
tion of stones in male and female patients, including age, inci- incidence and the population affected in the different decades
dence, and treatment: of the life span. His descriptions of the possible mechanisms by
which calculi might be formed remind one of much of the writ-
[A]s to the lithotomy, which has also lately been thought of, ings today. Finally, he considered therapy under conservative
in the gallbladder, do not be surprised that I made no mention medical management and warned about attempting to treat the
of it above. For in the first place, the pains which were excited condition by operation (Morgagni, 1960).
by gallstones, that were endeavoring to discharge themselves, As outlined by Wood (1979), numerous eponyms currently
are not only brought on by those which come from the cysts used pertain to the names of these early physicians. Johann
but also by those that come from the hepatic duct. In the second Wirsung (1600–1643) also studied in Padua and was the first
place, those cystic stones which are the largest, and on account to dissect the human pancreatic duct and to describe it in a
of which lithotomy seems, to some persons, to be chiefly desir- 1642 letter to Riola, professor of anatomy and botany at the
able, neither endeavor to disengage themselves nor create any University of Paris. Wirsung was subsequently murdered by a
great uneasiness; or at least for the most part. Dalmatian physician, in a dispute probably related to who had
described the duct first (Major, 1954; Morgenstern, 1965).
This is a remarkable analysis recognizing the presence of stones Abraham Vater (1684–1751) was the first to describe the
in the common bile duct and the relatively innocuous nature papilla of the duodenum. In 1720 he wrote that “those double
of the large stone. A further quotation is as follows: ducts (bile and pancreatic ducts) … come together in single
combination” (Boyden, 1936). He described not an ampulla
Last of all, although there were no danger in cutting, can you but an elevation of the mucosa of the duodenum and described
suppose there would be of no great difficulty in healing the the first reported case of an ampulla with two orifices. Likewise,
wound? We have, before our eyes, examples of three women, the duct of Santorini takes its name from the Venetian Giovanni
one of Bologna, of Frankfurt, and of Göttingen, in whom a Domenico Santorini (1681–1737), a brilliant anatomist and
4 Introduction Hepatobiliary and pancreatic surgery: historical perspective
one of the most exact and careful dissectors of his day. While
Vater was describing the tubercle at the confluence of the pan-
creatic and bile ducts, Santorini was relating the first detailed
observation of the orifice of the two ducts (Boyden, 1936). In
observations printed posthumously, Santorini noted a second
pancreatic duct of normal occurrence and named the upper one
the superior pancreatic duct and the lower one the main pan-
creatic duct. It was not until Oddi in 1864, working in Bologna,
rediscovered “Glisson’s sphincter” and did studies in dogs that
the holding quality of the sphincter of the outlet of the choledo-
chus was recognized (Boyden, 1936).
The work of Morgagni was seminal in the understanding of
liver and biliary disease. It started the movement toward ana-
tomic and pathologic appreciation. Belief in the humoral causa-
tion of disease became untenable, and scientific medicine was
launched. The end of the 17th century and the beginning of
the 18th could be said to mark the initiation of modern medical
science.
Direct anastomosis of the pancreatic duct to the gastroin- organ, without touching the duodenum. Codivilla of Italy is
testinal tract followed in the early part of the 20th century, reported to have resected the duodenum and head of the pan-
when Coffey (1909) performed an anastomosis of the tail of the creas and performed a cholecystojejunostomy in 1898, but the
pancreas to the small bowel. Ombredanne (1911) anastomosed patient died in the postoperative period (Codivilla, 1898). The
a pancreatic cyst to the duodenum, and Jedlicka (1923) anas- first surgeon to perform cephalic pancreaticoduodenectomy
tomosed a cyst to the posterior wall of the stomach. Chester- successfully was Kausch, a professor of surgery in Breslau and
man (1943) performed a cystojejunostomy, and König (1946) later in Berlin. On June 15, 1909, he performed a cholecysto-
carried out the same operation to a Roux-en-Y loop of jejunum. jejunostomy on a jaundiced 49-year-old man; on August 21,
Operations for pancreatic tumors were being done at about 1909, Kausch reoperated, performing a posterolateral gastro-
the same time. Ruggi (1890) reported a resection of a large enterostomy and resection of the head of the pancreas with the
lesion of the tail of the pancreas, and Briggs (1890) performed tumor, the pylorus, and the first and second part of the duode-
a similar operation. Biondi (1897) reported resection of a num. He anastomosed the third portion of the duodenum to
tumor arising from the inferior part of the head of the pancreas, the pancreatic stump. Kausch (1912) published a report enti-
and the patient was still alive 18 months later. tled “Cancer of the Duodenal Papilla and Its Radical Treat-
Whipple (Fig. 0.8) and associates (1935) published a tech- ment.” He gathered in that publication all reports that included
nique for cephalic duodenopancreatectomy, done in two stages, excisions of the papilla. Tenani (1922) reproduced this opera-
for cancer of the ampulla of Vater. In the first operation, they tion with success, also in two stages but with one difference:
performed a cholecystogastrostomy and gastroenterostomy. In Tenani performed a choledochojejunostomy, and the patient
the second and subsequent procedure, they resected the head survived 3 years. Kausch and Tenani, although cited by Whipple
of the pancreas with a portion of the duodenum without anas- (1941), are generally ignored in the English and American
tomosis to the stump of the pancreas, which they sutured. literature.
Whipple (1941) subsequently performed this operation in one Pancreatic resection was extended to manage cancers of the
stage and reported 41 cases, with a mortality rate of 27%. common bile duct and of the duodenum. Recognition of endo-
Eventually the technique of this operation was perfected. crine tumors of the pancreas later led to operations for these
Although English-speaking surgeons throughout the world con- conditions. Wilder and colleagues (1927) reported the first case
tinue to call this operation “Whipple’s operation,” the proce- of resection of an insulinoma arising from the islet cells of the
dure had been done many years earlier. pancreas. Mayo operated on a patient in whom he found a
Sauve (1908) reviewed the literature on pancreatectomy and tumor of the pancreas with metastases to the liver, and an
reported that several surgeons had resected small tumors from extract from one of the metastases produced an insulin-type
the head of the pancreas, and larger ones from the body of the reaction when injected into a rabbit. Graham and Hartmann
(1934) reported subtotal pancreatectomy for hypoglycemia,
and total pancreatectomy was performed by Priestley and col-
leagues (1944) for a patient in whom there was proven hyper-
insulinism, but in whom no tumor of the pancreas was evident.
The patient was cured by the operation, and the small tumor
causing the syndrome was discovered during the pathology
examination.
Later, Fallis and Szilagyi (1948) performed total pancreatec-
tomy for cancer in the hope that removal of the whole gland
would reduce rates of morbidity and mortality and perhaps lead
to better results. ReMine and colleagues (1970) and Brooks
and Culebras (1976) adopted this approach, but early sugges-
tions regarding efficacy were not fulfilled, and total pancreatec-
tomy for pancreatic cancer has largely been abandoned. Fortner
(1973) described the even more extensive procedure of regional
pancreatectomy. The operation included an extensive total
pancreatectomy and resection of the pancreatic segment of the
portal vein—and sometimes the hepatic and superior mesen-
teric arteries, if these vessels were invaded by tumor—together
with subtotal gastrectomy and regional lymph node dissection.
Fortner’s results have not been reproduced by others.
Surgery for pancreatitis also developed over the same period,
and the severity of acute pancreatitis was recognized. Ockinczyc
(1933) revealed the frustration of the times in the surgical
management of pancreatitis. He advocated “the use of drainage
of the pancreas and hope.” Because the mortality rate of
emergency surgery reached 78%, the conservative approach to
acute pancreatitis was advocated. Nevertheless, some patients
with acute pancreatitis still came to operation because of the
necessity to treat gallstone-related pancreatitis or to manage
complications, such as abscess and pseudocyst (Cattell &
FIGURE 0.8 Allen O. Whipple (1881–1963), surgeon. Warren, 1953).
Introduction Hepatobiliary and pancreatic surgery: historical perspective 9
The development of intensive care, antibiotics, and better which Prometheus’s liver grew back nightly after the eagle’s
metabolic management of patients with acute pancreatitis led daily and apparently bloodless “resections.” This oft-cited
to improvements in outcome, although the death rates remained myth does not necessarily mean that the ancient Greeks knew
unacceptably high. Ranson and colleagues (1976) and Imrie about liver regeneration; however, more recent evidence pro-
(1978) made important contributions in that they defined the vides dramatic proof of the liver’s power to grow back rapidly
evaluation of the severity of an attack. The surgical treatments (Blumgart et al, 1971).
of abscess and peritonitis were made systematic. The role of Knowledge of the liver’s lobar and segmental structures,
gallstones in acute pancreatitis was defined, particularly by functional reserves, and capacity to regenerate, as well as tech-
Acosta and Ledesma (1974), and endoscopic papillotomy to niques to prevent intraoperative hemorrhage are essential for
extract calculi impacted at the papilla of Vater was also described. major surgical resection. This knowledge also is relevant to
Surgical procedures aimed at the treatment of chronic pan- transplantation, particularly to split-liver homograft transplan-
creatitis had been developing since the beginning of the 20th tation and in the use of living, related donors.
century. As mentioned previously, Coffey (1909) had anasto- Early descriptions of operations on the liver usually con-
mosed the tail of the pancreas to a loop of jejunum, and in cerned complete or partial avulsion of some portion that was
1953, Link reported external drainage of a pancreatic duct in protruding externally as a result of abdominal trauma. Berta in
a patient who lived for a prolonged period but expelled calculi 1716 amputated a portion of liver protruding from the abdomen
periodically from the fistula tract. Roget (1958) described 50 after a wound, and Von Bruns in 1870 (Beck, 1902) removed
cases treated this way, but only a few patients were cured by a lacerated part of the liver of a soldier wounded in battle.
drainage. Doubilet and Mulholland (1948) attempted sphinc- Despite these anecdotal descriptions, true hepatobiliary opera-
terotomy in the treatment of pancreatitis. As a result of the tions were not possible until the advent of anesthesia (Fig. 0.9)
success of cystojejunostomy in the treatment of pancreatic and antisepsis (Lister, 1867a, 1867b; Fig. 0.10). Although
pseudocyst mentioned earlier, Cattell in 1947 used a side-to- Warvi (1945) recounted that Couzins performed a liver resec-
side anastomosis between a loop of jejunum and the pancreatic tion in 1874, Langenbuch (1888) recorded the first planned
duct in an attempt to relieve pain in a patient with cancer of hepatic resection in Germany. In the United States, Tiffany
the head of the pancreas. Subsequently, Longmire and associ- (1890) resected a liver tumor, and Lucke (1891) reported a
ates (1956) carried out end-to-end pancreaticojejunostomy to liver resection for cancer. Keen (1899), in the United States,
a Roux-en-Y loop of jejunum; however, this procedure proved reported 76 liver resections, of which 37 were for benign or
unsuccessful. Du Val (1957) performed a similar operation in malignant tumors.
an attempt to drain the pancreatic duct, but this too was About the time of these surgical developments, Rex (1888)
unsuccessful. and later Cantlie (1897) did detailed anatomic studies of the
Leger and Brehand (1956) and von Puestow and Gillespy liver and its intrahepatic architecture. These studies established
(1958) performed pancreatic ductal drainage in chronic pan- the lobar and segmental structure of the liver and of the Glis-
creatitis patients for the relief of pain. Longitudinal opening of sonian sheath enclosing structures that enter or leave the organ
the pancreactic duct allowed better decompression after anas- at the porta hepatis. They delineated the planes within the
tomosis to a jejunal loop. Mercadier (1964) performed a similar parenchyma of the organ that were relatively devoid of major
operation without the need for splenectomy, and further techni- blood vessels and bile ducts. These descriptions would make
cal variations were introduced more recently by Prinz and possible controlled hepatic resection.
Greenlee in 1981 and by Frey and Smith in 1987. Mallet-Guy
(1952) and Mercadier (1964) performed resection of the left
pancreas for chronic pancreatitis. This approach subsequently
was extended, so that only a small portion of the head of the
pancreas remained. A more modern approach aimed at con-
serving pancreatic parenchyma has since been developed (Beger
et al, 1985) and was further promoted by Buchler and col-
leagues (Di Sebastiano et al, 2007).
Liver Surgery
Liver surgery has evolved from being almost nonexistent to
comprising a repertoire of operations that can safely remove
nearly any amount of liver tissue (Chakravorty & Wanebo,
1987; Fortner & Blumgart, 2001). These operations are now
performed at numerous hospitals and medical centers through-
out the world. Courageous surgeons were enabled by extraor-
dinary developments in anesthesiology, blood transfusion,
infectious disease, and radiologic imaging.
Features of the anatomy and physiology of the liver that
allow major resection were known in ancient times. The struc-
tural arrangement of the liver into lobes was apparent to indi-
viduals preparing animals for food or for ceremony or to those
preparing humans for mummification. Two other properties FIGURE 0.9 The First Operation with Ether, by Robert Cutler Hinckley,
of the liver, functional reserve and rapid regeneration, were 1893. (Courtesy of Boston Medical Library in the Francis A. Countway
suggested by the early Greek mythology of Prometheus, in Library of Medicine.)
10 Introduction Hepatobiliary and pancreatic surgery: historical perspective
FIGURE 0.11 Claude Couinaud (1922–2008), surgical anatomist. FIGURE 0.12 Jean Louis Lortat-Jacob (1908–1992), surgeon.
attention, and many further case reports followed. As recounted mL of blood replacement. The surgical bluntness of this
by Fortner and Blumgart (2001), at the Southern Surgical approach and the absence of the customary surgical principles
Association meeting in the United States on December 10, and techniques precluded widespread acceptance of the tech-
1952, Quattlebaum (1953) described a right hepatic lobectomy nique. Similarly, a prominent figure in the early development of
for hepatoma. The operation had been done about 4 months liver surgery, Brunschwig (1953; Serrea & Brunschwig, 1955)
after that of Lortat-Jacob and Robert. Apparently unaware of advocated nonanatomic resection, but his results—with a very
Quattlebaum’s achievement, and thinking he would be the first high operative mortality rate for so-called simple right lobectomy,
to do a so-called right hepatic lobectomy in the United States, mostly from uncontrolled hemorrhage—led him to accept the
Pack at Memorial Sloan Kettering Cancer Center in New York approach of Lortat-Jacob. Brunschwig’s report of long-term
performed the operation on a 40-year-old woman on December survivors after hepatic resection for advanced cancer challenged
14, 1952 (Pack et al, 1955). the prevailing skepticism about resecting liver tumors.
Pack and colleagues (1962) recognized quickly the oppor- The laparothoracotomy approach of Lortat-Jacob and
tunity to study liver regeneration. Their studies were the first Robert in 1952 quickly became the standard for major hepatic
to describe and document regeneration of the human liver after resection. Opening the chest added operating time and increased
major resection and suggested that complete regeneration morbidity but gave needed exposure to the liver. Later, the
occurs over 3 to 6 months. Later, Lin and Chen (1965) studied introduction of costal arch retractors made thoracotomy exten-
metabolic function and regeneration of the cirrhotic liver and sion obsolete for most hepatic resections. Steps generally con-
found no discernible regeneration after resection. Blumgart and sidered unnecessary, such as T-tube drainage of the common
colleagues (1971) described the speed of liver regeneration as bile duct, were eliminated in the 1970s. Opinions were divided
recovery of liver size within 10 to 11 days after major hepatic in the 1970s and 1980s about the superiority of either intrahe-
resection for trauma. patic or extrahepatic management of the major hepatic veins.
Contrary to the trends toward anatomic precision, Lin Closed drainage was substituted for multiple Penrose drains
(1958) advocated a finger-fracture technique for liver resection, and packing, although these were still advocated by some in
removing a hepatic lobe in 10 minutes with an average of 2000 the 1980s. Many hepatic resections have been done without
12 Introduction Hepatobiliary and pancreatic surgery: historical perspective
drainage, as described by Franco and associates (1989) and laparoscopic liver resection remain under active investigation.
subsequently at Memorial Sloan Kettering Cancer Center by Robotic operative approaches to liver resection have been
Blumgart and colleagues (Fong et al, 1996). devised (Choi et al, 2012).
Methods for anatomically based segmental liver resection
that conserves parenchyma were developed and have proved Liver Tumors
valuable in hepatic resection for tumor. Numerous methods to The management of liver tumors has a relatively short history.
transect the liver parenchyma had been advocated, including After the initial reports of hepatic resection for tumors per-
the knife handle (Quattlebaum, 1953), nitrogen knife (Serrea formed by Langenbuch (1888), Tiffany (1890), Lucke (1891),
& Brunschwig, 1955), electrocautery (Fortner et al, 1978), and Keen (1899), no significant reports were published until
microwave tissue coagulator (Tabuse, 1979), waterjet (Papa- Foster’s review in 1970. He reported a multi-institutional
christou & Barters, 1982), ultrasonic aspiration dissector survey conducted on 296 adults who had liver resection for
(Hodgson & DelGuercio, 1984), and harmonic scalpel; other primary cancer and were followed for at least 5 years or until
techniques are described on an almost daily basis, and simple death. The operative mortality rate was 24%. Foster also
crushing of the liver tissue remains in use by many. studied the records of 115 patients who had undergone hepatic
Bleeding has remained a problem, and preliminary vascular resection for metastatic colorectal cancer. Operative mortality
control is difficult or impossible in some clinical settings. Inflow was 17.3%, and 21% survived for at least 5 years. Hemorrhage
occlusion using the Pringle maneuver for longer than 15 to 20 during operation was still a problem, and the operative mortal-
minutes was considered hazardous. Local and general hypo- ity rate was essentially the same or higher than the cure rate so
thermia was used in an effort to increase the liver’s tolerance of that skeptics remained unconvinced.
the presumed ischemic anoxia associated with the procedure In the 1970s, major hepatic resection for tumors became
(Longmire & Marable, 1961). More complete vascular control more frequent, and this coincided with improvements in anes-
was obtained by Heaney and colleagues (1966), without hypo- thesia, surgical technique, and postoperative support, and sig-
thermia, by employing aortic cross clamping and temporary nificantly, with the development of better imaging modalities.
occlusion of the porta hepatis and vena cava for 24 minutes In the United States, Wilson and Adson (1976), Fortner and
without ill effect. Fortner and colleagues (1971) described colleagues (1974), and Thompson and colleagues (1983) were
isolation-hypothermic perfusion of the liver, making prolonged major figures in this area of endeavor. In Asia, Ong (1977) and
vascular isolation for complicated resections possible. Huguet others were early explorers in the field, and other major centers
and associates (1978) challenged the long-held belief that the made significant technical improvements with encouraging
liver could tolerate only 15 to 20 minutes of normothermic results (Attiyeh et al, 1978; Cady et al, 1979; Starzl et al,
perfusion by extending the period to 65 minutes. This observa- 1975).
tion was subsequently confirmed (Bismuth et al, 1989; Huguet Morbidity and mortality rates decreased dramatically, and
et al, 1992, 1994). As described previously, however, major major centers began to provide encouraging preliminary long-
bleeding during liver resection usually arises from the major term survival figures. As described by Fortner and Blumgart
hepatic veins or vena cava, and development of techniques of (2001), by the 1980s the early reluctance by many surgeons to
low central venous pressure anesthesia during liver resection, accept the therapeutic benefit of hepatic resection for tumors
as first described by Blumgart and colleagues (Cunningham faded before the onslaught of encouraging reports from a
et al, 1994, Melendez et al, 1998), have proved simple and variety of institutions in the United States, Europe, and South-
efficacious and have rendered vascular isolation techniques east Asia.
rarely necessary (Jarnagin et al, 2002). Methods for limiting the extent of the parenchymal transec-
Apart from hepatic resection, many other techniques for the tion developed along with the emergence of surgical resection
enucleation of tumors and of hydatid cysts have been devel- for tumors in cirrhotic and noncirrhotic livers. Although sug-
oped. Garre (1907) had first noted that if he kept close to the gested originally by Pack and Miller (1961) and by McBride
line of the dense membrane around hydatid cysts—so as not to and Wallace (1972), Asian and European surgeons soon
enter the tissues of the liver too deeply, where large vessels may assumed a leadership role in developing isolated segmental
be encountered—it was possible to resect such lesions with resection and described various operations (Bismuth et al,
minimal blood loss. Enucleative techniques are now used by 1982; Hasegawa et al, 1989; Scheele, 1989; Ton, 1979). The
contemporary surgeons, not only for the removal of hydatid development of reliable intraoperative ultrasound allowed
cysts but also for the enucleation of giant hemangiomata (Baer further developments in liver resection (Bismuth et al, 1982;
et al, 1992; Blumgart et al, 2000; Hochwald & Blumgart, Makuuchi et al, 1985), and subsegmental resection was devel-
2000). As described in this book, enucleation also may be used oped. More recently, the segmental approach was reported and
for resection of certain neoplasms of the liver, such as fibronod- popularized in the United States, particularly by Blumgart and
ular hyperplasia. others (Billingsley et al, 1998; DeMatteo et al, 2000). The dif-
The widespread use of laparoscopic cholecystectomy led to ficulty of the approach to the caudate lobe was addressed, and
the development of techniques for laparoscopic resection of the the surgical anatomy and technique for caudate resection,
liver. First used by Gagner and colleagues (1992), laparoscopic either as an isolated segment or in combination with major
partial hepatectomy has been used by many surgeons. Ferzli resections, was described by Blumgart and colleagues (Lerut
and colleagues (1995) and Azagra and colleagues (1996) devel- et al, 1990; Bartlett et al, 1996).
oped the operation for anatomic resection of the left lateral Probes to perform cryosurgical ablation were developed
segment, and most such resections have involved this proce- (Ravikumar & Kaleya, 2000), and cryosurgery-assisted seg-
dure. More recently, major hepatectomy has been performed mental resection has been described (Polk et al, 1995). Radio-
using laparoscopic techniques (Gigot et al, 2002). Experience frequency ablation for liver tumors also has been evaluated
remains limited, however, and the indications and place of (Curley et al, 1999; Wood et al, 2000). Surgeons now perform
Introduction Hepatobiliary and pancreatic surgery: historical perspective 13
controlled tumor ablation or hepatic resection for tumors using The treatment of metastatic liver tumors by hepatic resec-
robotic techniques and refinements in the development of tion was viewed initially as highly dubious. Many regarded the
virtual reality techniques as originally suggested by Marescaux removal of tumor from the liver by hepatic resection as an
and colleagues in 1998 and by Satava and colleagues in 1999 irrational approach. The natural history of colorectal cancer
(Marescaux et al, 1998; Satava, 1999). Image-guided surgery offered the opportunity for resection of liver metastases
opens great possibilities for developments in hepatic surgery in more often than any other cancer in Western countries. The
the future (Lang et al, 2004). multiinstitutional report from Foster (1970) in the United
The evolution of liver surgery for cancer was influenced States suggested a 5 year survival rate of 25%, and multiple
profoundly by the geographic distribution of the disease. Sur- other reports supported that view. However, the question
geons in the United States and Europe were confronted much remained: How long could patients have lived without surgical
more often with metastatic cancer or hepatocellular carcinoma operations?
(HCC) in otherwise normal livers. In the 1980s and early A landmark article from Glasgow (Wood et al, 1976)
1990s, surgeons in the United States had no great drive to described the natural history of colorectal hepatic metastases.
conserve normal liver tissue. By contrast, surgeons in Asia were It was shown that survival depended on the extent of the
confronted frequently with HCC in patients with hepatitis B disease, and that multiple bilobar metastases indicated a much
and cirrhosis of the liver. Estimating the functional reserve of more serious prognosis than single or multiple nodules on one
the cirrhotic liver became a major concern, and methods for side of the liver. In Wood’s study, only one patient survived for
limiting the resection of nontumorous liver were developed. 5 years (1%). It was clear that if the operative mortality rate
Screening programs for the detection of HCC at an early stage declined, as it had in many reported series, the issue was closed.
were a natural corollary. A major study from Blumgart’s group at Memorial Sloan Ket-
Primary liver cancer (HCC) occurs mainly in areas where tering Cancer Center (Fong et al, 1999) described the results
viral hepatitis is endemic. Because of the prevalence of hepatitis in 1001 consecutive patients with a 5 year overall survival rate
B infection in Southeast Asia, most of the initial, significant, of 37% and an operative mortality rate of 3.4%. Five year
published experiences examining the treatment of primary survival reached more than 50% in patients with favorable
HCC are from Southeast Asia. Improved diagnostic and surgi- prognostic factors. Similar results are reported from many insti-
cal approaches in Japan permitted the Liver Cancer Study tutions worldwide. Tumor recurrence with the liver the only
Group of Japan (1990) to report a 5 year survival rate of 57.5% site of recurrence is common, and such hepatic recurrences are
for HCC; a high proportion of the cases were small, encapsu- often amenable to repeated resections, with risks and results
lated tumors. From China, Tang (1993) reported a 5 year similar to those of the initial operation (Elias et al, 1992; Fong
survival rate of 40.2%. et al, 1994; Scheele & Stangl, 2000).
In the West, experience with HCC differed from that More recently, the Memorial Sloan Kettering group reported
reported in the East in material ways: Tumors were generally a series of 1600 patients with metastatic colorectal cancer
large at presentation, the incidence of viral hepatitis was much treated since 1985 (House et al, 2010). They demonstrated an
lower, and many patients did not have underlying cirrhosis. improvement in results over time between 1999 and 2004, with
There were several reports of surgical mortality rates for hepatic a 5 year survival rate of 51% in 563 patients and an operative
resection in cirrhotic patients, ranging from 15% to 100%. In mortality rate of only 1%.
recent years, spread of hepatitis B and hepatitis C has changed Pichlmayr and colleagues (1990) did the first ex situ tumor
the demographics of the disease in the United States and in resection on the liver, removing the liver for bench surgery, then
Western Europe. This change has allowed a much greater surgi- autotransplanting it back into the patient. The liver was pre-
cal experience, and better techniques and improved patient served by hypothermic perfusion, as had been described earlier
selection have led to vastly improved results. Blumgart’s group for the in situ procedure (Fortner et al, 1974). This approach
(Fong et al, 1999) reported a mortality rate of 5% in 100 resec- may prove to have merit in highly selected cases, but it has not
tions, 57 being major resections, in patients with HCC and been accepted generally.
cirrhosis, and a 5-year survival rate of 37% was reported among Although initially completely ineffective, systemic chemo-
patients operated on since 1990. therapy improved dramatically with the development of new
Today the surgical mortality rate in noncirrhotic patients, agents, and its use as a neoadjuvant agent and as adjuvant
even for the most extensive resections, is uniformly less than chemotherapy after resection has been extensively explored.
5% in major centers. The overall 5 year survival rate is approxi- The use of neoadjuvant chemotherapy to convert unresectable
mately 35% in patients with HCC reported from Western tumors to resectable ones was reported by Bismuth and col-
series, in which small HCC is relatively rare (Bismuth et al, leagues (1996), and extensive studies were reported regarding
1986; Ringe et al, 1991). In a study reported by Blumgart and the possible benefits of chemotherapy after hepatic resection
others (Fong et al, 1999), patients who had HCC with a using hepatic arterial infusion of chemotherapy (Kemeny et al,
median tumor size of 10 cm but no cirrhosis had hepatic resec- 1999). Kemeny’s study followed the demonstration in 1982 by
tion with a surgical mortality rate of 3.7% and a 5 year survival Ensminger and colleagues of an implantable pump for hepatic
rate of 42%. Although survival rates have not changed substan- arterial infusion therapy. Others have studied regression of
tially, a great improvement has been seen in rates of morbidity advanced refractory cancer in the liver using isolated hepatic
and mortality. perfusion chemotherapy (Alexander et al, 2000).
In recent years a move toward hepatic transplantation has As described in this book, hepatic resection also has been
been seen in selected patients with small HCCs within a cir- shown to yield satisfactory results in terms of relief of symptoms
rhotic liver. Patients with small HCCs and compromised liver and prolongation of life in the management of hepatic metas-
function seem to be ideal candidates for total hepatectomy and tases from neuroendocrine cancer and sarcoma. Hepatic resec-
allotransplantation. tion for biliary and gallbladder cancer also has developed in a
14 Introduction Hepatobiliary and pancreatic surgery: historical perspective
(1987) reported on another powerful immunosuppressive (1990) were the first to report living-donor liver transplantation
agent, tacrolimus. using segments II and III of the liver; Yamaoka and colleagues
Serious complications of immunosuppressive therapy for (1994) reported using the right lobe of the liver. Use of split-
liver and other organ transplants have been described, includ- liver grafts and living, related donors for grafts of both the right
ing de novo malignancy (Penn, 1988; Penn & Brunson, 1988; and left lobes has been driven by cultural restrictions and by a
Penn & Starzl, 1972). In 1988 Iwatsuki and associates reported shortage of donor organs. This has been a major development,
an overall 54% survival rate of patients at 5 years. Development and the potential for mortality and morbidity not only of recipi-
was rapid, and by 1992, more than 3000 orthotopic liver trans- ents but also of the live donors has remained a major ethical
plantations were done annually in the United States (United concern.
Network for Organ Sharing). Liver transplantation for tumors has evolved considerably in
Total hepatectomy and liver transplantation were initially the field of primary HCC. Although liver resection remains the
disappointing for liver cancer. Iwatsuki and colleagues (1988) treatment of choice for HCC in patients with good liver func-
reported that three of every four patients who lived at least 2 tion, similar patients with compromised liver function and
months after transplantation for cancer had recurrence, and patients with hepatitis C and a small tumor in a portion of the
adjuvant chemotherapy had no demonstrable benefit. Ringe liver geographically unfavorable for resection are now consid-
and associates (1989) reported a 5 year survival rate of 15.2% ered best treated by liver transplantation. Liver transplantation
for such patients, and Calne and colleagues (1986) had similar has come to be a recognized therapy for many patients with
results. The best results and apparent cure were obtained when small HCCs (Bismuth et al, 1999), a wide range of benign
a cancer was an incidental finding in a liver removed for non- disease, and in particular for patients with compromised liver
cancerous disease (e.g., alcoholic cirrhosis). Geevarghese and function as a result of cirrhosis of the liver, Budd-Chiari syn-
associates (1998) reported a 1 year survival rate of 85% and a drome, polycystic liver and kidney disease, sclerosing cholan-
5 year survival rate of 78% for such cases. Liver transplantation gitis, and for patients with a wide variety of other parenchymal
for HCC was transformed with a publication by Mazzaferro and metabolic liver diseases. Liver transplantation for patients
and colleagues (Milan criteria, Mazzaferro et al, 1996), which with hilar cholangiocarcinoma is occasionally indicated, and
showed excellent long-term survival in patients with limited good results have been achieved in selected patients treated
disease and generated the patient selection criteria that are still with aggressive neoadjuvant chemotherapy and radiotherapy
widely used today. (Rea et al, 2005). Some patients with widespread neuroendo-
Current adjuvant chemotherapy may improve the results. crine metastatic disease of the liver may benefit from liver
Olthoff and colleagues (1995) reported a 3 year survival rate of transplantation. Patients with metastatic disease from adeno-
45% using fluorouracil, doxorubicin, and cisplatin, but only carcinoma have had poor results, and transplantation is no
three survivors had cancers larger than 5 cm. Laine and associ- longer used for this indication.
ates (1999) reported five children with advanced hepatoma who In writing this historical account, I have drawn freely on the
were alive at a mean of 4.6 years after transplantation that was work of the following excellent publications: Chakravorty and
preceded by induction chemotherapy. Wanebo (1987), Glenn (1971), Praderi (1982), and Starzl
Improved immunosuppression has allowed surgical tech- (2001). I have no doubt that there will be some inaccuracies
niques to blossom. Bismuth and Houssin (1984) reported and disputed claims as to “firsts,” but I have attempted to relate
reduced-size orthotopic liver grafts in children, and Pichlmayr a fascinating surgical story. I apologize for any disagreement I
and colleagues (1988) reported the use of one donor liver for may ignite.
two recipients (split-liver transplantation). Raia and associates
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CHAPTER 1
Embryologic development of the liver, biliary tract,
and pancreas
Yousef El-Gohary, Kai Zhao, and George K. Gittes
OVERVIEW OF LIVER AND BILIARY derm and the surrounding mesenchyme. The primitive gut
TRACT DEVELOPMENT tube, which is derived from the endodermal germ layer during
gastrulation, is divided into the foregut, midgut, and hindgut
Developmental biologists have often marveled at the enormous domains, each of which gives rise to specialized regions (Grapin-
regenerative capacity of the liver after injury, and such growth Botton, 2005). This specialization is initiated by transcription
represents one of the fastest by mammalian tissues. Presum- factors expressed in different regions (Table 1.1). For example,
ably, this process is based on the recapitulation of embryonic the coexpression of pancreatic and duodenal homeobox gene 1
signals in the liver, but our understanding of the mechanisms (PDX1) and pancreas-specific transcription factor (PTF1A) in
is relatively poor. The liver is considered the largest internal the endoderm gives rise to the pancreas (see Table 1.1;
organ and consists of diverse cell types that arise from various Fig. 1.2) (Grapin-Botton, 2005; Moore-Scott et al, 2007) (see
embryologic origins. It is a vital organ that has an array of Table 1.1). The definitive endoderm is formed at the ventral
diverse functions, including endocrine, exocrine, and essential side of the vertebrate embryo during gastrulation. Evagination
metabolic functions. The two principal cell types of the liver of the endoderm at the anterior end of the embryo generates
are the hepatocytes, which comprise nearly 70% of the mass of the ventral foregut, which will eventually give rise to the liver,
the adult organ and are responsible for the majority of the lung, thyroid, and the ventral pancreas. The dorsal region of
metabolic liver functions, and the cholangiocytes. Both cells are the definitive endoderm develops into the intestines and the
derived from the embryonic endoderm. Other cell types of the dorsal pancreas (see Fig. 1.2).
liver include hematopoietic, Kuppfer, stromal, and stellate This complex dialogue between the endoderm and meso-
cells, which are of mesodermal origin (Fig. 1.1). Despite their derm appears to be critical for the final patterning of the gut
homogenous appearance, hepatocytes do not all function iden- tube, where several signaling pathways have been implicated in
tically; they perform various tasks depending on their physical the regulation of foregut endoderm development, promoting
location within a hepatic lobule, the primary functional unit of organ specification along its anterior-posterior axis for organs
the liver. For instance, periportal hepatocytes are responsible such as the thyroid, lung, liver, and pancreas. The plasticity of
for the urea cycle enzymes, whereas pericentral hepatocytes the endoderm was demonstrated by experimentally recombin-
express glutamine synthase and utilize ammonia to generate ing the posterior mesoderm with early foregut endoderm,
glutamine. Thus, liver development entails not only hepatocyte leading to repression of liver and pancreatic development in
and cholangiocyte differentiation but also cellular differentia- favor of intestinal development (Kumar et al, 2003; Wells &
tion within the hepatocyte population (see Fig. 1.1). Melton, 2000).
During the third week of gestation, liver primordium first Specific signals from the surrounding mesoderm in the
appears as an outgrowth of the ventral foregut endoderm at the foregut region lead to hepatic specification and subsequent
caudal end of the foregut. The proliferation of the epithelial morphogenesis (Gualdi et al, 1996). The molecular pathway
cells in this liver bud leads to its outgrowth and branching into linking endodermal patterning to the initiation of liver and
the surrounding mesenchyme, giving rise to the liver and intra- pancreatic development has been partially elucidated by recent
hepatic biliary tree. As it grows caudally, traversing the septum studies in the Xenopus model, supporting a role for FGF4 and
transversum, the persistent connection between the branching WNT signaling from the posterior mesoderm in inhibiting
epithelium and the foregut develops into the extrahepatic bile foregut fate and promoting hindgut formation; these signals are
ducts and gallbladder (Sadler & Langman, 2006). The bipo- inhibited in the anterior endoderm to allow foregut develop-
tential hepatoblasts eventually differentiate into hepatocytes ment (McLin et al, 2007).
and cholangiocytes. The final liver structure continues to The β-catenin signaling pathway is essential in liver and
develop through the postnatal period. In addition to giving rise pancreas development. Specifically, repression of β-catenin (a
to the liver and biliary tract, the proximal endoderm (foregut) downstream mediator of canonical WNT signaling) in endo-
also gives rise to respiratory epithelium and the glandular cells derm is necessary to initiate reciprocal signaling from the meso-
of the thyroid, thymus, and pancreas due to its pluripotent derm, leading to hepatic induction. This role for β-catenin is
nature (Fig. 1.2). illustrated by the fact that forced β-catenin expression in the
anterior endoderm leads to downregulation of the hematopoi-
ENDODERMAL PATTERNING etically expressed homeobox gene (HHEX) and inhibition of
liver formation, whereas forced repression of β-catenin in the
Embryologically, the liver, biliary tract and pancreas develop posterior endoderm (future hindgut that normally expresses
through a series of reciprocal interactions between the endo- β-catenin) induced ectopic HHEX expression and ectopic liver
17
18 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
bud initiation (McLin et al, 2007). HHEX is a target of et al, 2009); and intestine (ENDOCUT) (Costa et al, 2003).
β-catenin and is one of the earliest foregut markers (Thomas Conversely, inhibiting β-catenin in the posterior mesoderm led
et al, 1998), which is essential for normal liver and ventral to ectopic expression of other liver and pancreas markers
pancreas development in mice (Bort et al, 2004; Keng et al, (FOR1, PDX1, elastase, and amylase) along with the inhibition
2000). In addition to repressing HHEX, β-catenin also down- of the intestinal marker ENDOCUT (McLin et al, 2007).
regulates other foregut markers for liver (FOR1) (Seo Conversely, inhibiting the WNT receptor FZD7 resulted in
et al, 2002); pancreas (PDX1); lung/thyroid (NKX2.1) (Goss loss of the liver primordium in Xenopus embryo. This result
indicates that low levels of WNT signaling are necessary to
maintain foregut fate, with hepatic specification a dynamic
process.
Stem cell
Studies in mouse and chick models demonstrate the need
for FGF2 signals from the cardiogenic mesoderm and bone
morphogenic proteins (BMPs) from the septum transversum
mesenchyme (Rossi et al, 2001; Zhang et al, 2004) for liver
Ectoderm Mesoderm
development. In addition, WNT2b has also been shown to be
Endoderm
Midgut Foregut Hindgut TABLE 1.1 Specialization of the Different Domains of the
Primitive Gut Tube is Initiated by Organ-Specific Transcription
Factors Expressed in Different Regions
Pancreas Lung Gallbladder
Liver Transcription Factor Organ
Notochord
Spinal cord
Forebrain
Pancreas: PDX1
Liver: HHEX
FIGURE 1.2. Schematic representation of the regional specification of the primitive foregut tube (E8.5) with the various transcription factors. WNT
and FGF4 (a fibroblast growth factor) are secreted from the posterior mesoderm in a gradient and repress foregut fate and promote hindgut develop-
ment. WNT and GFG4 inhibition in the anterior endoderm promote foregut fate. (Courtesy Mariam Hobeldin.)
Chapter 1 Embryologic development of the liver, biliary tract, and pancreas 19
an important signal for liver specification in zebrafish (Ober expression was seen (Lee et al, 2005a). This result indicates the
et al, 2006). necessity for FOXA1 and FOXA2 for hepatogenesis. In vivo
Other examples of transcription factors implicated in foregut DNA-binding studies revealed that the liver-specific ALB has
patterning include the HOX genes. HOXD13 is expressed in an important upstream regulatory binding site for FOXA factors
the hindgut of mouse and chick embryos (Dolle et al, 1991; (Bossard & Zaret, 1998; Gualdi et al, 1996). Before FOXA or
Roberts et al, 1995; Yokouchi et al, 1995). Knock out mice GATA4 binding, the ALB gene is transcriptionally silent, with
homozygous and null mutated for HOXD13 develop with a closed chromatin. After binding with FOXA and GATA4, the
hindgut defects (Kondo et al, 1996). Similarly, when HOXD13 chromatin domain is thought to become exposed (Cirillo et al,
is misexpressed in chick embryo midgut mesoderm, hindgut 2002), thus increasing the ability of the gene to be activated. By
features are seen in the midgut epithelium (Roberts et al, 1998). the E9.5 gestation age, other transcription factors CCAAT/
The exact mechanism of HOX genes in inducing endodermal enhancer binding protein-β and nuclear factor 1 bind to sites
patterning remains unknown, as the exact downstream targets adjacent to the FOXA site, and as a result, the albumin gene
are not clear. In addition to HOX genes, retinoic acid signaling becomes active (Zaret, 2002). Therefore, FOXA binding to
has been implicated in this foregut patterning, probably through chromatin is the critical step in hepatic competence by increas-
regulating HOX gene expression. Specifically, retinoic acid sig- ing gene expression and allowing binding of other transcription
naling appears to specify the position of the pancreatic domain factors.
in the foregut of Xenopus, zebra fish, and mice (Chen et al,
2004; Huang et al, 1998; Martin et al, 2005; Stafford et al, Hepatic Induction
2004). Goss and coworkers (2009) demonstrated that WNT2 FGF from the cardiogenic mesoderm and BMPs from the
and WNT2b play an essential role in specifying lung endoderm septum transversum mesenchyme (STM) have been implicated
without affecting the specification of other foregut-derived in the induction of liver fate in mouse and chick embryonic
tissues. WNT2/2b double knock out mutants display complete endoderm. In vitro studies demonstrated that when ventral
lung agenesis. NKX2.1, the earliest known transcription factor foregut and cardiogenic mesoderm were cocultured in the pres-
marker for the developing lung, was also lost from the anterior ence of fibroblast growth factor inhibitors, liver induction was
foregut, confirming the loss of trachea and lung development. inhibited (Jung et al, 1999). Culturing foregut endoderm
Despite our growing knowledge of molecular signals that without the cardiogenic mesoderm in the presence of low con-
govern endodermal patterning of the primitive foregut tube, centrations of exogenous FGF2 (2 to 5 ng/mL) rescued hepatic
most of the pathways remain poorly understood; exactly how gene expression (Jung et al, 1999) and simultaneously sup-
these pathways confer regional identity remains unresolved. pressed the expression of the pancreas program (PDX1)
(Deutsch et al, 2001), whereas a high concentration of FGF2
Hepatic Competence (10 to 500 ng/mL) induced NKX2-1, an early marker for respi-
Hepatic competence, or the ability to form liver from the foregut ratory epithelium, but not albumin gene expression (Serls et al,
endoderm, is considered the first of a two-step process for the 2005). When foregut endoderm was cocultured with noggin
specification of liver in vertebrates. Competence is a prerequi- (NOG), a BMP inhibitor, inhibited hepatic gene induction was
site for the endoderm to respond to specific signals, such as observed, an effect that was reversed when BMP2 or BMP4
FGFs from the surrounding mesoderm, which then leads to the were added. Despite these results, however, embryos that were
second step, the induction of liver-specific genes such as albumin homozygous mutants for BMP4 still exhibited normal hepatic
(ALB), α-fetoprotein (AFP), and hepatocyte nuclear factor 4α gene induction (Rossi et al, 2001; Smith & Harland, 1992).
(HNF4α). This “competence” is facilitated through the FOXA These data indicate that the cardiac mesoderm, a source for
gene transcription factor family that includes FOXA1 and FGF signaling, is crucial for the hepatic induction from the
FOXA2 (forkhead box proteins A1 and A2) and the GATA- ventral foregut endoderm and subsequent morphogenesis,
binding proteins 4 and 6. FOXA gene expression precedes the whereas BMP aides in the process (Fig. 1.3).
induction of the hepatic program by FGF signals in the endo-
derm, and FOXA2 binding reverses chromatin-mediated Morphogenesis of the Hepatic Bud
repression of AFP gene transcription in vitro (Crowe et al, Following hepatic specification (E8.5 to E9.0), the “liver” starts
1999). Deletion of FOXA1 and FOXA2 led to the absence of to express liver-specific genes (ALB, AFP, HNF4α), and even-
liver bud formation with the loss of AFP expression in the tually form the liver bud. Hepatic bud morphogenesis is facili-
ventral foregut, which indicates that hepatic specification had tated by two transcription factors, HHEX (hematopoietically
failed to initiate (Lee et al, 2005a). Similarly, deletion of either expressed homeobox, discussed earlier) (Crompton et al, 1992)
Gata4 or Gata6 in mouse embryos resulted in failed liver expan- and PROX1 (prospero-related homeobox 1) (Oliver et al,
sion, with the hepatic endoderm still expressing hepatic genes 1993). HHEX is expressed in the anterior endoderm at E7.0,
(Watt et al, 2007; Zhao et al, 2005). The forkhead box (FOX) which eventually gives rise to the liver as well as the ventral
proteins are an extensive family of transcription factors that pancreas. HHEX-null embryos grow without a liver or thyroid
share homology with the winged helix/fork head DNA-binding and develop forebrain defects at E11.5; however, evidence of
domains (Kaestner et al, 2000) that play important roles in endodermal epithelial thickening suggests a possible defect in
regulating expression of genes involved in cellular differentia- differentiation as evidence of possible hepatic induction (Mar-
tion, proliferation, transformation, and metabolic homeostasis tinez Barbera et al, 2000).
(Duncan, 2000; Wang et al, 2001; Zaret, 1999). In vitro explant In a separate study on HHEX-null embryos, liver genes ALB
cultures demonstrated that FGF was sufficient to induce ventral and PROX1 were expressed in the ventral foregut endoderm at
foregut endodermal cells to differentiate into hepatoblasts around E8.5, with the thickening of the hepatic endoderm
(Gualdi et al, 1996). However, when FOXA1/FOXA2-deficient region at E9.0 being smaller compared with heterozygote
endoderm was cultured with exogenous FGF2, no liver embryos. In addition, a significantly lower proliferation rate was
20 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
mariam hobeldin
FGF
contribute to hepatic induction and growth. This epithelial-
mesenchymal interaction is essential for liver bud formation,
1 expansion and differentiation. During this phase (E9.5 to E15),
FIGURE 1.3. Schematic for liver ontogeny controlled by factors the liver bud undergoes a tremendous amount of growth and
released from the cardiogenic mesenchyme 1, and septum transversum becomes an important site for hematopoiesis. Signals regulating
mesenchyme (STM, 2, which induce hepatic specification. Signaling this stage arise from both the hepatic mesenchyme and the STM.
molecules (eg, VEGFR2, HGF) and transcription factors (eg, PROX, HLX) These signals include FGF and BMP, which promote liver
from STM and endothelial cells leads to delamination and migration of growth in addition to aiding in hepatic specification. BMP4 is
endodermal cells into the STM to subsequently form the liver bud. BMP,
strongly expressed in the STM and continues to be expressed at
Bone morphogenetic protein; HGF, hepatocyte growth factor; c-MET,
E9.0, during which the liver bud migrates into the STM (Rossi
HGF receptor; VEGFR2, vascular endothelial growth factor receptor 2.
(Courtesy Mariam Hobeldin.) et al, 2001). BMP4-null mutant mice embryos had a delay in the
growth of the liver bud, which indicates that BMP constitutes
an important growth signal for the liver (Rossi et al, 2001).
Another factor that has been implicated in liver growth is
seen in the prospective hepatic domain when compared with HLX, which is expressed prominently in the visceral mesen-
the control group, demonstrated by bromodeoxyuridine (BrdU) chyme (STM), into which the liver will expand (Hentsch et al,
staining, with no evidence apoptosis (Bort et al, 2004). The 1996). HLX-null embryos exhibited severe liver hypoplasia
basal membrane layer, which is rich in laminin, surrounds the without affecting liver specification (Hentsch et al, 1996). A
hepatic endoderm and degrades around E9.0 to E9.5, so that similar finding was observed in embryos that were null mutants
the hepatocytes start migrating into the STM to form the liver for hepatocyte growth factor (HGF) (Schmidt et al, 1995). In
bud. This degradation is facilitated by the hepatoblasts, which contrast to HLX−/− embryos, apoptosis was the underlying
under normal conditions downregulate E-cadherin. However, cause for the severe liver hypoplasia in HGF-null embryos. HGF
in the PROX1-null mutant embryos, the progenitor liver cells is produced by the cells lining the sinusoids, which are of mes-
fail to migrate into the STM as a result of excess E-cadherin enchymal origin, mediating its effects through the c-MET tyro-
and basement membrane proteins laminin and collagen 4. The sine kinase receptor produced by hepatocytes (Schmidt
basal lamina fails to degrade, and the cells remain trapped in et al, 1995). Transforming growth factor-β (TGF-β) signaling
the hepatic diverticulum, with an overall reduction in liver size is also involved in mediating their signals through SMAD2 and
(Sosa-Pineda et al, 2000). The bulk of the liver lobe lacks SMAD3, which translocate to the nucleus to either upregulate
hepatocytes, suggesting that the mesenchymal component con- or downregulate gene expression. Embryos that were heterozy-
tributes most of the liver mass in PROX1-null mutant embryos. gous mutants for SMAD2 and SMAD3 exhibited severe liver
A similar phenotype is seen with ONECUT1 (also called HNF6) hypoplasia as a result of a decrease in β1-integrin expression
and ONECUT2 double mutants, which are required for basal (Weinstein et al, 2001). Intriguingly, this phenotype was rescued
lamina degradation (Margagliotti et al, 2007). Furthermore, a when HGF, a potent hepatotrophic growth factor, was added
pharmacologic inhibition of matrix metalloproteinases (MMPs), to the culture medium. Presumably, this was a result of β1-
extracellular matrix remodeling enzymes usually expressed by integrin expression (Weinstein et al, 2001), which plays an
the hepatoblasts and STM cells, inhibit hepatoblast migration important role in hepatocytic adhesion to the extracellular
in culture (Margagliotti et al, 2008). To further illustrate the matrix; TGF-β and HGF are known to induce β1-integrin
importance of the extracellular matrix in hepatic bud morpho- expression (Kagami et al, 1996; Kawakami-Kimura et al, 1997).
genesis, hepatoblasts deficient in laminin receptor β1-integrin
fail to colonize the liver bud (Fassler & Meyer, 1995). These OVERVIEW OF HEPATOBLAST
β1-integrins are among those that act as receptors for extracel- DIFFERENTIATION
lular matrix proteins, such as laminins and collagens (Hynes,
1992). Hepatoblasts begin to differentiate into mature hepatocytes and
In summary, PROX1 and ONECUT factors are important biliary epithelial cells at about E13.5. Before differentiation, the
in regulating delamination and in controlling hepatoblast hepatoblasts express genes for adult hepatocytes (albumin,
migration through regulating MMPs and hepatoblast interac- HNF4α), biliary epithelial cells (KRT19), and fetal liver (AFP)
tions with the extracellular matrix. Without an appropriate (Lemaigre, 2003; Shiojiri et al, 1991).
extracellular matrix, cell migration into the STM will be Hepatoblasts in proximity to the portal vein form a bilayer
disrupted. architecture and eventually differentiate into biliary epithelial
Chapter 1 Embryologic development of the liver, biliary tract, and pancreas 21
E12 HEPATOBLASTS
AFP/ALB
HNF4
CK19
PORTAL
MESENCHYME IMMATURE IMMATURE
BILE DUCT CELLS HEPATOCYTE
Jagged-1/Notch CK19 ALB
EGF HNF6 HNF4 HNF1α
HGF HNF1β C/EBP
FOXF1
E18
OSM
DEX
HGF
WNT
PERINATAL
mariam hobeldin
FIGURE 1.4. Overview of differentiation of hepatoblasts into mature hepatocytes and bile duct cells. Bipotential hepatoblasts initially express markers
for both hepatocytes (ALB, AFP) and biliary epithelial cells (KRT19). Hepatoblasts in the periportal mesenchymal area upregulate KRT19 and down-
regulate hepatogenic transcription factors (HNF4, CEBP) to form mature biliary epithelial cells, further signaling from the portal mesenchyme (NOTCH,
HGF) and duct remodeling. The rest of the hepatoblasts upregulate hepatogenic factors. Other factors (OSM, dexamethasone) help in maturation of
mature hepatocytes. HGF, Hepatocyte growth factor; EGF, epidermal growth factor; OSM, oncostatin M; DEX, dexamethasone; ALB, albumin;
AFP, α-fetoprotein; HNF, hepatocyte nuclear factor. (Courtesy Mariam Hobeldin.)
cells by upregulating biliary specific cytokeratin-19 (KRT19) are derived from bipotential hepatoblasts that can differentiate
and downregulating the other hepatic genes. This bilayer into either hepatocytes or biliary epithelial cells. This theory is
around the portal vein begins to form focal dilatations incorpo- based on the observation that immature hepatoblasts coexpress
rated into the portal mesenchyme to form intrahepatic biliary markers of both hepatocytes (ALB) and biliary epithelial cells
duct at E17.0 until birth. Areas of the ductal bilayer plate not (KRT19). The biliary specific marker KRT19 becomes strongly
involved in the formation of the ducts progressively regress. expressed at a later gestational age, as the cells become ductal
The remaining hepatoblasts differentiate into mature hepato- cells, whereas other cells transiently express the hepatocyte
cytes, arranged in hepatic chords with the bile canaliculi on the markers ALB and AFP as they develop into mature hepatocytes
apical surfaces (Lemaigre, 2003). In the mature hepatobiliary (Shiojiri et al, 1991). This theory was further supported when
system, the bile is produced by the hepatocytes and is secreted embryonic liver, before the intrahepatic biliary ducts form, was
into the canaliculi, which are connected to the network of transplanted into the testis of syngeneic animals, giving rise to
intrahepatic biliary ducts. The bile then flows to the hepatic both hepatocytes and typical bile ducts (Shiojiri et al, 1991).
ducts, transits through the cystic duct, and is stored in the Suzuki and colleagues (Suzuki et al, 2002) used in vitro studies
gallbladder; eventually, the bile is excreted into the bowel via on hepatic “stem” cells from E13 embryonic livers, identified
the common bile duct. The biliary epithelial cells delineate the with self-renewing capability and multilineage differentiation
lumen of the intrahepatic, extrahepatic biliary tree (hepatic, potential, to demonstrate that these cells could form differenti-
cystic and common bile duct), and the gallbladder (Fig. 1.4). ated hepatocytes, biliary epithelial cells, pancreatic, and intes-
tinal cells.
Biliary Epithelial Cell Differentiation and Formation The first step in triggering the initiation of the transition
of the Ductal Plate from hepatoblast to a biliary epithelial cell is thought to be
The exact origin of the biliary epithelial cells has been greatly facilitated through the ONECUT transcription factor hepato-
debated; however, the popular school of thought is that they cyte nuclear factor 6 (HNF6), which is expressed in the biliary
22 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
epithelial cells of the developing intrahepatic biliary ducts and for the development of organs derived from foregut endoderm
in hepatoblasts, gallbladder primordium, and the extrahepatic such as the pancreas, liver, gallbladder and lung (Kalinichenko
bile ducts (Landry et al, 1997; Rausa et al, 1997). HNF6−/− et al, 2002). FOXF1 expression is restricted to the gallbladder
embryos displayed severe biliary anomalies. Extrahepatically, mesenchyme and STM. In FOXF1+/−embryos, the gallblad-
this mutation resulted in the absence of gallbladder and the der develops severe structural abnormalities with significant
normal bile ducts; instead, there was an enlarged structure reduction in size with reduced mesenchymal cell numbers, an
connecting the liver to the duodenum. Intrahepatically, absent biliary epithelial cell layer, and a deficient external
however, it caused abnormal differentiation of biliary epithelial smooth muscle layer. The reduction in mesenchymal cell
cells, resulting in cholestasis. Closer histologic examination numbers was attributed to the reduction in vascular cell adhe-
revealed an increased number of KRT19-positive cells com- sion molecule and cell adhesion α5-integrin, both of which
pared with control cells at E13.5, with the development of are essential for mesodermal formation (Mahlapuu et al,
abnormal large cysts at E15.5 to E16.5 that contained an epi- 2001; Yang et al, 1993). Defective smooth muscle layer for-
thelium of KRT19-expressing cells. These abnormal cysts are mation was attributed to diminished levels of platelet-derived
similar to those seen in Caroli disease, an autosomal recessive growth factor receptor α, which is essential for smooth muscle
disorder with ductal plate malformation and ectasias. The cell differentiation (Jacob et al, 1994). FOXF1 is not expressed
abnormal increase in KRT-positive cells at E13.5 lacked any in intrahepatic biliary duct mesenchyme in wild-type mice,
proliferative marker, suggesting that they are postmitotic, and no defects were seen in the intrahepatic biliary ducts of
resulting from hepatoblasts that have differentiated toward a FOXF1+/− mice; however, FOXF1 mRNA levels in the liver
biliary lineage prematurely (Clotman et al, 2002). In addition, were increased, suggesting that it may be a compensatory
the excess KRT-positive biliary epithelial cells formed cordlike mechanism to prevent defects in the liver (Kalinichenko et al,
extensions within the liver parenchyma, compared with the 2002). All these suggest that FOXF1 is crucial for the devel-
control group, which is restricted to the vicinity of the portal opment of the extrahepatic biliary duct and gallbladder with
vein. This observation supports the role of HNF6 in control- the mesenchyme playing an essential role in biliary epithelial
ling the differentiation of hepatoblasts into biliary epithelial cell differentiation. The interaction between the biliary epithe-
cells and the morphogenesis of the intrahepatic biliary ducts, lial cell and the extracellular matrix is also thought to contrib-
confining biliary epithelial cells to the periportal area. A ute to biliary epithelial cell differentiation.
similar morphologic defect of intrahepatic biliary ducts was Integrins are membrane receptors for extracellular matrix
observed in HNF1β−/− embryos, which suggests that HNF6 proteins where they play an important role in mediating the
controls intrahepatic biliary duct development via HNF1β interaction between differentiating cells and the extracellular
(Clotman et al, 2002). In contrast to the intrahepatic ducts matrix (Couvelard et al, 1998; Hynes, 1992). Hepatoblasts
that are derived from bipotential hepatoblasts, the cholangio- express integrin heterodimers containing the β1 subunit (α1β1,
cytes that line the extrahepatic bile ducts are derived from the α5β1, α6β1, and α9β1), and when hepatoblasts differentiate
common ventral pancreatobiliary bud. The bile duct fate of into immature intrahepatic biliary epithelial cells while in
these primitive embryonic bud–derived cells is determined by contact with the mesenchyme, the morphology of the integrins
the transcription factor SOX17, which is coexpressed with changes. The primitive intrahepatic biliary epithelial cells
PDX1 in these pancreaticobiliary progenitor cells (Spence et upregulate α6β1 expression and loses α1β1 while acquiring
al, 2009). The cell fate decision between pancreas-lineage several other integrin dimmers not previously expressed on
PDX1-positive cells versus biliary primordium SOX17- hepatoblasts such as α2β1, α3β1, αVβ1, and α6β4 (Couvelard
positive cells is determined by hairy and enhancer of split 1 et al, 1998). Intrahepatic biliary epithelial cells are contacted
(HES1) (see later in the PANCREAS section). Deleting by a basement membrane containing collagen, enactin, and
SOX17 at E8.5 resulted in ectopic expression of pancreatic laminin (Desmet, 1985); however, hepatocytes are surrounded
tissue in the common bile duct with PDX1-positive cells in by the perisinusoidal matrix, which is devoid of laminin or
the liver bud along with the loss of biliary structures. Con- enactin (Schuppan, 1990). The increase in α6β1 expression
versely, overexpression of SOX17 suppressed pancreas devel- along with the acquisition of biliary-specific expression of α2β1,
opment and promoted ectopic biliary-like tissue in the α3β1,and α6β4, which are integrin receptors for laminin, cor-
PDX1-positive domain tissue (Spence et al, 2009). Further- related with the deposition of laminin at the contact points of
more, it has been demonstrated that SOX17 regulates insulin the portal mesenchyme with the ductal plate (Couvelard et al,
secretion postnatally, with the mice becoming prone to devel- 1998).
oping diabetes with the deletion of SOX17 gene in the pan-
creas (Jonatan et al, 2014). Remodeling of the Ductal Plate
With regard to mesenchymal-epithelial induction of liver As mentioned earlier, the double-layered ductal plate around
primordium and gallbladder, studies have suggested that the the portal vein begins to form focal dilatations incorporated
mesenchyme contributes to biliary epithelial cell differentia- into the portal mesenchyme to form intrahepatic biliary ducts,
tion, where differentiation of hepatoblasts into biliary epithe- while the parts of the ductal bilayer plate not involved in the
lial cells was stimulated when cocultured with hepatic or lung formation of the ducts progressively regress. This mechanism
mesenchyme (Shiojiri & Koike, 1997). It was also noted in the of regression is thought to be carried out by apoptosis (Sergi
study of HNF6−/− mice that biliary epithelial cell differentia- et al, 2000; Terada & Nakanuma, 1995). Cell-matrix interac-
tion occurred at the interface between the portal mesenchyme tions are also thought to contribute to the remodeling process.
and the liver parenchyma (Clotman et al, 2002). Tenascin was found to be expressed in the mesenchyme around
A recent study revealed that the forkhead box f1 (FOXF1) the biliary epithelial cells of primitive ducts migrating into the
transcription factor may play an important role in the mesenchyme. In contrast, tenascin was absent in the mesen-
mesenchymal-epithelial signaling, an interface that is required chyme of peripheral ducts (Terada & Nakanuma, 1994).
Chapter 1 Embryologic development of the liver, biliary tract, and pancreas 23
Hepatocyte Differentiation
During later stages of development, hepatocytes undergo a
transition period from a hematopoietic support role to a mature
MATURE adult hepatocyte. This change occurs under the control of the
PERINATAL HEPATOCYTE transcription factor CEBP with HNF4, the latter being a crucial
mariam hobeldin
BILE
factor in hepatocyte differentiation. Loss of HNF4 function led
DUCT to the disruption of the expression of several genes associated
with a mature hepatocyte phenotype. In HNF4−/− mice, hepa-
tocytes failed to express many mature hepatic enzymes and
FIGURE 1.5. Overview of intrahepatic bile duct formation around the lacked normal morphology, leading to low glycogen storage,
portal vein. Hepatoblasts in the portal mesenchyme vicinity begin to disrupted sinusoids, and gap junction disruption. These results
acquire the biliary epithelial cell marker (KRT19) and downregulate demonstrate that HNF4 is essential for liver differentiation.
hepatic genes, first forming a single layer at E14, then a bilayer at E18 Other factors that have been shown to promote hepatocyte
with focal dilatations that eventually form the intrahepatic bile ducts. The differentiation include oncostatin M (OSM), an interleukin-6
rest of the bilayer regresses. (Courtesy Mariam Hobeldin.) (IL-6) family cytokine, HGF, and WNT (Michalopoulos et al,
2003; Tan et al, 2008). Although as discussed earlier in the
chapter, the repression of WNT signaling in the foregut endo-
Tubulogenesis of ductal cells is thought to be contributed derm is necessary for hepatic specification, its role is reversed
by soluble factors secreted from hepatocytes or biliary epithelial at later gestational stages to promoting hepatocyte differentia-
cells. When coculturing human biliary epithelial cells with tion. β-Catenin, a central component of the canonical WNT
hepatocytes, a marked ductular morphogenic response was pathway, is essential for normal development; its aberrant acti-
induced, and the biliary epithelial cells formed well-organized vation in liver was associated with tumors, including hepatic
luminal ducts. This result was reproduced when biliary epithe- adenomas and hepatocellular cancers (de La Coste et al, 1998;
lial cells were grown in a conditioned medium from previous Peifer & Polakis, 2000; Zucman-Rossi et al, 2006). Livers that
hepatocyte and biliary epithelial coculturing (Auth et al, 2001); were deficient in β-catenin displayed decreased numbers of
however, it remains unclear whether soluble factors contribute hepatocytes, with hepatoblasts that lacked maturation, prolif-
to tubulogenesis in in vivo studies (Fig. 1.5). eration, and function (Tan et al, 2008). In addition, CEBPα,
a fundamental regulator of hepatocyte differentiation and mat-
Developmental Relationship Between the Ducts, uration (Tan et al, 2008), was decreased. Also noted in these
Vessels and Mesenchyme of the Portal Tract livers was a complete absence of CK-19–positive intrahepatic
A functional relationship appears to exist between the contents biliary ducts, suggesting that β-catenin may play a role in biliary
to the portal tract (bile duct, hepatic artery, and portal vein) differentiation (Tan et al, 2008). In vitro studies showed that
24 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Branching morphogenesis
mariam hobeldin
Pancreatic bud Salivary gland bud Ureteric bud
FIGURE 1.7. Pancreatic branching morphogenesis is different than in other organ systems, such as lungs, kidneys, and salivary glands, which
branch in a 90-degree pattern to be fully exposed to the mesenchyme. However, the pancreas has an acute branching pattern; thus some areas
are excluded from mesenchymal contact. Mesenchyme contains factors that regulate pancreatic growth and differentiation. (Courtesy Mariam
Hobeldin.)
specification with the transcription factor PDX1, followed by rise to mature islets (Jensen, 2004; Pictet et al, 1972). In a
PTF1A (Grapin-Botton, 2005; Moore-Scott et al, 2007; Sadler similar gestational window, the exocrine pancreatic precursors
& Langman, 2006). The first morphologic evidence of pancreas undergo rapid branching morphogenesis and acinar cell dif-
development is in the form of mesenchymal condensation over- ferentiation (see Fig. 1.7). During this secondary wave of dif-
lying the dorsal aspect of the primitive foregut tube at the level ferentiation, the simple stratified epithelium of the early
of the duodenal anlagen, distal to the stomach. Shortly after, pancreatic bud restructures into a branched network, with pro-
at about E9.5 of gestation in mice and day 26 of gestation in genitor cells becoming segregated to the distal “tips” expressing
humans, the dorsal bud begins to evaginate into the overlying acinar-specific enzymes, with transcription factors including
mesenchyme (Kallman & Grobstein, 1964; Pictet et al, 1972). PTF1A, and proximal “trunks” expressing duct markers such
Approximately 12 hours later in mice, and 6 days after dorsal as SOX9 and endocrine precursor markers such as NEUROG3
bud evagination in humans, the ventral bud begins to arise. (Kesavan et al, 2009; Villasenor et al, 2010). All the various
The morphologic development of the ventral pancreatic bud pancreatic cell types are eventually derived from PDX1+ cells,
is similar to the dorsal pancreas; however, it is markedly differ- whereas cell progenies from NEUROG3-positive cells will
ent at the molecular level. After this initial bud evagination, the delaminate from the main “trunk” and specifically form clusters
pancreatic bud undergoes elongation of the stalk region, a of islet cells. It was originally thought that toward the end of
precursor to the main pancreatic duct and branching morpho- gestation, different transcription factors, such as in PDX1-
genesis of the apical region of the bud. Unlike growth patterns positive, PTF1A-positive, and SOX9-positive cells, become
seen in the developing lung, kidney, and salivary glands, in gradually restricted to β cells, acinar cells, and duct cells,
which the branching morphogenesis undergoes a typical respectively. However, with the advent of lineage tracing experi-
90-degree pattern, the pancreas grows in an acute branching ments using the Cre-LoxP and the new Dre-Rox system, this
pattern that can lead to the exclusion, or “squeezing out,” of has proven not to be the case. For instance, PDX1-positve cells
mesenchyme from between the closely apposed branches of have now been shown to be expressed in pancreatic duct glands
epithelium. This exclusion of mesenchyme may influence (Strobel et al, 2010) (see later) and also give rise to the extra-
epithelial-mesenchymal interactions and lineage selection (Fig. hepatic biliary system (Spence et al, 2009).
1.7). The ventral pancreatic bud, which arises from the base of
the hepatic diverticulum, rotates dorsally, eventually fusing Endodermal Patterning of the Pancreas
with the dorsal pancreatic bud (sixth to seventh week of gesta- As mentioned earlier in the chapter, the pancreas develops
tion in humans, E12 to E13 in mice) contributing to the forma- through an epithelial-mesenchymal interaction. Before this, the
tion of the uncinate process and inferior part of the head of the dorsal foregut becomes competent to receive propancreatic
pancreas, with the rest of the pancreas arising from the dorsal signals from the notochord (FGFs) (Wells & Melton, 2000) and
pancreatic bud. The entire ventral pancreatic bud and the distal from the anterior foregut (retinoic acids and BMPs) (Stafford
part of the dorsal pancreatic duct fuse together to form the main and Prince, 2002; Tiso et al, 2002). The prepancreatic region
pancreatic duct of Wirsung. The remaining proximal part of of the definitive foregut comes into contact with the notochord,
the dorsal pancreatic duct is either obliterated or persists as a whereas the ventral pancreas contacts the lateral plate meso-
small accessory pancreatic duct of Santorini (Sadler & Langman, derm (Kumar et al, 2003).
2006).
During development, the pancreas undergoes a major Dorsal and Ventral Pancreatic Bud Development
amplification of the endocrine cell population through two The notochord is crucial to the development of the dorsal
waves of differentiation: an early primary transition (pre-E13.5 pancreas, where it remains in contact with the dorsal prepan-
in mice), marked by the expression of the homeobox transcrip- creatic endoderm until the paired dorsal aortae fuse in the
tion factor PDX1 at E8.5, followed by the secondary transition midline (≈E8.0). The dorsal pancreas failed to form when
(E13.5 to E16.5 in mice), which is marked by a dramatic the notochord was removed from early chick embryos in vitro
increase in endocrine and exocrine cell differentiation, giving (Kim et al, 1997), but no effect was seen on ventral pancreas
26 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
(Dichmann et al, 2003), while overexpressing BMP4-enhanced pancreatic development. It appears that the downstream factors
ductal cell proliferation (Hua et al, 2006). of NOTCH targets are variably expressed at a certain time in
The intracellular mediators of TGF-β signaling, SMADs, development of the pancreas. The early pattern of downstream
have gained interest among developmental biologists. Specifi- molecules is a key mediator of NOTCH signaling in determin-
cally, the intracellular mediators of TGF-β signaling, SMAD2 ing endocrine versus exocrine differentiation of progenitor cells
and SMAD3, along with their inhibitor SMAD7, have been and in maintaining a stem cell state in some progenitor cells.
found to play an intricate role in regulating pancreatic endo- Later in gestation, the downstream molecules for NOTCH
crine maturation and development. Genetic inactivation of signaling change to foster cell maturation and differentiation
SMAD2 and SMAD3 led to both a significant expansion of the beyond this initial lineage decision between endocrine and exo-
embryonic endocrine compartment and a more robust islet crine differentiation.
proliferation in adult mouse pancreas after partial pancreatec-
tomy. Whereas genetic inactivation of SMAD7 led to a signifi- HEDGEHOG Signaling
cant decrease in the endocrine compartment with little β-cell As mentioned earlier, SHH suppression in the prospective pan-
proliferation after pancreatectomy in the adult mouse pancreas creatic endoderm is a prerequisite need for pancreas formation;
(El-Gohary et al, 2013; El-Gohary et al, 2014). Furthermore, however, HEDGEHOG signaling in pancreatic development
SMAD4 was specifically identified to be mutated in 50% of appears to be complex. SHH-null mutant mice do not exhibit
pancreatic cancers (Hahn et al, 1996). However, a key role for an expanded pancreatic field; in contrast, Indian Hedgehog
SMAD4 has not been identified yet in pancreatic development (IHH)-null mutant mice develop with a small pancreas, indicat-
(Bardeesy et al, 2006; Simeone et al, 2006). These results ing a propancreatic role for IHH (Hebrok et al, 2000). However,
identify the SMAD2/3/7 network as a legitimate target for regu- when combining a SHH-null mutation with a heterozygous
lating β-cell proliferation, and for generating more β-cells for mutation for IHH, an annular pancreas develops. Mice that are
future treatment of diabetes. null mutants for Hedgehog Patched receptor Ptc lack PDX1
and glucagon expression at E9.5, supporting the need to sup-
NOTCH Signaling press SHH for early pancreatic development (Hebrok et al,
A key step in pancreatic development is the lineage decision by 2000). Similarly, transgenic overexpression of SHH or IHH
pancreatic progenitor cells between the endocrine and exocrine under PAX4 promoter led to significant decrease in endocrine
lineage. NOTCH signaling has been identified as a master and exocrine tissue mass (Smith et al, 2000). Furthermore,
regulator of this fate decision switch (Apelqvist et al, 1999). a novel and distinct anatomic compartment has been described
However, the exact mechanism for NOTCH signaling in pan- within the pancreatic ducts, known as the pancreatic
creatic lineage selection remains elusive, and ambiguity still duct glands (McMinn and Kugler, 1961; Strobel et al, 2010;
surrounds the exact role of NOTCH signaling through Wilcox et al, 2013) (Fig. 1.8). They are present throughout the
A B
C D
FIGURE 1.8. A, Whole-mount image of the main common pancreatic duct containing the pancreatic duct glands (PDGs). Stained with Dolichos
Biflorus Agglutin (DBA), with a higher magnification seen in (B). C, Cross-section of the main common pancreatic duct, with duct glands seen in the
periphery. D, These blind-ending pouches communicate with the lumen. (Courtesy Mariam Hobeldin.)
28 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
pancreatic ductal network in both humans and rodents, with Zhou et al, 1999) and ARIP cells (Hui et al, 2001) into insulin-
little known about the function of these duct glands other than expressing cells. Together, these studies strongly support the
that they are blind-ending pouches that unexpectedly express role of glucagon signaling, through its receptor, in initiating
Sonic Hedgehog, HES1, and PDX1 (Strobel et al, 2010). Both early insulin differentiation.
HES1 and PDX1 are markers of pancreatic progenitors (Gittes, Current treatments for diabetes, such as insulin replacement
2009), and their specific expression in these blind-ending therapy, do not address the actual physical loss of β cells, a
pouches, reminiscent of intestinal crypts, which are known to hallmark of the disease. Hence extensive efforts are focused on
harbor intestinal stem cells, possibly indicate that they may trying to establish alternate sources for the replenishment of the
have a role in pancreas regeneration. depleted β-cell population. For many years there has been a
dogma that once a cell reaches its terminal differentiation, it
WNT can no longer switch cell fate. Therefore the issue of whether
As mentioned earlier in the chapter, β-catenin repression in the β-cell neogenesis does occur within the mature adult pancreas
anterior endoderm is necessary to initiate liver and pancreas has been vigorously disputed in the literature. However, evi-
development. Consistent with this, Pdx1-Wnt1 and Pdx1- dence from recent studies has demonstrated the plasticity that
Wnt5a transgenic mice developed pancreatic agenesis and exists between α and βcells. Forced PDX1 expression in NGN3
severe hypoplasia, respectively, confirming that early WNT sig- progenitor cells resulted in nearly all of the α cells converting
naling is detrimental for pancreatic development (Heller et al, to β cells by postnatal day 12, without any obvious evidence of
2002). Similar to NOTCH signaling, the role of WNT signal- the α cells regenerating (Yang et al, 2011). Furthermore, near
ing beyond endodermal patterning is complex and depends on total ablation of β cells (about 99%) using a diphtheria toxin
time and place of WNT signaling. β-Catenin, which is mostly transgenic model led to α cell conversion to β cells via a bihor-
expressed in the mesenchyme (Heller et al, 2002), when ablated monal cell stage (glucagon positive/insulin positive) after 10
from PDX1-positive cells resulted in the loss of acinar tissue at months (Thorel et al, 2010). Also, ectopic expression of PDX1
birth, confirming earlier studies that exocrine tissue develop- or PAX4 has been shown to induce α cells or α-cell progenitors
ment is mesenchyme dependent (Murtaugh et al, 2005; Wells to convert to β cells (Collombat et al, 2009; Piccand et al,
et al, 2007). Others found a role for Wnt signaling in promoting 2014). To illustrate that α cells can genuinely act as a source
postnatal pancreatic growth (Heiser et al, 2006), illustrating for new β cells in the future, Thorel and coworkers (2011) used
the complex and multiple roles that it plays in pancreatic the diphtheria toxin model to ablate 98% of α cells, with the
development. transgenic mice able to maintain a euglycemic state. The previ-
ous notion that terminally differentiated cells in the pancreas
Endothelial Cells lack plasticity is no longer accepted, with several studies dem-
Recently, an important role for endothelial cells in pancreatic onstrating that their fate is flexible (Chera et al, 2014; Puri
endocrine development has been demonstrated. As mentioned et al, 2015).
earlier, the notochord separates from the gut endoderm by the
fusion of the dorsal aortas at about E8.0. Lammert and cowork- Extracellular Matrix
ers demonstrated that the removal of the dorsal aorta from The pancreatic epithelium is contained within a continuous
Xenopus embryos led to the absence of pancreatic endocrine sheath of basement membrane, which constitutes the epithelial-
development (Lammert et al, 2001). In addition, aortic endo- mesenchymal interface and plays an important role in guiding
thelial cells were able to induce pancreatic bud formation and pancreatic development (Hisaoka et al, 1993). Basement mem-
subsequent insulin cell differentiation in the adjacent endo- brane has also been shown to play an important role in regulat-
derm. Of importance, ectopic VEGFA in the intestine and ing branching morphogenesis in many other organs. Laminin-1
stomach led to ectopic formation of islets in the stomach was found to induce duct formation in isolated E11 mouse
(Lammert et al, 2001). Of interest, it appears that the ventral pancreatic epithelium (Gittes et al, 1996) and to mediate the
pancreas development seems to be independent of the endo- proexocrine effect of the mesenchyme and the pro–β-cell role
thelium, despite its close proximity to the vitelline veins (Yoshi- in later gestation (Jiang et al, 2001; Li et al, 2004). Cadherins
tomi & Zaret, 2004). (calcium-dependent adhesion molecules), critical for cell-cell
adhesions, play an essential role in migration and differentiation
Glucagon of pancreatic endocrine progenitor cells. E-cadherin and
The first endocrine cells to appear during pancreatic develop- R-cadherin are initially localized to the ducts, but they become
ment are the glucagon-containing α-granules at about E9.0 in downregulated as cells move out of the ducts to form islets
the mouse, and recent studies have shown that glucagon signal- (Dahl et al, 1996; Sjodin et al, 1995). N-CAM, another cell-
ing is necessary for early differentiation of insulin expressing adhesion molecule expressed in mature α and PP cells (Cirulli
cells, which appear at about E13.0 (Pictet et al, 1972; Prasadan et al, 1994), when knocked out led to improper aggregation of
et al, 2002). Glucagon hormone is generated from proglucagon endocrine cells within the islet (Esni et al, 1999). Thus cell-
by the action of prohormone convertase 2 (PC2). When PC2 adhesion molecules regulate the adhesive properties of endo-
is knocked out, mutant mice are generated being without glu- crine cells, and these adhesive properties are essential for
cagon and displaying a delay in islet cell differentiation and endocrine cell aggregation into islets.
maturation but still retaining the large amplification of insulin-
positive cells (“secondary-wave”) later in gestation (Vincent et Transcription Factors
al, 2003). Exogenous addition of exendin-4, a glucagon-like The role of transcription factors has been extensively studied
peptide-1 (GLP-1) analogue, was able to rescue the delay in in pancreatic development, and much of our understanding of
early insulin differentiation (Prasadan et al, 2002). Exendin-4 pancreatic development has been facilitated by the develop-
was also shown also to convert AR42J cells (Yew et al, 2004; ment of the various transcription factor–specific knock-out
Chapter 1 Embryologic development of the liver, biliary tract, and pancreas 29
mice. Especially with the advent of the Cre-LoxP system, with no pancreatic endocrine cells form (Gradwohl et al, 2000); thus
or without tamoxifen-inducible (Cre-ERT2), allowing spatio- it appears to be a critical and essential factor for endocrine
temporal control of lineage labeling (Guo et al, 2013). The differentiation.
most heavily studied of the transcription factors is PDX1, an
early marker for pancreatic progenitors that later “restricts” to RFX6. RFX6 is a transcription factor downstream of NGN3 that
the β-cells and is clearly required for maintenance of β-cell fate has recently been identified as a key proendocrine regulator that
and function (Gao et al, 2014). It is expressed in the prepan- directs islet cell differentiation. It is initially expressed broadly
creatic region of the primitive foregut tube at E8.5, then in gut endoderm, particularly in PDX1-positive cells in the
expands to be expressed in distal stomach, common bile duct, prospective pancreatic region, and then becomes restricted to
and duodenum by E10.5 to 11.5 (Guz et al, 1995; Offield et the endocrine lineage, in postmitotic islet progenitor cells. Null-
al, 1996). Pdx1 is initially expressed throughout the epithelium; mutant mice for RFX6 fail to generate all islet cell types except
however, its expression becomes suppressed in cells as they pancreatic polypeptide cells (insulin, glucagon, somatostatin,
commit to the endocrine (Jensen et al, 2000) lineage or ducts and ghrelin). A human syndrome of neonatal diabetes (patients
(Gu et al, 2002). Its expression reappears as cells differentiate who lack pancreatic endocrine cells) with bowel atresia were
to insulin-positive β-cell lineage. More recently, Pdx1 has been shown to have mutations in the RFX6 gene (Smith et al, 2010).
shown to be expressed in pancreatic duct glands in addition to Thus RFX6 is dependent on NGN3 and is a unique regulator
β cells (Strobel et al, 2010). PDX1-null mutant mice and of islet cell development. It is also essential in maintaining func-
humans developed pancreatic agenesis (Jonsson et al, 1994; tional identity in adult pancreatic β cells (Piccand et al, 2014).
Stoffers et al, 1997a; Stoffers et al, 1997b; Yee et al, 2001).
Delayed PDX1 inhibition using tetracycline regulatable trans- PAX6. PAX6 is also another marker of endocrine lineage, but
genic knock-in system demonstrated severe blunting of pancre- unlike NEUROG3, it is not absolutely necessary for endocrine
atic development with complete absence of acini and β cells formation because null-mutant mice for PAX6 still formed
(Holland et al, 2002), indicating that PDX1 continues to play endocrine cells, albeit at a reduced rate (St-Onge et al, 1997).
a role in pancreas development beyond regional specification PAX6 expression is retained in cells that are committed to the
during endodermal patterning. endocrine lineage as early as E9.5 in glucagon-positive cells or
in insulin-positive cells at E12.5, thereafter beginning hormone
PTF1A. Pancreas-specific transcription factor 1A (PTF1A) is expression (St-Onge et al, 1997). Transgenic expression of
an early marker of pancreatic progenitor cells, expressed PAX6 under the PDX1 promoter led to islet and ductal hyper-
slightly later than PDX1 at around E9.5; by E18.5 it becomes plasia, indicating that it may have roles in the formation of
progressively restricted to acinar cells (Cras-Meneur et al, ducts and in islet growth (Yamaoka et al, 2000). However,
2009). PTF1A-null mutant mice develop a phenotype similar when PAX6 was ectopically expressed in β cells under the
to that seen with PDX1-null mutants, with severe pancreatic insulin promoter, it led to β-cell apoptosis, indicating that
hypoplasia and absent acini and ducts; however, endocrine PAX6 promotes proliferation only in pancreatic progenitors,
cells still develop. Of interest, the endocrine cells migrate out not in mature cells.
through the pancreatic mesenchyme to populate the spleen
(Kawaguchi et al, 2002; Krapp et al, 1998). A PTF1A non- PAX4/ARX
functioning mutation has been seen in humans born without PAX4 is another endocrine cell marker and is expressed as early
a pancreas (Sellick et al, 2004). Furthermore, PTF1A has as E9.5; it then peaks at about E13 to E15, coinciding with the
complex interactions with downstream targets of NOTCH to secondary transition of insulin-positive cells (Wang et al, 2004).
control exocrine lineage selection and differentiation. Overex- Its importance was further delineated when β cells and δ cells
pressing PTF1A in pancreatic progenitors represses the pro- failed to develop in PAX4-null mutant mice. Early embryonic
endocrine marker NKX6.1, stopping endocrine differentiation insulin-positive cells were present in these mice, indicating that
(Puri et al, 2015). This further emphasizes the role of PTF1A PAX4 is needed for the formation of mature β cells (Sosa-
as a promoter of acinar fate while suppressing the endocrine Pineda et al, 1997; Wang et al, 2004). In these mice, the β and
program fate. δ cells seems to have been replaced by cells coexpressing glu-
cagon and ghrelin, indicating that PAX4 may act as transcrip-
NEUROG3. NEUROG3 is one of the earliest markers specific to tional inhibitor for this inhibitor (Wang et al., 2008). PAX4
the pancreatic endocrine lineage, and it is a key driver of endo- seems also to inhibit the expression of ARX, a homeobox-
crine differentiation (Li et al, 2014). It is first expressed at E9.0 containing gene that enhances glucagon-positive cell differen-
and peaks at around E15.5; it is thought to be antagonized by tiation (Collombat et al, 2005). ARX, which is downstream of
NOTCH signaling in cells with an acinar fate (Gradwohl et al, NEUROG3 and is absent in NEUROG3-null mutant mice,
2000; Jensen et al, 2000). NEUROG3 cells then proliferate, when overexpressed in PDX1-positive progenitor cells, diverted
giving rise to proendocrine postmitotic cells expressing tran- most β- and δ-cell precursors toward α- and PP-cell lineages,
scription factors RFX6, NEUROD, NKX6.1, and PAX6. without a change in the overall number of endocrine cells.
NEUROG3 shuts off at around E17.5 (Gu et al, 2002; Jensen When ARX was knocked out, no α cells were seen with the
et al, 2000), and forced overexpression of NEUROG3 leads to appearance of the β-cell marker (Collombat et al, 2003; Court-
cells prematurely committing to an endocrine lineage, with the ney et al, 2013; Wilcox et al, 2013 ). These findings further
development of only glucagon-positive clusters (Johansson et emphasize the opposing roles for PAX4 and ARX in α and PP
al, 2007). Overexpressing NEUROG3 at different time points cells versus β and δ cells (Collombat et al, 2007). In summary,
later in gestation (E11 to E12) resulted in the formation of PAX4 and ARX mutually repress each other, with PAX4 pro-
insulin- and pancreatic polypeptide–positive cells (Johansson moting β-cell fate at the expense of α cells, whereas ARX
et al, 2007). However, when NEUROG3 is deleted from cells, promotes α cells at the expense of β cells.
30 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
FIGURE 1.9. Overview of the pancreatic endocrine and exocrine cell lineage. (Courtesy Mariam Hobeldin.)
NKX2.2. NKX2.2 is expressed as early as E9.5, is coexpressed NKX6.1 AND NKX6.2. Single- and double-null mutant studies for
with PDX1, acting as a marker of multipotent pancreatic pro- NKX6.1 and NKX6.2 have been performed and suggest that
genitor cells, and eventually becomes restricted to NEUROG3- both molecules, which are expressed early in pancreatic endo-
positive cells, persisting in all endocrine lineages except for δ dermal cells, play central roles in pancreatic development, espe-
cells (Chiang & Melton, 2003; Sussel et al, 1998). NKX2.2- cially in β-cell development (Henseleit et al, 2005). NKX6.1,
null mutant mice develop with no β cells, reduced PP cells, an which is downstream of PDX1 and is an endocrine progenitor
80% reduction in α cells, and no effect on δ cells. However, a marker, becomes restricted to insulin-positive cells; whereas
large number of ghrelin-positive ε cells were found with no NKX6.2 is restricted to glucagon-positive and amylase-positive
glucagon coexpression, indicating that NKX2.2 normally cells; after E15.5, it disappears (Sander et al, 2000). In NKX6.1-
induces insulin-positive differentiation and represses ε-cell for- null mutant mice, an 85% reduction in β cells is seen, whereas
mation (Sussel et al, 1998). NKX6.1 and NKX6.2 double-null mutants developed a 92%
Chapter 1 Embryologic development of the liver, biliary tract, and pancreas 31
and 65% reduction in β cells and α cells, respectively, suggest- as described earlier (Haumaitre et al, 2005; Jacquemin et al,
ing that NKX6.1 has an important role in generating β cells. 2003). HNF6 is expressed in the foregut-midgut endoderm
Deletion of NKX 6.1 in the adult pancreas leads to β cells junction at E8.0 under the control of HNF1β (Poll et al, 2006).
converting into somatostatin-expressing δ cells (Schaffer et al, HNF6 in turn regulates the expression of FOXA2, which is
2013). NKX6.2 plays an important role in α-cell formation and essential for gut formation (Weinstein et al, 1994). FOXA2,
can compensate for NKX6.1 absence in β-cell formation however, is not necessary for pancreas formation because its
(Henseleit et al, 2005; Sander et al, 2000). β-Cell loss was deletion did not affect pancreatic development (Lee et al,
rescued with transgenic expression of NKX6.1 or NKX6.2 2005b). As discussed earlier, in the bile duct formation, HNF6
under the PDX1 promoter (Nelson et al, 2007). also acts upstream from HNF1β, where HNF6 activates HNF1β
to initiate the formation of endocrine progenitors (Clotman
MAFA AND MAFB. The transcription factor MAFA is a critical et al, 2002).
regulator of the insulin gene, and it also regulates glucose-
responsive expression of insulin (Matsuoka et al, 2003; SRY (SEX-DETERMINING REGION Y)-BOX: SOX9
Nishimura et al, 2015). MAFA is first expressed in insulin- SOX9 acts as a marker and maintenance factor for pancreatic
positive cells during the “secondary transition” wave of insulin- progenitor cells. It is initially expressed throughout the early
cell differentiation; however, it is not absolutely necessary for pancreatic epithelium, then later becomes restricted to trunk
β-cell formation, because MAFA-null mutant mice have a progenitors and mature ducts, eventually giving rise to all pan-
normal proportion of insulin-positive cells at birth (Nishimura creatic cell types. It is seen as necessary for maintaining cells in
et al, 2009). MAFB is expressed early in pancreatic endocrine a progenitor state (Akiyama et al, 2005). SOX9 mutants display
development and, as the pancreas develops, it switches off in pancreatic hypoplasia as a result of depletion of the pancreatic
insulin-positive–forming cells as they form mature β cells, to progenitor pool (Seymour, 2014). It has also been suggested
then express MAFA (Nishimura et al, 2006). It was demon- that SOX9 mediates HNF6 and the control of NEUROG3-cell
strated that early expression of MAFA under the PDX1 pro- formation, because conditional deletion of SOX9 led to the
moter was detrimental for pancreatic development, with a formation of cystic structures similar to that seen in HNF6−/−
severe reduction in pancreatic mass and proliferation of pro- embryos, associated with absent pancreatic endocrine cells
genitors, suggesting that MAFA is a key regulator for the matu- (Seymour et al, 2007). Furthermore, it was found that SOX9 is
ration of pancreatic β cells rather than specification (Nishimura transiently coexpressed with NEUROG3 and frequently
et al, 2009). The same conclusion was drawn in MAFB-null colocalizes with HES1, which acts as a precursor to NEUROG3-
mutant mice, in which there was a delay in the development of positive cells. It was suggested that SOX9 helps mediate
early insulin- and glucagon-positive cells, with a reduction by the transition of endocrine progenitors from nonendocrine
almost half of their total mass (Artner et al, 2007). HES1-positive, NEUROG3-negative state to a HES1-negative,
NEUROG3-positive endocrine-committed state (Seymour
HNF CASCADE. Three HNF factors: HNF6/ONECUT1, et al, 2007). Thus SOX9 acts a key mediator for the commit-
HNF1β, and HNF3β (renamed FOXA2), appear to have an ment of NEUROG3-positive endocrine progenitors (Seymour,
interwoven, complex set of interactions that all have an impact 2014). More recently, it has been shown that SOX9 is a marker
on pancreatic development, starting from the earliest pancreatic of a common pool of progenitors cells in the intestinal crypts
specification all the way through to mature pancreatic cell dif- and the biliary and pancreatic ductal trees that are intercon-
ferentiation and function. They are all expressed in the pancre- nected in a contiguous epithelial lining (Furuyama et al, 2011)
atic epithelium at about E9.0 to E10.0, with HNF6 appearing (Fig. 1.9). SOX9 is also seen as a useful marker in clinical
to be the key determinant of pancreatic specification (Maestro pathology (Shroff et al, 2014) and key player in the initiation of
et al, 2003). This conclusion comes from observations that pancreatic cancer (Grimont et al, 2015; Seymour, 2014).
HNF6−/− embryos developed ventral pancreatic agenesis, with
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CHAPTER 2
Surgical and radiologic anatomy of the liver, biliary
tract, and pancreas
Leslie H. Blumgart, Lawrence H. Schwartz, and Ronald P. DeMatteo*
32
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 33
Gallbladder
Quadrate lobe
Umbilical
fissure
Left lobe
Right lobe
Left lobe
Right adrenal
vein
Ligamentum Right triangular
venosum ligament
Ligamentum
teres
M
L
R
IVC
FIGURE 2.4. The anterior surfaces of the major extrahepatic veins and
the inferior vena cava are retroperitoneal and masked behind the layers
of the falciform ligament, while it splits and passes to the right and left
triangular ligaments. The left and middle hepatic veins usually join within
the liver, and not outside the liver as depicted here for visual simplicity.
FIGURE 2.2. Transverse ultrasound image of the hepatic vein conflu-
ence shows the left (L), middle (M), and right (R) hepatic veins as they
join the inferior vena cava (IVC).
M
M
IVC
IVC
R
R
A B
R
PV IVC
IVC A
C D
FIGURE 2.3. Two inferior accessory right hepatic veins. A, Contrast-enhanced computed tomographic (CT) image of the hepatic vein confluence.
IVC, inferior vena cava; M, middle hepatic vein;R, Right hepatic vein. B, A small right inferior accessory vein (arrow) enters the IVC below the hepatic
venous confluence. C, The second, larger right inferior accessory right hepatic vein (arrow) is seen more inferiorly. PV, Portal vein. D, CT coronal
reconstruction image shows the right hepatic vein (R) and one right inferior accessory vein (arrow). A, Aorta.
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 35
VII
RIGHT MAIN LEFT
VIII
SCISSURA SCISSURA SCISSURA
II
V I
III
IV
VI
Umbilical
fissure
Right portal pedicle Left portal pedicle II
VIII
RIGHT LIVER LEFT VII
FIGURE 2.5. The portal vein, hepatic artery, and draining bile ducts
are distributed within the liver in a beautifully symmetric pedicular pattern, III
which belies the asymmetric external appearance. Each segment (I to
VIII) is supplied by a portal triad composed of a branch of the portal vein
and hepatic artery and drained by a tributary of the right or left main
hepatic ducts. The four sectors demarcated by the three main hepatic IV
veins are called the portal sectors (now referred to as sections in the V
Brisbane terminology); these portions of parenchyma are supplied by
independent portal pedicles. The hepatic veins run between the sectors
in the portal scissurae; the scissurae containing portal pedicles are called VI
the hepatic scissurae. The umbilical fissure corresponds to a hepatic
scissura. The internal architecture of the liver consists of two hemilivers,
the right and the left liver separated by the main portal scissura, also
known as Cantlie’s line. It is preferable to call them the right and left liver, B
rather than the right and left lobes because the latter nomenclature is FIGURE 2.6. The functional division of the liver and its segments
erroneous; there is no visible mark that permits identification of a true according to Couinaud’s nomenclature. A, As seen in the patient. B, In
hemiliver. the ex vivo position.
36 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
referred to as sections (Table 2.1) (see Chapter 103B for differ- This prolongation of the left portal pedicle turns anteriorly and
ences in the terminology of the various hepatic resections). Also, caudally within the umbilical fissure, giving branches of supply
note that the left medial section, in the terminology of Strasberg to segment II first and then segment III and recurrent branches
(2005), is composed of one segment (i.e., segment IV). (“feedback vessels”) to segment IV (Fig. 2.8; see Fig. 2.6).
At the hilus of the liver, the right portal triad pursues a short Beneath segment IV, the pedicle is composed of the left branch
course of approximately 1 to 1.5 cm before entering the sub- of the portal vein and the left hepatic duct, but it is joined at
stance of the right liver (Fig. 2.7). In some cases, the right the base of the umbilical fissure by the left branch of the hepatic
anterior and posterior pedicles arise independently, and their artery.
origins may be separated by 2 cm. In some cases, it appears as The branching of the portal pedicle at the hilus (Fig. 2.9),
if the left portal vein arises from the right anterior branch (see the distribution of the branches to the caudate lobe (segment
Fig. 2.40). On the left side, however, the portal triad crosses I) on the right and left sides, and the distribution to the seg-
over approximately 3 to 4 cm beneath segment IV (formerly ments of the right (segments V through VIII) and left (segments
called the quadrate lobe), embraced in a peritoneal sheath at the II through IV) hemiliver follow a remarkably symmetric pattern
upper end of the gastrohepatic ligament and separated from the and, as described by Scheele (1994), allow separation of
undersurface of segment IV by connective tissue (hilar plate). segment IV into segment IVa superiorly and segment IVb
4 3
U
2
p
B
FIGURE 2.7. A, Transverse sonogram at the level of the portal vein
bifurcation. The main portal vein (MPV) bifurcates into the left and right
portal veins (LPV and RPV). The RPV bifurcates shortly into the right IVC
anterior (RAPV) and right posterior (RPPV) branches, but the LPV has a
longer horizontal course within the hilar plate. The inferior vena cava
(IVC) is seen posteriorly. B, Coronal view of computed tomographic FIGURE 2.8. Transverse sonogram shows the branching pattern of
angioportography. Reconstruction shows the right hepatic vein (open the left portal vein (P), which courses horizontally and into the umbilical
arrow) and the portal vein (large arrow); anterior and posterior sectional fissure. The umbilical portion of the left portal vein (U) gives branches to
branches of the RPV (small arrows) are seen to arise directly and sepa- the left hepatic segments (II to IV). The left hepatic vein (arrow) and
rately from the main portal trunk. inferior vena cava (IVC) also are shown.
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 37
II/III
IV
LPV
Lesser
omentum
VII
L
I
IVC
RA R
FIGURE 2.11. The main bulk of the caudate lobe (segment I; dark
area) lies to the left of the inferior vena cava (IVC); the left and inferior
margins are free in the lesser omental bursa. The gastrohepatic (lesser)
omentum separates the left portion of the caudate from segments II and
RP
III of the liver, while it passes between them to be attached to the liga-
mentum venosum. The left portion of the caudate lobe inferiorly tra-
verses to the right between the left portal vein (LPV) and IVC as the
caudate process, where it fuses with the right lobe of the liver. Note the
position of the middle hepatic vein (MHV).
IVC
MHV
LHV
II/III
Ligamentum
venosum
*
RPV IVC
v
a
PV
LPV
FIGURE 2.12. The caudate lobe (shaded) and segments II and III,
rotated to the patient’s right. Superiorly, the left portion of the caudate
lobe is linked by a deep anterior portion, embedded in the parenchyma
immediately under the middle hepatic vein (MHV), reaching inferiorly to
the posterior margin of the hilus of the liver and fusing anterolaterally to
the inferior vena cava (IVC) on the right side to segments VI and VII of
the right liver. The major blood supply arises from the left branch of the A
left portal vein (LPV) and the left hepatic artery close to the base of the
umbilical fissure of the liver. The hepatic veins (MHV, LHV) are short in
course and drain from the caudate directly into the anterior and left
aspect of the vena cava. LHV, Left hepatic vein; RPV, right portal vein;
PV, main trunk of portal vein.
BILIARY TRACT
A Biliary exposure and precise dissection are the most important
steps in any biliary operative procedure. A thorough under-
standing of biliary anatomy is necessary.
II
VIII V IV
VI
III
III
IV
V
V
VII II
Right Left
A B
II
VIII
VII
IV
III
V
Common hepatic
duct
VI
vein, which pursues an ascending course. The junction of these system only. In about 7%, the drainage is into the right hepatic
two main right biliary channels usually occurs above the right system.
branch of the portal vein. The right hepatic duct is short and
joins the left hepatic duct to constitute the confluence lying in Extrahepatic Biliary Anatomy and Vascular Anatomy of
front of the right portal vein and forming the common hepatic the Liver and Pancreas
duct.
The caudate lobe (segment I) has its own biliary drainage The extrahepatic bile ducts are represented by the extrahepatic
(Healey & Schroy, 1953). The caudate lobe is divided into right segments of the right and left hepatic ducts, joining to form the
and left portions and a caudate process. In 44% of individuals, biliary confluence and the main biliary channel draining to the
three separate ducts drain these three parts of the lobe, whereas duodenum. (Figs. 2.17 and 2.18). The confluence of the right
in another 26%, a common duct lies between the right portion and left hepatic ducts occurs at the right of the hilar fissure of
of the caudate lobe proper and the caudate process and an the liver, anterior to the portal venous bifurcation and overlying
independent duct that drains the left part of the caudate lobe. the origin of the right branch of the portal vein. The extrahe-
The site of drainage of these ducts varies. In 78% of patic segment of the right duct is short, but the left duct has a
cases, drainage of the caudate lobe is into the right and left much longer extrahepatic course. The biliary confluence is
hepatic ducts, but in 15%, drainage is by the left hepatic ductal separated from the posterior aspect of segment IVB of the liver
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 41
Right posterior
VIII sectoral duct
A VII
Left hepatic duct
VI
Right anterior
sectoral duct
B
FIGURE 2.16. A, Biliary and vascular anatomy of the right liver. Note the horizontal course of the posterior sectional duct and the vertical course
of the anterior sectional duct. B, Transtubal cholangiogram shows a common normal variant: the right posterior sectional duct drains into the left
hepatic duct. In this case, the posterior duct is anterior to the posterior sectional duct. Frequently in this variant, the posterior duct passes posteriorly
to the anterior sectional pedicle.
by the hilar plate, which is the fusion of connective tissue et al, 1981). The commonly accepted working definition of
enclosing the biliary and vascular elements with the Glisson the triangle of Calot recognizes, however, the inferior surface
capsule (Fig. 2.19). Because of the absence of any major vas- of the right lobe of the liver as the upper border and the cystic
cular interposition, it is possible to open the connective tissue duct as the lower border (Wood, 1979). Dissection of the
constituting the hilar plate at the inferior border of segment IV triangle of Calot is of key significance during cholecystectomy,
and, by elevating it, to display the biliary confluence and left because in this triangle runs the cystic artery, often the right
hepatic duct (Fig. 2.20). branch of the hepatic artery, and occasionally a bile duct,
which should be displayed before cholecystectomy (see
Main Bile Duct and Sphincter of Oddi Chapter 35). If there is a replaced or accessory common or
The main bile duct, the mean diameter of which is approxi- right hepatic artery, it usually runs behind the cystic duct to
mately 6 mm, is divided into two portions: the upper is called enter the triangle of Calot (Fig. 2.21).
the common hepatic duct and is situated above the cystic duct, The common variations in the relationship of the hepatic
which joins it to form the lower portion, the common bile artery and origin and course of the cystic artery to the biliary
duct (CBD). The common duct courses downward anterior apparatus are shown in Figure 2.22. Ignorance of these varia-
to the portal vein, in the free edge of the lesser omentum; it tions may provoke unexpected hemorrhage or biliary injury
is closely applied to the hepatic artery, which runs upward on (Champetier et al, 1982) during cholecystectomy and may
its left, giving rise to the right branch of the hepatic artery, result in bile duct injury during efforts to secure hemostasis
which crosses the main bile duct usually posteriorly, although (see Chapter 42). The union between the cystic duct and the
in approximately 20% of cases, it crosses anteriorly. The cystic common hepatic duct may be located at various levels. At its
artery, arising from the right branch of the hepatic artery, may lower extrahepatic portion, the CBD traverses the posterior
cross the common hepatic duct posteriorly or anteriorly. The aspect of the pancreas, running in a groove or tunnel. The
common hepatic duct constitutes the left border of the triangle retropancreatic portion of the CBD approaches the second
of Calot, the other corners of which were originally described portion of the duodenum obliquely, accompanied by the ter-
as the cystic duct below and the cystic artery above (Rocko minal part of the pancreatic duct of Wirsung.
42 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
a b
c
i
d
j e
f
g
h
k
V VIII
VII
C
FIGURE 2.17. Anterior aspect of the biliary anatomy and of the head
of the pancreas: right hepatic duct (a), left hepatic duct (b), common II
hepatic duct (c), hepatic artery (d), gastroduodenal artery (e, cystic duct VI
(f), retroduodenal artery (g), common bile duct (h), neck of the gallbladder B
(i), body of the gallbladder (j), fundus of the gallbladder (k). Note particu-
larly the position of the hepatic bile duct confluence anterior to the right III
branch of the portal vein, the posterior course of the cystic artery behind IV
the common hepatic duct, and the relationship of the neck of the gall-
bladder to the right branch of the hepatic artery. Note also the relation- A
ship of the major vessels (portal vein, superior mesenteric vein, and
superior mesenteric artery) to the head of the pancreas.
FIGURE 2.19. Anatomy of the plate system. A, Cystic plate, above the
Gallbladder and Cystic Duct gallbladder. B, Hilar plate, above the biliary confluence and at the base
The gallbladder is a reservoir located on the undersurface of of segment IV. C, Umbilical plate, above the umbilical portion of the portal
vein. Large, curving arrows indicate the plane of dissection of the cystic
the right lobe of the liver, within the cystic fossa; it is separated
plate during cholecystectomy and of the hilar plate during approaches
from the hepatic parenchyma by the cystic plate, which is com-
to the left hepatic duct.
posed of connective tissue that extends to the left as the hilar
plate (see Fig. 2.19). Sometimes the gallbladder is deeply
embedded in the liver, but occasionally it occurs on a mesen-
teric attachment and may be susceptible to volvulus. The gall- The cystic duct arises from the neck or infundibulum of the
bladder varies in size and consists of a fundus, a body, and a gallbladder and extends to join the common hepatic duct. Its
neck (Fig. 2.23). The fundus usually, but not always, reaches lumen usually measures approximately 1 to 3 mm, and its
the free edge of the liver and is closely applied to the cystic length varies, depending on the type of union with the common
plate. The cystic fossa is a precise anterior landmark to the main hepatic duct. The mucosa of the cystic duct is arranged in spiral
liver incisura. The neck of the gallbladder makes an angle with folds known as the valves of Heister (Wood, 1979). Although the
the fundus and creates Hartmann’s pouch, which may obscure cystic duct joins the common hepatic duct in its supraduodenal
the common hepatic duct and constitute a real danger point segment in 80% of cases, it may extend downward to the ret-
during cholecystectomy. roduodenal or retropancreatic area. Occasionally, the cystic
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 43
A B
Umbilical
fissure
Ligamentum
teres
Gallbladder
fossa
C
FIGURE 2.20. A, Relationship between the posterior aspect of segment IV and the biliary confluence. The hilar plate (arrow) is formed by the fusion
of the connective tissue enclosing the biliary and vascular elements with the Glisson capsule. B, Biliary confluence and left hepatic duct exposed by
lifting segment IV upward after incision of the Glisson capsule at its base. This technique, lowering of the hilar plate, generally is used to display a
dilated bile duct above an iatrogenic stricture or hilar cholangiocarcinoma. C, Line of incision (left) to allow extensive mobilization of segment IV. This
maneuver is of particular value for high bile duct strictures and in the presence of liver atrophy or hypertrophy. The procedure consists of lifting
segment IV upward (A and B), then not only opening the umbilical fissure but also incising the deepest portion of the gallbladder fossa. Right, Inci-
sion of the Glisson capsule to gain access to the biliary system (arrow). (B, From Hepp J, Couinaud C: L’abord et l’utilisation du canal hépatique
gauche dans les reparations de la voie biliare principale. Presse Med 64:947-948, 1956.)
duct may join the right hepatic duct or a right hepatic sectional 16% the right anterior sectional duct, and in 4% the right
duct (Fig. 2.24). posterior sectional duct, may approach the main bile duct in
this fashion. In 6%, a right sectional duct may join the left
BILIARY DUCTAL ANOMALIES hepatic duct (the posterior duct in 5% and the anterior duct in
1%. In 3%, there is an absence of the hepatic duct confluence,
Full knowledge of the frequent variations from the described and the right posterior sectional duct may join the neck of the
normal biliary anatomy is required when any hepatobiliary gallbladder, or it may be entered by the cystic duct in 2%
procedure is performed (Fig. 2.25). The constitution of a (Couinaud, 1957). In any event, these multiple biliary ductal
normal biliary confluence by union of the right and left hepatic variations at the hilus are important to recognize in resection
ducts, as described previously, is reported in only 72% of and reconstructive surgery of the biliary tree at the hilus and
patients (Healey & Schroy, 1953). There is a triple confluence during partial hepatectomy and cholecystectomy.
of the right anterior and posterior sectional ducts and the left Intrahepatic bile duct variations also are common (Fig.
hepatic duct in 12% of individuals (Couinaud, 1957), and a 2.26) (Healey & Schroy, 1953). The main right intrahepatic
right sectional duct joins the main bile duct directly in 20%. In duct variations are represented by an ectopic drainage of
44 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
A B
CBD HA
CD
Replaced or
accessory
RHA
C
FIGURE 2.21. Hepatic artery variations shown by angiography. A, Replaced common hepatic artery arises from the superior mesenteric trunk. B,
Left, The hepatic artery (large arrowhead) arises from the celiac axis. The small arrowheads indicate a drainage catheter in the bile duct. Right, An
accessory right hepatic artery (large arrowhead) is arising from the superior mesenteric artery and lies lateral to the catheter (small arrowheads) in
the common bile duct (CBD). C, The accessory right hepatic artery usually courses upward in the groove posterolateral to the CBD, appearing on
the medial side of the triangle of Calot, usually running just behind the cystic duct (CD). This common variation occurs in about 25% of individuals.
HA, Hepatic artery; RHA, right hepatic artery.
segment V in 9%, of segment VI in 14%, and of segment VIII In 67% of patients (Healey & Schroy, 1953) a classic distri-
in 20%. In addition, a subvesical duct has been described in bution of the main left intrahepatic biliary ductal system exists.
20% to 50% of cases. This duct, sometimes deeply embedded The main variation in this region is represented by a common
in the cystic plate, joins either the common hepatic duct or the union between the ducts of segments III and IV in 25%, and
right hepatic duct. It does not drain any specific liver territory, in only 2% does the duct of segment IV join the common
never communicates with the gallbladder, and is not a satellite hepatic duct independently. Several anomalies of drainage of
of an intrahepatic branch of the portal vein or hepatic artery. the intrahepatic ducts into the neck of the gallbladder or cystic
Although not of major anatomic significance, injury may occur duct have been reported (Fig. 2.27) (Albaret et al, 1981;
during cholecystectomy if the cystic plate is not preserved. This Couinaud, 1957), and these must be kept in mind during cho-
may lead to a postoperative biliary leak. lecystectomy (see Chapter 33).
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 45
a b c
d e f
g h
A
FIGURE 2.22. The main variations of the cystic artery: typical course
(a), double cystic artery (b), cystic artery crossing anterior to main bile
duct (c), cystic artery originating from the right branch of the hepatic
artery and crossing the common hepatic duct anteriorly (d), cystic artery
originating from the left branch of the hepatic artery (e), cystic artery
originating from the gastroduodenal artery (f), cystic artery arising from
the celiac axis (g), cystic artery originating from a replaced right hepatic
artery (h).
GB
PV
IVC
B
FIGURE 2.23. Longitudinal sonogram shows the relationship of the
FIGURE 2.24. A, T-tube cholangiogram shows a very low insertion of
liver, gallbladder (GB), portal vein (PV), inferior vena cava (IVC), hepatic
a right sectional duct into the common hepatic duct (arrow). B, Endo-
artery (curved arrow) and common bile duct (straight arrow).
scopic retrograde choledochopancreatogram shows a low right sec-
tional duct (large arrow), into which is draining the cystic duct (small
arrow), an uncommon but important normal variant.
46 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
VIII D seg IV
VII
A seg V
VI a 67% b 1%
II II
91%
VI VI c 1%
II
5% 4%
III
VII
d 25% e 1% II
B seg VI II
VIII 86%
V
VII VII III III
VII
VIII VIII
VIII f 1%
II
V 10% V 2% V 2%
III
VII VII
VI g 4%
VI II
V
80% V 20%
C seg VIII
III
FIGURE 2.26. The main variations of the intrahepatic ductal system. A, Variations of segment V. B, Variations of segment VI. C, Variations of
segment VIII. D, Variations of segment IV. There is no variation of drainage of segments II, III, and VII. seg, Segment.
described a technique whereby lifting the segment IV upward Frequently, by a simultaneous opening of the deepest portion
and incising the Glisson capsule at its base offers a good expo- of the gallbladder fossa and the umbilical fissure (see Fig.
sure of the hepatic hilar structures (see Fig. 2.20). This tech- 2.20C), good exposure of the biliary duct confluence, and
nique is referred to as lowering of the hilar plate. It can be carried especially the right hepatic duct, can be obtained without the
out safely because only exceptionally (in 1% of cases) is there necessity for full hepatotomy.
any major vascular interposition between the hilar plate and the
inferior aspect of the liver, although tiny venules are common. Umbilical Fissure and Segment III (Ligamentum
This maneuver is of particular value in exposing the extrahe- Teres) Approach
patic segment of the left hepatic duct because it has a long
course beneath the segment IV. It is not as effective in exposing The round ligament, which is the remnant of the obliterated
the extrahepatic right duct or its secondary branches, which are umbilical vein, runs through the umbilical fissure to connect
short. The technique is of major importance for the identifica- with the left branch of the portal vein. The round ligament is
tion of proximal biliary mucosa during bile duct repair after sometimes deeply embedded in the umbilical fissure. At the
injury. Basically, an incision is required at the posterior edge of junction of the round ligament and the termination of the left
segment IV, where the Glisson capsule is attached to the hilar portal vein, elongations containing channels that are elements
plate. The upper surface of the hilar plate can be separated from of the left portal system course into the liver. The bile ducts of
the hepatic parenchyma and, by lifting segment IV upward, the left lobe of the liver (Figs. 2.30 and 2.31A) are located above
display of the hepatic duct convergence, which is always extra- the left branch of the portal vein and lie behind these elonga-
hepatic, is effected. Bile duct incision allows performance of a tions, whereas the corresponding artery is situated below the
mucosa-to-mucosa anastomosis. Rarely, it may be hazardous to vein. Dissection of the round ligament on its left side and divi-
approach the biliary confluence in this manner, especially when sion of one or two vascular elongations of segment III allow
anatomic deformity has been created by atrophy or hypertrophy display of the pedicle or anterior branch of the duct of segment
of liver lobes and in patients in whom there appears to be a III (Fig. 2.32). In the event of biliary obstruction with intrahe-
very deep hilus that is displaced upward and rotated laterally. patic biliary ductal dilation, a dilated segment III duct is
VI
A B C d
RP a
D
b f
RP
g
c
h
E F
FIGURE 2.27. The main variations of ectopic drainage of the intrahe-
patic ducts into the gallbladder and cystic duct. A, Drainage of the cystic
duct into the biliary confluence. B, Drainage of cystic duct into the left
hepatic duct, associated with no biliary confluence. C, Drainage of
segment VI duct into the cystic duct. D, Drainage of the right posterior
(RP) sectional duct into the cystic duct. E, Drainage of the distal part of
the right posterior sectional duct into the neck of the gallbladder. F,
Drainage of the proximal part of the right posterior sectional duct into FIGURE 2.29. The bile duct blood supply. Note the axial arrangement
the body of the gallbladder. of the vasculature of the supraduodenal portion of the main bile duct
and the rich network enclosing the right and left hepatic ducts: right
branch of the hepatic artery (a), 9 o’clock artery (b), retroduodenal artery
(c), left branch of the hepatic artery (d), hepatic artery (e), 3 o’clock artery
A (f), common hepatic artery (g), gastroduodenal artery (h).
1 2 3
C
IV
B
II
1
1 2
1 2
III
E
FIGURE 2.30. Biliary and vascular anatomy of the left liver. Note the
location of the segment III duct above the corresponding vein. The
75% 20% 5% anterior branch of the segment IV duct is not represented.
a b c
FIGURE 2.28. Main variations in gallbladder and cystic duct anatomy.
A, Duplicated gallbladder. B, Septum of the gallbladder. C, Diverticulum
of the gallbladder. D, Variations in cystic ductal anatomy. E, Different
types of union of the cystic duct and common hepatic duct: angular
union (a), parallel union (b), spiral union (c).
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 49
II
b
a
III
b
IV
c
c
d
A B
FIGURE 2.31. A, The biliary and vascular anatomy of the left liver. Note the relationship of the left horn of the umbilical recess with the segment
III ductal system: left portal vein (a), left hepatic duct (b), segment III system—note that the duct (black) lies adjacent to the portal venous branch
indicated (c), ligamentum teres (d). B, Segment III ductal approach: exposure of the left horn of the umbilical recess (a), division of the left horn of
the umbilical recess including segment III portal vein branches (b), exposure and opening of segment III duct: hepaticojejunostomy to the segment
III ductal system (c; see also Chapters 31 and 42).
A B
FIGURE 2.32. A, The liver is split to the left of the ligamentum teres in the umbilical fissure. It may be necessary to remove a small wedge of liver
tissue (c). B, Segment III duct is exposed at the base of the liver split, above and behind its accompanying vein, and is ready for anastomosis (see
also Chapters 31 and 42).
50 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
A B
FIGURE 2.33. A, Anterior sectional approach. If necessary, the liver substance is opened through a short distance in the line of the right anterior
sectional pedicle. B, The duct is displayed anterior and to the left side of the corresponding vein. This can be facilitated by using a posterior pedicular
approach as described by Launois (see Chapter 103B).
generally easily located above the left branch of the portal vein. of the mobilization of segment IV after opening of the principal
It is often preferable to split the normal liver tissue just to the scissura and the umbilical fissure as described previously.
left of the umbilical fissure to widen the fissure further, which
allows access to the ductal system with no need to divide any EXTRAHEPATIC VASCULATURE
elements of the portal blood supply to segment III (see Fig.
2.32). Celiac Axis and Blood Supply of Liver, Biliary Tract,
and Pancreas
Surgical Approaches to the Right Hepatic Biliary
Ductal System The usual classic description of the arterial blood supply of the
Because of the lack of precise anatomic landmarks, exposure liver, biliary system, and pancreas is found in only approxi-
of the right intrahepatic ductal system is much more hazardous mately 60% of patients (Figs. 2.34 to 2.36). The right and the
and imprecise than that of the left. In some cases of hilar left hepatic arteries, the former in the right of the hilus of the
cholangiocarcinoma, the planned surgical procedure—partial liver and the latter in the left at the base of the umbilical fissure,
hepatectomy (see Chapters 51B and 103B) or segment III become enclosed in the sheath of peritoneum, forming the right
duct bypass (see Chapters 31 and 42)—seems impossible at and left portal triads. In this sheath, further branching to the
operation. In such a critical operative situation, intrahepatic right anterior and posterior sections of the liver and on the left
right ductal system drainage is an option. Anatomically, the to segments II, III, and IV occurs within the respective pedicles,
anterior sectional duct and its branches run on the left side which also come to enclose the portal vein branches and the
of the corresponding portal vein. In essence, the end of the tributary bile ducts from these sections and segments. The arte-
liver scissura, within which lies the right branch of the portal rial supply of the CBD was described earlier; it arises from
vein, is opened through a short distance. The anterior sectional branches of the hepatic artery, the gastroduodenal artery, and
duct is displayed on the left aspect of the vein, and the dilated the pancreaticoduodenal arcades.
duct is opened longitudinally and sewn to a Roux-en-Y loop For practical surgical issues, the most important relation-
of jejunum (Fig. 2.33). Although this technique is rarely used, ships in the anatomy of the pancreas concern the arterial blood
it may be valuable in selected cases. Preferably, the right-sided supply and the venous drainage. The dorsal pancreatic artery
pedicles can be encircled and exposed by the technique used is a major branch, usually arising from the splenic artery, but
for pedicle exposure and control described for right-sided liver it can arise directly from the hepatic artery. When splenectomy
resection. is performed, it is important to establish the site of origin of the
dorsal pancreatic artery to avoid distal pancreatic ischemia. The
Exposure of the Bile Ducts by Liver Resection superior mesenteric artery (SMA) arises from the aorta poste-
This chapter does not detail exposure of the bile ducts by resec- riorly behind the pancreas and runs forward and upward to run
tion of liver substance. In essence, a segment of the left lobe first behind and then to the left of the superior mesenteric vein
may be amputated to expose the segment II or III ducts, or a (SMV) (see Fig. 2.35).
similar procedure may be carried out after removal of the infe-
rior tip of the right lobe. Finally, in some instances, removal of Variations in the Hepatic Artery
segment IV may be carried out to effect exposure of the biliary As a result of the complex embryologic development of the
confluence. This procedure really represents a simple extension celiac axis and SMA, wide variations in the arterial supply of
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 51
MH LH Left gastric
Aorta LGA SA
PV
RH HA
Celiac trunk RGA DP
GDA
Cystic Splenic SPDA
Proper hepatic
Pancreas
Supraduodenal Post PDA
MCA
Gastroduodenal MCV
Right Common hepatic GEA
gastric
FIGURE 2.34. The celiac trunk is a short, thick artery originating from Ant PDA
the aorta just below the aortic hiatus of the diaphragm and extending
horizontally and forward above the pancreas, where it divides into the IPDA
left gastric, common hepatic, and splenic arteries. An inferior phrenic SMA
artery, usually arising from the aorta or the splenic artery, occasionally SMV
arises from the celiac trunk. The left gastric artery curves toward the FIGURE 2.35. The primary arteries that supply the pancreas are the
stomach and extends along its lesser curve, forming anastomoses with gastroduodenal artery (GDA), which arises usually from the common
the right gastric artery. The splenic artery, the largest of the three celiac hepatic artery (HA) while it crosses the portal vein (PV) above the pan-
branches, takes a tortuous course to the left, behind and along the creas proper, and the dorsal pancreatic artery (DP), arising from the
upper border of the pancreas and at the hilus of the spleen, where it splenic artery (SA). The superior pancreaticoduodenal arteries (SPDAs)
splits into numerous terminal branches. The splenic artery usually arise from the GDA and join the inferior pancreaticoduodenal arteries
approaches and runs superiorly to the splenic vein. An uncommon but (IPDAs) from the superior mesenteric artery (SMA), forming two arcades
dangerous abnormality can occur when the splenic artery runs inferiorly along the anterior and posterior aspects of the head of the pancreas.
and behind the splenic vein, close to the splenic vein–mesenteric vein The GDA, after giving rise to the pancreaticoduodenal artery (PDA),
confluence. The left gastroepiploic artery and the short gastric arteries passes forward and to the left as the right gastroepiploic artery (GEA).
originate from one of these terminal branches. The common hepatic The GDA is a good landmark for the identification of the portal vein above
artery passes forward into the retroperitoneum then curves to the right the pancreas, and surgical division of the GDA just at its origin from the
to enter the right margin of the lesser omentum, just above the pancreas, common HA gives much greater access to the anterior surface of
and ascends; it approaches the common bile duct (CBD) on its left side the portal vein at this site. The right gastric artery (RGA) also usually
and runs usually anterior to the portal vein. While it turns upward just arises from the common HA just distal to the GDA, but it can arise from
above the pancreas, it gives rise to the gastroduodenal artery, which various sites. The GDA commonly divides into a larger right GEA and
also may originate from the right hepatic artery. This descends to supply smaller SPDA. The right GEA runs forward between the first part of the
the anterior, superior, and posterior surfaces of the first inch of the duodenum and pancreas; the SPDA divides into anterior and posterior
duodenum. The gastroduodenal artery can be duplicated and often has branches. The anterior superior PDA continues downward on the ante-
a small branch running with it toward the pylorus. The right gastric artery rior surface of the head of the pancreas to anastomose with the IPDA,
passes to the left along the lesser curve of the stomach, and anasto- which arises from the SMA. The posterior superior PDA behaves simi-
mosis is to the left gastric artery. The continuation of the common larly. Ant, Anterior; LGA, left gastric artery; MCA, middle colic artery;
hepatic artery, beyond the origin of the gastroduodenal artery and right MCV, middle colic vein; Post, posterior; SMV, superior mesenteric vein.
gastric artery, is known as the proper hepatic artery and usually soon
divides into a right and a left branch. The left branch extends vertically,
directly toward the base of the umbilical fissure, and usually gives off a
branch known as the middle hepatic artery (MH), which is directed
toward the right of the umbilical fissure and is destined to supply
segment IV of the liver. A further branch of the left hepatic artery (LH)
courses to the left to supply the caudate lobe, and further smaller
caudate branches arise from the left and right hepatic artery. The right
hepatic artery (RH) usually passes behind the common hepatic duct and
enters the cystic triangle of Calot; in some cases, it passes in front of
the bile duct, which is important in surgical exposure of the CBD. The p
cystic artery usually arises from the right hepatic artery but has many c
variations. IVC a s
the liver are found (Fig. 2.37). These variations are important posteriorly to the right renal vein and the anterior surface of
to recognize. Failure to show all arteries feeding the liver at the IVC. The neck and body of the pancreas lie atop the SMA
angiography may not only result in errors of diagnosis but may and the splenic vessels and their branches, the left renal vein,
also seriously mislead the surgeon or the interventional radiolo- and, more laterally, the left kidney. The right gastroepiploic vein
gist. In most cases, the hepatic artery arises from the celiac axis commonly drains into the anterior surface of the SMV just at
as described earlier, but it may be entirely replaced by a common the inferior border of the pancreas; this can often be involved
hepatic artery that originates from the SMA. In this instance, by tumor, as can the anterior branch of the inferior pancreati-
the hepatic artery passes posterior and then lateral to the portal coduodenal vein; the middle colic vein may also join at this
vein while it ascends and lies posterolateral to the CBD in the point. In mobilizing the SMV, these vessels are ligated so as to
hepatoduodenal ligament, where it is susceptible to operative avoid bothersome hemorrhage. Abnormalities of the IVC are
injury if not recognized. This applies to a right replaced or an uncommon, with duplication of the vena cava and a left-sided
accessory hepatic artery. Other variations in the origin of the vena cava seen rarely.
common hepatic artery include its origin directly from the aorta Several variations in anatomy and rare congenital anomalies
and the persistence of a primitive embryologic link between the of the portal vein are of surgical significance (Figs. 2.40 to
celiac and superior mesenteric systems. These variations are of 2.43). For example, performance of right hepatic resection,
considerable importance in controlling the arterial blood supply with division of what appears to be the right portal vein in a
to the liver during hepatic resection, liver transplantation, devas- patient with absence of the left portal vein (see Figs. 2.42 and
cularization of the liver, placement of intraarterial hepatic infu- 2.43) can be fatal. Agenesis of the right branch of the portal
sion devices, and in the resection of the head of the pancreas. vein is associated with agenesis of the right hemiliver and left
liver hypertrophy. This may be associated with biliary and
Portal Vein hepatic venous anatomic anomalies, which can compromise
The portal vein (Fig. 2.38) is formed behind the neck of the surgical approaches to the liver and to biliary repair (Fields
pancreas by confluence of the superior mesenteric and splenic et al, 2008).
veins (Fig. 2.39). The venous drainage of the pancreas usually Portal venous blood is derived from the venous drainage of
runs parallel to the arterial supply. There are anterior and the stomach, small bowel, spleen, and pancreas, and this drain-
posterior and superior and inferior pancreaticoduodenal veins age is important when considering surgery of the pancreas and
that drain to the portal vein and the SMV. The left gastric vein in patients with portal hypertension; it is described in detail
and the inferior mesenteric vein (IMV) usually drain into the along with the description of the anatomy of the pancreas.
splenic vein, but they can drain directly into the portal vein,
whereas the various small splenic tributaries drain directly to PANCREAS
the splenic vein.
The anatomic relationship of the pancreas to the SMV, the The pancreas is a posteriorly situated retroperitoneal organ that
splenic vein, and the portal vein (see Fig. 2.38) is important in lies transversely (Fig. 2.44). The organ is composed of a head,
pancreatic resection (see Chapter 66). The uncinate process can neck, body, and tail. The head is encompassed by the duode-
extend behind the SMV to well behind the SMA (see Fig. 2.35). num, whereas the tail rests in the splenic hilum (Figs. 2.45 and
Access to the portal vein behind the pancreas usually is obtained 2.46). A portion of the head inferiorly is termed the uncinate
from below by elevating the pancreas from the surface of the process and is intimately related to the SMV and SMA. Poste-
SMV just before it joins the splenic vein. With the exception of riorly, the pancreas is related to the IVC, aorta, left renal vein
the inferior pancreaticoduodenal veins, which enter the SMV and kidney, and spleen. The portion lateral to the portal vein
at the inferior border of the pancreas, it is uncommon to see averages 56.4% of the total weight. The pancreatic capsule is
branches from the pancreas run directly posteriorly into the loosely attached to the surface of the pancreas and is contiguous
SMV. Fixation here is usually by some inflammatory or neo- with the anterior layer of the mesocolon such that it can be
plastic process. Superiorly, the portal vein runs behind the dissected in continuity if necessary. The mesenteric attach-
pancreas and is identified first in the gap between the curvature ments to the pancreas tend to be contiguous (see Fig. 2.46).
of the splenic vein, splenic artery, common hepatic artery, and The arterial blood supply and venous drainage and the relation-
gastroduodenal artery. Division of the gastroduodenal artery ships to the CBD are described and illustrated earlier (see Figs.
provides much greater access to the superior surface of the 2.17, 2.29, 2.34, 2.35, and 2.38).
portal vein. If difficulty is encountered in this area, division of
the CBD, usually above the cystic duct, can provide excellent Pancreatic Duct
access to the right lateral aspect and anterior surface of the The duct of Wirsung, beginning in the distal tail as a confluence
portal vein. The SMA can be approached behind the pancreas of small ductules, runs through the body to the head, where it
above the point at which it is embraced by the uncinate process usually passes downward and backward in close juxtaposition
at the origin from the aorta. This allows dissection of the most to the CBD (see Fig. 2.45). The sphincter of Oddi (Fig. 2.47)
proximal part of the SMA. has been thoroughly studied (Boyden, 1957; Delmont, 1979)
Occasionally, the middle colic artery and other vessels of and consists of a unique cluster of smooth muscle fibers distin-
supply to the colon can arise from the more proximal SMA, guishable from the adjacent smooth muscle of the duodenal
such that they pass through the pancreas; this abnormality wall. The papilla of Vater at the termination of the CBD is a
should be searched for carefully. Division of the middle colic small, nipple-like structure that protrudes into the duodenal
artery is usually not a problem, however, because the colon is lumen and is marked by a longitudinal fold of duodenal mucosa.
well supplied with blood, and ischemia typically does not occur. The duct of Wirsung runs downward and parallel to the CBD
Of special importance to the surgeon is the direct relation- for approximately 2 cm and joins it within the sphincter
ship of the head of the pancreas to the duodenum and Text continued on p. 58
FIGURE 2.37. In approximately 25% of individuals, the right hepatic artery arises
partially or completely from the superior mesenteric artery (A, C, E); in a similar propor-
tion of patients, the left hepatic artery may be partially or completely replaced by a
branch arising from the left gastric artery, coursing through the gastrohepatic omentum
to enter the liver at the base of the umbilical fissure (D, F). Rarely, the right or left
hepatic arteries originate independently from the celiac trunk or branch after a very
short common hepatic artery origin from the celiac, and the gastroduodenal artery
may originate from the right hepatic artery (B, C). Multidetector computed tomography
(CT) angiogram demonstrating an accessory right hepatic artery (arrow) arising from
the superior mesenteric artery (G). Multidetector CT angiogram demonstrating a A B
replaced left hepatic artery arising from the left gastric artery (H). Another common
arterial variant is the hepatic trifurcation (I).
C D
E F
G I
H
RAS LPV
Ligamentum teres
IVb
RAS III
RPS IVa
II
LPV
RPS
PV
RPV
CV
B
RAS LPV
SV
SMV
IMV PV
RPS
A C
FIGURE 2.38. A, The superior mesenteric vein (SMV) at the root of the lesser omentum is usually a single trunk; two, or sometimes even three,
branches may unite as the vessel enters the tunnel beneath the neck of the pancreas (shaded) to form a superior mesenteric trunk. This trunk
ascends behind the neck of the pancreas and is joined by the splenic vein (SV), which enters it from the left to form the portal vein (PV), which
emerges from the retroperitoneal upper border of the neck of the pancreas and ascends toward the liver within the free edge of the lesser omentum,
lying behind the bile duct and the hepatic artery and surrounded by the lymphatics and nodes of the lesser omentum. During this course, it receives
blood through the coronary vein (CV), which communicates with esophageal venous collaterals, which connect with the gastric vein and the esopha-
geal plexus. Sometimes a separate right gastric vein enters the PV in this area. A superior pancreaticoduodenal vein often enters the PV just above
the level of the pancreas, and several smaller veins enter the SMV and PV from the right side beneath the neck of the pancreas. As the PV ascends
behind the common bile duct and common hepatic duct, it approaches the hilus of the liver and bifurcates into two branches, a larger right (RPV)
and a smaller left portal vein (LPV). The branch on the left courses below the left hepatic duct to enter the umbilical fissure, in company with the left
hepatic artery, and subsequently branches to supply the left liver segments (II-IV). Just before its entry into the umbilical fissure, it gives off a major
caudate vein, segment I, which runs posteriorly and laterally to the left. Sometimes this vein consists of two or more branches; the right portal branch,
which is much shorter in length before its entry into the liver, divides at the extremity of the hilus into the right anterior (RAS) and posterior (RPS)
sectional branches and is accompanied by the respective arterial branches and biliary tributaries. B, The division of the portal vein may arise more
proximally, however, and C, the right anterior and posterior sectional portal veins may arise independently from the portal venous trunk. IMV, Inferior
mesenteric vein.
L
RA
M
p s
RP
sm
A C
FIGURE 2.41. A, The portal vein anterior to the head of the pancreas and the duodenum may be in an abnormal position. B, Another rare but
interesting anomaly is the entrance of the portal vein into the inferior vena cava. C, Very rare, the entrance of a pulmonary vein into the portal vein.
D
S
v
v
a
i a
r IVC
A
A B
FIGURE 2.44. A, Magnetic resonance imaging of the pancreas, oblique axial reconstruction, T1-weighted three-dimensional gradient-echo tech-
nique. Aorta (a), inferior vena cava (i), common bile duct (CBD) (arrow), inferior mesenteric vein at the splenoportal confluence (v), superior mesenteric
artery (arrowhead), and left renal vein (r) are shown. B, Normal pancreatic anatomy. Postcontrast computed tomographic scan at the level of the
pancreas. A, Aorta; a, superior mesenteric artery; D, duodenum; IVC, inferior vena cava; S, stomach; v, superior mesenteric vein;. Long arrow, CBD;
short arrow, inferior pancreaticoduodenal artery; open arrow, gastroduodenal artery.
Aorta
NECK BODY
HEAD POSITION OF THE COMMON BILE DUCT
Superior mesenteric
vein and artery
Uncinate
process
B
UNCINATE PROCESS
a b c
(i) (ii)
A C
FIGURE 2.45. A, The head of the pancreas is globular with an extension, the uncinate process, which curves behind the superior mesenteric
vessels and may end even before it embraces the superior mesenteric vein (a), or it may pass completely behind between the aorta and the left of
the patient’s superior mesenteric artery (b, c). All variations are commonly seen. Posteriorly, the head of the pancreas lies in juxtaposition to the
inferior vena cava at the level of the entry of the left and right renal veins. The head of the pancreas forms a narrow neck in front of the superior
mesenteric and splenic vein confluence. The neck joins to the body of the gland, which forms a narrow tail. B, The common bile duct (CBD) passes
through the pancreas, either directly in the substance of the gland or initially with a posterior groove. C, The duct of Wirsung courses from left to
right within the pancreas, curves downward approaching the CBD, and runs parallel with but separated from it by the transampullary septum to
enter the duodenum, 7 to 10 cm distal to the pylorus, at the papilla of Vater after traversing the sphincter of Oddi. An accessory duct, the duct of
Santorini, runs more proximally in the head of the pancreas and usually terminates in the duodenum at an accessory papilla. Multiple variations of
the ductal system occur, depending on the extent of development of the duct of Santorini, such that rarely the accessory duct can enter the duo-
denum inferior to the main duct. It can be in communication with the main duct directly (i), or it can occur in duplicate version known as pancreas
divisum (ii). The duct of Santorini drains the body and tail of the organ, and the duct of Wirsung drains the head and the uncinate process.
Aorta
Portal vein
Vena cava Aorta
Peritoneum
Uncinate process
of pancreas
Middle
Superior mesenteric artery colic
artery Third part of
Superior mesenteric vein duodenum
Superior
mesenteric
artery
A B
Pancreas posterior view
Portal Common
vein bile duct
Superior
mesenteric
artery
Uncinate
FIGURE 2.46. A, The anterior surface of the pancreas, covered by the posterior process Superior
layer of the omental bursa or lesser peritoneal sac, can often be obliterated by adhe- mesenteric vein
sions. The transverse mesocolon arises from the lower border of the pancreas and Left Right
envelops the middle colic vessels as they arise from the superior mesenteric vessels Related Related to left kidney, Related to
just beneath the pancreatic neck. B, The relationship of the pancreatic neck and unci- to spleen left renal vein and inferior
nate process to the aorta and superior mesenteric artery. Note the position of the left adrenal gland vena cava
and aorta
renal vein and duodenum. C, The posterior relationships of the duodenal loop and
pancreas. Note the relationship to the inferior vena cava, aorta, and hilum of the spleen. C
b
c
d
e
f
FIGURE 2.47. Schematic representation of the sphincter of Oddi: notch (a), biliary sphincter (b), transampullary septum (c), pancreatic sphincter
(d), membranous septum of Boyden (e), common sphincter (f), smooth muscle of duodenal wall (g).
58 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
B
Posterior Anterior
FIGURE 2.48. A, Magnetic resonance imaging cholangiography (MRCP), T2-weighted coronal image at the level of the ampulla, shows the duo-
denum (D) and the pancreatic head with common bile duct (curved arrow) and pancreatic duct (straight arrow). B, MRCP of pancreas divisum.
Anterior projection shows variant anatomy with the duct of Santorini (vertical arrow) between the duodenum above the duct of Wirsung (angled
arrow). The two ducts are separate; the duct of Santorini drains mainly the neck and body of the pancreas, and the duct of Wirsung drains mainly
the uncinate process portion of the head of the pancreas.
Splanchnic nerves
Vagal nerves
Celiac ganglion
LYMPHATIC DRAINAGE
Liver and Pancreas
The lymphatic drainage of the liver and gallbladder is mainly
to nodes in the hepatoduodenal ligament and along the hepatic
artery; this is shown in Figure 2.49. The lymphatic drainage of
i PV the pancreas is predominantly to the nodes that lie in juxtaposi-
tion to the arteries and veins (Fig. 2.50B).
HA BD
SA
NERVE SUPPLY TO THE LIVER AND PANCREAS
The nerve supply to the liver and pancreas (see Fig. 2.50) is
from branches of the celiac ganglion. It is composed of sympa-
thetic and parasympathetic elements.
SV
IMV
References are available at expertconsult.com.
SMA SMV
B ii
FIGURE 2.49. A, The liver drains principally to hepatoduodenal nodes
at the hilus and along the hepatic artery and portal vein. The gallbladder
drains partly to the liver, but it also drains via the cystic node to nodes
of the hepatoduodenal ligament and to suprapancreatic nodes.
B, Numerous nodes (i) lie along the superior mesenteric vein along the
borders of the pancreas, draining back into the splenic hilar nodes; along
the superior border of the pancreas to the superior pancreatic nodes;
and to the celiac trunk and nodes at the base of the common hepatic
artery. A large node commonly lodges in intimate association with the
surface of the superior border of the pancreas and the right side of the
common hepatic artery. This node often needs to be dissected and
elevated to gain access to the anterior surface of the portal vein. Removal
of this node often improves access, as does division of the gastroduo-
denal artery. Posterior pancreaticoduodenal nodes (ii) lie along the pos-
terior pancreatic duodenal arterial arcade. BD, Bile duct; HA, hepatic
artery; IMV, interior mesenteric vein; PV, portal vein; SA, splenic artery;
SMA, superior mesenteric artery; SMV, superior mesenteric vein; SV,
splenic vein.
Chapter 2 Surgical and radiologic anatomy of the liver, biliary tract, and pancreas 59.e1
REFERENCES Hjörtsjö CH: The topography of the intrahepatic duct systems, Acta
Anat (Basel) 11:599–615, 1931.
Albaret P, et al: À propos des caneaux hépatiques directement abou- Hobby JAE: Bilobed gallbladder, Br J Surg 57:870–872, 1970.
chés dans la voie biliaire accessorie, Ann Chir 35:88–92, 1981. Kune GA: The influence of structure and function in the surgery of
Bismuth H, et al: Major and minor segmentectomies—“réglées”—in the biliary tract, Ann R Coll Surg Engl 47:78–91, 1970.
liver surgery, World J Surg 6:10–24, 1982. McIndoe AH, Counseller VX: A report on the bilaterality of the liver,
Boyden EA: The accessory gallbladder: an embryological and compara- Arch Surg 15:589, 1927.
tive study of aberrant biliary vesicles occurring in man and the Newcombe JF, Henley FA: Left-sided gallbladder: a review of the lit-
domestic mammals, Am J Anat 38:177–231, 1926. erature and a report of a case associated with hepatic duct carci-
Boyden EA: The anatomy of the choledochoduodenal junction in man, noma, Arch Surg 88:494–497, 1964.
Surg Gynecol Obstet 104:641–652, 1957. Northover JMA, Terblanche J: A new look at the arterial blood supply
Champetier J, et al: Aberrant biliary ducts (vasa aberrantia): surgical of the bile duct in man and its surgical implications, Br J Surg
implications, Anat Clin 4:137–145, 1982. 66:379–384, 1979.
Couinaud C: Le foi: études anatomogiques et chirurgicales, Paris, 1957, Perelman H: Cystic duct reduplication, JAMA 175:710–711, 1961.
Masson. Rachad-Mohassel MA, et al: Duplication de la vésicule biliaire, Arch
Delmont J: Le sphincter d’Oddi: anatomie traditionelle et fonction- Fr Mal App Dig 62:679–683, 1973.
nelle, Gastroentrol Clin Biol 3:157–165, 1979. Rocko JM, et al: Calot’s triangle revisited, Surg Gynecol Obstet 153:410–
Eelkema HH, et al: Partial duplication of the gallbladder, diverticulum 414, 1981.
type: report of a case, Radiology 70:410–412, 1958. Rogers HI, et al: Congenital absence of the gallbladder with choledo-
Fields RC, et al: Biliary injury after laparoscopic cholecystectomy in a cholithiasis: literature review and discussion of mechanisms, Gastro-
patient with right liver agenesis: case report and review of the litera- enterology 48:524–529, 1975.
ture, J Gastrointest Surg 12:1577–1581, 2008. Scheele J, Stangl R: Segment-orientated anatomical liver resections. In
Goldsmith NA, Woodburne RT: Surgical anatomy pertaining to liver Blumgart LH, editor: Surgery of the liver and biliary tract, ed 2, New
resection, Surg Gynecol Obstet 195:310–318, 1957. York, 1994, Churchill Livingstone, pp 1557–1578.
Gross RE: Congenital abnormalities of the gallbladder: a review of 148 Strasberg SM, et al: Nomenclature of hepatic anatomy and resections:
cases with report of a double gallbladder, Arch Surg 32:131–162, a review of the Brisbane 2000 system, J Hepatobiliary Pancreat Surg
1936. 12:351–355, 2005.
Healey JE, Schroy PC: Anatomy of the biliary ducts within the human Ton That Tung: La vascularisation veineuse du foie et ses applications aux
liver: analysis of the prevailing pattern of branchings and the major resections hépatiques, Hanoi, 1939, Thèse.
variations of the biliary ducts, AMA Arch Surg 66:599–616, 1953. Ton That Tung: Les resections majeures et mineures du foie, Paris, 1979,
Hepp J, Couinaud C: L’abord et l’utilisation du canal hépatique gauche Masson.
dans les reparations de la voie biliare principale, Presse Med 64:947– Wood D: Eponyms in biliary tract surgery, Am J Surg 138:746–754,
948, 1956. 1979.
CHAPTER 3
Assessment of hepatic function: implications for the
surgical patient
Paul J. Karanicolas
60
Chapter 3 Assessment of hepatic function: implications for the surgical patient 61
Volumetric Thresholds
Despite the refinement in methods to measure the FLR, the
clinical application of the information gathered remains contro-
versial. It has long been clear that patients with lower FLR are
at increased risk of hepatic dysfunction, but the exact threshold
below which resection should not be performed is debated.
587.805 cm3 Several studies have attempted to address this fundamental
question, yielding different conclusions (Ferrero et al, 2007;
Kishi et al, 2009; Lin et al, 2014; Pulitano et al, 2014; Schindl
FIGURE 3.1. Volumetric assessment based on magnetic resonance et al, 2005; Shoup et al, 2003). The variable results may be
imaging. attributable to the heterogeneity of included patients (some
having background liver disease and others healthy livers),
methods used to calculate the FLR (TLV vs. TELV), indica-
the TLV to yield the total functioning liver volume can correct tions for PVE, and definitions of hepatic dysfunction. Further-
this but is very labor intensive and prone to measurement error more, only two studies analyzed their results using a formal
(Kubota et al, 1997). The direct measurement technique of receiving operator characteristic (ROC) curve to determine the
TLV is further limited by the fact that the parenchyma beyond optimal FLR threshold, and both studies were limited by small
tumors may be abnormal due to biliary or vascular obstruction. sample sizes (Ferrero et al, 2007; Schindl et al, 2005). Allowing
These limitations typically do not apply to the assessment of for these admittedly crucial differences, the optimal cutoff for
the FLR, which usually does not contain tumors. patients with a normal background liver appears to be between
An alternative method referred to as the total estimated liver 20% and 30%.
volume (TELV) was first proposed by Urata and colleagues Patients who have received preoperative chemotherapy are
(1995) in Japan for use in liver transplantation. Rather than at risk of background liver injury that impairs regeneration fol-
measuring the TLV directly and subtracting the volume of liver lowing partial hepatectomy (Dello et al, 2014; Narita et al,
tumors, this technique estimates the TLV based on body surface 2011; Kele et al, 2013) (see Chapters 71 and 100). There is
area (BSA). The formula was subsequently modified to apply to general consensus that patients treated with extensive preopera-
Western patients, based on the observation that Urata’s formula tive chemotherapy or who have evidence of background liver
underestimated TELV by an average of 323 cm3 (Heinemann injury require a larger FLR to allow safe hepatectomy, although
et al, 1999; Vauthey et al, 2000). The resulting equation, the exact threshold is again controversial. Two studies exam-
TELV = −794 + 1267 × BSA, has been extensively studied and ined this question and performed formal ROC curve analyses,
found to yield a precise estimate of TLV across institutions with reporting optimal thresholds of 31% and 48.5%, respectively
different CT scanners and three-dimensional reconstruction (Ferrero et al, 2007; Narita et al, 2012). The largest study
techniques (Vauthey et al, 2002). When the TELV is used as the includes 194 patients undergoing extended hepatectomy on the
denominator to calculate the FLR ratio (i.e., FLR/TELV), the right side, stratified by extent of preoperative chemotherapy,
resultant ratio is referred to as the standardized FLR (sFLR). with long-duration chemotherapy defined as greater than 12
The measured TLV was compared with the TELV in a weeks (86 patients) (Shindoh et al, 2013b). Using a minimum
recent study of 243 patients who underwent major liver resec- P-value approach, the authors concluded that the optimal
tion (three or more segments) (Ribero et al, 2013). There was cutoff value of FLR for preventing postoperative liver insuffi-
a strong correlation between the two measures across the popu- ciency in these patients was 30%.
lation; however, in overweight patients (body mass index [BMI] The optimal FLR threshold in patients with documented
> 25), TELV was significantly higher, yielding a lower sFLR in underlying liver disease is even less certain, given the additional
these patients. Based on the surgeons’ thresholds, 47 patients variability of defining the extent of background liver injury (see
were deemed to have insufficient liver volume for resection Chapters 71 and 103D). Some authors advocate for PVE in all
using TLV compared with 73 patients using TELV. According patients with chronic liver disease prior to right side hepatec-
to institutional practices at the time, patients who had sufficient tomy, and others apply a conservative threshold as high as 40%
liver volume based on TLV underwent resection, and the subset (Farges et al, 2003; Suda et al, 2009). Given the importance
of patients who had insufficient volume based on TELV had of background liver function, additional functional tests to
significantly worse outcomes than the patients who had suffi- assess the liver remnant should be considered prior to embark-
cient volume based on both calculations. The authors conclude ing on major hepatectomy in the setting of significant back-
that TELV (i.e., sFLR) is a better measure of postoperative ground liver disease.
hepatic insufficiency risk.
Over the past several years, a number of more sophisticated Response to Portal Vein Embolization
software packages have been developed to simplify the process In patients at increased risk of posthepatectomy liver failure,
of volumetric assessment. Several studies suggest that these hypertrophy of the FLR may be induced by preoperative
62 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
ipsilateral PVE (Hemming et al, 2003) (see Chapter 108C). (alanine aminotransferase, aspartate aminotransferase, and
Cross-sectional imaging is typically repeated 2 to 6 weeks fol- alkaline phosphatase), and markers of hepatic metabolism [bili-
lowing PVE, and the FLR (or sFLR) may be recalculated. The rubin] and synthetic function (albumin and international nor-
post-PVE FLR can be interpreted with the same thresholds malized ratio [INR]). Aberrations in any of these laboratory
previously discussed, although the degree of hypertrophy (DH), measures should prompt further investigation of background
defined as absolute difference between FLR before and after liver dysfunction, although none of them are sensitive or spe-
PVE, may be more informative (Ribero et al, 2007). In addition cific enough for surgeons to rely on exclusively.
to its therapeutic intent, PVE functions as a diagnostic test The Child-Turcotte and subsequent Child-Pugh scoring
analogous to a cardiac stress test; patients who do not experi- systems were developed to predict the risk of death in patients
ence substantial growth in the FLR following PVE should be undergoing surgical management of portal hypertension. Child-
suspected of harboring background liver disease and approached Pugh has since been applied to predict risk in patients with
with caution. hepatic cirrhosis undergoing a variety of other procedures. The
Recognizing that the DH is contingent upon the duration Child-Pugh score is easily calculated from three readily avail-
from PVE to reimaging, surgeons have proposed incorporating able laboratory tests (bilirubin, albumin, and INR) and two
some measure of growth rate into consideration. The kinetic clinical findings (ascites and encephalopathy). The Child-Pugh
growth rate (KGR) may be calculated by dividing the DH by score is a good marker of global liver function in a patient with
the number of weeks elapsed since PVE (Shindoh et al, 2013a). cirrhosis and may help in selection of patients appropriate for
In one study of 107 patients who underwent liver resection for resection, particularly in the setting of hepatocellular carci-
colorectal liver metastases with an sFLR volume of greater than noma. In general, surgery is reasonable to consider in patients
20%, KGR was a more accurate predictor of postoperative with class A cirrhosis, should be approached cautiously in
hepatic insufficiency than absolute sFLR or DH (area under patients with class B cirrhosis, and should be avoided in patients
the curve [AUC] 0.830) (Shindoh et al, 2013a). In this study, with class C cirrhosis. In patients without cirrhosis, the Child-
patients with a KGR less than 2% per week suffered a 21.6% Pugh score will almost always be normal even when there is
hepatic insufficiency rate and a 8.1% 90-day mortality rate, substantial background liver dysfunction; in this setting, it does
compared with no hepatic insufficiency or 90-day mortality in not predict postoperative liver dysfunction, and other tests are
patients with a KGR greater than 2% per week. In a similar needed.
study of 153 patients who underwent major hepatectomy after The Model for End-Stage Liver Disease (MELD) score is
PVE, post-PVE absolute FLR correlated poorly with liver a mathematical equation frequently used in liver transplanta-
failure (Leung et al, 2014). Both DH and KGR were good tion to allocate organs. The MELD score is similar to the
predictors of liver failure (AUC 0.80 and 0.79, respectively). Child-Pugh score in that it incorporates simple laboratory
Notably, posthepatectomy liver failure did not develop in any investigations, including serum bilirubin, creatinine, and INR,
patients with a KGR greater than 2.66% per week. although it is more cumbersome to calculate. It was initially
In summary, for patients with insufficient FLR (or sFLR) validated for the prediction of short-term survival in patients
to safely undergo hepatectomy, response to PVE provides a with cirrhosis and has subsequently been validated for long-
good measure of the remnant liver’s ability to hypertrophy. term survival as well. In patients with cirrhosis undergoing
Post-PVE FLR should be interpreted in combination with partial hepatectomy, a MELD score greater than 8 is a strong
some measure of extent of hypertrophy (either DH or KGR), predictor of perioperative mortality and decreased long-term
to optimally predict a patient’s risk of posthepatectomy liver survival (Delis et al, 2009; Hsu et al, 2009; Teh et al, 2005).
insufficiency. In contrast, in patients without documented background liver
injury, a MELD score is not strongly associated with inferior
FUNCTIONAL ASSESSMENT outcomes (Rahbari et al, 2011; Schroeder et al, 2006; Teh
OF LIVER REMNANT et al, 2008).
Thus, in patients with cirrhosis being considered for partial
Although a thorough assessment of the anticipated FLR volume hepatectomy, Child-Pugh and MELD scores provide good
is required prior to embarking on major hepatectomy, a com- measures of global liver function. Surgeons should approach
plete assessment should ideally also account for the quality of patients with Child-Pugh class B/C or MELD score greater
the background liver that will be preserved. The optimal than 8 with caution, and consider alternative treatment
method to assess hepatic function would be accurate, noninva- approaches. Clinical scoring systems are not sensitive enough
sive, inexpensive, specific to the remnant portion of the liver, to detect background liver injury and subsequent risk of post-
and widely reproducible. Unfortunately, none of the techniques operative liver dysfunction in patients without cirrhosis; other
currently available fulfill all of these criteria, and therefore methods of functional liver assessment are needed in these
none are frequently utilized in routine assessment. However, patients.
several newer techniques show promise, and with further inves-
tigation may find a role in routine assessment of liver function
Measurement of Hepatic Uptake, Metabolism,
(Table 3.1).
and Elimination
Clinical Scoring Systems Indocyanine Green Clearance
The simplest, most widely available method to assess liver func- Indocyanine green (ICG) clearance is the quantitative measure
tion relies on laboratory investigations either in isolation or of hepatic function most used worldwide. ICG is a water-
combined into clinical scoring systems. Clinicians are familiar soluble tricarbocyanine dye that binds to albumin and distrib-
with conventional liver laboratory tests routinely used in clinical utes rapidly and uniformly in the blood after intravenous
practice, including enzymatic measures of hepatocyte injury injection. ICG is exclusively cleared from the bloodstream by
Chapter 3 Assessment of hepatic function: implications for the surgical patient 63
Volume of liver Lower liver remnant volume is Can be easily calculated with Does not incorporate measure of
remnant (MRI, associated with worse conventional imaging underlying liver function
CT) outcomes Can be performed by surgeons Threshold for safe resection in setting of
Incorporates planned resection background liver disease unclear
Response of liver Failure of liver to hypertrophy Can be easily calculated with Requires invasive procedure that may not
remnant to in response to portal vein conventional imaging be necessary in some patients
portal vein embolization indicates Can be performed by surgeons
embolization underlying liver injury Incorporates planned resection
Clinical scoring Scoring systems are Easy to calculate Not sensitive enough for background liver
systems associated with poor Noninvasive dysfunction
(Child-Pugh, outcomes following other
MELD, etc.) procedures
ICG clearance ICG is metabolized by the Good measure of underlying liver Time consuming
liver, poor ICG clearance is function Measures total liver function, not specific
indicative of underlying liver to remnant
dysfunction Altered based on environmental conditions
99m
Hepatobiliary Tc- GSA binds to Provides anatomic and functional High interrater and interinstitution variability
scintigraphy hepatocyte receptors; information Limited availability
99m
Tc- IDA derivatives are May be specific to remnant liver
metabolized by the liver; May be combined with SPECT
poor uptake of either are
indicative of liver
dysfunction
Other measures of Metabolized almost Correlated with other measures Not widely available
metabolic exclusively by the liver of total liver function Limited data related to clinical outcomes
function (P450), poor clearance High interrater variability
(lidocaine, indicates underlying liver Time consuming
galactose, 13C dysfunction Measures total liver function, not specific
breath tests) to remnant
Altered based on environmental conditions
MRI with Taken up and cleared by Routinely available Not directly correlated with postresection
Gd-EOB-DTPA hepatocytes, poor uptake Frequently used in preoperative clinical outcomes
contrast indicates liver dysfunction assessment
May be specific to remnant liver
Provides other information
Transient Provides assessment of liver Noninvasive User dependent
elastography fibrosis Fast Not correlated with clinical outcomes
CT, Computed tomography; Gd-EOB-DTPA, gadolinium ethoxybenzyl dimeglumine; ICG, indocyanine green; MRI, magnetic resonance imaging; SPECT, ; 99mTc- GSA, technetium-99m–labeled galactosyl
serum albumin; 99mTc- IDA, technetium-99m–labeled iminodiacetic acid.
the liver in a similar manner to bilirubin and toxins, and then capillarization. Further, ICG clearance testing is a measure of
excreted unchanged into bile. Thus ICG clearance tests reflect global liver function, so if there is heterogeneous uptake in the
blood flow-dependent clearance, hepatocyte uptake and biliary liver (e.g., the portion being resected does not function as well
excretion. due to tumor, biliary obstruction, etc.), the results may be mis-
The conventional measurement of ICG clearance involves leading. Finally, ICG testing does not incorporate the extent of
intravenous injection of ICG, followed by serial collection resection, or conversely, the volume of the remnant that will
of venous blood at 5 minute intervals for 15 minutes. ICG remain. Researchers have attempted to mitigate some of these
clearance can also be measured noninvasively by pulse- limitations by creating scoring systems and decision trees that
spectrophotometry, which allows real-time monitoring of liver incorporate ICG (Du et al, 2011; Kim et al, 2015).
function (Okochi et al, 2002; Sakka et al, 2000;). The results
of ICG tests may be expressed as the percentage of ICG Nuclear Imaging Techniques
retained in the circulation 15 minutes after injection (ICG- Theoretically, nuclear imaging represents an attractive preop-
R15), the plasma disappearance rate (ICG-PDR), and the erative hepatic assessment, combining anatomic considerations
elimination rate constant (ICG-k). Several studies have identi- (FLR volume) with both total and regional liver functional
fied an association between elevated ICG-R15 and posthepa- assessment. Several scintigraphic tests have been developed
tectomy complications, with proposed threshold values of over the past few decades, but the most widely used radiophar-
ICG-R15 ranging from 14% to 20% (Das et al, 2001; Fan maceutical imaging methods for liver functional assessment are
et al, 1995; Lau et al, 1997). technetium-99m–labeled galactosyl serum albumin (GSA)
Despite the theoretical attractiveness of ICG clearance as scintigraphy and hepatobiliary scintigraphy (HBS) with 99mTc-
a simple measure of hepatic function, several limitations labeled iminodiacetic acid (IDA) derivatives. Both of these
have hampered enthusiasm for its widespread use. The results of methods provide quantitative data on the total and regional
ICG clearance tests are not reliable in patients with hyperbiliru- hepatic function, although they are based on different principles
binemia, or in patients with intrahepatic shunting or sinusoidal and therefore interpretation varies.
64 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
99m
Tc-GSA is an analogue of a glycoprotein (ascites sialo- (Oellerich et al, 2001; Reichen, 1993). Unfortunately, the test
glycoprotein) that binds to receptors on the hepatocyte cell is limited by poor reliability and the need for frequent monitor-
membrane and is taken up by the hepatocytes. Chronic liver ing; therefore its present application in preoperative assessment
disease results in diminished hepatocyte glycoprotein receptors of liver function is investigational only. Galactose elimination
and subsequent accumulation of plasma glycoproteins. To capacity also accurately reflects metabolic function of the liver
perform dynamic scintigraphy, an intravenous bolus of 99mTc- but is similarly limited by practical constraints and alterations
GSA is administered, and images are obtained by using a due to environmental conditions (Ranek et al, 1976). Finally,
gamma camera positioned over the heart and liver. Several there are a variety of 13C breath tests available that follow the
parameters may be calculated to document the extent of hepatic same principles, including the 13C-methacetin breath test
99m
Tc-GSA uptake, including the hepatic uptake ratio (LHL15 (LiMAx; Humedics, Berlin) (Cieslak et al, 2014; Stockmann
[receptor index: uptake ratio of the liver to the liver plus heart et al, 2009). Unfortunately, these tests also suffer from poor
at 15 min]) and the blood clearance ratio (HH15 [blood clear- interobserver reliability and alterations based on physiologic
ance index: uptake ratio of the heart at 15 min to that at conditions so should be viewed as experimental at present
3 min]). In patients with cirrhosis, 99mTc-GSA uptake corre- (Afolabi et al, 2013).
sponds well with other conventional liver function tests, includ-
ing ICG clearance, and predicts histologic severity of disease Magnetic Resonance Imaging Hepatic Agents
better than ICG clearance in a substantial proportion of patients MRI with contrast enhancement offers high-resolution cross-
(Kwon et al, 1995; Nanashima et al, 2004). Several small sectional assessment of background liver anatomy and accurate
studies have demonstrated an association between poor 99mTc- characterization of hepatic tumors. MRI is more sensitive and
GSA uptake and postoperative complications after liver resec- specific than CT for the detection of primary and metastatic liver
tion (Kim et al, 1997; Nanashima et al, 2004; Takeuchi et al, neoplasms and is used routinely at most centers before embark-
1999). However, 99mTc-GSA uptake is limited by interoperator ing on liver resection (Zech et al, 2014). Gadolinium ethoxyben-
and interinstitutional differences and does not provide a zyl dimeglumine (Gd-EOB-DTPA) is a liver-specific contrast
measure of regional liver function (Koizumi et al, 1997). To agent that has as much as 50% hepatobiliary excretion in a
address this limitation, 99mTc-GSA scintigraphy may be com- normal liver (Van Beers et al, 2012). Gd-EOB-DTPA improves
bined with static single-photon emission computed tomography– the detection and characterization of focal liver lesions and
CT (SPECT-CT) to allow a three-dimensional measurement diffuse liver disease. Given the hepatic uptake and elimination of
of 99mTc-GSA uptake. Results of dynamic SPECT-CT may Gd-EOB-DTPA, contrast-enhanced MRI may also provide
help to predict postoperative liver failure; however, this method functional assessment of the background liver (Fig. 3.2).
suffers from the same interobserver variability and environmen- Several small studies have demonstrated correlation
tal factors as dynamic 99mTc-GSA scintigraphy (Beppu et al, between Gd-EOB-DTPA uptake on MRI and conventional
2011; Iimuro et al, 2010; Satoh et al, 2003). Thus, although measures of liver function (Nilsson et al, 2013; Nishie et al,
this is a promising tool with some utility in the preoperative 2012; Saito et al, 2014). There are several theoretical and
assessment of patients, further work is needed to standardize practical advantages to using Gd-EOB-DTPA–enhanced MRI
measurement before wide implementation. to assess liver function. First, MRI is routinely available and
99m
Tc-mebrofenin is an organic IDA derivative with similar frequently used in the preoperative assessment of these
properties to ICG: It has high hepatic uptake, low displacement patients, so no additional testing is required. Second, func-
by bilirubin, and low urinary excretion. The test is administered tional assessment may be focused on the planned FLR in
in an identical manner to 99mTc-GSA scintigraphy, using a cases of heterogeneous uptake, rather than calculating uptake
gamma camera and calculating similar parameters and ratios. for the whole liver as is the case in most other functional
However, the uptake ratio is divided by the patient’s BSA to quantitative tests. Finally, MRI provides visual assessment of
compensate for differences in metabolic requirements. 99mTc- background liver injury, including steatosis and fibrosis, which
mebrofenin HBS correlates well with ICG clearance, and may further assist in preoperative decision making. However,
appears to be a good marker of post resection liver function enthusiasm for the use of MRI for functional liver assessment
(Bennink et al, 2004; de Graaf et al, 2010a; Dinant et al, 2007; must be tempered by the lack of prospective data demonstrat-
Erdogan et al, 2004). HBS may also be combined with ing a clear relationship between Gd-EOB-DTPA uptake and
SPECT-CT to allow three-dimensional assessment of the FLR, clinical outcomes postresection. Further research is needed to
particularly in patients undergoing PVE (de Graaf et al, 2010b). determine whether MRI with Gd-EOB-DTPA contrast will
The main limitation of HBS is, again, interobserver and inter- indeed be the panacea of functional liver assessment that it
institution variability. Although these techniques offer great appears to be.
advantages compared with more conventional methods, further
research is needed to ensure that results are reproducible across Transient Elastography
different settings before wider application. Ultrasound transient elastography (TE) has been reported as a
test to estimate the extent of liver fibrosis. Ultrasound TE has
Other Measures of Metabolic Function the clear advantages of being noninvasive and fast but is limited
In addition to ICG, several other compounds are metabolized by significant interobserver variability and anatomic variations
almost exclusively by the liver cytochrome P450 system and (Kawamoto et al, 2006; Sandrin et al, 2003). Furthermore,
have been investigated as potential markers of hepatic function. although results of ultrasound TE are correlated with extent of
For example, lidocaine is metabolized to monoethylglycinexyli- fibrosis, the impact of abnormal TE on clinical outcomes fol-
dide (MEGX) primarily in the liver. The MEGX test has lowing resection is unknown. Thus further research is needed
been studied in transplantation and critical care medicine and before incorporating this imaging modality into routine clinical
appears to correlate with other measures of hepatic metabolism practice.
Chapter 3 Assessment of hepatic function: implications for the surgical patient 65
Texture Analysis
Texture analysis is an established technique that characterizes
regions of interest in an image based on spatial variations in pixel
intensity. On CT imaging, texture analysis can potentially quan-
tify regional variations in enhancement that cannot be assessed
by inspection. Several studies have shown potential utility of this
new technique for tumor diagnosis and characterization and
prognostication. In a recent study by Simpson and coworkers
(2015) analyzing patients submitted to major hepatic resection,
texture variables of preoperative CT scans showed promise for
predicting postoperative hepatic failure, and may represent a
new means of preoperative risk stratification.
A
CONCLUSION
Hepatobiliary surgeons now have a variety of tools at their
disposal to assist with preoperative assessment of hepatic func-
tion. The gold standard remains volumetric-based assessment
of the FLR with cross-sectional imaging (CT or MRI). In
patients in whom there is concern about insufficient liver
volume or background liver injury, response to PVE provides
a functional assessment of the FLR in addition to its therapeu-
tic role. Quantitative measures of hepatic uptake, metabolism,
and elimination, including ICG clearance, nuclear scintigraphy,
and MRI hepatic-specific contrast agents, may have a role in
assessment of patients with borderline FLR volume or back-
ground liver disease but are currently limited by physiologic
alterations and poor reproducibility. Further refinement of
these techniques may allow the development of algorithms or
B decision aids that incorporate both volumetric and functional
assessment of the FLR.
FIGURE 3.2. Magnetic resonance imaging with gadolinium ethoxy-
benzyl dimeglumine contrast on two patients demonstrating normal References are available at expertconsult.com.
uptake (A) and diffusely decreased uptake (B).
Chapter 3 Assessment of hepatic function: implications for the surgical patient 65.e1
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CHAPTER 4
Pancreatic Physiology and Functional Assessment
Alessandro Paniccia and Richard D. Schulick
66
Chapter 4 Pancreatic Physiology and Functional Assessment 67
The islets of Langerhans receive approximately 20% of the The main glucose transporters on pancreatic β cells are
pancreatic arterial flow, with distribution significantly influ- GLUT-2, which are highly expressed in rodents (van de Bunt
enced by the different phases of digestion (Bonner-Weir, 1993). & Gloyn, 2012), and GLUT-1 and GLUT-3, both recently
Furthermore, an insuloacinar portal system responsible for recognized to be expressed at high levels on human β cells (Fig.
draining blood and secreted hormones from the islets of Lang- 4.1) (McCulloch et al, 2011). The GLUT transporters allow
erhans to the acinar element of the pancreas has been described equalization of the intracellular and extracellular glucose con-
in several species, including humans (Merkwitz et al, 2013). centrations. If the glucose concentration exceeds 5 mmol/L,
Therefore hormones secreted by the islet of Langerhans are intracellular β-cell glucokinase enzymes activate to allow fine
directly transported to the acinar cells, where they can exert a regulation of insulin secretion (Tan, 2014). Acting as a “glucose
local regulatory function. In addition, a local regulatory effect sensor,” these enzymes are responsible for the phosphorylation
on endocrine and exocrine pancreatic function is exerted by of glucose to glucose-6-phosphate (Lenzen, 2014; Matschinsky
several neuropeptides, including neuropeptide-Y, gastrin- et al, 1998). Glucose-6-phosphate accumulates in the β cell, is
releasing peptide, and calcitonin gene–related peptide (CGRP). metabolized, and contributes to an increase in cellular adenos-
ine triphosphate (ATP). The β-cell membrane is rich in ATP-
SYNTHESIS AND STORAGE OF INSULIN dependent potassium channels, which subsequently undergo
closure in response to the surge in ATP, resulting in membrane
In 1923 Banting and McLeod, two Canadian surgeons, were depolarization (Rorsman et al, 2014; Yang et al, 2014). Depo-
awarded the Nobel Prize in Physiology or Medicine for the larization activates voltage-gated L-type calcium channels,
discovery of insulin (Banting, 1926). This 51 amino acid poly- leading to influx of calcium into the cell (Rorsman & Braun,
peptide is primarily responsible for maintaining serum glucose 2013; Rutter & Hodson, 2013) The increased intracellular
between 4 mM and 8 mM (70 to 140 mg/dL) during periods calcium concentration leads to margination of secretory gran-
of feeding and fasting (Rorsman & Braun, 2013). In addition, ules, their fusion with the cell membrane, and exocytosis of
insulin regulates lipid and protein metabolism. The gene their content, including insulin and its intermediate products
responsible for encoding insulin is located on the short arm of (e.g., C-peptide) (Yang et al, 2014). This process characterizes
chromosome 11 and leads to the translation of a preprohor- the “first phase” of insulin release, in which insulin is rapidly
mone protein known as preproinsulin within the β cell. Prepro- secreted within 3 to 5 minutes of glucose administration and
insulin consists of a leading sequence of 24 amino acids, terminates within 10 minutes. The loss of the first phase of
followed by three domains named “B,” “C,” and “A.” Succes- insulin secretion is one of the earliest metabolic defects identi-
sive cleavage processes take place starting at the time of transla- fied in type 2 diabetes mellitus (T2DM) (Nagamatsu et al,
tion until the final secretion. First, cleavage of the leading 2006). The “second phase” of insulin secretion is longer lasting
sequence in the endoplasmic reticulum leads to the formation (reaching a plateau in insulin secretion after 2 to 3 hours), and
of proinsulin. As the proinsulin is arranged into secretory gran- its regulation is not completely understood (Henquin, 2009;
ules in the trans-Golgi, additional proteases cleave the central Huang & Joseph, 2014). However, recent mathematic models
31 amino acid C-peptide. This leads to the formation of a suggest that the second phase is characterized by the recruit-
mature insulin peptide composed of an A-chain and B-chain ment and mobilization of intracellular granules containing
held together by two disulfide bonds, ready to be released in insulin (as opposed to predocked granules as in the first phase)
the secretory vesicle. Cleaved C-peptide and other intermediate in a dose-dependent glucose response (Stamper & Wang, 2013).
products, such as proinsulin, remain present in the secretory The amino acid arginine (L-arginine) is another well-known
granules and are eventually released together with the mature insulin secretagogue. Following uptake into the β cells through
insulin (Boron & Boulpaep, 2012). The mature insulin peptide a cationic amino-acid transporter (CAT), arginine leads to
has a plasma half-life of 4 minutes. It is rapidly internalized by depolarization of cell membrane, which triggers calcium influx
target organs expressing its receptor and degraded by the (Smith et al, 1997). Furthermore, L-arginine can stimulate the
kidneys and liver (Marques et al, 2004). Notably, C-peptide release of GLP-1, which acts at its receptor (GLP-1R) to
has a plasma half-life of 30 minutes and is excreted unchanged augment glucose-stimulated insulin secretion from pancreatic
by the kidneys, making it a clinically important marker of β cells (Clemmensen et al, 2013; Tolhurst et al, 2009).
endogenous insulin secretion (Jones & Hattersley, 2013). The secretion of insulin from pancreatic β cells is further
potentiated by the incretin effect through the enteroinsular axis
STIMULUS-SECRETION COUPLING (Diab & D’Alessio, 2010; Opinto et al, 2013). The incretin
FOR INSULIN SECRETION effect is the phenomenon whereby the presence of nutrients,
especially carbohydrates, in the duodenal lumen stimulates
The rise of islet cell transplantation has led to a renewed under- cells in the gut mucosa to release potent insulin secretagogues
standing of human β-cell regulation, building on earlier work (Drucker, 2013). The ingestion of nutrients stimulates duode-
completed in rodents. Insulin is released from β cells through nal and jejunal K cells to produce and release GIP, a well-
two mechanisms: unstimulated and stimulated secretion. studied incretin. In addition, GLP-1 is produced and release
Unstimulated secretion or basal insulin secretion occurs every by the L cells (also known as enteroglucagone cells), located in
6 to 8 minutes (Song et al, 2002). Stimulated secretion of the distal small bowel, colon, and rectum. It has been shown
insulin occurs in response to several stimuli, including glucose, that orally administered glucose is able to stimulate insulin
amino acids (e.g., arginine), acetylcholine (ACh), glutamate, secretion as much as 25% more than intravenously adminis-
and incretins such as gastric inhibitory peptide (GIP) and tered glucose, likely through the incretin effect (Ahrén, 2013).
glucagon-like peptide-1 (GLP-1). The change in extracellular GIP and GLP-1 play major roles in the enteroinsular axis,
glucose concentration, however, is the dominant factor control- mainly through activation of adenylate cyclase and subsequent
ling β-cell function. increase in intracellular cyclic adenosine monophosphate
68 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Incretin
Acetylcholine GIP/GLP-1
Glucose
GLUT-1 M3
GLUT-2 M1 †Gαs
GLUT-3 Gαq*
Glucokinase PIP2
Glucose-6-P Phospholipase-C Adenylate
Cyclase
Pyruvate
L-Arginine CAT
IP3 DAG cAMP
KREBS
CYCLE Protein Kinase C Protein Kinase A
Voltage-gated
Open ↑Cytosolic
Ca2+ channel
Ca2+ Insulin
Insulin
FIGURE 4.1. Stimulus-secretion coupling for insulin secretion. Insulin is secreted following food ingestion; glucose, acetylcholine (ACh), incretins,
and amino acids are the most important physiologic secretagogues. Glucose enters the human β cell mainly via the glucose transporters GLUT-1
and GLUT-3 and, to a lesser extent, via GLUT-2. Once in the β cell, glucose is phosphorylated to glucose-6-phosphate by an intracellular glucokinase
(GCK) and eventually is metabolized to produce adenosine triphosphate (ATP), leading to an elevation of the cytosolic ATP/diphosphate (ADP) ratio.
The increase in the intracellular ATP content is responsible for the closure of the ATP-dependent K+ channel. The resulting increased membrane
potential, caused by the closure of the ATP-dependent K+ channel, prompts the opening of voltage-dependent Ca2+ channels, leading to an increase
in intracellular Ca2+ levels. Arginine is a positively charged amino acid that leads to depolarization of the β cell following its uptake by a cationic
amino-acid transporter (CAT); the membrane depolarization leads to opening of voltage-dependent Ca2+ channels, allowing entry of Ca2+ into the
cell. The increase in intracellular Ca2+ triggers exocytosis of insulin-containing secretory granules. ACh, released from vagal efferent and α cell, binds
to the muscarinic ACh receptor M3, which is coupled with a phospholipase C, resulting in the production of inositol-1,4,5-triphosphate (IP3) and
diacylglycerol (DAG). Eventually, IP3 triggers the release of intracellular Ca2+, and DAG causes activation of protein kinase C (PKC). The incretins
(gastric inhibitory peptide [GIP] and glucagon-like peptide-1 [GLP-1]) bind to the extracellular domain of a G protein-coupled receptor to mediate
signal transduction by activation of adenylate cyclase, which acts to elevate intracellular cyclic adenosine monophosphate (cAMP) concentrations
and leads to activation of protein kinase A. Ultimately, the activation of protein kinase C and protein kinase A leads to protein phosporylation and
secretion of insulin. *Gαq, Membrane-associated heterotrimeric G protein that activates phospholipase C (PLC); †Gαs, membrane-associated het-
erotrimeric G protein that activates the cAMP-dependent pathway by activating adenylate cyclase; PIP2, phosphatidylinositol-4,5-bisphosphate.
(cAMP). The increase in cAMP leads to activation of protein increase in inositol-1,4,5-triphosphate (IP3) (Ruiz de Azua
kinase A, with subsequent phosphorylation and activation of et al, 2011). Additionally, ACh stimulates the somatostatin-
exocytosis-related proteins. Furthermore, cAMP activates secreting δ cell via M1 receptors. As somatostatin is known to
L-type calcium channels, culminating in insulin release (see inhibit insulin secretion, it appears that endogenous cholinergic
earlier). signaling provides a direct stimulatory and indirect inhibitory
Acetylcholine plays a pivotal role in glucose homeostasis. input to β cells, allowing further regulation of insulin secretion
Recently, it has been reported that in human islets, ACh acts (Molina et al, 2014).
primarily as a nonneuronal paracrine signal released from α cells
rather than as a neural signal, as previously described in rodent GLUCAGON AND OTHER ISLET HORMONES
islets (Rodriguez-Diaz, et al, 2011b). In fact, ACh stimulates
the insulin-secreting β cell via the muscarinic ACh receptors The islets of Langerhans secrete many additional hormones,
M3 and M5, causing release of insulin (Molina et al, 2014). including glucagon (α cells), somatostatin (δ cells), pancreatic
The activation of the M3 receptor leads to the release of calcium polypeptide (F cells), and ghrelin (ε cells) (Jain & Lammert,
from intracellular stores through a phospholipase C–mediated 2009). Furthermore, islets contain a variable, but small, number
Chapter 4 Pancreatic Physiology and Functional Assessment 69
of cells responsible for secreting pancreastatin, serotonin, and pancreatitis (Ito et al, 2007; Levy et al, 2006) (see Chapters 56
vasointestinal polypeptide (VIP) (Ohta et al, 2011; Sanlioglu to 58).
et al, 2012; Valicherla et al, 2013).Glucagon, a 29–amino-acid
peptide (molecular weight, 3.5 kDa), counteracts the effect of EXOCRINE PANCREAS
insulin by increasing blood glucose concentration through stim-
ulation of glycogenolysis, gluconeogenesis, and ketogenesis The exocrine pancreas constitutes 80% to 90% of the gland
(Cryer, 2012). Secretion from islet α cells directly into the mass and secretes the majority of digestive enzymes, as well as
portal system is largely in response to protein ingestion. Glu- approximately 2000 mL of colorless, odorless, and isosmotic
cagon at physiologic concentration exerts its function primarily alkaline protein-rich fluid (pH, 7.6-9.0) daily. It is mainly regu-
in liver tissue through activation of cAMP pathways, where lated by the neuroendocrine system, and it is integrated ana-
it promotes gluconeogenesis and indirectly ketogenesis tomically and physiologically with the endocrine pancreas,
(Ramnanan et al, 2011). In addition, glucagon indirectly stim- which helps modulate its function (Barreto et al, 2010).
ulates fatty oxidation through the carnitine acylcarnitine trans-
locase system (CAT). This leads to an increase in the ketone EXOCRINE PANCREAS STRUCTURE
bodies β-hydroxybutyric acid and acetoacetic acid, which exit
the liver to be used by other tissues as metabolic fuel. Glucagon The exocrine pancreas consists primarily of two distinct but
inhibition is caused by increased blood glucose concentration integrated units: the acinus and the ductal network.
of glucose as well as through paracrine effects of insulin and
somatostatin within the islet (Gylfe & Gilon, 2014). Acinus
Somatostatin, which acts primarily as an inhibitory hormone, The acinus is a functional unit mainly dedicated to the produc-
is secreted by the islet δ cell in addition to several other organs, tion and secretion of digestive enzymes (6 as much as 20 g
including the hypothalamus and the D cells of the gastrointesti- daily). It is composed of 15 to 100 pyramidal-shaped cells (as
nal tract. Among others, somatostatin inhibits insulin, glucagon, much as 30 µm apical base height) known as acinar cells
gastrin, and VIP. Its broad inhibition makes somatostatin and its (Cleveland et al, 2012). The acinar cells are polarized epithelial
pharmacologic analogues (e.g., octreotide) useful therapeutic cells rich in rough endoplasmic reticulum and characterized by
agents in the medical management of secreting pancreatic neu- an abundance of secretory zymogen granules within the apex.
roendocrine tumors (e.g., insulinoma) along with other medical The acinus is organized concentrically around a central lumen
diseases (e.g., Cushing disease, acromegaly, carcinoid, etc.) that is in continuity with the proximal end of an intercalated
(Lamberts et al, 1996) (see Chapter 65). Furthermore, soma- duct, where it drains its secretions. Several acini form a pancre-
tostatin analogues are used in treatment of some surgical com- atic lobule, which is separated from other lobules by thin layers
plications. Recently, pasireotide, a multisomatostatin receptor of connective tissue.
ligand, significantly decreased pancreatic leak complications fol-
lowing pancreatic surgery (Allen et al, 2014) (see Chapter 27). The Ductal Network
Pancreatic polypeptide (PP) is produced and released by The ductal network serves two critical functions: transport of
islet F cells; however, its physiologic role remains under inves- exocrine secretions from the acini to the duodenum and pro-
tigation (Holzer et al, 2012). Some studies suggest that absence duction of a solution rich in bicarbonate and electrolytes (Fig.
of PP secretion, resulting from removal of the uncinate process 4.2). The bicarbonate and water released in the ductal network
(rich in islet F cells) during pancreaticoduodenectomy, can lead facilitate the transport and flushing of acinar secretions through-
to pancreatogenic diabetes (Maeda & Hanazaki, 2011). out the pancreatic ducts and, most important, optimize the pH
Ghrelin, produced by the ε cells, also known as the “hunger of the solution in which pancreatic enzymes are secreted (Hegyi
hormone,” is a centrally active neuropeptide that participates & Petersen, 2013).
in metabolic regulation, growth hormone release, and energy The ductal network starts with small intercalated ducts
balance (Wierup et al, 2014; Heppner & Tong, 2014). originating from different acini, which then join to form an
intralobular duct. This serves to drain an individual pancreatic
PANCREATITIS CONSEQUENCES ON lobule. Intralobular ducts then drain into larger interlobular
ENDOCRINE PANCREAS FUNCTION ducts, which then empty into the main pancreatic duct, releas-
ing the pancreatic secretions into the duodenum, through the
Pancreatic endocrine insufficiency is a dreaded consequence of ampulla of Vater (Pandiri, 2014; Ashizawa et al, 2005).
acute pancreatitis. Recent studies suggest that following hospi- The ductal network is composed of highly specialized epi-
talization for the first episode of acute pancreatitis there is as thelial cells with varying morphologies and functions (Cleve-
much as a 40% risk of prediabetes and/or diabetes mellitus land et al, 2012). Cells of the intercalated duct are characterized
(Das et al, 2014). Approximately 15% of newly diagnosed dia- by minimal cytoplasm and by a squamous-shaped appearance.
betes mellitus occurs within 12 months from the first episodes On the contrary, cells in the main pancreatic duct have an
of acute pancreatitis, and the risk remains high, increasing abundance of cytoplasm rich in mitochondria and are charac-
significantly with time. It appears that development of endo- terized by a cuboidal shape.
crine insufficiency is independent from the severity of the Ductal cells contain substantial levels of cytoplasmic car-
episode of acute pancreatitis (Das et al, 2014). This suggests bonic anhydrase, an enzyme necessary for bicarbonate produc-
that the mechanisms that lead to endocrine insufficiency might tion (Ishiguro et al, 2012).
be partially unrelated to the amount of pancreatic necrosis.
Alternative mechanisms have been proposed and are currently Centroacinar Cells
under investigation. It is worth mentioning that the risk for Cuboidal-shaped centroacinar cells are present at the junction
diabetes mellitus can be as high as 80% in patients with chronic between the acinus and the ductal cells of the intercalated
70 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
A B C D
Centroacinar
cell
Intralobular
Intercalated duct
duct
Small
interlobular duct
Main/large
interlobular duct
Acinar Ductal
FIGURE 4.2. Anatomic organization of the pancreatic ductal network. A, Centroacinar cells are present at the junction between the intercalated
duct and the acinar cell (white arrowhead; scale bar: 10 µm). B, Intercalated duct (also known as terminal duct) originates at the level of the acini
and are composed of cell characterized by minimal cytoplasm and by squamous-shaped appearance. The intercalated ducts merge into intralobular
ducts (white arrowhead) that are lined by cuboidal epithelia and serves to drain an individual pancreatic lobule (scale bar: 10 µm). C, Intralobular
ducts join to form small interlobular ducts that eventually merge into (D) larger interlobular ducts that are lined by cuboidal epithelium (scale bar: 10
µm). Exocrine pancreatic secretions ultimately reach the main pancreatic duct and are released in the duodenum through the ampulla of Vater (not
shown). (Adapted from Reichert M, Rustgi AK: Pancreatic ductal cells in development, regeneration, and neoplasia, J Clin Invest 121:4572–
4578, 2011.)
duct. Recognized as morphologically distinct from acinar cells, compartment could contribute, at least in part, to the develop-
centroacinar cells are smaller than acinar cells (≈10 µm in ment of mucinous metaplasia and pancreatic intraepithelial
diameter), have a high nuclear-to-cytoplasm ratio, and have neoplasia (Strobel et al, 2010) (see Chapter 9B).
long cytoplasmic processes that allow contact with other cells
(i.e., centroacinar, acinar, and islet cells) (Cleveland et al,
2012; Leeson & Leeson, 1986; Pour, 1994). The role of the NEUROHORMONAL REGULATION OF EXOCRINE
centroacinar cells remains under investigation, but some PANCREATIC FUNCTION
authors suggest that centroacinar cells could represent progeni-
tor multipotent pancreatic cells and potentially be involved in
Digestive and Interdigestive Periods
malignant transformation (Seymour et al, 2007; Stanger et al, of Pancreatic Secretion
2005). Pancreatic exocrine secretion can be temporally categorized
into an interdigestive and digestive secretion period. Between
Ductal Epithelial Compartment meals, the intestinal migrating myoelectric complex (MMC) is
Ductal epithelial compartments (also known as pancreatic duct responsible for the cyclic stimulation of the exocrine pancreas
glands) are distributed along the pancreatic ducts and resemble (interdigestive period) (Zimmerman et al, 1992). The cholin-
blind outpouches or small branches originating from the pan- ergic stimuli that regulate the MMC cause cyclic pancreatic
creatic ducts. The cell lining of these outpouches consists of secretion of a fluid rich in bicarbonate (every 60 to 120 minutes).
columnar-shaped cells, characterized by abundant supranu- These secretions appear to facilitate the removal of bacteria and
clear cytoplasm and basally located nuclei (Cleveland et al, food debris from the small intestine; however, definitive agree-
2012). Their physiologic function remains under investigation; ment of their function has not been reached (Pandol, 2010).
however there is evidence to suggest that these cells undergo The digestive secretion period begins following the ingestion
selective expansion during chronic epithelial injuries. Some of a meal bolus and is characterized by three distinct phases:
authors have hypothesized that cells in the ductal epithelial cephalic, gastric, and intestinal. Each phase is determined by
Chapter 4 Pancreatic Physiology and Functional Assessment 71
the location of the meal bolus in the gastrointestinal tract, and Evidence suggests that muscarinic receptors (M1 and M3)
it is regulated by different secretory signals (Pandol, 2010). are predominantly expressed on acinar cells and are involved
The cephalic phase, elicited by the anticipation of food, the in regulating exocrine function, making ACh the principal neu-
smell, the taste, and the act of chewing, stimulates exocrine rotransmitter (Nakamura et al, 2013). This is supported by
secretion via the vagus nerve (Power & Schulkin, 2008). In this studies examining the mechanism of action of CCK. During
initial phase, pancreatic secretions are mainly composed of the intestinal phase of pancreatic secretion, the I cell of the
digestive enzymes and low levels of bicarbonate, indicating duodenum (also present in the jejunum), releases CCK primar-
principally an acinar-type secretion. ACh is the primary neu- ily in response to products of the digestion of fat, protein, and,
rotransmitter, although acinar cells have been shown to express to a lesser extent, starch. CCK then causes the release of diges-
G protein–coupled receptors (GPCRs) for gastrin-releasing tive enzymes and bile from the pancreas and gallbladder,
peptide (GRP) and VIP, suggesting a role for these peptides in respectively. Although only low levels of CCK receptor protein
the cephalic phase (Anagnostides et al, 1984; Holst et al, 1983). have been identified on human acinar cells, intrapancreatic
The gastric phase is initiated once the meal reaches the vagal nerve terminals express CCK receptors (Miyasaka et al,
stomach and is stimulated by gastric distention (Kreiss et al, 2002; Niebergall-Roth & Singer, 2006; Singer & Niebergall-
1996). A low volume of enzyme-rich secretion characterizes Roth, 2009). These receptors bind CCK and release ACh in
this phase, and it is accompanied by minimal water and bicar- the proximity of acinar cells. This suggests that the cholinergic
bonate secretion. pathway regulates exocrine function. Additional studies support
The intestinal phase begins with the entry of chyme and this hypothesis as the effect of CCK on pancreatic exocrine
gastric acid juice into the duodenum. In this phase, one of the secretion can be prevented and almost abolished by atropine
main regulatory mechanisms is the vasovagal enteropancreatic administration (Li et al, 1997; Mussa & Verberne, 2013;
reflex that is mediated through the dorsal vagus center. The Owyang, 1996; Soudah et al, 1992).
presence of chyme in the duodenum activates efferent fibers of Some ingested nutrients exert direct or indirect regulatory
enteric neurons that stimulate intrapancreatic postganglionic effects on pancreatic cells. Amino acids, especially phenylala-
neurons to release ACh. In addition, the presence of hydrogen nine, valine, methionine, and tryptophan are potent stimulants
ions (pH, ≤ 4.5) stimulates duodenal S cells to release secretin of exocrine pancreatic secretion. Furthermore, intraluminal
into the bloodstream. Secretin acts primarily on ductal cells fatty acids, monoglycerides, and, to a lesser extent, glucose
through its receptor GPCR, causing release of fluid and bicar- stimulate the secretion of digestive enzymes during the intesti-
bonate and, to a lesser extent, acinar secretion (Chey & Chang, nal phase (Pandol, 2010).
2014).
Feedback Inhibitory Regulation
Water, Bicarbonate, and Ion Secretion From the Feedback regulation to the exocrine pancreas is provided by
Ductal Network signals originating in the proximal and distal intestine. The
The role of the ductal network is of paramount importance for main factors identified are monitor peptide, luminal CCK-
the optimal function of the exocrine pancreas. The cells of the releasing factor (LCRF), secretin-releasing factors (e.g., phos-
ductal network are primarily under the control of secretin, pholipase A2), and peptide tyrosine tyrosine (PYY) (Barreto
which stimulates the centroacinar and ductal cells to release et al, 2010; Li et al, 2001; Liddle, 1995; Moran & Kinzig,
water and bicarbonate (Chey & Chang, 2014). These secre- 2004; Naruse et al, 2002). The action of these enzymes is
tions act as a vehicle for the transport of inactive digestive dependent on the presence or the absence of intraluminal
zymogens from the acinar cells to the duodenum. Furthermore, trypsin. Evidence suggests that trypsin inactivates monitor
their alkaline nature (pH, 7.6 to 9.0) helps neutralize the acidic peptide and LCRF, therefore preventing augmentation of CCK
chyme, in which nutrients are delivered from the stomach, release from the I cell. Once trypsin is occupied by the presence
resulting in an optimal neutral pH for the action of digestive of meal chyme, monitor peptide and LCRF are not digested
enzymes. The concentration of sodium bicarbonate (NaHCO3) and can augment CCK release from the I cell. Eventually, the
in pancreatic secretions can reach up to 140 to 150 mM, and excess of digestive protease in the duodenal lumen leads to
chloride secretion varies inversely to bicarbonate concentration, digestion of both monitor peptide and LCRF, preventing
keeping [HCO3−] + [Cl−] constant at approximately 160 mM further pancreatic enzyme secretion (Pandol, 2010).
(Ishiguro et al, 2012). Neuroendocrine L cells present in ileum and colon are stim-
Secretin also promotes an increase of blood flow to the ulated by the presence of intraluminal oleic acid to release PYY.
entire organ (Chey & Chang, 2014). During a meal, the blood This is a centrally active neuropeptide that exerts its action on
flow to the pancreas increases as much as 4 mL/min from a the area postrema of the brain, decreasing vagal cholinergic
baseline of 0.2 or 0.3 mL/min (Pandol, 2010). mediation of CCK-stimulated pancreatic secretion (Lin &
Taylor, 2004; Mussa & Verberne, 2013).
Regulation of Exocrine Secretion
Pancreatic secretions are tightly regulated through an intricate Digestive Enzymes
network of neural, humoral, and paracrine mediators. Many The exocrine pancreas releases proteolytic, amyolytic, lipolytic,
neurotransmitters, hormones, and growth factors have been and nuclease digestive enzymes. These enzymes are stored in
reported to influence pancreatic exocrine function. These zymogen granules either as proenzymes (i.e., trypsinogen, chy-
agents include, but are not limited to, ACh and catecholamine, motrypsinogen, procarboxypeptidase, prophospholipase, pro-
secretin (as earlier), nitric oxide (NO), VIP, GRP, neuropeptide elastase, mesotrypsin) or as active enzyme (i.e., a-amylase,
Y, galanin, substance P, CGRP, gastrin/cholecystokinin (CCK), lipase, DNase, RNase) (Whitcomb & Lowe, 2007). In addition,
and enkephalins (Barreto et al, 2010; Chandra & Liddle, 2012; the zymogen granules contain a trypsin inhibitor molecule
Chandra & Liddle, 2014). known as pancreatic secretory trypsin inhibitor (PSTI) (Kazal
72 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
ACINAR LUMEN
Gα q* CENTROACINAR CELL
ACh
IP3
CCK Gα q
Intracellular
PIP2
Phospholipase-C Ca2+ store ACINAR CELL
SUBSTANCE P Gα q
DAG
↑ Cytosolic
Ca2+
BOMBESIN Gαq
Secretion
Protein Kinase C
Protein
Phosphorylation
Protein Kinase A
SECRETIN †Gas
Adenylate cAMP
Cyclase
VIP Gα s
CENTROACINAR CELL
FIGURE 4.3. Stimulus-secretion coupling in pancreatic acinar cell. The primary secretagogues for acinar secretions bind to two types of cell
surface heterotrimeric G protein receptors. Acetylcholine (ACh; the primary secretagogue for acinar secretion), cholecystokinin (CCK), substance P,
and bombesin act through heterotrimeric G protein–coupled receptors (GPCRs) associated with phospholipase C. This results in the production of
two main messengers: inositol-1,4,5-triphosphate (IP3), which promotes the release of Ca2+ from intracellular stores; diacylglycerol (DAG), which
prompts the activation of protein kinase C (PKC). The increase in cytoplasmic Ca2+ concentration and activated PKC leads to protein phosphorylation
and digestive enzyme secretion. Secretin and vasoactive intestinal peptide (VIP) act through heterotrimeric GPCRs associated with adenylate cyclase.
Elevation in cytoplasmic cyclic adenosine monophosphate (cAMP) levels cause activation of protein kinase A (PKA), which ultimately leads to protein
phosphorylation and digestive enzyme secretion. The centroacinar cells are terminal ductal cells that are in close contact with acinar cells and could
represent progenitor multipotent pancreatic cells. *Gαq, Membrane-associated heterotrimeric G protein that activates phospholipase C (PLC);
†Gαs, membrane-associated heterotrimeric G protein that activates the cAMP-dependent pathway by activating adenylate cyclase; PIP2,
phosphatidylinositol-4,5-bisphosphate.
et al, 1948). PTSI forms a stable complex with trypsin near its adaptation remain under investigation, it is reasonable to
catalytic site, preventing its undesired activation (Pubols et al, believe that the regulation occurs at the level of gene
1974). transcription.
Following acinar stimulation, the zymogen granules fuse
with the apical acinar cell membrane, releasing their contents Stimulus-Secretion Coupling in Acinar Cell
in the pancreatic intercalated ducts that will eventually reach Increase in intracellular concentration of calcium is the funda-
the intestinal lumen. A brush-border glycoprotein peptidase mental event that stimulates the acinar cells to release the
present on the duodenal lumen, known as enterokinase, activates secretory granules containing the digestive enzymes (Fig. 4.3)
trypsinogen by removing its N-terminal hexapeptide fragment. (Low et al, 2010). Transmembrane heterotrimeric G proteins
The active form of trypsin is responsible for the catalytic activa- are the principal receptors for pancreatic acinar cell secreta-
tion of the remaining pancreatic proenzymes (Whitcomb & gogues and produce secondary messengers that ultimately act
Lowe, 2007). to release intracellular calcium (Messenger et al, 2014). Secre-
One characteristic of the acinar cell is its capacity to adapt tin and VIP bind to their specific GPCRs and cause activation
synthesis of digestive enzymes as a function of diet. Although of adenylate cyclase, generation of cAMP, and activation of
the mechanisms by which acinar cells are capable of this protein kinase A (Chey & Chang, 2014).
Chapter 4 Pancreatic Physiology and Functional Assessment 73
SLC26A3/A6
CFTR
HCO3–
Cl–
Protein Kinase A CO2 + H2O
Carbonic Anhydrase
cAMP
H+ + HCO3–
Adenylate
Cyclase
H+ Na+ Na+ K+
Gαs*
ATP
SECRETIN Capillary
FIGURE 4.4. Stimulus-secretion coupling in pancreatic ductal cell. Carbon dioxide (CO2) diffuses from the blood across the basolateral mem-
brane of the duct cell and is hydrated by carbonic anhydrase within the duct cell to form carbonic acid (H2CO3). Eventually, carbonic acid dissociates
into H+ and HCO3−. The extrusion of H+ via Na+-H+ exchanger, located across the basolateral membrane, leads to the accumulation of bicarbonate
(HCO3−) in the ductal cell. The intracellular bicarbonate (HCO3−) is then secreted into the ductal lumen by a chloride/bicarbonate (Cl−/HCO3−) exchanger
(SLC26A3/A6) in exchange for luminal Cl−. The cystic fibrosis transmembrane conductance regulator (CFTR) channel recycles Cl− back into the ductal
lumen, making it available for a new exchange. Secretin, the most important ductal cell secretagogue, binds to its heterotrimeric G protein–coupled
receptors, associated with adenylate cyclase located in the basolateral membrane. The resulting increase in cyclic adenosine monophosphate (cAMP)
leads to activation of protein kinase A (PKA) resulting in the activation of the CFTR channel. The activated CFTR channel accelerates the extrusion
of Cl− from the cell to the ductal lumen, causing the apical Cl−/ HCO3− to operate at a faster rate, leading to an increase in HCO3− secretion into the
ductal lumen. The net passage of bicarbonate across the duct cell generates an ionic and osmotic gradient, which favors paracellular passage of
sodium and water into the ductal space. ATP, Adenosine triphosphate; *Gαs, membrane-associated heterotrimeric G protein that activates the
cAMP-dependent pathway by activating adenylate cyclase.
CCK, ACh, bombesine/GRP, PAR-2–activating protease, the cellular receptor causing activation of protein kinase C and
and substance P bind to their respective GPCRs, which ulti- increase in intracellular calcium concentration. The end result is
mately act through the activation of phospholipase C and the the activation of cAMP-dependent Cl− channel that releases
production of IP3 (Singer & Niebergall-Roth, 2009; Weiss et al, intracellular Cl− into the ductal space, increasing the amount of
2008). IP3 binds act on its receptor in the endoplasmic reticu- Cl− available for the Cl−-HCO3− exchanger.
lum and stimulates Ca+2 release. Ultimately, activated protein The high concentration of ductal Cl− activates a Cl−-HCO3−
kinase A and protein kinase C phosphorylate specific intracel- antiport that results in an exchange of Cl− for HCO3−. Further-
lular proteins that lead to the secretion of pancreatic enzymes. more, Na+ and H2O are released into the ductal space drowned
by the ionic and osmotic gradient generated by the presence of
Stimulus-Secretion Coupling in the Ductal Cell bicarbonate in the duct lumen. Several K+ channels are present
The apical and the basolateral portion of the ductal cells are in the ductal cell membrane and appear to have an essential
involved in the stimulus-coupling secretion (Fig. 4.4). The apical role in generating and maintaining the electrochemical driving
membrane of ductal cells is equipped with cAMP-activated force for anion secretion. Ductal HCO3− secretion is not only
Cl−channels (also known as the cystic fibrosis transmembrane regulated by gastrointestinal hormones and cholinergic nerves
conductance regulator), Cl−-HCO3− exchanger (SLC26A3/A6), but is also influenced by luminal factors: intraductal pressure,
and water channels aquaporin 5 (AQP5). The basolateral mem- calcium concentration, and pathologic activation of protease
brane is rich in a Na+-H+ exchanger, N+,K+-ATPase, K+ conduc- and bile reflux (Ishiguro et al, 2012; Steward & Ishiguro 2009).
tance channels, and AQP1 (localized in both apical and
basolateral membrane). The interstitial portion of the ductal cells FUNCTIONAL ASSESSMENT
express receptors for the two major stimulants of ductal secre-
tion: secretin and ACh (Ishiguro et al, 2012; Steward & Ishiguro, Assessment of Endocrine Function
2009). Secretin binds to its cellular receptor, leading to the acti- The evaluation of the endocrine pancreas revolves around the
vation of adenylate cyclase and protein kinase A. ACh binds to assessment of β-cell function. These assessments should take
74 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
days and to collect the complete volume of feces for 3 days, spot fecal sample) are diagnostic for pancreatic insufficiencies
starting on day 3. Fecal content greater than 7 g/day is consid- in patients with chronic pancreatitis (Benini et al, 2013).
ered abnormal, and it is diagnostic for steatorrhea. This test However, fecal elastase-1 tests are often unreliable following
poses an unpleasant burden on laboratory personnel, and its pancreatic resection, where pancreatic insufficiency results
diagnostic utility is limited to the advanced stages of pancreatic from a combination of factors not solely depended on decreased
insufficiency. pancreatic function (e.g., abnormal hormonal stimulation,
Previously considered one of the most accurate of the non- abnormal mixing of food with digestive secretions, acidic intra-
invasive tests, the pacreolauryl test has limited value in patients luminal pH) (Benini et al, 2013). Furthermore, fecal elastase-1
with bile salt deficiency, renal failure, celiac disease, and post- levels are not influenced by the exogenous administration of
gastrectomy symptoms, and its use has been abandoned in pancreatic enzyme, and therefore this test cannot be utilized to
clinical practice (Elphick & Kapur, 2005; Friess & Michalski, evaluate the response to pancreatic enzyme replacement therapy
2009; Lankisch et al, 1983). (Leeds et al, 2011; Nøjgaard et al, 2012).
Another test available to quantify fat malabsorbtion is the Invasive direct PFTs require the use of a double-lumen col-
13
C–mixed triglyceride breath test. This test requires the oral lection tube, with one lumen terminating in the duodenum to
administration of a 13C–market substrate and relies on the pres- collect pancreatic secretions and one lumen resting in the
ence of intestinal pancreatic lipase activity. Ultimately, the 13C– gastric antrum to prevent gastric fluid from entering the duo-
market substrate is hydrolyzed by the intestinal lipase, yielding denum. Correct tube placement is confirmed via fluoroscopy
13
CO2 that is absorbed and eventually released across the pul- prior to administration of meal or segretagogues, and then
monary endothelium and quantified via mass spectrometry or pancreatic secretions are collected for 1 to 2 hours. Alterna-
infrared analysis. This test could represent a practical alterna- tively, an endoscope can be used, and pancreatic fluid can be
tive to the fecal fat test, although it is subject to similar limita- collected directly either through cannulation of the pancreatic
tions of all indirect tests with limited accuracy for the early duct or through the suction channel of the endoscope under
phases of pancreatic insufficiency (Keller et al, 2014; Naka- direct visualization from the duodenum. Of historic interest is
mura et al, 2009a). the Lundh test (Lundh,1962), where a physiologic stimulus to
pancreatic secretion is obtained through the administration of
Direct Pancreatic Function Test a standardized meal (composed of 300 mL of solution contain-
Noninvasive direct PFTs aim to quantify the fecal or serum ing 15% carbohydrate, 6% fat, and 5% protein). Endogenous
levels of pancreas-derived enzymes (e.g., serum trypsinogen, secretin and CCK, released in response to the standardized
fecal chymotrypsin, and fecal elastase). Although easy to meal, are necessary to stimulate pancreatic secretion, making
perform and well tolerated by patients, noninvasive PFTs are the Lundh test dependent on normal duodenal mucosal func-
hindered by their low sensitivity, often leading to inconclusive tion (Lundh, 1962; Pandol, 2010). The hormone-stimulated
results, especially in the early phases of chronic pancreatitis. tests are the cornerstone of the direct invasive pancreatic tests.
Furthermore, fecal measurement of pancreatic enzyme can lead These tests utilize the exogenous administration of secretin,
to false-positive results in the setting of nonpancreatic gastro- CCK, or a combination of secretin-CCK as a more reliable
intestinal disturbances and diarrhea. method of pancreatic stimulation (Jowell et al, 2000; Somogyi
Serum trypsinogen is considered a sensitive and specific test et al, 2003).
for advanced pancreatic insufficiency, although its accuracy for The secretin test requires intravenous administration of a
earlier stages of pancreatic insufficiency is low. A serum tryp- synthetic secretin bolus (0.2 µg/kg), followed by a continuous
sinogen concentration of less than 20 ng/mL is considered a collection of duodenal fluid in four aliquots of 15-minute inter-
reasonable cutoff for the diagnosis of pancreatic insufficiency vals each. The test measures bicarbonate concentration in each
(Jacobson et al, 1984). of the four aliquot samples. Exocrine insufficiency is evident
Fecal chymotrypsin concentration can be utilized for the when bicarbonate concentrations less than 80 mEq/L are
evaluation of pancreatic insufficiency. Chymotrypsin is specifi- recorded in each of the four aliquots, and severe exocrine insuf-
cally synthesized and secreted by the acinar cells of the pan- ficiency is diagnosed when bicarbonate concentration is less
creas. This test is influenced by exogenous pancreatic enzyme than 50 mEq/L (Chowdhury & Forsmark, 2003). Moreover,
administration and requires suspension of enzyme administra- the test can quantify the total volume output as well as the total
tion for at least 2 days before the test (Molinari et al, 2004). amount of bicarbonate secreted. These measurements are
Furthermore, chymotrypsin is not an ideal marker as it is employed as a secondary diagnostic test when bicarbonate con-
degraded during intestinal transit and can be diluted in the centrations are equivocal. Although theoretically useful, these
presence of diarrhea, leading to false-positive results. tests are not commonly employed because they are hindered by
Fecal elastase-1 appears to be a more reliable test compared the low accuracy caused by incomplete recovery of duodenal
to fecal chymotrypsin. Elastase-1 is not influenced by exoge- fluid.
nous pancreatic enzyme administration, and it is more stable Alternative approaches have been developed to overcome
than chymotrypsin during intestinal transit. Evidence suggests the challenges of gastroduodenal tube placement. One of these
that this study has a reasonably high sensitivity and specificity approaches is the purely endoscopic secretin test (ePFT). This
for pancreatic insufficiency (Leeds et al, 2011). Results obtained test has been shown to have similar accuracy to the classic
with the fecal elastase-1 test reliably correlate with the one secretin test. Duodenal aspirates are obtained through an endo-
obtained using imaging studies (ERCP, magnetic resonance scope at 0, 15, 30, 45, and 60 minutes after secretin stimulation
neurography [MRN]) (Bilgin et al, 2008), or the more sensitive and analyzed for bicarbonate concentration (Stevens et al,
direct invasive pancreatic tests (secretin test) (Löser et al, 1996; 2007; Tayler & Parsi, 2011).
Stein et al, 1996). Level of fecal elastase-1 less than or equal Another attempt made to overcome the limitations of duo-
to 15 µg/g of stool (enzyme-linked immunoabsorbent assay on denal fluid collection consists of the use of ERCP for the
76 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
analysis of pure pancreatic secretion collected directly from the CCK-stimulated gallbladder contraction, ultimately results in
pancreatic duct. However, the results obtained with this method dilution of the digestive enzymes. To avoid false-positive results,
have been unsatisfactory (Draganov et al, 2005). CCK tests some authors have advocated the use of perfusion markers,
using either CCK or a receptor agonist (e.g., cerulein) have although no definitive agreement exists.
been developed to measure pancreatic enzyme secretion. A Of recent interest are tests combining secretagogues with
simplified version of these tests measures lipase concentration imaging techniques. Examples of these tests are the secretin-
from duodenal fluid collected over an 80-minute period and enhanced MRI and the secretin-enhanced MRCP (Balci et al,
utilizes a cutoff lipase value of 780 IU/L (Conwell et al, 2002). 2010; Bian et al, 2013; Hansen et al, 2013). Secretin-enhanced
Acinar and ductal pancreatic exocrine function can be evalu- MRI utilizes diffusion-weighted MRI imaging to evaluate
ated simultaneously using the secretin-CCK test. This test increase in pancreatic capillary blood flow and pancreatic secre-
requires continuous collection of duodenal fluid and measure- tion following stimulation with secretin. In addition, secretin-
ment of total secretion output, bicarbonate concentration, and enhanced MRCP allows evaluation of duodenal filling as a
digestive enzyme concentration (Lieb & Draganov, 2008). function of pancreatic secretion (Sanyal et al, 2012). Although
Some patients may have a more pronounced deficit of one growing enthusiasm is developing around these tests, further
specific enzyme; therefore measuring more than one digestive studies are necessary to evaluate their performances with stan-
enzyme (i.e., amylase, lipase, and tryptase) in addition to bicar- dard invasive tests.
bonate can increase the sensitivity of this test. One pitfall of the
secretin-CCK test is that the large amount of fluid released by References are available at expertconsult.com.
the pancreas following secretin stimulation, combined with
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CHAPTER 5
Liver blood flow: physiology, measurement,
and clinical relevance
Simon Turcotte
Circulation in the liver is unique because of a dual afferent because of the greater oxygen content found in arterial blood.
blood supply, derived from the hepatic artery (HA) and the In addition, the HA provides the exclusive blood supply to the
portal vein (PV) (see Chapter 2). The oxygen-rich arterial intrahepatic bile ducts through the peribiliary plexus (Fig. 5.2).
blood and the nutrient-rich portal venous blood merge in the In the hepatic lobules, the hepatic arterioles empty directly or
hepatic parenchymal microcirculation to sustain the complex via peribiliary plexi into the sinusoids. Direct artery-to-HV
functions of the liver, prior to returning to the heart through connections do not usually exist but may arise in liver disease.
the hepatic veins (HVs). This chapter outlines how liver blood Within the liver parenchyma, the pressure in the arterial
flow (LBF) is controlled to maintain the hepatic perfusion system is reduced toward that existing in the portal circulation
within an acceptable physiologic range, describes techniques and sinusoids. This is suggested to be achieved mainly by (1)
used for LBF measurement, and explores clinical situations in the presinusoidal arteriolar resistance in the peribiliary plexus
which blood flow is altered. and (2) the intermittent closure of the arterioles, which protect
the portal bloodstream from arterial pressure (Rappaport,
PHYSIOLOGY 1973). In the event of hepatic arterial occlusion, numerous
intrahepatic collaterals can provide a source of arterial blood.
Liver Blood Supply Additionally, extrahepatic collateral supply can develop after
The peculiar double afferent blood supply to the liver results hepatic arterial ligation and depends on the site of occlusion.
in 75% to 80% of the entering blood being partially deoxygen- If the common HA is interrupted, revascularization occurs
ated portal venous blood draining the stomach, intestine, through extrahepatic collaterals arising from (1) the inferior
spleen, and pancreas. The remainder is well-oxygenated blood phrenic arteries and (2) from the gastroduodenal arteries,
from the aorta, carried by the HA. Mixing of arterial and portal which derive blood flow from the superior mesenteric artery
blood occurs in terminal branches in the sinusoidal microcir- (Rappaport & Schneiderman, 1976). Ligation of the proper
culation around hepatocytes arranged into roughly polyhedral- hepatic arteries leads to revascularization mainly via a hyper-
shaped lobules, from their periphery toward their centrilobular trophied inferior phrenic circulation, which can develop con-
venule (Fig. 5.1). The centrilobular venules drain into the HVs nections with hepatic arteries within the liver (Jefferson et al,
and into the inferior vena cava (IVC). Although the liver mass 1956). If only the right or left HA is interrupted, intrahepatic
constitutes approximately 2.5% of the total body weight, the translobar anastomoses reestablish arterial flow in the ligated
liver receives nearly 25% of the cardiac output. The total LBF, system (Mays & Wheeler, 1974). Thus complete long-term
ranges between 800 to 1200 mL/min, which is equivalent to dearterialization of the liver by any form of arterial vascular
approximately 100 mL/min per 100 g liver wet weight. The occlusion is difficult to achieve.
liver blood volume is estimated to range from 25 to 30 mL per
100 g of liver wet weight, which accounts for 10% to 15% of Portal Vein
the total body blood volume. The sinusoids hold 60% of the The PV normally carries approximately 75% of the total blood
blood volume, whereas the remaining 40% lies in large vessels flow to the liver (90 mL/min per 100 g of liver weight) in a
(HA, PV, and HV) (Greenway & Stark, 1971; Lautt, 1977a). valveless, low-pressure/low-resistance venous system. The
Of note is the high compliance of the liver, calculated as the inferior and superior mesenteric veins join with the splenic vein
change in its blood volume per unit change in venous pressure. to form the PV, and jointly they collect the venous outflow from
The liver thus acts as an important blood reservoir because its the entire prehepatic splanchnic vascular bed (the intestinal
blood volume can expand considerably in cardiac failure or, in tract from the lower esophagus to the rectum plus the pancreas
case of bleeding episodes, can compensate as much as 25% of and spleen). The PV pressure ranges between 6 and 10 mm Hg
the hemorrhage by rapid expulsion of blood into the circulation in humans when measured by direct cannulation (Balfour et al,
(Lautt, 2007; Lautt & Greenway, 1976). 1954). Portal venous pressure depends primarily on the degree
of constriction of mesenteric and splanchnic arterioles, coupled
Hepatic Artery with the intrahepatic vascular resistance. Because portal blood
The HA normally supplies approximately 25% of the total is derived from postcapillary beds, it is partly deoxygenated.
blood flow to the liver (25 to 30 mL/min per 100 g of liver However, because of its large volume flow rate, it may supply
tissue) in a high-pressure/high-resistance system. The mean 50% to 70% of the liver’s normal oxygen requirement. During
pressure in the HA is similar to that in the aorta. The HA fasting states, the oxygen saturation in the portal blood
provides as much as 50% of the liver’s oxygen requirement approaches 85%, which is greater than other systemic veins.
77
78 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Hepatic sinusoid
Centrilobular
venule
Hepatocytes Hepatic Bile canaliculi
lobule
Reticuloendothelial
Centrilobular cell
venule Hepatic sinusoid
Bile canaliculi
Hepatocyte
Portal triad
Branch of
A Hepatic lobules bile duct
Branch of
hepatic portal vein
Branch of
hepatic artery
Portal triad
Branch of
bile duct
Branch of
Hepatic hepatic
sinusoid portal vein
Hepatocytes
Branch of B Hepatocytes and sinusoids
hepatic artery
C Portal triad
FIGURE 5.1. The liver microcirculation. The liver is composed of thousands of roughly polyhedral structures called hepatic lobules, which are the
basic functional units of the organ. Hepatic lobule of some mammals, such as the pig, are delimited on all sides by connective tissue but have much
less connective tissue, and their boundaries are more difficult to distinguish in humans. A, A small central vein projecting through the center of each
hepatic lobule and several sets of blood vessels defining the periphery. The peripheral vessels are grouped primarily in connective tissue comprising
the portal tracts in the space of Mall, which include a branch of the portal vein and a branch of the hepatic artery, as well as a branch of the bile
duct. These comprise the portal triad. B, Both blood vessels to each lobule give off sinusoids, which run between plates of hepatocytes and drain
into the central vein. C, Micrograph showing components of the portal triad within the space of Mall (hematoxylin and eosin; ×220). (From Mescher
AL: Junqueira’s Basic Histology: Text and Atlas, 12th ed. New York, 2009, McGraw-Hill.)
Hepatic Veins
The hepatic venous system is the systemic drainage tract of
the entire splanchnic circulation. A total LBF of 1.5 L/min is
PP
considered the normal value in the average male, but the range
can be quite wide (1 to 2 L/min). In normal conditions, the
A free pressure in the HVs and IVC is 1 to 2 mm Hg and is 1 to
5 mm Hg lower than the pressure measured in the sinusoids
and PV. The portal pressure gradient, defined as the difference
in pressure between the PV and the IVC, has been a useful
clinical indicator of the perfusion pressure of the liver with
portal blood (Berzigotti et al, 2013). The pressure gradient
in the liver is thus extremely low, in the range of 5 mm Hg
FIGURE 5.2. Arterial peribliary plexus. A cast of the portal vein (P), compared with all other organs, where it is in the range of
hepatic artery (A), and peribiliary arterial plexus (PP) of a rat, showing a
115 mm Hg (Lautt, 2009). Hepatic venous blood is normally
connection between a small artery and the plexus (arrow). The peribiliary
plexus forms a dense sheath around the bile duct. Bar = 100 µm. approximately two-thirds saturated with oxygen, but this may
(From Grisham JW, Nopanitaya W: Scanning electron microscopy of be markedly reduced during periods of low delivery of oxygen
casts of hepatic microvessels: review of methods and results. In Laut to the liver, when oxygen is extracted by hepatocytes. In resting
W: Hepatic Circulation in Health and Disease. New York, 1981, Raven states, the liver accounts for approximately 20% of the total
Press, Figure 4, p 98.) oxygen consumption of the body.
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 79
Central vein
Hepatic arteriole
Zone III
Bile duct least
oxygenated
Portal vein
Zone II
Centrilobular Zone I
venule most
oxygenated
FIGURE 5.3. Structure-function conceptual liver units. To this day, there is no complete consensus on whether the microvascular unit of the liver
should be referred to as a lobule, centering on a hepatic vein, or an acinus, centering on a “portal triad” consisting of a terminal branch of the hepatic
artery, portal vein, and bile duct, encased within a limiting plate of cells defining the space of Mall. Three related conceptual units emphasizing different
aspects of hepatocyte activity have been proposed. A, The classic lobule emphasizes the endocrine function of hepatocytes as blood flows past
them toward the centrilobular venule. B, The portal lobule emphasizes the hepatocytes’ exocrine function and the flow of bile from regions of three
classic lobules toward the bile duct in the portal triad at the center. The area drained by each bile duct is roughly triangular. C, The liver acinus
concept proposed by Rappaport emphasizes the different oxygen and nutrient contents of blood at different distances along the sinusoids, with
blood from each portal area supplying cells in two or more classic lobules. Each hepatocyte’s major activity is determined by its location along the
oxygen/nutrient gradient: periportal cells of zone I get the most oxygen and nutrients and show metabolic activity generally different from the pericentral
hepatocytes of zone III, exposed to the lowest oxygen and nutrient concentrations. (From Boron WF, Boulpaep EL (eds): Medical Physiology: A
Cellular and Molecular Approach. Philadelphia, 2005, Saunders Elsevier.)
Hepatic Microcirculation with a diameter of 150 to 175 nm (Fig. 5.4). The sieve plates
Although the organization of the liver into morphologic and occupy as much as 8% of the endothelial surface and are not
functional units has been a matter of debate, the hexagonal uniform in size or distribution throughout the length of the
polyhedral-shaped hepatic lobule, encompassing hepatic micro- sinusoids. There is a decrease in diameter but an increase of
vascular subunits consisting of a portal triad of terminal frequency from periportal to centrilobular zones, which results
branches of the HA, PV, and bile duct; a network of sinusoids; in higher centrilobular porosity (Braet & Wisse, 2002; Wisse
and an efferent centrilobular venule is a widely accepted frame- et al, 1985). The fenestrae are dynamic structures that contract
work (Ekataksin & Kaneda, 1999; Malarkey et al, 2005) (see and dilate in response to alterations of sinusoidal blood flow
Fig. 5.1). The portal triads, surrounded by lymphatics and and perfusion pressure (Smedsrød et al, 1994). Red blood cells
autonomous nerves, all travel together in parallel in the space (RBCs) remain restricted within the sinusoids, whereas mol-
of Mall, through the liver parenchyma, and form portal tracts. ecules as large as albumin can pass through the fenestrations
Lymphatics transport proteins and other macromolecules that and enter the small space of Disse before making contact with
are trapped extravascularly due to hindrance of hepatocellular the microvilli of the hepatocytes (Lautt, 2009).
uptake, as in the case of cirrhosis, which will in turn contribute As represented in Fig. 5.5, other unique cellular compo-
to ascites formation (see Chapter 76). The hepatic sinusoids nents, such as the hepatic stellate cell (HSC) (Friedman, 2008)
correspond to the capillary bed of the liver and represent the and the Kupffer cell (KC), are found in the hepatic sinusoids
segment of the microcirculation in which supply of nutrients and may regulate the sinusoidal microcirculation in response to
and removal of metabolic products by hepatocytes takes place. various mediators (McCuskey, 2000). External to the endothe-
Bile canaliculi closely assemble around hepatocytes and collect lium cell lining, HSCs (also known as fat-storing cells, Ito cells,
bile flowing in an opposite direction from blood in the sinusoids. or hepatic perisinusoidal lipocytes) are contractile cells distrib-
As depicted in Fig. 5.3, histologic and physiologic studies of uted homogeneously around the exterior of the endothelial cells
the liver have given rise to three related ways to view the liver’s in the space of Disse, which is the space between the basal
microcirculation, emphasizing different functional aspects microvilli-rich surfaces of the hepatocytes and the sinusoidal
useful for the classification of various pathologic processes. lining cells. In addition to their well-known importance in
Apart from the absence of a basement membrane, the retinol metabolism and as key actors in the hepatic fibrogenic
structural peculiarity of hepatic sinusoids is their unique lining, response to injury (see Chapters 7 and 76), HSCs are capable
consisting of endothelial cells with flattened processes perfo- of compressing the sinusoidal diameter by squeezing the endo-
rated by small fenestrae. These open fenestrations are arranged thelial cells and therefore play a central role in the regulation
in clusters of 10 to 50 pores, forming so-called “sieve plates” of blood flow through hepatic sinusoids (Rockey, 2001; Zhang
80 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
et al, 1994). KCs are liver-specific macrophages, and, in con- direct regulation role of the sinusoidal microcirculation is
trast to HSCs, are anchored to the luminal side of the sinusoids. debated (Lautt, 2009; Vollmar & Menger, 2009).
They account for approximately 15% of the liver-cell popula-
tion and constitute approximately 80% of the total population Control of Liver Blood Flow
of macrophages in the body (Lautt, 2009). By their large bodies, The hepatic blood flow required to meet the physiologic func-
with cytoplasmic process that sometimes reach the opposite tion of the liver is mainly controlled by intrinsic physiologic
wall of a sinusoid, KCs represent a flow hindrance and can mechanisms that are independent of extrinsic innervation and
secrete large amounts of the vasodilator nitric oxide, but their vasoactive agents. Instead, the interrelationship of arterial and
portal inflow circuits is the major contributor to hepatic
perfusion.
Space of Disse
Hepatocyte Endothelial
Hepatic sinusoid cell
Hepatic Kupffer
stellate cell cell
FIGURE 5.5. Hepatic stellate and Kupffer cells relation to the liver microcirculation. Contractile hepatic stellate cells are distributed homogeneously
around the exterior of the endothelial cells in the space of Disse, the space between the basal microvilli-rich surfaces of the hepatocytes and the
sinusoidal lining cells. Kupffer cells, which are liver-specific macrophages, are anchored to the luminal side of the sinusoids. They can secrete vasoac-
tive mediators, and their large bodies may represent sinusoidal flow hindrance.
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 81
20 20
18 18
16 16
14 14
Blood flow (mL/min)
10 10
§
8 † 8
† †
6 * 6 *
4 4
2 2
0 0
A I II III IV V B I II III IV V
FIGURE 5.6. Hepatic arterial buffer response in cirrhotic (A) and control livers (B). Upon reduction of portal venous blood flow (open circles, black
line), there is a constant increase of hepatic arterial blood flow (solid circles, gray line). The portal flow is markedly diminish in cirrhotic liver, but the
buffer response is preserved. Values are means ± standard error of triplicate measurements per animal (n = 6). *P < .05 vs. I and II; †P < .05 vs. I,
II, and III. §P < .05 vs. I, II, II, and IV. (From Richter S, et al (eds): Impact of intrinsic blood flow regulation in cirrhosis: maintenance of hepatic arterial
buffer response. Am J Physiol Gastrointest Liver Physiol 279:G454-G462, 2000.)
blood flow decreases, less adenosine is washed away, and the arrangement precludes substances diffusing back from the
elevated adenosine concentration leads to dilation of the HA. hepatic parenchyma or venous blood into the hepatic arterial
Of importance, the source of the adenosine found in the space resistance vessels. Among other studies, this concept has been
of Mall remains to be elucidated. If portal blood flow is severely exemplified by isovolemic hemodilution or upregulation of
reduced, the buffer response results in the HA dilating maxi- hepatic enzymes, leading to oxygen deprivation to the liver
mally, as demonstrated by the inability to produce additional parenchyma, which does not result in HA dilation (Lautt &
dilation in response to intraarterial infusion of adenosine. Greenway, 1987). Therefore the hepatic metabolic demands do
Conversely, when portal flow is doubled, the HA constricts to not control the hepatic arterial flow, even if the liver parenchy-
a maximal extent, as demonstrated by the inability of intraarte- mal cells can release large quantities of potent vasoactive
rial norepinephrine to produce further constriction (Lautt et al, molecules during metabolic stress.
1990). Although the HABR is sufficiently powerful to regulate The term autoregulation refers to the tendency for local
the vascular tone in the HA over the full range from maximal arterial blood flow to remain constant in the face of pressure
vasodilation to maximal vasoconstriction, this mechanism is changes in the arteries that perfuse a given organ. Overall, the
capable of buffering 25% to 60% of the decreased portal flow degree of autoregulation is considered small in the liver, and
(Lautt et al, 1985). mixed results have been reported in animal models (Eipel et al,
Although adenosine appears to be the main mediator of 2010). In fact, the adenosine washout may well account for HA
the HABR, a possible contribution of the afferent sensory autoregulation because endogenous adenosine produced by the
nerves and neuropeptides is suggested by studies in fully HA tributaries can contribute to high presinusoidal adenosine
denervated animal livers (Mathie et al, 1980) and in trans- concentration in situations where hepatic clearance is impaired
planted human livers (Henderson et al, 1992; Payen et al, by a reduction in the portal flow, leading to hepatic arterial
1990), in which the HABR upon partial PV occlusion is par- vasodilation (Ezzat & Lautt, 1987).
tially impaired (Biernat et al, 2005; Ishikawa et al, 1995). It
has also recently been shown that hydrogen sulfide (H2S), a REGULATION OF INTRAHEPATIC RESISTANCE AT THE SINUSOIDAL
vasoactive gaseous mediator produced within the liver, appears LEVEL. Sinusoidal blood pressure and vascular resistance are so
to almost double the HABR by increasing the hepatic arterial low that a pressure gradient across the liver from the portal
conductance, and in turn, its inhibition has the opposite effect venous inflow to the hepatic venous outflow is only approxi-
(Siebert et al, 2008). mately 5 mm Hg. The low pressure gradient is remarkable,
considering that 30% of the inflow to the liver sinusoids is
THE HEPATIC INFLOW IS NOT CONTROLLED BY LIVER-INTRINSIC META- provided by the HA under arterial pressure. How the hepatic
BOLIC NEEDS. Until the mid-1970s, the hepatic arterial flow was pressure gradient is maintained has been studied in multiple
believed to be under metabolic control of the liver. As for most animal models. About 60 years ago, Knisley suggested the pres-
organs, the liver metabolism, estimated by its oxygen require- ence of sphincter-like structures at the entrance and exit of
ments, was postulated to participate in vascular inflow control. sinusoids that maintain the portal venous pressure gradients,
It has, however, been established that the liver normally receives but these proved to be species dependent (Lautt, 2009; Knisely
more oxygen than it requires and can extract more oxygen to et al, 1957; Vollmar & Menger, 2009). In humans, although
compensate for reduced delivery (Bredfeldt et al, 1985; Lautt, smooth muscle cells are found throughout all segments of
1976, 1977b). Additionally, the unique one-way sinusoidal flow the hepatic microvascular subunits, no such sphincter-like
82 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
TABLE 5.1 Liver-Intrinsic Vasoactive Molecules and Pathways Regulating the Microcirculation
Cellular Source and
Vasoactive Agent Function Enzyme System Distribution Target Cell Pathways
structures have been described for controlling the intrahepatic hypercarbia, whereas metabolic alkalosis has essentially no
blood flow. significant effect (Hughes et al, 1981). The sympathetic nervous
In contrast, there is a growing body of evidence that con- system is thought to be responsible for the hepatic arterial
tracting cells associated with the sinusoids, such as the HSCs vasoconstriction observed in hypercarbia and hypoxia (Mathie
and the sinusoidal endothelial cells, through a complex inter- & Blumgart, 1983).
play with vasoactive mediators, may dynamically regulate the Sympathetic Nervous System. The liver is a significant blood
hepatic microvascular blood flow. With such a low sinusoidal reservoir, and 50% of its blood volume may be mobilized by
perfusion pressure, local regulators at a single-cell level may nerve stimulation (Greenway & Lautt, 1989). Denervation
actively control the flow within the sinusoids toward the HVs. experiments have shown that the sympathetic nervous system
It seems plausible that the HSCs could dilate to pull outward is not involved in basal arterial tone in the liver (Mathie &
on the endothelial cells and enlarge the sinusoidal space (see Blumgart, 1983). Hepatic sympathetic nervous stimulation
Fig. 5.5); however, this does not seem to have been shown causes hepatic arterial vasoconstriction and reduced blood flow,
(Vollmar & Menger, 2009). Many endothelial mediators known which appears secondary to an autoregulatory response (Gre-
to control vascular tone by acting on HSC contractility have enway & Stark, 1971). Sensory denervated rats and pigs have
been described (Table 5.1), notably, (1) the endothelium- a diminished arterial buffer response on partial occlusion of the
derived relaxing factor nitric oxide (NO) (Palmer et al, 1987), PV (Ishikawa, 1995). Portal pressure increases as a result of an
(2) the endothelium-constricting factor endothelin-1 (ET-1) increase in portal venous resistance, but portal flow does not
(Hickey et al, 1985; Yanagisawa et al, 1988), and (3) two decrease unless there is a decrease in intestinal or splenic blood
vasodilatory gaseous molecules: carbon monoxide (CO) flow caused by simultaneous sympathetic stimulation of these
(Furchgott & Jothianandan, 1991; Lin & McGrath, 1988) and vascular beds. Although the HA contains both α-adrenergic and
H2S (Hosoki et al, 1997; Zhao et al, 2001). With the exception β-adrenergic receptors, the portal venous system is believed to
of H2S, a direct contribution of these vasoactive agents to the contain only α-receptors (Richardson & Withrington, 1981). At
HABR is not well established (Eipel et al, 2010). low doses, epinephrine causes hepatic and mesenteric arterial
vasodilation, whereas at high doses, vasoconstriction occurs in
Liver-Extrinsic Factors Affecting Liver Inflow the hepatic arterial and portal venous vascular beds and in the
ENDOGENOUS FACTORS mesenteric circulation (Greenway & Stark, 1971; Richardson
Blood Gas Tensions. Hypercarbia (partial pressure of carbon & Withrington, 1981).
dioxide in arterial blood [PaCO2] > 70 mm Hg) increases Other Endogenous Vasoactive Agents. Intraportal administra-
portal venous flow and decreases hepatic arterial flow in tion of exogenous vasoactive agents affects hepatic arterial
dogs (Hughes et al, 1979a), whereas hypocarbia (PaCO2 < resistance (Lautt et al, 1984). The mechanisms underlying this
30 mm Hg) decreases both (Hughes et al, 1979b). Systemic intrahepatic transvascular effect are not understood, but it is
hypoxia (partial pressure of oxygen in arterial blood [PaO2] < likely that the close anatomic association between arterioles and
70 mm Hg) causes a decrease in arterial flow but has no effect venules could permit this and may be a means by which hepatic
on the contribution from the PV (Hughes et al, 1979c). The arterial blood flow is finely controlled by endogenous agents,
response to metabolic acidosis is similar to that induced by such as gut hormones. Gastrin, secretin, cholecystokinin, and
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 83
Noninvasive Techniques
DOPPLER ULTRASOUND. Named after Christian Doppler for the
phenomenon he described, the principle of flow estimation by
Doppler is simple: Flow is a product of the average velocity of
the blood measured in the vessel of interest and the cross-
sectional area of the vessel. Two forms of D-US devices exist.
The first consists of a flowmeter with a US probe that is placed
directly on the vessel; measurement with such a device is
invasive. The second consists of a combined image scanner and
flowmeter (duplex) by which flow in a vessel can be measured
transcutaneously and noninvasively (see Chapter 15). In experi-
ments performed on anesthetized dogs, good correlation was
FIGURE 5.7. Experimental arrangement for measuring liver blood flow
found between portal venous flow measured by a transcutane-
in the dog with electromagnetic flow probes. Probes are placed around ous Doppler duplex system and electromagnetic flow probes
the portal vein (PV) and common hepatic artery (CHA). The gastroduo- fitted to the PV (Dauzat & Layrargues, 1989). Because the
denal vein (GDV) and gastroduodenal artery (GDA) are ligated as illus- development of color Doppler and better probe resolution with
trated to ensure that the flows measured by the probes are those that high-frequency transducers has improved accuracy, and because
actually perfuse the liver. the technique provides morphologic assessment of the liver, is
cheap, and can be performed at bedside, D-US has become a
widespread first-line technique. In patients with known cir-
are fitted directly to the vessel, such systems have been used rhosis, D-US has greater than 80% specificity diagnosing clini-
successfully in the investigational setting of intraoperative cally significant portal hypertension, but the sensitivity does not
(Henderson et al, 1992) and postoperative measurement of exceed 4% to 70%, particularly in compensated patients (Ber-
portal venous and hepatic arterial blood flow in liver transplant zigotti et al, 2013). Inversion of flow within the PV is 100%
patients (Payen et al, 1990). specific for clinically significant portal hypertension. D-US is
very accurate for detecting PV, HV, and HA thrombosis (Rossi
TRANSJUGULAR HEPATIC VENOUS PRESSURE MEASUREMENT. Because et al, 2006). Additionally, D-US is useful in the noninvasive
portal hypertension is responsible for most clinical consequences follow-up of transjugular intrahepatic portosystemic shunt
of cirrhosis, measurement of portal venous pressure is critical (TIPS) (Abraldes et al, 2005) (see Chapter 87).
to guide the clinical management of patients with chronic liver
diseases. Currently, the accuracy of invasive techniques has not Total Blood Flow
been surpassed by noninvasive measurement. Direct measure- Clearance Techniques
ments of portal pressure can be performed through transhepatic Substances reaching the liver via the HA or PV are equally well
or transvenous catheterization of the PV but are rarely used extracted (Lautt et al, 1984), and the rate of disappearance
because of the risk of intraperitoneal bleeding and visceral from the bloodstream of an indicator substance exclusively
perforation. Instead, measurement of hepatic venous direct and cleared by the liver is proportional to LBF. First applied to
wedge pressure by a transjugular approach has been developed humans by Bradley and colleagues in 1945, indirect clearance
as a safe and reproducible technique to assess portal hyperten- methods of LBF measurement rely on the Fick equation. The
sion (Fig. 5.8). As mentioned earlier, the pressure gradient flow measurement obtained by Bradley’s group depended on
between the PV and the IVC represents the liver portal perfu- the fact that intravenously injected bromosulfophthalein is
sion pressure, and its normal value is as high as 5 mm Hg. The removed from the bloodstream and excreted into the bile
HVPG is calculated with the difference between wedged hepatic entirely by hepatocytes. They derived a value for the rate of
venous pressure (WHVP) and free hepatic venous pressure hepatic bromosulfophthalein removal indirectly by determining
(FHVP) (see Chapter 87). It is based on the concept that when the rate of IV infusion of dye that maintained the arterial
the blood flow in a HV is blocked by a wedged catheter, concentration at a constant level, and by measuring the arte-
the static column of blood transmits the pressure from the riovenous concentration difference of bromosulfophthalein,
preceding communicated vascular territory, in this case, the they were able to calculate total hepatic blood flow. The mean
hepatic sinusoids. Thus WHVP is a measurement of the hepatic value obtained in a group of healthy individuals was 1.5 L/min.
sinusoidal pressure and not of portal pressure itself. As in cir- Indocyanine green (ICG) is another substance dependent
rhosis, the intersinusoidal communications are lost due to on hepatocyte extraction into bile. It was initially devised
fibrous sept and nodule formation, and the sinusoidal pressure for the measurement of blood flow and later used for the assess-
equilibrates with portal pressure. It has been well demonstrated ment of liver function by measuring functional hepatocyte
that WHVP adequately reflects portal pressure in alcoholic mass (see Chapter 3). HV canulation was initially performed
liver disease, hepatitis C–related (Perelló et al, 1999), and hepa- to calculate the true extraction efficiency of ICG because
titis B–related cirrhosis (Iwao et al, 1994), which are the most of its incomplete hepatic removal (Caesar et al, 1961). Many
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 85
2-4 cm
A B
mmHg
40
WHVP WHVP
20
FHVP FHVP
0
C D
FIGURE 5.8. Measurement of hepatic venous pressure. A, Free hepatic venous pressure (FHVP) is measured bymaintaining the tip of the catheter
free in the hepatic vein at 2 to 4 cm from its opening into the inferior vena cava. B, Wedged hepatic venous pressure (WHVP) is measured by
occluding the hepatic vein by inflating the angiographic balloon (arrow) at the tip of the catheter. Adequate occlusion of the hepatic vein is confirmed
by slowly injecting 5 mL of contrast dye into the vein with the balloon inflated. Please note the typical wedged pattern distal to the balloon. C, A
washout of contrast dye through communications with other hepatic veins (arrow) prevents a correct measurement of the hepatic venous pressure.
D, Typical tracing of pressures measured in the hepatic vein obtained using a multichannel recorder and adequately calibrated transducers. (From
Berzigotti et al: Assessing portal hypertension in liver diseases. Expert Rev Gastroenterol Hepatol 2013;7:141-155.)
investigators now use a simplified version of the original (Combes, 1960), or propranolol (George, 1979). The more
method, in which ICG is administered as a single IV bolus complete hepatic extraction of these substances overcomes the
instead of as an infusion, and hepatic extraction efficiency is need to cannulate a HV in patients with normal liver function.
determined from an analysis of the clearance curve derived A modification of the colloid extraction method developed in
from peripheral blood sampling or pulse dye densitometry, by the 1980s allows the derivation of the ratio of hepatic arterial
using an optical sensor placed on the finger (Akita et al, 2008; to total LBF, termed the “hepatic perfusion index.” The basis
Okochi et al, 2002). ICG plasma disappearance rate is the most of the technique is the ability to determine by dynamic scintig-
commonly used parameter, with a normal range between 16% raphy the temporal separation of accumulating hepatic activity
and 25% per minute and near-complete disappearance at 20 from the arterial and portal supplies after the IV administration
minutes (Sakka, 2007). It is now the most widely used quantita- of a bolus of technetium-99m–sulfur colloid (Fleming et al,
tive liver function test in the clinical setting (Clavien et al, 1981).
2007). Limitations of this technique include variations in
hepatic blood flow caused by intrahepatic and extrahepatic Other Techniques of Physiologic Interest
shunting, or portal thrombosis, which is common in liver INDICATOR DILUTION. The indicator dilution method relies on the
disease. application of the Stewart-Hamilton principle, also derived
Other hepatic clearance techniques have been investigated from the Fick equation (Stewart, 1897). In principle, the
in the past, such as colloidal clearance by the hepatic Kupffer hepatic blood flow is proportional to the amount of hepatic
cells (Dobson & Jones, 1952) and hepatocyte removal of galac- blood that has diluted an introduced indicator. This method
tose (Keiding, 1988), sorbitol (Zeeh et al, 1988), rose bengal involves the injection into the HA and PV of a labeled substance
86 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
that is not removed by the liver; changes in HV concentration γ-emissions of 133Xe after the injection of a saline solution of the
are measured by blood sampling or by monitoring the hepatic isotope into the PV.
isotope activity with an external detector. Such a method is
therefore independent of hepatocellular function and reliable, Laser Doppler Flowmetry
provided the indicator remains in the vascular space and is not Laser Doppler flowmetry (LDF) is a more recent but estab-
excreted prior to sampling. A modified thermal dilution tech- lished technique for the real-time measurement of microvascular
nique has been used to measure portal blood flow in humans RBC perfusion in the liver. By illuminating the tissue with
(Biber et al, 1983). Indicator dilution methods overestimate low-power laser light and capturing the backscattered light with
true blood flow to hepatic tissue when intrahepatic or extrahe- independent photodetectors, the Doppler shift of moving cells
patic shunts are present, although it is possible to measure can be transmitted as an electrical signal. Linearity of the LDF
azygos blood flow by thermal dilution in patients with cirrhosis signal from the liver with total-organ perfusion has been shown
(Bosch & Groszmann, 1984). (Shepherd et al, 1987), and the technique has been shown to
be sensitive to rapid changes in organ flow (Almond & Wheatley,
INDICATOR FRACTIONATION. The measurement of regional blood 1992). The technique has been applied successfully to measure
flow by fractional distribution of cardiac output was first LBF during liver transplantation in humans (Seifalian et al,
described by Sapirstein in 1956. Briefly, a known amount of 1997). A major drawback of the technique is that, owing to the
radioactive microspheres is injected into the left ventricle, and small volume of tissue interrogated by the laser, the LDF signal
a reference sample is withdrawn from a peripheral artery at a can only be used to measure arbitrary, instead of absolute blood
known rate. The microspheres are then extracted from the perfusion in a single area.
various vascular beds, where they have lodged in proportion
to the cardiac output. The hepatic arterial blood flow can be In Vivo Fluorescent Microscopy
determined directly by this method, but the portal flow con- Intravital microscopy was first described in the microvessels of
tribution is found indirectly by addition of the flow values in the frog tongue by Waller in 1846. Using this technique, indi-
the prehepatic splanchnic organs. Examination of the intrahe- vidual sinusoids and terminal venules can be visualized, and
patic distribution of microspheres has provided a means of changes in their diameters and the velocities with which eryth-
assessing the pattern of arterial flow in different liver regions rocytes pass through them can be seen (Menger & Messmer,
(Greenway & Oshiro, 1972). Because the microsphere method 1991). The introduction of fluorescent dyes has broadened the
requires the postmortem removal of the organs of interest for spectrum of in vivo microscopy in the liver from morphologic
radioactivity or colorimetric measurement, the additional analysis to the study of pathologic events. However, from a
determination of tissue weight enables flow per gram (i.e., hemodynamic point of view, intravital fluorescent microscopy
tissue perfusion) to be calculated. Microspheres may be used has problems of interpretation (Sherman et al, 1990). In per-
to determine the extent of portosystemic shunts. The frac- fused liver, a 2.5-fold increase in portal venous blood flow has
tional distribution in the liver may be measured with respect been found to be associated with only a 22% increase in sinu-
to systemic (lung) activity after PV injection, or it may be soidal RBC velocity, suggesting that changes in portal venous
estimated by injecting a second radioactive microsphere blood flow have only a minor effect on the capillary transit time
directly into the splenic or mesenteric venous system (Sherman et al, 1996).
(Groszmann et al, 1982).
Near-Infrared Spectroscopy
Hepatic Tissue Perfusion Near-infrared spectroscopy is a noninvasive technique that uses
Inert Gas Clearance light transmission and absorption to measure hemoglobin and
By exploiting the fact that radioactive gases such as krypton mitochondrial oxygenation. In contrast to visible light, which
(85Kr) and xenon (133Xe) distribute equally between tissue and can only penetrate a few millimeters, near-infrared light (700
blood according to a specific partition coefficient, the rate of to 1000 nm) can be detected through as much as 80 mm of
clearance of such gases can be measured after their injection tissue. The application of this technology to monitor liver
into the hepatic blood supply. After injection and rapid diffusion oxygenation has been validated in models of endotoxic shock
throughout the liver, the gas clears from the tissue into the blood in pigs (Nahum et al, 2006) and by intraoperative quantifica-
and is almost completely eliminated from the body after a single tion of congestion and mitochondrial redox during HV occlu-
passage through the lungs. The clearance rate is proportional to sion in living-donor transplantation (Ohdan et al, 2003).
hepatic tissue perfusion, which may be calculated by using a
standard formula (Leiberman et al, 1978). β-Emissions of 85Kr Investigational Techniques
are recorded by a Geiger-Müller tube or semiconductor (silicon) Orthogonal polarized spectral imaging has been used to obtain
detector placed on or immediately above the exposed liver images of the liver microcirculation comparable to those of fluo-
surface, whereas the γ-emissions of 133Xe are monitored trans- rescence microscopy but without the need for fluorescent dyes
cutaneously by a single scintillation crystal or a γ-camera; the (Langer et al, 2001). This system relies on the absorbance of
latter device allows simultaneous measurement of hepatic tissue hemoglobin and can discriminate a single RBC in an individual
perfusion in many regions of interest. Inert gas techniques capillary with a diameter of 5 µm. Studies with handheld devices
involve minimal trauma to the patient, and their accuracy is not using this technology have been applied to healthy living donors
markedly affected by the presence of hepatic cellular disease or to obtain sinusoidal RBC velocity and blood flow (Puhl et al,
nonperfusion shunts; however, some variability does occur, even 2003). A more recent successor to spectral imaging is sidestream
within the same subject, when multiple studies are performed. darkfield imaging, whereby a light guide surrounded by diodes
The first to use the inert gas method in the hepatic circulation can detect both red and white blood cells in the microcirculation
were Aronsen and colleagues (1968a), who recorded the without the surface reflections (Cerný et al, 2009).
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 87
Portal venous blood flow measured by magnetic resonance prioritized versus production of other hepatic proteins, such as
imaging (MRI) has been found to correlate well with flow albumin and transferrin (Sganga et al, 1985). More recently,
measured by D-US flow probes (Pelc et al, 1992). Subsequently, hemorrhagic shock has been recognized to result in generalized
the technique has been used to measure portal venous blood vascular endothelial dysfunction and impaired endothelial
flow in human liver transplantation candidates (Kuo et al, biosynthesis of NO. Endothelial NO that continues to be
1995). Further methodologic improvements in MRI with high- expressed by the liver during ischemia is believed to protect
resolution phase contrast and compressed sensing may lead to against the initial hepatic injury arising from severe hemor-
their increasing use in the study of hepatic arterial and venous rhage. By contrast, more prolonged hemorrhagic shock (>6
circulation in humans (Dyvorne et al, 2015). hours duration) induces greatly increased production of NO
Transient elastography (TE) is a well-validated technique owing to activation of an inducible NO synthase enzyme in
for the noninvasive assessment of liver fibrosis (Castera et al, hepatocytes and Kupffer cells (Peitzman et al, 1995).
2012) (see Chapter 3). Measurements are performed with a US In the transplantation era, the consequences of ischemia and
transducer built on the axis of a vibrator so that a vibration of reperfusion for the liver have been increasingly investigated
mild amplitude and low frequency is transmitted, inducing a and understood. The damage to the hepatic endothelium and
wave that propagates through the liver tissue, and pulse-echo parenchyma that results from postischemic reperfusion is
acquisitions are performed to measure the velocity of propaga- caused by numerous interrelated phenomena, including the
tion of the wave, which is directly correlated to tissue stiffness. action of locally liberated oxygen-derived free radicals and
Because fibrosis is the main determinant of tissue stiffness and excess formation of vasoconstrictor agents (Wendon, 1999).
of hepatic resistance to portal blood flow, TE has been tested Endogenous NO tends to protect the liver in the early reperfu-
in recent years as a novel way of obtaining numerical, objective, sion period after hepatic ischemia (Wang et al, 1995). Ischemia
and operator-independent noninvasive surrogate value of is also the primary signal for heat-shock protein production in
HVPG (Castera et al, 2012). In this emerging field, several liver tissue. Experimental studies of heat-shock protein precon-
publications support that high liver stiffness (≥21.1 kilopascal ditioning through intermittent portal clamping demonstrated
[kPa]) and low liver stiffness (<13.6 kPa) are accurate to respec- attenuated aminotransferase elevations and improved bile
tively rule in or out clinically significant portal hypertension, production after ischemia (Terajima et al, 1999).
but a considerable indeterminant zone (between 13.6 and 21.1
kPa) limits the use of TE in the precise assessment of HVPG Liver Atrophy
(Berzigotti et al, 2013). Liver atrophy results from a significant reduction of LBF
containing hepatotrophic substances (see Chapter 6). The
degree of atrophy depends on the degree of blood flow depriva-
CLINICAL RELEVANCE tion and may be distributed according to the source of depriva-
tion, including PV or HA blood flow or their combination.
Hemorrhagic Shock, Hypoperfusion, Atrophy and fatty degeneration of the canine liver after total
and Ischemia-Reperfusion Injury portal diversion through an Eck fistula initially was reported
Total LBF decreases approximately in relation to the degree of more than a century ago (Hahn et al, 1893). Partial or complete
the hemorrhage, and portal venous blood flow decreases in diversion of PV blood flow from the liver results in atrophy.
parallel to cardiac output; but similar to the coronary, pulmo- Complete portal venous flow diversion with interruption of all
nary, and cerebral circulations, hepatic arterial flow does not portal venous collaterals results in more profound liver atrophy
decrease until extremely low blood pressures are reached. As a than the partial deviation of portal venous flow resulting from
result, the hepatic oxygen supply tends to be maintained, side-to-side portacaval anastomoses (Bollman, 1961). A precise
although oxygen extraction greatly increases to preserve normal relationship between the degree of liver atrophy and the reduc-
total oxygen consumption (Smith et al, 1955). Hepatic blood tion of portal venous blood flow is still to be determined, pri-
volume can increase significantly in cardiac failure and can marily because of the relative composition and contribution of
compensate as much as 25% of hemorrhage from its large- portal flow and resultant compensatory hepatic arterial flow.
capacitance vessels (Lautt, 2007). Liver atrophy after portal diversion is not believed to be the
The clinical entity known as shock liver has long been recog- result of a decrease in absolute volume flow, but instead it is
nized, typically related to cardiogenic or hemorrhagic shock due to the effective loss of hepatotrophic substances in the
(Birgens et al, 1978). Hepatic dysfunction caused by hypoperfu- portal blood. Rats subjected to portal flow diversion with
sion is manifested pathologically by centrilobular necrosis and portacaval transposition had a decrease in relative liver weight
clinically by abdominal pain, cholestatic jaundice, and marked (Guest et al, 1977) despite the effective preservation of portal
elevation of serum aminotransferases. Three phases of liver perfusion from the IVC (Ryan et al, 1978). Dogs with “partial
injury attributed to ischemia were proposed by Champion and portacaval transposition” (Marchioro et al, 1967) or “splanch-
colleagues (1976), whereby the initial hepatic dysfunction nic flow division” (Starzl et al, 1973) with diversion of pancre-
would resolve as long as no additional insults (e.g., sepsis) were aticogastroduodenosplenic blood had atrophy in liver lobes,
incurred. Gottlieb and colleagues (1983) showed that hepatic although normal tissue perfusion was shown in all regions of
dysfunction in humans after trauma was related to a reduced the liver (Mathie et al, 1979).
hepatic blood flow rate as much as 70% of resting levels. Hepatic Histologically, arterial obstruction results in ischemic
blood flow was markedly reduced after injury, and although total changes, such as mitochondrial swelling, cell membrane disrup-
splanchnic oxygen delivery was decreased, oxygen consumption tion, platelet aggregation, and widening of the spaces of Disse
remained normal as a result of increased hepatic extraction. (Mallet-Guy et al, 1972). The fate of the liver after ligation of
In the ischemic state, upregulation of acute-phase proteins the HA depends largely on the extent of a functional collateral
(C-reactive protein, fibrinogen, ceruloplasmin, haptoglobin) is arterial circulation (Rappaport & Schneiderman, 1976). If
88 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
limited collaterals are present, liver infarction and necrosis may secondary biliary fibrosis (see Chapter 76) and shock after
occur after HA ligation, resulting in death. However, HA liga- biliary tract decompression. Approximately 20% of patients
tion results only in transient ischemic changes in the periphery with prolonged biliary obstruction experience clinically signifi-
of the hepatic acinus (zone III, see Fig. 5.3) in the presence of cant portal hypertension (Blumgart et al, 1984; Sedgwick et al,
adequate collaterals. Atrophy after HA ligation can occur 1966). The operative risk of biliary decompression in these
in liver segments that have compensatory collateral supply patients is significant. Technical difficulties of stricture repair—
to prevent necrosis. The effects of HA flow absence are magni- dense fibrous adhesions, hilar ductal involvement, and
fied by the presence of low portal venous blood flow, limited infection—are complicated by the risk of hemorrhage from
oxygen saturation, and superimposed infection (Rappaport & subhepatic and periductal varices and potential postoperative
Schneiderman, 1976). liver failure. In addition to the hemodynamic consequences of
chronic bile duct obstruction, sudden decompression of the
Impact of Acute and Chronic Bile Duct Obstruction on obstructed biliary tree also causes an abrupt decrease in
Liver Blood Flow wedged HV pressure, PV pressure, and arterial pressure within
Bile duct obstruction can affect hepatic hemodynamics signifi- 30 minutes of decompression in jaundiced dogs, leading to
cantly. In general, LBF is reduced in the presence of chronic hypotension and shock (Tamakuma et al, 1975). Similarly,
biliary obstruction, leading to hepatic dysfunction. Conversely, Steer and colleagues (1968) reported that rapid needle decom-
acute increases in bile duct pressure from early obstruction pression of an obstructed biliary tree in jaundiced dogs induced
result in a reflexive increase in LBF, which attempts to maintain a decreased arterial pressure, central venous pressure, and
adequate flow in the face of an increased pressure gradient portal venous pressure within 1 hour; they concluded that
opposing secretion and excretion of bile (see Chapter 8). Most sudden decompression of chronic biliary obstruction leads to
evidence suggests that the hemodynamic response of the liver sequestration of fluid within the liver, resulting in a decrease
to biliary obstruction is related, directly or indirectly, to changes in the effective circulating plasma volume and subsequent
in bile duct pressure. Given the limited space of Mall in the hypotension.
portal triad (see Fig. 5.1), it is conceivable that increased biliary
pressures may compress the portal capacitance vessels, leading Liver Resection and Regeneration
to increased arterial flow (Kanda et al, 1996). Acute serial The adult liver exhibits a remarkable potential to restore its
increases in bile duct pressure in dogs with complete bile duct cellular mass in response to injury through hepatocyte hyper-
obstruction increased hepatic arterial blood flow by 250% but plasia. Hepatic regeneration of the normal liver remnant pro-
did not affect portal venous blood flow. The precise mechanism ceeds rapidly after partial hepatic resection (Aronsen et al,
for reduction in LBF after chronic bile duct obstruction is 1970; Blumgart et al, 1971) (see Chapters 6 and 108D). Partial
unknown. Although increased portal vascular resistance is the liver resection without devascularization normally produces
accepted underlying cause, the primary site of this resistance little change in total blood flow to the liver. This occurs because
change has been considered to be presinusoidal (Reuter & the major contributor to total flow, the PV, is affected less by
Chuang, 1976), sinusoidal (Bosch et al, 1983), or postsinusoi- events occurring within the liver than by control mechanisms
dal (Tamakuma et al, 1975). The development of significant in the arterial resistance vessels of the prehepatic splanchnic
portosystemic shunting with an inverse correlation between bed. On the other hand, the failure of the liver to directly
shunting and portal venous blood flow can also contribute to control its portal venous flow may result in portal hyperperfu-
extrahepatic shunting (Bosch et al, 1983; Ohlsson, 1972). sion of a reduced parenchymal mass. Because essentially the
Relief of long-term obstruction does not result in the return same total blood flow is redistributed to a smaller mass of liver
of normal hemodynamics, suggesting irreversible intrahepatic tissue, a corresponding increase in tissue perfusion (mL/min
vascular damage (Aronsen et al, 1969). Furthermore, a 23% per unit tissue weight) would be anticipated in the in situ
reduction in effective LBF persisted for 1 to 5 years after remnant. Experimental studies support these expectations; an
operative decompression in patients with choledocholithiasis increase in hepatic tissue perfusion was observed in rats imme-
and jaundice for more than 2 weeks preoperatively (Aronsen, diately after two-thirds hepatectomy (Rice et al, 1977; Wheatley
1968b). Hunt (1979) serially measured LBF daily for 1 week et al, 1993; Wu et al, 1993). This increase in hepatic perfusion
after bile duct ligation in rats, using the 133Xe clearance tech- is due primarily to portal venous inflow, because hepatic arterial
nique to document the early hemodynamic response. Total LBF blood flow is low, and hepatic arterial resistance is high even
decreased steadily after the first postoperative day to a plateau 24 hours after partial hepatectomy in rats.
level of approximately 50% of the preoperative value 5 days In humans, an immediate increase in tissue perfusion of
after operation. Mathie and colleagues (1988) confirmed the approximately 120% occurs in the liver remnant (Mathie &
decrease in total LBF after bile duct ligation by measuring the Blumgart, 1982). A 60% partial hepatectomy results in a
individual portal venous and hepatic arterial components of doubling of the portal flow in the 40% of remnant liver tissue
LBF. Using electromagnetic flowmeters in dogs with complete (Troisi et al, 2005). Experimental evidence has suggested that
bile duct ligation, hepatic arterial and portal venous blood flow intrahepatic shear stress from increased portal flow is a regula-
were observed to decrease by 36% and 44%, respectively; they tor of liver regeneration (Nobuoka et al, 2006; Schoen et al,
also showed a 200% increase in intrahepatic portal resistance 2001). The significance of blood flow in relation to liver regen-
but a lesser increase in hepatic arterial resistance. Similarly, eration, however, continues to be debated since Mann (1944)
dogs with chronic bile duct ligation had decreased portal venous suggested that regenerative hyperplasia of the liver after partial
flow and had developed sinusoidal portal hypertension and resection was a function of portal blood flow and that the
extensive portosystemic shunting (Bosch et al, 1983). process could be prevented by portal flow diversion. However,
Chronic biliary obstruction can thus result in two hemody- regenerative hyperplasia normally occurs after partial liver
namic consequences: portal hypertension associated with resection in portacavally transposed animals, in which there is
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 89
no direct supply of portal blood nor the usual posthepatectomy et al, 2003). This phenomenon describes the impaired HA flow
increase in hepatic tissue perfusion (Fausto, 2000). by shifting of the main blood flow to the splenic or gastroduo-
denal artery in patients with hypersplenism. In whole-organ
Liver Blood Flow and Hemodynamic Studies liver recipients analyzed by D-US, HA vasoconstriction in
in Liver Transplantation response to portal hyperperfusion and exaggerated HABR
The HA buffer reponse is conserved following orthotopic liver produces a high resistive index with poor arterial perfusion
transplantation (OLT) despite denervation (Eipel et al, 2010; (Quintini et al, 2008). In a retrospective analysis of 650 OLTs,
Henderson et al, 1992). In a series of experiments by Payen a 5.1% incidence of splenic artery syndrome has been reported,
and colleagues (1990), serial clamping of the PV every 12 hours and prophylactic treatment with ligation of the splenic artery
for 7 days following OLT resulted in reciprocal increases in for patients at risk for development of splenic artery syndrome
hepatic arterial flow. OLT of a normal donor organ does not has been advocated (Mogl et al, 2010). A prospective study has
normalize the splanchnic and systemic hemodynamic altera- suggested that preoperative embolization of the splenic artery
tions of end-stage liver disease (Henderson, 1993). In fact, total leads to improved postoperative living-donor graft function
hepatic blood flow remains elevated 6 months after OLT (Umeda et al, 2007). Because splenic artery occlusion reduces
(Hadengue et al, 1993; Navasa et al, 1993) mainly because of the resistance to distal HA flow by reducing flow in the splenic
portal venous blood flow (Henderson et al, 1992; Paulsen & circulation, and consequently portal venous flow, it has been
Klintmalm, 1992). This suggests that baseline LBF may be suggested to revise the name of splenic artery steal syndrome
under direct sympathetic control, which is lost after OLT, to splenic artery syndrome, thereby underlining that the cause
leading to an unopposed rise. Azygos flow also remains elevated, is portal hyperperfusion and not arterial siphoning (Quintini
and other portosystemic shunts have been documented up to et al, 2008).
4 years after OLT (Navasa et al, 1993). Ligation of these por-
tosystemic collateral pathways has been shown to increase Portal Hypertension
portal venous blood flow (Fujimoto et al, 1995). Portal hypertension is a state of sustained increase in the
The hemodynamic consequences of OLT in human patients intraluminal pressure of the PV and its collaterals, associated
are difficult to interpret for several reasons: (1) The causes of with the most severe complications of cirrhosis, including
liver failure in end-stage transplant candidates are diverse; ascites, hepatic encephalopathy, and bleeding from gastro-
(2) immunosuppressive drugs are used, such as cyclosporine, esophageal varices (de Franchis et al, 2010) (see Chapters 76,
which causes arterial hypertension; and (3) to control systemic 81, and 82). A mean HVPG greater than 12 mm Hg has clas-
hypertension after OLT, patients may also be given vasodilators, sically been used to define portal hypertension, as variceal
which can cause persistently increased cardiac output. Cardiac bleeding does not occur at lower pressures than this (Garcia-
output data have been conflicting, with one group reporting Tsao et al, 1985). Measurement of HVPG is now considered
persistently elevated values (Hadengue et al, 1993) and others as one of the best surrogates of clinical events, using different
showing decreases 2 weeks and 2 months after OLT (Navasa thresholds to guide the management of cirrhotic patients, and
et al, 1993). Gadano and colleagues (1995) emphasized that a value of 10 mm Hg and greater is predictive of varices
factors such as anemia and sepsis may account for the deranged formation and liver decompensation (Table 5.2) (Berzigotti
hemodynamics after OLT. In a recent retrospective series of et al, 2013).
970 patients, new-onset heart failure developed in as many as
10% of patients following OLT after a median follow-up of 5.3 Hemodynamics
years, the majority of which were of nonischemic etiology Hemodynamic factors that influence portal hypertension are
(Qureshi et al, 2013). best understood by the flow-resistance principle that applies to
the portal venous system. Portal pressure depends on two basic
Small-for-Size Syndrome components: portal blood flow and hepatic portal vascular
The advent of living-donor partial liver transplantation and the resistance. Portal hypertension may result from a significant
enlargement of the resectable limit has introduced the phenom- increase in hepatic portal inflow from the prehepatic splanchnic
enon of small-for-size syndrome, whereby the pressure of the vasculature, an increase in intrahepatic portal resistance
full portal flow traveling through a small liver remnant leads to (IHPR), or both. Although simple in concept, multiple factors
a marked decreased arterial inflow, hypothesized to result from may influence both the components of the system and the
an intact HABR (Michalopoulos, 2010). In a porcine model, pathophysiology of portal hypertension.
portal flow to split grafts with a graft-to-recipient liver volume Increased portal pressure, diminished hepatic portal blood
ratio of 2 : 3 and 1 : 3 was inversely correlated to graft size flow, and an extensive extrahepatic collateral venous network
(Smyrniotis et al, 2002). In patients with right lobe living- supplied by a hyperdynamic splanchnic and systemic circula-
donor transplantation, the grafts are subjected to more than tion characterize the hemodynamics of portal hypertension in
double increases of portal blood flow, whereas the arterial flow cirrhotic patients. Extrahepatic shunts may account for at least
is strikingly decreased, likely to maintain total blood flow within 50% of the portal flow, whereas 80% of portal flow actually
an acceptable physiologic range (Marcos et al, 2000; Rocheleau reaching hepatocytes has been observed to bypass the sinusoidal
et al, 1999). The consequence of inadequate hepatic arterial vascular bed via intrahepatic shunts (Okuda et al, 1977). The
flow range from mild cholestasis and delayed synthetic function magnitude of extrahepatic shunt flow in patients with cirrhosis
to ischemic cholangitis and parenchymal infarct (Demetris was measured directly by thermal dilution assessment of azygos
et al, 2006) (see Chapter 120). blood flow; a value 300 mL/min greater than in patients without
Although arterial flow impairment appears to result from an portal hypertension was noted (Bosch & Groszmann, 1984).
active HABR, it has repeatedly been ascribed to the splenic The HA probably provides a greater relative contribution to the
artery steal syndrome in the past (Manner et al, 1991; Nüssler total LBF in patients with cirrhosis than in healthy individuals,
90 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
TABLE 5.2 Prognostic Significance of Hepatic Venous Pressure Gradient Thresholds According to the Compensated or Decompensated
Stage of Cirrhosis
Clinical Setting HVPG (mm Hg) Increased Risk of Threshold
Compensated cirrhosis 10 Presence (Garcia-Tsao et al, 1985) and development of gastroesophageal varices
(Groszmann, 2005)
First clinical decompensation in patients without varices (Ripoll, 2007)
Development of HCC (Ripoll, 2009)
Decompensation after surgery for HCC (Bruix, 1996; Llovet, 1999)
12 Variceal bleeding (Garcia-Tsao et al, 1985; Gluud, 1988; Lebrec, 1980; Merkel, 1992;
Vorobioff, 1996)
16 First clinical decompensation in patients with varices (Berzigotti, 2011) and mortality
(Merkel, 2000)
Decompensated cirrhosis 16 Variceal rebleeding and mortality (Stanley, 1998)
20 Failure to control variceal bleeding in patients actively bleeding from varices (Abraldes,
2008; Moitinho, 1999)
22 Mortality in patients with alcoholic cirrhosis and acute alcoholic hepatitis (Rincon, 2007)
30 Spontaneous bacterial peritonitis (Sersté, 2006)
HCC, Hepatocellular carcinoma.
From Berzigotti A, et al: Assessing portal hypertension in liver diseases. Expert Rev Gastroenterol Hepatol 7:141-155, 2013.
although it also was shown that 33% of the arterial blood may mediators, cytokines, growth factors, and endothelin (Lee et al,
flow through intrahepatic shunts to the systemic venous circula- 2015) (see Chapter 11). Capillarization of sinusoidal endothe-
tion (Groszmann et al, 1977). Vallance and Moncada proposed lial cells occurs by defenestration or loss of endothelial cell
the hypothesis that the low peripheral vascular resistance in pores and the appearance of a basement membrane (Varin &
portal hypertension may be caused by the stimulated produc- Huet, 1985). In the cirrhotic liver, the sites of vascular resistance
tion of NO induced by endotoxemia in 1991. The initial are still unclear. However, because portal and hepatic venules
experimental evidence was provided by Pizcueta and others can be found within fibrous septa, constriction or distortion of
(1992), who showed an increase in systemic and splanchnic portal venules, hepatic venules, or both may be involved (Kelty
vascular resistance in cirrhotic rats after the administration of et al, 1950). Disruption of hepatic architecture, with the devel-
an NO inhibitor. Although endotoxemia is likely responsible for opment of fibrous septa and abnormal nodules and circulation
the decompensation in end-stage cirrhosis, the hemodynamic leads to a sustained IHPR and portal pressure. While portal
alterations are due to NO in animal models (Lee et al, 1996; venous blood flow progressively decreases in cirrhosis, arterial
Niederberger et al, 1995). Constitutive NO synthase seems to resistance decreases and arterial flow increases, suggesting an
be upregulated in discrete anatomic locations, such as in the intact buffer response. Studies in cirrhotic rats have demon-
endothelium of the mesenteric artery and in the esophageal, strated higher hepatic arterial flows compared with normal
gastric, and jejunal mucosa (Mathie, 1999). control rats under baseline conditions (Richter et al, 2000).
The direction of portal blood flow has been proposed as a This finding was confirmed by using intraoperative measure-
contributor to the pathophysiology of portal hypertension. The ments in patients with end-stage cirrhosis undergoing living-
progression of intrahepatic disease and increasing sinusoidal donor liver transplantation (Aoki et al, 2005). Clinically, the
pressure has been postulated as contributing to reversal of flow vasodilaton of the splanchnic circulation likely serves to increase
in the PV, which further aggravates the injury by depriving the flow in the extrahepatic collateral circulation, leading to variceal
liver of nutrients (Warren & Muller, 1959). However, reversed, hemorrhage.
or hepatofugal, PV flow is relatively infrequent. Gaiani and
colleagues (1991) reported an incidence of 3.1% in 228 patients Treatments
assessed, whereas intrahepatic portal flow reversal has been Medical and surgical management strategies for portal hyper-
described in as many as 9% of patients and seen almost exclu- tension strive to improve patient survival by the reduction of
sively in those with Child-Turcotte-Pugh C cirrhosis (Tarantino pressure and flow in extrahepatic variceal vessels, mainly
et al, 1997). esophageal and gastric vessels, while preserving adequate portal
In portal hypertension, the increased mesenteric blood flow flow to the liver (see Chapters 81 to 87). Portosystemic shunting
in the hyperdynamic stage may be relatively less important and pharmacologic reduction of portal flow can provide effec-
than the elevated IHPR caused by the interplay of local regula- tive decompression, but both deprive the liver of portal flow.
tory mechanisms affecting sinusoidal hemodynamics (Grosz- Multiple pharmacologic agents have been investigated to
mann 1990). The traditional view of the source of increased reduce portal hypertension by diminishing hepatic portal inflow
portal pressure is fibrotic encroachment around portal radicles, from the mesenteric vascular bed. At a dose that decreases the
leading to increased IHPR. The pathogenesis of cirrhosis heart rate by 25%, the β-blocker propranolol significantly
involves initial hepatocyte necrosis and inflammation with reduced the risk of rebleeding in cirrhotic patients who were
subsequent transformation of HSCs into myofibroblasts. HSC otherwise in good condition (Lebrec et al, 1981) (see Chapter
activation results in the collagenization of the space of Disse 82). Propranolol exerts its action by two mechanisms: decreased
(Martinez-Hernandez, 1985) (see Chapter 7). Several factors cardiac output as a result of β1-adrenergic cardiac receptor
have been implicated in HSC activation, such as inflammatory blockade and antagonism of β2-adrenoceptors in the splanchnic
Chapter 5 Liver blood flow: physiology, measurement, and clinical relevance 91
vasculature, which leaves the vasoconstrictive influence of PREVENTION OF VARICEAL BLEEDING. All patients with cirrhosis
α-adrenergic receptors unopposed, resulting in a decrease should be screened by endoscopy for varices at diagnosis. The
portal flow and pressure. Vasopressin causes generalized periph- treatment of underlying liver disease, when possible, may
eral vasoconstriction (Bosch et al, 1988), whereas the effect of reduce portal hypertension and prevent its clinical complica-
somatostatin is specific to the splanchnic vascular bed (Kravetz tions. There is no pharmaceutical agent proven effective to
et al, 1984) and resultsg from glucagon-release inhibition and prevent the formation of varices. Patients with small varices
direct vasoconstriction. Serotonin may play a significant role in with red marks or Child-Turcotte-Pugh C cirrhosis have an
maintaining increased portal pressure, and smooth muscle increased risk of bleeding and should thus be treated with
serotonin-receptor antagonists have been shown to lower the nonselective β-blockers. Patients with medium to large varices
pressure in cirrhosis (Hadengue et al, 1987; Mastaï et al, 1989). also can benefit from endoscopic band ligation for the preven-
Although it was originally thought that IHVR in cirrhosis tion of the first variceal bleeding episode (primary prophylaxis)
was irreversible, evidence has supported that it can be reduced (see Chapter 82). In centers where adequate resources and
pharmacologically (Bhathal & Grossman, 1985). The nitrova- expertise are available, HVPG measurements can routinely be
sodilators isosorbide dinitrate and isosorbide mononitrate were used for prognostic and therapeutic indications (see Table 5.2).
observed to lower the portal pressure in portal hypertensive A decrease in HVPG of at least 20% from baseline or to
animals (Blei & Gottstein, 1986) and to increase hepatic (but 12 mm Hg or less after chronic treatment with a nonselective
not azygos) blood flow in patients with cirrhosis (Navasa et al, β-blocker has been demonstrated clinically relevant in the
1989), suggesting that they may act by reducing intrahepatic setting of primary prophylaxis of variceal bleeding.
portal vascular resistance. Application of nitroglycerin by
transdermal tape to patients with cirrhosis resulted in a reduc- TREATMENT OF ACUTE BLEEDING (SEE CHAPTER 83). Critical initial
tion in portal pressure without affecting hepatic blood flow steps include airway protection, particularly in patients with
(Iwao et al, 1991), and IV nitroglycerin caused a 24% decrease altered mental status or those with hemodynamic instability,
in IHVR in patients with cirrhosis (Groszmann, 1990). In resuscitation with fluid and blood products, and correction of
animal models, IHVR can be reduced by prostaglandin E2, the coagulopathy and thrombocytopenia. Patients with variceal
endothelin receptor antagonist isoprenaline, nitroprusside, hemorrhage are often bacteremic as a result of a concomitant
papaverine, and verapamil. (Ballet, 1991; Bhathal & Grossman, infectious process (spontaneous bacterial peritonitis, urinary
1985; Reichen & Le, 1986; Reichen et al, 1998). tract infection, or pneumonia), and clinical trials have shown
The use of TIPS, first reported by Rössle and colleagues better outcomes when empiric antibiotic therapy is initiated
(1989), now largely replaces shunt surgery. TIPS is currently early. Vasoconstrictive drugs that reduce portal pressure (soma-
the treatment of choice for recurrent variceal bleeding in tostatin and vasopressin analogues) and endoscopic variceal
patients who are refractory to conservative medical manage- ablation (ligation and sclerotherapy) are the mainstay of initial
ment (Parker, 2014) (see Chapter 87). management (see Chapters 82 and 83). As shown in single trials
Surgical treatment of portal hypertension may be performed and by meta-analysis, this initial strategy controls 80% to 85%
by one of the many portosystemic shunt procedures; the initial of bleeding episodes (Gonzalez et al, 2008). Early assessment
clinical application of the portacaval shunt was reported 50 of prognosis is important to guide further management, because
years after its description by Eck (Whipple, 1945) (see Chapter patients at high risk of treatment failure benefit from early TIPS
85 and 86). The hemodynamic consequences of shunt surgery placement (within 72 hours) (García-Pagán et al, 2010) (see
depend on the particular shunt performed, the nature and Chapter 87). An HVPG of 20 mm Hg or higher, Child-Pugh
severity of the disease, and the hemodynamic condition of the class C, and active bleeding at endoscopy are the variables most
patient. End-to-side portacaval shunts divert all portal blood consistently found to predict 5 day rebleeding treatment failure
flow away from the liver, whereas less complete diversions (Bambha et al, 2008). TIPS may not be an option in some cases,
reduce portal flow in proportion to the degree to which the for example, in face of portal thrombosis, in which situation a
shunt reduces portal pressure. The HA flow may increase by surgical shunt or a devascularization procedure (Dagenais et al,
100%, but even a maximal flow increase can usually only partly 1994) is indicated (see Chapters 84, 85, and 86). Emergency
compensate for loss of portal flow (Mathie & Blumgart, 1983b). portacaval shunt has a success rate of 95% in stopping bleeding
Hepatic oxygen consumption tends to be maintained by in this context. The death rate of the operation is, however, not
increased oxygen extraction from the available arterial supply. insignificant, but generally related to the status of the patient’s
Total portacaval shunts are very effective in reducing portal liver function. Approximately 40% of patients experience
pressure and preventing bleeding from esophageal varices. encephalopathy after portacaval surgical shunting. Hepatic
However, because of bypass of the hepatic circulation, liver insufficiency is accelerated, and liver failure is the cause of death
failure and encephalopathy are common complications of the in approximately two-thirds of those who die after an emergency
operation. Therefore partial shunts, such as the side-to-side, portacaval shunt. Balloon tamponade should only be used in
mesocaval, and proximal or distal splenorenal shunts, are pre- massive bleeding as a temporary measure until definitive treat-
ferred when technically feasible. Selective shunts, such as the ment is instituted (Garcia-Tsao & Bosch, 2010).
distal splenorenal (Warren) shunt, in which the gastrosplenic
collaterals are decompressed via the splenic vein into the left Blood Flow in Hepatic Tumors
renal vein, leaving the PV intact, are affective but usually too It has been demonstrated that tumors of the liver, whether
time consuming for use in emergency operations. primary or secondary, are perfused almost exclusively with
Current consensus on treatment approaches are here sum- arterial blood (Breedis & Young, 1954). Hepatocellular carci-
marized for prevention and treatment of variceal bleeding in noma and liver metastases from neuroendocrine tumors are,
patients with cirrhosis (de Franchis et al, 2010; Garcia-Tsao & however, more arterialized and less necrotic than most other
Bosch, 2010). primary or metastatic liver tumors. The arterial uptake of
92 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
hepatic solid lesions thus provides important differential diag- can also be effectively used to deliver high doses of chemo-
nosis information when assessed by computed tomography therapy directly to the liver for the treatment of patients with
scan and MRI performed with IV contrast, provided that colorectal cancer liver metastasis and unresectable intrahepatic
images are acquired at time of arterial enhancement in addition cholangiocarcinoma (Goéré et al, 2010; Jarnagin et al, 2009;
to venous enhancement (Forner et al, 2008) (see Chapters 18, Kemeny, 2013; Kemeny et al, 2009) (see Chapter 99).
19, 91, and 93). The neovasculature of tumor tissue lacks
smooth muscle and therefore does not respond to vasocon Effect of Laparoscopy on Liver Blood Flow
strictor agents, enabling increased delivery and retention of The use of a CO2 pneumoperitoneum in laparoscopic surgery
chemotherapeutic drugs. The vasoconstrictors epinephrine, has been demonstrated to substantially reduce portal venous
phenylephrine, and angiotensin have improved cytotoxic drug flow in parallel with the intraperitoneal pressure (Jakimowicz
delivery to liver tumors in human and animal models, but this et al, 1998; Schilling et al, 1997). Conflicting data exist in
has not translated into common clinical practice (Bloom et al, support of the maintenance of the HABR effect in high-pressure
1987; Goldberg et al, 1991; Hemingway et al, 1991). pneumoperitoneum. Rat models using fluorescent microspheres
A variety of transarterial techniques have been used to supported preserved hepatic arterial flow during decreased
selectively embolize and deliver chemotherapy to liver tumors, portal venous flow (Yokoyama et al, 2002), but this was not
taking advantage of the fact that they derive disproportionately supported by others (Richter et al, 2001), who saw a parallel
greater blood supply from the hepatic arterial circulation com- decrease in arterial and portal venous flows during laparoscopy.
pared with the surrounding liver (see Chapter 96). Emboliza- Most surgical teams use a 10 to 14 mm Hg pneumoperitoneum
tion is often performed with Gelfoam, which dissolves after a during laparoscopic liver resection, which allows good control
few weeks, but other inert agents are also used and are probably of bleeding (Tranchart et al, 2015) (see Chapter 105). A case-
more effective for occluding vessels. Some centers use inert matched analysis suggested that the positive pressure of pneu-
particles without chemotherapy (i.e., bland embolization), but moperitoneum was probably the main factor explaining the
most combine the procedure with chemotherapy (i.e., transar- decreased blood loss during laparoscopy when compared with
terial chemoembolization, or TACE). Doxorubicin, mitomycin, open liver surgery (Tranchart et al, 2013). Some groups have
and cisplatin in various combinations are the drugs most often suggested the avoidance of head-up positioning and pressures
given. The embolized material causes temporary blood flow greater than 15 mm Hg during laparoscopy to preserve LBF
interruption and potentially improves the uptake of chemo- (Junghans et al, 1997; Klopfenstein et al, 1998). So far, no
therapeutic agents in tumor tissue and, consequently, reduces major accident related to the use of a CO2 pneumoperitoneum
systemic toxicity (Liapi & Geschwind, 2010). Lipiodol and during laparoscopic liver resection has been reported in
drug-eluting beads, which lodge in the tumor, have also been approximately 6000 cases (Dagher et al, 2014). Furthermore,
used as a carrier for chemotherapy. More recently, radioactive a swine model has been used to prospectively demonstrate that
microspheres emitting yttrium-90 have been used. These pro- multiple gas embolisms frequently occur during laparaoscopic
cedures are mainly performed in the palliative setting for liver resection without significant modification of hemodynam-
patients with hepatocellular carcinoma not amenable to liver ics (Jayaraman et al, 2009; Schmandra et al, 2004).
resection or transplantation. It remains unclear if the addition
of chemotherapeutic agents provides much benefit beyond the Acknowledgements
necrosis produced by occlusion of the hepatic arterial supply Thank you to Drs. Blumgart, Wheatley, Mathie, and Rocha for
alone (Lammer et al, 2010; Llovet et al, 2002; Lo et al, 2002; their previous contributions to this chapter.
Malagari et al, 2010; Maluccio et al, 2008; Salem et al, 2011).
Hepatic arterial infusion of chemotherapy delivered by References are available at expertconsult.com.
catheters connected to subcutaneously placed ports or pumps
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CHAPTER 6
Liver regeneration: mechanisms and clinical
relevance
Jeroen de Jonge and Kim M. Olthoff
And now the last recess of the Black Sea opened up and they regain most of its functional mass within 2 weeks (Humar et al,
[the Argonauts] caught sight of the high crags of the Kaukasos, 2004; Kamel et al, 2003; Marcos et al, 2000; Pomfret et al,
where Prometheus stood chained by every limb to the hard 2003). Factors that limit the achievement of curative tumor
rock with fetters of bronze, and fed an eagle on his liver. The resection and small-for-size (SFS) transplantations are the high
bird kept eagerly returning to its feed. They saw it in the morbidity and mortality rates associated with insufficient
afternoon flying high above the ship with a strident whirr. It volume of the liver remnant or graft (Fig. 6.1). While hepatobili-
was near the clouds, yet it made all their canvas quiver to its ary and transplant surgeons continue to expand the magnitude
wings as it beat by. For its form was not that of an ordinary and complexity of liver resection, understanding liver regenera-
bird: the long quill-feathers of each wing rose and fell like a tion becomes increasingly relevant. Many tumors that were
bank of polished oars. Soon after the eagle had passed, they previously considered to be unresectable are now amenable to
heard Prometheus shriek in agony as it pecked at his liver. The complete resection through induction chemotherapy and inno-
air rang with his screams till at length they saw the flesh- vative treatment strategies to increase liver remnant volume
devouring bird fly back from the mountain by the same way (Clavien et al, 2007). Portal vein embolization (PVE), portal
as it came. vein ligation, and to the extreme, in Associating Liver Partition
Argonautica 2.1238f and Portal vein ligation for Staged hepatectomy (ALPPS),
causes atrophy of the ipsilateral hemiliver and hypertrophy of
The ability of the liver to regenerate was recognized by the the contralateral side and are particularly valuable in patients
Greeks in the ancient myth of Prometheus, the Titan god of who have underlying liver disease. Because of the increased
forethought, who gave fire to the mortals and angered Zeus. success of liver surgery, more patients with underlying liver
Prometheus was chained to the Caucasus Mountains, and each disease are now considered suitable candidates for liver resec-
day he would be tormented by Zeus’ eagle Ethon as it devoured tion, even with Child-Pugh grade A cirrhosis and some degree
his liver. Each night, the damaged liver would heal so the eagle of portal hypertension (Boleslawski et al, 2012; Chen et al,
could begin anew, illustrating the incredible capacity of the liver 2012; Zhong et al, 2014). Patients with the metabolic syn-
to regenerate. drome, morbid obesity with concomitant steatosis, or nonalco-
In contrast to other solid organs, the human liver has the holic steatohepatitis (NASH) have, however, increased risk of
unique ability to regenerate after toxic injury, chronic inflam- liver failure after liver surgery (Belghiti et al, 2000; McCormack
mation, and surgical resection. The terms regeneration, hyper- et al, 2007), as are elderly patients older than 70 years with
plasia, and hypertrophy are used synonymously in literature, restricted hepatic reserve capacity.
but hyperplasia is the most precise from a cellular standpoint. In colorectal malignant disease, approximately 50% of the
The damaged hepatic lobes do not grow back in the same way patients will experience liver metastasis in the course of their
a lizard’s tail regrows, but rather, there is a hyperplastic response disease. With the substantially improved chemotherapy for
(defined as increasing cell number) in the remnant liver, leading colorectal cancer during the last decade, the resectability rate
to its hypertrophic appearance (defined as enlarging liver size) has gradually increased to 20% to 30% (Chua et al, 2010;
(Lory et al, 1994). This process is highly regulated, involving Robinson et al, 2011; Uetake et al, 2015). As a consequence,
multiple cell types, extrahepatic signals, complex molecular more patients are having liver surgery after neoadjuvant or
pathways, and cellular interactions. A delicate balance in initia- induction chemotherapy, which has considerable effects on liver
tion of regeneration and exerting an intracellular growth parenchyma and can inhibit liver regeneration.
response to restore lost liver mass, while maintaining normal Regeneration also is crucial in liver transplantation. In
metabolic function, is necessary for survival. The inability to deceased-donor transplantation, hepatocyte loss occurs in the
maintain this process leads to poor liver function and ultimately form of ischemia/reperfusion (I/R) injury owing to the neces-
liver failure after surgery. sary preservation period from procurement to implantation
and damage that may have occurred in the donor. Due to the
CLINICAL RELEVANCE OF LIVER scarcity of organs, more “marginal” organs are accepted for
REGENERATION transplantation, which increases the need for regeneration and
recovery in the environment of I/R injury and use of immuno-
Today, liver surgery is routinely and safely accomplished for suppressive drugs. One of the landmark advances in liver
malignant and benign disease. This substantial progress in both transplantation is the ability to use segmental liver grafts
resection and transplantation relies on the ability of the liver to obtained from either a deceased donor or a living donor. In the
93
94 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Vascular endothelial
Stellate cell
growth factor Hepatocyte
Platelets
Tumor Farnesoid X
Kupffer cell
necrosis
receptor
factor-α
G1 phase
Leukocyte
Interleukin-6
Nucleus
G0 or G1 Release
phase Matrix
Sinusoidal metalloproteases
endothelial cell Transforming
Epidermal growth factor-α
Bile acids growth factor
FIGURE 6.2 Pathways of liver regeneration initiated by major hepatectomy. After hepatectomy, nonparenchymal cells, such as stellate cells, Kupffer
cells, leukocytes, and platelets, are activated by soluble factors. As a result, Kupffer cells release tumor necrosis factor-α and interleukin-6. The
cytokines cause a priming of the remnant hepatocytes, and concurrently, extracellular proteases such as urokinase-type plasminogen activator convert
inactive hepatocyte growth factor to its active form. The cytokines and the growth factors act in concert to initiate the reentry of quiescent hepatocytes
(in the G0 phase) into the cell cycle from the G1 phase to the S phase, resulting in DNA synthesis and hepatocyte proliferation. The metabolic burden
is indicated by the accumulation of bile acids in the blood, which enter the hepatocytes and drive increased protein and DNA synthesis. To signal
the end of proliferation, transforming growth factor-β blocks further replication. (From Clavien, et al: Strategies for safer liver surgery and partial liver
transplantation. N Engl J Med 356:1545-1559, 2007.)
(Roskams et al, 1998). The human HPC originates from the flow after PHx resulted in hepatocyte proliferation and hyper-
canals of Hering (Carpentier et al, 2011; Carpino et al, 2011; plasia (Starzl et al, 1977). From a recent experimental partial
Rodrigo-Torres et al, 2014) and play an important role in liver transplant model, we know that increased portal flow
acetaminophen-induced injury (Kofman et al, 2005). Huch (from a universal 100 mL/100 g liver tissue/min to 200 mL/
and colleagues (2015) described conditions allowing long-term 100 g/min) is essential for liver regeneration. However, if portal
expansion of these adult bile duct–derived bipotent progenitor flow exceeds 250 mL/100 g/min (portal hyperperfusion), the
cells from human liver, which enables disease modeling, toxi- process is completely abolished (Hessheimer et al, 2011).
cology studies, and regenerative medicine. Experiments in parasymbiotic rats demonstrated the existence
In common with other tissues, there is persuasive evidence of humoral factors in the induction of liver growth after PHx
that, in the liver, stem cells can be the founder cells of primary (Moolten & Bucher, 1967).
hepatic malignancies, such as hepatocellular carcinoma (HCC). Interleukin-6 (IL-6) and tumor necrosis factor-α (TNF-α)
Prominin-1 (CD133) and Sal-like protein 4 (SALL4) have have since then been identified as the earliest factors triggering
been identified as cancer stem cell markers in HCC (Ma, 2012; activation of several transcription factors during regeneration
Oikawa et al, 2013; Song et al, 2008; Tang et al, 2008, 2012; (Cressman et al, 1996; Yamada et al, 1997) (Fig. 6.3). In
You et al, 2010). IL-6–deficient or TNF-α receptor–deficient mice, liver regen-
eration after hepatectomy is delayed (Streetz et al, 2000) but
Induction of Proliferation: Priming and not completely abolished (Fujita et al, 2001; Michalopoulos
Cell-Cycle Progression et al, 1984). Therefore other blood-derived mitogens, such as
Within minutes after PHx, specific immediate early genes are hepatocyte growth factor (HGF), were identified as putative
activated in remnant hepatocytes (Haber et al, 1993). These hepatic growth factors during liver regeneration (Fausto, 2000).
genes include protooncogenes that play an important role in Hepatocytes in normal liver are not ready to respond to mito-
normal cell-cycle progression, such as JUN, FOS, MYC, and genic signals without a set of “priming” events that switch them
KRAS (Morello et al, 1990; Taub, 2004; Thompson et al, 1986) into a responsive state. This has been described by Webber and
and the transcriptional factors nuclear factor (NF)-κB, signal colleagues (1994), who identified priming factors involved in
transducer and activator of transcription 3 (STAT3), activator initiating and triggering of the hepatic response to injury and
protein-1 (AP-1), and CCAAT enhancer–binding protein-β (C/ concomitant growth factors and their receptors, allowing com-
EBPβ) (Cressman et al, 1995; FitzGerald et al, 1995). petent hepatocytes to progress through the cell cycle. Priming
Historically, the onset of liver regeneration has been attrib- is accomplished by the release of preformed cytokines that
uted to a flow-dependent response by which increased relative subsequently activate transcription factor complexes and allow
96 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Hepatocyte
STAT3
gp130 JAK P
Kupffer cell
C3a/C5a IL-6
TNF-α TLR
IL-6R JAK P –VE
P
P SOCS3
Activated
NF-κB STAT3 homodimer
IL-6
SOCS3
TNF IL-6 mRNA P mRNA
mRNA P
TNF-α
Multiple biological responses:
Cell survival/proliferation
FIGURE 6.3 Stimulated by components of the innate immune system, Kupffer cells produce and secrete interleukin-6 (IL-6) and tumor necrosis
factor-α (TNF-α) to kick-start the regenerative response. IL-6 helps stimulate hepatocyte proliferation via signal transducer and activator of transcription
3 (STAT3) activation; in turn, this response is negatively regulated by suppressor of cytokine signaling 3 (SOCS3). gp130, Glycoprotein 130; IL-6R,
interleukin-6 receptor; JAK, Janus activating kinase; mRNA, messenger RNA; NF-κB, nuclear factor kappa B; P, phosphate; TLR, Toll-like receptor;
VE, negative feedback. (From Alison et al: Stem cells in liver regeneration, fibrosis and cancer: the good, the bad and the ugly. J Pathol 217:282-
298, 2009.)
the cell to exit G0 into G1 of the cell cycle. This group includes poor activation of nuclear factor kappaB (NF-κB) and STAT3.
TNF-α and IL-6 (Aldeguer et al, 2002). Growth factors include In the initiation of growth factors, uPA appears to play an
the potent hepatocyte mitogens HGF, transforming growth important role. uPA and its downstream effector plasminogen
factor-α (TGF-α), and heparin-binding epidermal growth increase within 1 to 5 minutes after PHx and rapidly cleave the
factor (HB-EGF). This process is further controlled by HGF precursor pro-HGF. Blocking uPA delays the appearance
co-mitogens, such as insulin, glucagon, steroid hormones, par- of HGF and thereby delays liver regeneration, whereas blocking
ticularly estradiol, and epinephrine, which facilitate activity of plasminogen-activator inhibitor (PAI) accelerates the release of
the mitogens, and by downregulation of growth factor inhibi- HGF and liver regeneration (Currier et al, 2003).
tors such as activin A and TGF-β. The nuclear receptor (NR) superfamily is a set of transcrip-
So far, a few factors have been identified to be possibly tion factors, acting as conductors of differentiated liver func-
responsible for the release of these priming cytokines and tions. NRs are master transcriptional regulators of different
growth factors in the onset of liver regeneration. The first is homeostatic processes (e.g., development, cell differentiation,
endotoxin lipopolysaccharide (LPS), produced in the gut by metabolism, proliferation, and apoptosis), and can be modu-
gram-negative bacteria. Circulating LPS is an extremely strong lated by different signals (e.g., hormones, vitamins, lipids)
signal for Kupffer cells to start the cascade resulting in hepato- (Karpen & Trauner, 2010; Wagner et al, 2011). NRs (48 in
cyte replication. Rats treated with antibiotics and germ-free humans, 49 in rodents) are key players in the modulation of
rodents have a delayed peak of DNA replication after PHx, liver physiology and development, being also involved in cell
confirming the importance of LPS (Cornell et al, 1990). This growth and differentiation (Mangelsdorf et al, 1995). Some
signal is MyD88 (myeloid differentiation primary response NRs are regulated by small lipophilic ligands (e.g., hormones,
gene 88) dependent, but the LPS receptor Toll-like receptor vitamins, dietary lipids, bile acids (BAs), and xenobiotics),
(TLR) 2, TLR2, and CD14 do not play roles in regulating whereas other NRs, namely ‘‘true orphans,’’ regulate trans
cytokine production or DNA replication after PHx (Campbell cription independently from binding to specific ligands (Man-
et al, 2006). Another major finding is the demonstration that gelsdorf & Evans, 1995). NRs are also implicated in liver
cytokine activation and DNA replication are severely impaired regeneration modulation (Huang et al, 2006; Vacca et al, 2014)
in mice lacking the complement components C3a and C5a and in the pathophysiology of liver disease.
(Strey et al, 2003). In particular, mice lacking both C3a and NRs are suitable targets for pharmacologic approaches
C5a have impaired production of TNF and IL-6 after PHx and aimed to the control of hepatocyte proliferation (Vacca et al,
Chapter 6 Liver regeneration: mechanisms and clinical relevance 97
2013) because they may modulate a number of early changes several mechanisms, including binding by CDK-inhibitory
essential for the liver regeneration and HCC, such as the activa- proteins, such as p21. Feedback signals to this process are
tion of transcription factors (AP-1; NF-κB; STAT3; and C/ provided by suppressor of cytokine signaling 3 (SOCS 3) and
EBPβ, and the expression of immediate early genes (FBJ TGF-β, also regulated by IL-6. Other studies confirmed the
murine osteosarcoma viral oncogene homolog FOS, JUN, importance of NF-κB (Arai et al, 2003; Fukuhara et al, 2003;
MYC avian myelocytomatosis viral oncogene homolog [c-Myc], Togo et al, 2004) and showed immediate upregulation of apop-
liver regenerating factor-1 [LRF-1], early growth response-1, totic genes (Fas and caspases) in livers that failed owing to
[EGR-1]), cytokines, and growth factors (Huang et al, 2006; excessive resection (Morita et al, 2002) (Fig. 6.4).
Turmelle et al, 2006). In addition, many NR ligands can induce As shown above, the initiation of liver regeneration is associ-
hepatocyte proliferation, also in the absence of liver injury (i.e., ated with strong inflammatory cell signals. It is necessary for
‘‘direct hyperplasia’’) (Columbano & Shinozuka, 1996; Colum- this inflammation to be controlled to allow progression of the
bano et al, 2005; Locker et al, 2003). This is the case of fibrates regenerative pathways. The NF-κB inhibitory and ubiquitin-
(agonists of PPAR-α), thyroid hormones, and the halogenated editing A20 protein (TNFAIP3) plays a key role in the liver’s
hydrocarbon TCPOBOP (agonist of the constitutive androstane protective response to injury, particularly to its antiinflamma-
receptor, CAR) (Columbano & Ledda-Columbano, 2003; tory armamentarium (da Silva et al, 2014).
Ohmura et al, 1996). In a model of 70% mouse hepatectomy, A20 is significantly upregulated in the liver following PHx
the NRs FXRβ, PPAR-δ, and THRA mRNA expression levels and protects hepatocytes from apoptosis and ongoing inflam-
represented the identity card of proliferating cells, thus high- mation by inhibiting NF-κB( da Silva et al, 2013; Longo et al,
lighting these NRs as candidate biomarkers of liver prolifera- 2005). A20 also allows proliferation and optimizes metabolic
tion, and as potential targets for novel pharmacological control and energy production following LR (liver regeneration,
approaches (Vacca et al, 2014). liver resection), as demonstrated by increased enzymatic activ-
Another humoral factor that triggers the concerted regen- ity of cytochrome c oxidase or mitochondrial complex IV
erative response in hepatocytes was discovered. Extracellular (Damrauer et al, 2011). A20-based therapies could be benefi-
adenosine triphosphate (ATP) has emerged as a rapidly acting cial in future prevention and treatment of hepatic failure after
signaling molecule that, after PHx, leads to rapid and transient liver resection.
activation of c-Jun–amino-terminal kinase (JNK) signaling, The cytokine-induced form of nitric oxide synthase (iNOS)
induction of immediate early genes FOS and JUN, and also seems to play an important role in scavenging oxygen radi-
AP-1 DNA-binding activity (Gonzales et al, 2010; Tackett et al, cals and protection from apoptosis, caused by an uncontrolled
2014). inflammatory reaction mediated through IL-6 and TNF-α (Rai
et al, 1998).
Distinct Intracellular Pathways in Liver Regeneration The HGF/c-Met pathway is important for sustaining DNA
The importance of liver regeneration in sustaining life is dem- synthesis after injury and activates various downstream path-
onstrated by the plethora of well-characterized pathways ways that involve phosphoinositide 3-kinase (PI3K), ERK, and
involved and the fact that liver regeneration is usually only serine-threonine kinase Akt/protein kinase B (AKT) (Huh et al,
blunted or delayed in experimental models that lack a “critical” 2004). This pathway cross-talks with the Wnt/β-catenin signal-
pathway. The immediate early genes that are activated in regen- ing pathway, which has come to the forefront in liver biology
erating liver were first identified by Mohn and colleagues (1990) during the last several years (Monga, 2011). Increased levels of
and Haber and colleagues (1993), who described induction HGF results in β-catenin dissociation along with nuclear trans-
patterns of more than 70 genes activated in the first week after location (Monga et al, 2002) and upregulation of downstream
two-thirds PHx in a rat model, normally not expressed in the targets of this pathway, such as cyclin D1, MYC, uPAR, matrix
quiescent liver. A mouse complementary DNA (cDNA) array metalloproteinases (MMPs), and EGF receptor (Michalopou-
has also been used to study the crucial role of IL-6 in liver los et al, 1997). Vascular endothelial growth factor (VEGF)
regeneration in IL-6–deficient mice posthepatectomy, showing interacts with endothelial cells in the liver to increase HGF
a 36% reduction in the early gene expression compared with production from nonparenchymal cells (LeCouter et al, 2003).
wild-type mice. In the absence of IL-6, activation of genes such In the transplant setting, microarray analysis of SFS rat liver
as those encoding the uPA receptor (uPAR) and PAI-1, crucial grafts showed upregulation of vasoconstrictive and adhesion
for HGF activation and the MAPK pathway, were remarkably molecule genes at early time points postreperfusion, with later
delayed (Li et al, 2002). IL-6 activates the JAK/STAT3 and increases in genes associated with inflammation and cell death
MAPK signaling pathways via the gp130/IL-6R complex. This and downregulation of genes related to energy metabolism
leads to activation of an array of immediate and delayed early (Man et al, 2003), which was confirmed in the situation of
genes required for normal liver-specific metabolic functions, clinical deceased-donor and living-donor liver transplantation
repair and hepatoprotection from injury (Taub, 2003; Wueste- (LDLT) (de Jonge et al, 2009).
feld et al, 2003; Zimmers et al, 2003). STAT3 is crucial for cells
to progress from G1 to S phase and for activating the MYC gene, Remodeling of the Liver
a gene required for cell cycle progression. Other intracellular Remodeling of the newly regenerated liver tissue begins with
signaling pathways that involve the receptor tyrosine kinases the repopulation and maturation of nonparenchymal cells, such
p38, mitogen-activated protein kinase (MAPK), phosphorylated as endothelial cells, stellate cells, and biliary epithelial cells.
extracellular signal-regulated kinases (pERKs), and JNK are Newly formed hepatocytes form clusters into which replicating
also rapidly activated. Progression through the cell cycle is regu- endothelial cells invade to form new sinusoids. To restore
lated by cyclins and cyclin-dependent kinases (CDKs). Various normal architecture, stellate cells, which are located between
combinations bind to form kinase complexes that are active at endothelial cells and hepatocytes, synthesize extracellular
distinct points within the cell cycle and tightly controlled by matrix (ECM) proteins and TGF-β1, which can regulate the
98 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Chemokines,
Hormones,
Transmitters
Survival factors Growth factors Extracellular
(e.g., interleukins,
(e.g., IGF-1) (e.g., TGF- α, EGF ) matrix
serotonin)
GPCR Integrins
RTK RTK
cdc42 Wnt
Grb2/SOS Fyn/Shc
PLC
Frizzled
P13K G-Protein Ras FAK Dishevelled
Src
AKT Raf GSK-3 β
PKC Adenylate
cyclase MEK Hedgehog
Akk α NF- κB APC
Patched
(e.g., EPC)
STAT3, 5
TCF
Cytokine receptor
SMO
Cytochrome C CREB CyclD
p16 Gli
Rb CDK4
Caspase-9 p15
E2F
Gene regulation
CyclE p27
Caspase-8 Apoptosis
ARF CDK2
p21
Cell
FADD mdm2
Bcl-2 proliferation
p53
Bad
Mt Bax
abnormality
FasR sensor Bim
Death factors
(e.g. FasL,TNF)
FIGURE 6.4 Intracellular pathways of liver regeneration. Multiple intracellular signaling pathways are rapidly activated. Progression through the cell
cycle is regulated by cyclins and cyclin-dependent kinases (CDKs), tightly controlled by several mechanisms, including binding by CDK-inhibitory
proteins, such as p21. APC, Activated protein C; ARF, ADP-ribosylation factor; Bcl, B-cell lymphoma 2; CREB, cAMP response element-binding
protein; EGF, epidermal growth factor; EPC, endothelial progenitor cell; ERK, extracellular signal-regulated kinase; FADD, Fas-associated death
domain; FAK, focal adhesion kinase; FasR, Fas receptor; GPCR, G-protein–coupled receptors; GSK, glycogen synthetase kinase; IGF-1, insulin-like
growth factor-1; JAK, Janus activating kinase; JNK, c-Jun–amino-terminal kinase; MAPK, mitogen-activated protein kinase; MEK, MAP/ERK kinase;
MEKK, MAP/ERK kinase kinase; Mt, mitochondrion; NF-κB, nuclear factor kappa B; PI3K, phosphoinositide 3-kinase; PKA, PKC, protein kinases A
and C, respectively; PLC, phospholipase C; RTK, receptor tyrosine kinase; SMO, Smoothened (protein); SOS, Son of Sevenless protein; Src, sarcoma;
STAT, signal transducer and activator of transcription; TCF, T-cell factor; TGF, transforming growth factor; TNF, tumor necrosis factor. (Original from
http://en.wikipedia.org/wiki/File:Signal_transduction_pathways.png.)
production of hepatic ECM. VEGF, angiopoietins 1 and 2, inhibitory effect on proliferating hepatocytes, potentially signal-
TGF-α, fibroblast growth factor (FGF)-1 and FGF-2, and ing the end of rapid regeneration (Kim et al, 1998).
HGF all are likely involved in the angiogenic process. Angio-
statin, an inhibitor of angiogenesis, causes delayed and sup- Maintaining Liver Function During Regeneration
pressed liver regeneration in mice (Drixler et al, 2002; Vogten After volume loss, hepatocytes must adapt rapidly and seek a
et al, 2004). Remodeling of the ECM is associated with the compromise between maintenance of continued differentiated
activation of the urokinase/plasminogen pathway and the function and cellular replication to permit survival. After toxic
membrane-bound MMP pathway. MMP-9 is one of the most injury, resection, or transplantation, the balance is dramatically
active proteins during liver remodeling and regeneration (Kim shifted to the crucial tasks of recovery and regeneration at the
et al, 2000). MMPs not only remodel the ECM but also expense of normal hepatic metabolism. The success of restoring
regulate immune responses (Duarte et al, 2015). Compared lost liver mass, repairing tissue injury, and resolving inflamma-
with fatty controls, MMP-9(−/−) steatotic livers showed signifi- tion determines the ability of the liver to support normal meta-
cantly reduced leukocyte infiltration, proinflammatory cytokine bolic function and determines the ability of the liver to recover
expression, and liver necrosis. Loss of MMP-9 activity preserved (Huang & Rudnick, 2014; Strey et al, 2004) (Fig. 6.5). Several
platelet endothelial cell adhesion molecule-1 expression, a of the expressed immediate early genes encode enzymes and
modulator of vascular integrity at the endothelial cell-cell junc- proteins that are involved in regulating gluconeogenesis, a very
tions in steatotic livers after I/R injury (Kato et al, 2014). important process after PHx to compensate for the lost glyco-
The MMPs in combination with HGF, EGF, and TGF-β1 gen content and to produce sufficient glucose for the whole
act to remodel the ECM, changing the levels of several ECM organism (Haber et al, 1995; Rosa et al, 1992). There is rapid
proteins, such as collagen, fibronectin, laminin, and entactin. increased expression of genes involved in glucose homeostasis
The maturation and thickening of the ECM seems to have an after PHx. Most notably, these include phosphoenolpyruvate
Chapter 6 Liver regeneration: mechanisms and clinical relevance 99
Liver function
Recovery Metabolic
regeneration function
carboxykinase (PEPCK), glucose-6-phosphatase (G6Pase), after PHx require mitochondrial fatty-acid β-oxidation. PPAR-
and insulin-like growth factor binding protein-1 (IGFBP-1), α may be a crucial modulator controlling energy flux important
controlled at the level of transcription by insulin (downregula- for repair of liver damage and regeneration (Anderson et al,
tion), glucagon/cyclic adenosine monophosphate (upregula- 2002).
tion), and glucocorticoids (upregulation) (Diamond et al, 1993; In a microarray analysis of gene expression profiles after
Mohn et al, 1990). Livers lacking IGFBP-1 display abnormal living-donor liver transplantation, we demonstrated that C/
liver regeneration (Leu et al, 2003). Decreased expression of EBPα was downregulated, as well as HNF-4α and PPAR-α (de
genes that oppose gluconeogenesis also occurs rapidly pos- Jonge et al, 2009). Expression of many other liver-specific
thepatectomy. Insulin itself can be a potent growth factor genes, such as IGFBP-1 and G6Pase, are regulated in the basal
mediated through the insulin receptor, and insulin and gluca- state by HNF-1. The transcriptional activity of HNF-1 is
gon have long been established as important “gut-derived” upregulated during liver regeneration by binding of HNF-1 to
growth factors (Starzl et al, 1975). Liver-specific transcription the growth-induced transcription factors STAT3 and AP-1
factors (hepatocyte nuclear factors [HNFs]), have an important (Leu et al, 2001).
role in determining the level of glucose production, fatty-acid New insights into how the liver fulfills the adaptive response
metabolism, and liver-specific secreted proteins. C/EBPα regu- to metabolic needs during regeneration, may come from the
lates expression of genes involved in hepatic glucose and lipid tight regulation of lipid, glucose, and bile acid (BA) metabolism
homeostasis, has antiproliferative proprieties, and is downregu- through the class III NAD1-dependent histone deacetylase
lated during liver regeneration after hepatectomy (Costa et al, SIRT1 (Ruderman et al, 2010). SIRT1 is activated in situations
2003; Mischoulon et al, 1992). of low energy availability and links nutritional status with meta-
During early regeneration, the liver accumulates fat. Neither bolic homeostasis. It regulates adenosine monophosphate
the mechanisms responsible for nor the functional significance activated protein kinase (AMPK). Contrary to SIRT1, mam-
of this transient steatosis has been determined. Suppression of malian target of rapamycin (mTOR) is activated in high-energy
hepatocellular fat accumulation is associated with impaired conditions and controls cell growth and proliferation (Sengupta
hepatocellular proliferation after PHx, indicating that hepato- et al, 2010). mTOR promotes protein synthesis and this axis is
cellular fat accumulation is specifically regulated during, and essential to regulate the cell cycle during liver regeneration after
may be essential for, normal liver regeneration (Shteyer et al, PHx. BA is also essential for the regeneration of the liver after
2004). Some data show that decreasing lipid peroxidation levels PHx (Huang et al, 2006), although, when present in excess,
by vitamin treatment after PHx produces an attenuation of BA can be toxic and promote hepatocyte death. Therefore a
cellular apoptosis and a marked increase in the proliferation fine regulation of BA metabolism comes from the tight regula-
process, suggesting that the modulation of lipid peroxidation tion of lipid, glucose, and BA metabolism through the class
has a role in the liver regeneration process (Ronco et al, 2002). III nicotinamide adenine dinucleotide-1–dependent histone
Hepatocytes in the periportal regions that divide and replicate deacetylase sirtuin 1 (SIRT1) (Ruderman et al, 2010). SIRT1
100 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
is activated in situations of low-energy availability and links the role of C/EBPα, a key regulator of liver proliferation, in the
nutritional status with metabolic homeostasis. It regulates termination of regeneration was demonstrated. Complex forma-
adenosine monophosphate–activated protein kinase. Contrary tion of C/EBPα and the chromatin remodeling protein HDAC1
to SIRT1, mammalian target of rapamycin (mTOR) is activated represses other key regulators of liver proliferation: C/EBPα,
in high-energy conditions and controls cell growth and prolif- p53, FXR, SIRT1, PGC1α (peroxisome proliferator-activated
eration (Sengupta et al, 2010). mTORC1 promotes protein [PPAR]-γ coactivator-1), and telomerase reverse transcriptase
synthesis, and this is essential to preserve liver homeostasis and (TERT). The C/EBPβ-HDAC1 complexes also repress promot-
a proper response to injury. The farnesoid X receptor FXR ers of enzymes of glucose synthesis PEPCK and G6Pase. Proper
(NR1H4) is the master regulator of BA, lipid, and glucose cooperation of C/EBP and chromatin remodeling proteins
metabolism. Recently, the role of SIRT1 as a key regulator of seems essential for the termination of liver regeneration after
the regenerative response of the liver, controlling BA homeo- surgery and for maintenance of liver functions (Jin et al, 2015).
stasis, protein synthesis, and cell proliferation through deacety- Additional work strongly implicates the detection of blood
lation of FXR and histones, and regulation of mTOR was BA levels by nuclear receptors, as a regulator of liver growth
established (Garcia-Rodriguez et al, 2014). (Huang et al, 2006). In addition, Mst1 and Mst2, mammalian
genes comparable to those in the Drosophila Hippo kinase
Termination of Proliferation signaling cascade, which regulates wing mass during develop-
The size of the liver is highly regulated and is controlled by the ment, can also control hepatocyte proliferation (Dong et al,
functional needs of the organism. This observation infers the 2007). Overexpression of YES-associated protein (YAP), the
existence of a master regulator of the liver/body-mass ratio, that mammalian counterpart to Yorki—the last gene in the Dro-
is a “hepatostat.” sophila Hippo kinase cascade—in a transgenic mouse model
From LDLT, we know that differences are present between leads to massive liver hyperplasia, reaching 25% of body weight.
donors and recipients in the percentage reconstitution of the YAP transcriptionally activates cell-cycle proteins such as Ki-67
standard liver volume (LV) (80% vs. 93% at 3 months), prob- and c-Myc and also inhibitors of apoptosis, and its phosphory-
ably caused by the need for functional liver mass to compensate lation by way of activation of the Hippo pathway blocks its
for long-standing liver disease (Olthoff et al, 2015). ability to shuttle to the nucleus (Reddy & Irvine, 2008). It is
The most well-known antiproliferative factors within the therefore possible that the Hippo kinase pathway has a decisive
liver are TGF-β and related family members such as activin role in determining overall liver size (Hong et al, 2014; Plouffe
(Derynck & Zhang, 2003). TGF-β is produced mainly by et al, 2015; Wu et al, 2015; Zheng et al, 2011).
hepatic stellate cells, but in the early phase, it forms inhibitory
complexes with SKI proto-oncogene (SKI) and SKI like proto- LIVER ATROPHY
oncogene (SnoN) (Macías-Silva et al, 2002), rendering hepato-
cytes initially resistant to TGF-β (Koniaris et al, 2003). Later Classically, atrophy is triggered by an obstruction of portal
on, TGF-β acts through a heteromeric receptor complex, which venous blood flow or is the result of chronic obstruction of the
subsequently phosphorylate proteins of the SMAD family bile duct. When atrophy occurs unilaterally, the opposite lobe
(protein homologs of both the Drosophila protein mothers of the liver responds with a hypertrophic response, and the
against decapentaplegic (MAD) and the Caenorhabditis elegans anatomic result is a rotation of the liver around the hilar axis.
protein SMA), particularly SMAD2 and SMAD3 (Lonn et al, The liver frequently is grossly distorted, and anatomic land-
2009). The downregulation of microRNA 23b (miR23b) may marks are markedly changed, most commonly seen accompa-
further contribute to activation of the TGF-β1/SMAD3 signal- nied by a rotation of the portal triad structures (Fig. 6.6). In
ing pathway during the termination stage (Yuan et al, 2011). recent years, surgeons have sometimes used preoperative embo-
Upon activation, Smad2, Smad3 and Smad4 assemble in a lization of the right portal vein to induce hypertrophy when the
common complex, translocate into the nucleus and activate. future liver remnant (FLR) is small.
The Smad2/3-Smad 4 complex translocates into the nucleus
and activates target genes that negatively regulate the cell cycle Mechanisms of Liver Atrophy
(Nakao et al, 1997). Reactive oxygen species (ROS) enhance The death of liver cells in atrophy generally is divided into
synthesis and activation of TGF-β (Koli et al, 2008), which may necrosis and apoptosis. The distinction is important because
account for the reduced regeneration after ischemia and reper- necrosis is a nonregulated traumatic disruption of a cell occur-
fusion. Interacting with the TGF-β/Smad signaling could restore ring when it encounters overwhelming injury, whereas apoptosis
regeneration in a model of SFS liver grafts (Zhong et al, 2010). is an inducible, highly orchestrated cascade of events that is
Similarly, activin A blocks hepatocyte mitogenesis and shows physiologic. Necrotic cells lose membrane integrity, leak lyso-
diminished signaling during liver regeneration when its cellular- somal enzymes, and induce a large inflammatory response.
receptor level is reduced. Its receptor level is restored once liver Apoptosis is energy dependent and allows cells to shrink and
regeneration is terminated (Date et al, 2000). The level of die without inducing inflammation. Apoptotic cells are charac-
activin receptor messenger RNA (mRNA) expression was terized by plasma membrane blebbing, chromosomal conden-
shown to be an important determinant in the magnitude of sation, and nuclear DNA fragmentation (Steller, 1995).
regeneration in portal vein ligation and PHx (Takamura et al,
2005a, 2005b). SOCSs are important negative regulators of Portal Vein–Induced Hepatic Atrophy
cytokine signaling that prevent the tyrosine phosphorylation of The most common clinical scenario of hepatic atrophy is portal
STAT proteins. It has been shown that IL-6 signaling in the liver vein–induced atrophy; occlusion of the portal vein leads to
causes the rapid upregulation of SOCS3, which correlates with ischemia in areas of the liver, and atrophy in this setting is a
the subsequent downregulation of phosphorylated STAT3, result of liver cell death secondary to necrosis and apoptosis
thereby terminating the IL-6 signal (Campbell et al, 2001). Also (Ikeda et al, 1995; Shibayama et al, 1991). Ischemic necrosis
Chapter 6 Liver regeneration: mechanisms and clinical relevance 101
A B
C
FIGURE 6.6 Hepatic atrophy. A, Computed tomography appearance of the liver in a patient with papillary hilar cholangiocarcinoma involving the
left hepatic duct. Note the atrophic left lobe and intrahepatic ductal dilation predominantly on the left. B, Gross appearance of the liver in the same
patient. Inset shows intraluminal view of the common bile duct with tumor extruding from the left hepatic duct (arrow).
of centrilobular areas of the liver predominates in the first 3 impaired apoptosis and less injury and fibrosis compared with
days of cell death. Areas peripheral to the necrotic liver cells wild-type mice (Canbay et al, 2002; Gujral et al, 2004; Miyoshi
predominantly undergo apoptotic cell death, and apoptosis et al, 1999). More recent data, however, suggest a nonischemic
persists long after necrosis subsides. Oxygen levels and mito- model of necrosis/oncosis as the predominant process leading
chondrial function help determine which cells will undergo to cell death after common bile duct ligation, with cell swelling
necrosis or apoptosis (Nishimura et al, 1998). Models of portal and without apoptotic caspase-3 activation (Fickert et al, 2005).
vein ischemia in rats have confirmed a caspase-dependent
apoptosis and have indicated that Kupffer cells are involved in Clinical Causes of Atrophy
generating reactive oxygen substrates and other acute-phase Hilar cholangiocarcinoma is a frequent cause of biliary atrophy,
reactants, culminating in mitochondrial dysfunction and apop- induced by occlusion of a major bile duct. Biliary occlusion,
tosis (Kohli et al, 1999). often accompanied by portal vein compromise leading to
atrophy of the liver, occurs approximately 20% of the time with
Biliary-Induced Hepatic Atrophy this disease and has significant surgical implications. Also
The molecular mechanisms involved in biliary obstruction postcholecystectomy bile duct strictures lead to hepatic atrophy
leading to hepatic atrophy are much more centered on apopto- 10% to 15% of the time (Hadjis & Blumgart, 1987; Pottakkat
sis, with little or no involvement of acute necrosis. Cholestasis et al, 2009). Choledocholithiasis and hepatolithiasis are infre-
results in the accumulation of toxic bile salts, which induce quent causes of atrophy, as are benign tumors, such as papil-
apoptosis through the Fas-mediated pathway. In this case, lomas, cystadenomas, and granular cell tumors (Blumgart &
TNF-α and Fas ligand bind to the Fas death receptors, leading Kelly, 1984). Strictures caused by parasitic biliary infections,
to a cascade of intracellular events, including cytochrome c such as Clonorchis sinensis and Ascaris lumbricoides, also have
release from mitochondria and activation of apoptosis-mediating been known to cause biliary obstruction and associated atrophy
caspases. In Fas-deficient mice, bile duct ligation resulted in of the liver. Occlusion of the hepatic artery alone would not
102 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
induce atrophy, although arterial radioembolization techniques due to high mitochondrial susceptability to oxidative stress
are currently used to increase resectability in the treatment (Lenaz et al, 2000).
of HCCs (Toso et al, 2010). Lobar radioembolization with
yttrium-90 or holmium-166 can cause atrophy of a lobe through Biliary Obstruction
β-emission, causing necrosis. This way “radiohepatectomy” Cholestasis results in the accumulation of toxic bile salts, which
allows growth of the contralateral lobe with a median increase induce apoptosis through the Fas-mediated pathway. In this
of 24% after 3 months (Garlipp et al, 2014; Vouche et al, 2013), pathway, TNF-α and Fas ligand bind to the Fas death recep-
which may enable resection. tors, leading to cytochrome c release from mitochondria and
activation of apoptosis-mediating caspases. In Fas-deficient
Compensatory Regeneration Triggered by Atrophy mice, bile duct ligation resulted in impaired apoptosis and less
In the embolized portion of liver, Kupffer cells release TNF-α, injury and fibrosis compared with wild-type mice (Canbay et al,
inducing hepatocyte swelling and hyperplasia in the contralateral 2002; Gujral et al, 2004; Miyoshi et al, 1999). Other molecular
liver. Additionally, increased portal flow in the nonembolized mechanisms involved in reduces regenerative capacity with
lobe induces proliferation and activates several cytoplasmic biliary obstruction are much suppressed expression of c-Myc
growth-promoting signal transduction pathways involved in (Tracy et al, 1991), C/EBP, and cyclin E (Nakano et al, 2001).
hepatic regeneration, including c-Jun and the MAPK pathways. Production of HGF (Hu et al, 2003), EGF (Bissig et al, 2000),
Kupffer cells in the contralateral liver begin to produce TNF-α and IL-6 (Fujiwara et al, 2001) is also altered. Finally, biliary
as well, stimulated either by increased portal flow or through obstruction also impairs enterohepatic circulation and thus
the direct effect of circulating growth factors (Kim et al, 2001). negatively affects the regenerative capacity. Clinically relevant
Stellate cells in the injured portion of the liver produce HGF is that external biliary drainage for obstructive jaundice mark-
(Parekkadan et al, 2007; Skrtic et al, 1999). mRNA levels of edly suppresses liver regeneration after PHx (Suzuki et al,
HGF in the ischemic portion of liver were noted to be 10 to 1994), whereas internal biliary drainage preserves this capacity
20 times that of normal, with most upregulation occurring in (Saiki et al, 1999). The mechanism was demonstrated in a rat
Kupffer cells (Hamanoue et al, 1992). model in which oral BAs were given before PHx. Liver regen-
eration was significantly increased through activation of the
FACTORS INFLUENCING LIVER REGENERATION FXR signaling pathway (Ding et al, 2015).
regeneration following PHx (Skullman et al, 1990). When Steatohepatitis, or acute inflammation in the setting of fatty
improving nutritional status, enteral feeding should be pre- infiltration, carries an even higher risk and eventually results in
ferred, because rats given enteral nutrition showed much better fibrosis and cirrhosis.
weight gain after 70% hepatectomy than those given isocaloric In transplantation, liver grafts with moderate to severe ste-
nutrition parenterally (Delany et al, 1994). atosis (>30% to ≥60%) have higher rates of primary nonfunc-
Recently, a small trial with supplementation with branched- tion, higher aminotransferases, and poorer graft survival in the
chain amino acids–enriched nutrients showed improved nutri- transplant setting (Verran et al, 2003), possibly as a result of
tional state in LDLT recipients in the early posttransplant increased inflammation and the inability to initiate repair and
period and shortened the posttransplant catabolic phase regeneration mechanisms.
(Yoshida et al, 2012). Supplementation of glutamine, one of Progressive scarring and hepatic fibrosis leads to accumula-
the sources of DNA and protein synthesis, has been shown tion of abnormal collagen secreted into the ECM by stellate
to promote liver regeneration (Ito & Higashiguchi et al, 1999). cells (Kim et al, 1998). Impaired regeneration is thought to
Essential fatty acids, components of the cell membrane be the result of the decreased diffusion of nutrients and
and precursors of several functional mediators, also play an hepatotrophic factors to the hepatocytes, and ultimately the
important role in hepatic regeneration. Interestingly, dextrose architectural liver abnormalities created by scar contracture
supplementation has an inhibitory effect of on liver regenera- form a physical barrier, preventing hepatocytes from proliferat-
tion, associated with increased expression of C/EBP-α, p21, ing (Poynard et al, 1997).
and p27 (Weymann et al, 2009), although this effect was not
found in a previous study (Nishizaki et al, 1996). Pharmacologic Therapy
Many exogenous agents can affect liver regeneration, including
Gender frequently prescribed drugs and neoadjuvant chemotherapy.
Sex steroids are known to induce transient hepatocellular pro- Numerous medications associated with impaired liver regenera-
liferation and to improve fatty-acid metabolism (Repa et al, tion, secondary to the induction of steatosis, are certain antiar-
2000). Estrogen receptors are found on hepatocytes, and serum rhythmic agents, antibiotics, antiviral agents, anticonvulsants,
estradiol is increased substantially after PHx in rodents and steroids, calcium channel blockers, statins, and antiglycemic
humans (Francavilla et al, 1989). Pretreatment of rats with medications. β-Blockers and nonsteroidal antiinflammatory
17β-estradiol induces hepatocyte DNA synthesis in vitro and drugs (NSAIDs) exert a more direct negative influence on liver
accelerates liver regeneration in vivo; administration of tamoxi- regeneration. β-Blockers impair liver regeneration by decreas-
fen, a mixed-estrogen agonist/antagonist, slows regeneration ing portal blood flow to the liver and blocking the trophic
when given soon after PHx (Francavilla et al, 1989). In contrast, effects of epinephrine. NSAIDs directly inhibit cyclooxygenase,
testosterone levels decline in men and in male rats after PHx. part of the C/EBP-β–mediated liver regenerative pathway. Liver
However, there is no clinical evidence that shows significant regeneration after PHx is delayed in rodents treated with either
differences between the sexes in humans after liver resection. β-blockers or NSAIDs (Hong et al, 1997; Rudnick et al, 2001).
Although this effect has not been reflected in increased morbid-
Intrinsic Liver Disease: Steatohepatitis ity or mortality after liver resection in patients taking β-blockers
The regenerative response of the liver can be seriously affected or NSAIDs, the potential harmful effect of any medication on
by preexisting intrinsic liver conditions, such as steatohepatitis, hepatic regeneration must be considered before resection.
fibrosis, and cirrhosis. Steatohepatitis is a condition met more There are an increasing number of patients having liver
frequently in the general population (Adams et al, 2005; Bhala surgery after neoadjuvant or induction chemotherapy. Major
et al, 2011) and poses challenges in the management of patients drawbacks of hepatotoxic chemotherapy are the sinusoidal
undergoing liver resection. Hepatic steatosis affects regenera- obstruction syndrome (SOS), associated with oxaliplatin
tion on several molecular levels. Lipid accumulation has been (Eloxatin, Sanofi Aventis, Bridgewater, NJ) (Rubbia-Brandt
associated with hepatocyte mitochondrial damage caused by et al, 2004) and the chemotherapy-associated steatohepatitis
free radical injury. Steatotic livers in rats show delayed mitosis (CASH) (Vauthey et al, 2006), which is associated with irino-
and increased mortality after PHx, which may be due to abnor- tecan (Campto, Pfizer, New York). This chemotherapy-
mal TNF and IL-6 signaling (Selzner et al, 2000). The coordi- associated steatohepatitis increases postoperative mortality and
nated induction of JNKs and ERKs is disrupted after PHx in specifically deaths from postoperative liver failure (Fernandez
fatty livers of ob/ob mice (a model for steatohepatitis), with et al, 2005). Sinusoidal obstruction also impairs liver regenera-
enhanced AKT and inhibition of PEPCK (Yang et al, 2001). tion after extensive liver resections and increases postoperative
Cyclin D1 induction is abolished along with STAT3 and morbidity but may be prevented by concomitant administration
reduced ATP levels, which may arrest cell-cycle progression. of bevacizumab (Avastin, Hoffmann-LaRoche, Indianapolis,
Hepatocyte mitochondrial damage associated with lipid accu- IN) (Rubbia-Brandt et al, 2011; Vigano et al, 2013). Bevaci-
mulation is caused by free radical injury from fatty-acid oxida- zumab, a monoclonal antibody targeting VEGF, is given in
tion. Abnormalities in induction of cytochrome P-450 may be combination with cytotoxic chemotherapy to improve resect-
one mechanism in the pathophysiology of these findings in fatty ability (Gruenberger et al, 2015) and survival in patients with
livers and may contribute to poor regeneration (Farrell, 1999; metastatic colorectal cancer (Hurwitz et al, 2004). Well-
Kurumiya et al, 2000; Neuschwander-Tetri et al, 2003). The designed preclinical studies have demonstrated that inhibition
presence of underlying steatosis has a considerable impact on of angiogenesis can inhibit wound healing (Scappaticci et al,
operative morbidity and mortality after major hepatic resection 2005). Bevacizumab does not appear to adversely affect the
(Behrns et al, 1998; de Meijer et al, 2010; Vetelainen et al, results of PHx in humans (D’Angelica et al, 2007). Animal
2007), with a significantly higher rate of complications if studies have demonstrated that liver regeneration depends on
marked steatosis (≥30%) is present (Kooby et al, 2003). VEGF and angiogenesis (Drixler et al, 2002). In a murine
104 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
model, anti–VEGF receptor therapy slightly impaired liver and activation of cytokines, transcription factors, and immedi-
regeneration and cell proliferation after PHx compared with ate early genes and a greater magnitude of hepatocellular rep-
control individuals (Van Buren et al, 2008). Clinically, no dif- lication (Debonera et al, 2001). The liver can tolerate ischemic
ferences in postoperative liver insufficiency were seen if stopped injury only to a certain “point of no return;” however, after
at least 6 to 8 weeks before hepatic resection (Reddy SK et al, which the damage is too extensive, and the liver or allograft is
2008; Zorzi et al, 2008). unable to maintain functional homeostasis and regenerative
Regarding the effect of sorafenib (Nexavar, Bayer), a multi- capabilities, which results in liver dysfunction and graft failure
kinase inhibitor used for treatment of HCC, conflicting results (Debonera et al, 2002).
have been reported in experimental research. Sorafenib did In addition, recent studies have demonstrated that lack of
not impact on liver regeneration when ceased before surgery; blood flow occurring during cold preservation for transplanta-
however, administration after hepatectomy affected late liver tion markedly deteriorates the liver sinusoidal endothelial cells
regeneration in a mouse study, and reduced phospho-ERK (LSEC) protective phenotype by downregulating the expres-
levels and wound-healing complications were observed (Hora sion of the transcription factor Kruppel-like factor 2 (KLF2),
et al, 2011). In another rat experiment, however, no significant which orchestrates the transcription of a variety of protective
change in liver regeneration related to sorafenib exposure was genes, including the endothelial synthase of NO (eNOS), the
found (Shi et al, 2012). antithrombotic molecule thrombomodulin, or the antioxidant
transcription factor NRF2 ( Gracia-Sancho et al, 2010; Peralta
Liver Transplantation et al, 2013; Russo et al, 2012).
Regeneration also is crucial in liver transplantation. In cadaveric
transplantation, hepatocyte loss occurs in the form of I/R injury Minimal Liver Mass
owing to the necessary preservation period from procurement The amount of liver mass transplanted has been shown to be
to implantation and damage that may have occurred in the an important factor after transplantation. Early experimental
donor. Regenerative mechanisms are actively engaged after studies addressing regeneration after transplantation showed
transplantation, depending on the length and degree of preser- that a SFS graft adapts to its environment and achieves a size
vation injury (Debonera et al, 2001; Olthoff, 2002). Similarly, equal to the original native liver (Kam et al, 1987). It became
hepatocytes lost to the alloimmune response require replace- apparent that the graft size-to-recipient ratio was crucial in that
ment. Regeneration also is necessary in the setting of trans- grafts that were too small had decreased survival (Francavilla
planting a SFS graft into a larger recipient. This is the case in et al, 1994). These findings correlated with early clinical experi-
the setting of adult-to-adult living-donor liver transplantation ence in living-donor transplantation in that some SFS segmental
(AALDLT) (Olthoff, 2003). Ischemic injury is minimized in grafts developed a “SFS syndrome” that was associated with
AALDLT, in that the preservation period is short; however, this significant functional impairment, shown by prolonged cho-
technique supplies a graft that is by definition too small, requir- lestasis and histologic changes consistent with ischemic injury
ing vigorous immediate hepatocyte proliferation. By transplant- and associated with poor outcome. Liver grafts with a graft
ing only 50% to 60% of what is the expected LV in adults, volume of less than 40% of calculated standard LV were associ-
recipients (and donors) must rely on the rapid regeneration of ated with poor graft survival and prolonged hyperbilirubinemia
a partial liver in addition to maintaining the basic metabolic (Emond et al, 1996; Kiuchi et al, 1999; Lo et al, 1999; Zhong
functions required of the liver. The National Institutes of Health et al, 2006). The development of segmental graft dysfunction
(NIH)-sponsored study in adult-to-adult living-donor trans- in the A2ALL study was also associated with worse patient
plantation (A2ALL) has investigated the role of numerous outcome (Olthoff et al, 2015). Animal models of partial liver
donor and recipient factors in regeneration. The size of the graft transplantation have studied the interplay between the
remnant liver or graft had the greatest impact on rate and regenerative response and ischemic injury in the setting of 50%
quantity of regeneration (Olthoff et al, 2015). and 30% size grafts. The partial grafts showed a robust regen-
In a pilot study investigating molecular mechanisms associ- erative response if the ischemic injury was minimal. It became
ated with human liver regeneration, we noted differences in apparent, however, that when these partial grafts were subjected
hepatic gene expression between donors with complete regen- to ischemic injury of moderate to prolonged time periods, there
eration compared with those with less successful regeneration— was a significant effect on survival, with extensive hepatic
genes mainly related to cell proliferation, inflammation, necrosis, the inability to initiate or maintain the regenerative
metabolism (aminoacyl transfer RNA synthesis), and stress response, and decreased survival. These findings show the
pathways (acute-phase response) were among the most signifi- diminished tolerance of SFS grafts for additional injury beyond
cantly regulated pathways. In contrast, the poor regeneration transplantation itself ( Debonera et al, 2004; Selzner et al,
group demonstrated very little change in expression before and 2002).
after resection. The lack of significant change in genomic profile Although ischemic injury in AALDLT is minimized, the
in the poorly regenerating livers suggests a possible inhibition amount of critical liver mass required for transplantation in
or delay in initiation of recovery and regeneration molecular living donation remains in question. Most centers have defined
pathways (Hashmi et al, 2015). liver mass as graft-to-recipient body-weight ratio or as a per-
centage of the standard LV. No uniform method of measuring
Ischemic Injury or reporting graft volume in relation to the recipient has been
Warm and cold ischemic injury is an unavoidable component established. Clinical experience with living-donor and split
of transplantation. After prolonged cold ischemia of whole-liver grafts has led to an accepted lower limit of 0.8% graft-to-
grafts, there is initiation of the cell-cycle pathways with upregu- recipient body-weight ratio, or 40% of the standard LV. Donor
lation of markers of liver regeneration as described earlier. and recipient characteristics, and graft factors, significantly
When ischemic injury is significant, there is a greater expression influence these minimal accepted standard volumes. Patients
Chapter 6 Liver regeneration: mechanisms and clinical relevance 105
with fulminant hepatic failure, severe portal hypertension, and 2004; Tralhao et al, 2002), have been reported to inhibit
significant disease severity, as manifested by a high Model for hepatic regeneration. The precise mechanism responsible for
End-Stage Liver Disease (MELD) score, and patients with viral infection–related suppression is unclear, although it may
significant metabolic stress may require more LV than stable be partly mediated by the inhibition of cell-cycle–dependent
patients transplanted under elective conditions (Marcos et al, molecules. Because most transplant patients in the United
2000). Although AALDLT in acutely ill patients with fulminant States have hepatitis C, it is important to know whether this
failure is often performed successfully, usually in parts of the vigorous regenerative response in the transplanted graft has a
world with no access to deceased donor transplantation, many significant effect on the kinetics of viral replication in hepatitic
centers in the West are not performing them because of the C virus (HCV)–positive individuals. Investigators have noted
uncertainty of knowing if a partial graft has enough volume to that HCV RNA replication is enhanced in proliferating cells,
support the recovery of such a recipient (Campsen et al, 2008; suggesting that viral replication is regulated by cell-cycle–
Olthoff et al, 2011). The accumulation of additional stressful dependent factors (Erhardt et al, 2002). Clinically, progressive
stimuli, such as sepsis or renal failure, may push a relatively liver disease has been reported to be associated with increased
small graft into failure. hepatocyte proliferation (Poynard et al, 1997). Alternatively,
HCV core proteins have been shown to have significant inter-
Effect of Immunosuppression action with cellular promoters and regulators of cell growth,
Within the graft environment, the host immune response needs which may affect liver regeneration (Blindenbacher et al, 2003;
to be inhibited to avoid acute allograft rejection, and inhibition Hayashi et al, 2000; Lee et al, 2002; Ray et al, 1998; Shrivas-
of this response may interfere with the recovery of liver grafts tava et al, 1998). Early single-center studies suggested
requiring active regeneration of hepatocytes. Glucocorticoids, that recipients of living-donor liver transplants may have an
routinely used in immunosuppression protocols, have been earlier and more severe recurrence of HCV compared with
shown to inhibit cell-cycle progression markedly in PHx recipients of whole deceased-donor grafts; however, this was
models and in transplant models with ischemic injury not validated in any of the prospective controlled studies
(Debonera et al, 2003; Nagy et al, 1998; Tamasi et al, 2001). (Berenguer, 2006; Ghobrial et al, 2002; Shiffman et al, 2004;
Cyclosporine and tacrolimus may have differential effects on Terrault et al, 2007).
regeneration in a dose-dependent fashion (Francavilla et al, Concomitant bacterial infections also alter liver regenera-
1991). Sirolimus, with its antiproliferative action, interferes tion. Earlier reports showed enhanced liver regeneration in rats
with hepatocyte replication (Francavilla et al, 1992; Palmes after inflammation prior to hepatic resection, due to stimula-
et al, 2008). The rapid hepatocyte replication and smaller liver tion of LPS; upregulation of proinflammatory cytokines, such
mass also may interfere with metabolism and pharmacokinet- as IL-6 and TNF-α; and HGF ( Sekine et al, 2004; Weiss et al,
ics of certain drugs. Preliminary studies have shown that 2001), all of which are chief mediators of hepatic regeneration.
AALDLT recipients require lower doses of tacrolimus in the A recent study showed—more in line with clinical observations—
early postoperative period than patients receiving whole grafts a significantly delayed regeneration kinetic in a rat model
(Trotter et al, 2002). The ability to measure functional recov- of combined liver resection and intraperitoneal sepsis, with
ery of these recipients would help in the assessment of hepa- hyperinflammation and increased liberation of proinflamma-
tocellular function and metabolic demands in these regenerating tory cytokines (Seehofer et al, 2007). The relation between
partial liver grafts. inflammation and poor liver regeneration was confirmed in
patients with early allograft dysfunction (EAD) occurring in
Donor Age the first week post liver transplantation. EAD was associated
As with liver regeneration in the nontransplant setting; old with an inflammatory response in the perioperative period and
grafts do not regenerate as quickly as young livers. A clinical a specific pattern of 25 cytokines, chemokines, and immuno-
study of living donors showed a greater graft/standard LV receptors. Patients with EAD showed higher MCP-1 (mono-
in the young donor livers posttransplant compared with middle- cyte chemoattractant protein-1 [CCL2]), IL-8 (CXCL8), and
aged and old donor grafts. The old livers also had a higher RANTES ((regulated on activation, normal T-cell expressed
prothrombin time in the early period postoperatively (Ikegami and secreted; CCL5) chemokine levels in the early postopera-
et al, 2000). Statistics from the UNOS database show that the tive period, suggesting upregulation of the NF-κB pathway,
graft survival of older living-donor grafts is inferior to younger in addition to higher levels of chemokines and cytokines
grafts (Abt et al, 2004) and increasing donor and recipient age associated with T-cell immunity, including MIG (monokine
affected both short- and long-term survival in the NIH A2ALL induced by interferon-γ; CXCL9), IP-10 (interferon-γ–induc-
study (Olthoff et al, 2005, 2015). In the deceased-donor trans- ible protein-10; CXCL10) and IL-2R (interleukin-2 receptor)
plant setting, grafts older than 55 to 60 years have poorer (Friedman et al, 2012).
long-term survival combined with longer cold ischemic times
(Cassuto et al, 2008). Age may affect the regeneration and Other Factors
recovery of the living donor and the recipient. Many groups Several other factors may influence the regenerative response
limit the upper age limit of the donor in the 50- to 60-year after transplantation. Increased portal venous flow has been
range, although no definite age has been specified. implicated in more rapid regeneration (Jiang et al, 2009). In
addition to the reduced cell mass of the graft itself, portal
Inflammation: Viral Hepatitis and Bacterial Infections blood flow dynamics are altered, and the graft is subjected to
Very little is known about how rapid hepatocellular prolifera- increased portal blood flow and pressure. Increased portal
tion affects other processes. Inflammation in general, and some flow to about two times baseline level is associated with
viral infections, such as hepatitis B and C and murine cyto- increased recovery (Eguchi et al, 2003); however, significant
megalovirus specifically (Marshall et al, 2005; Sun & Gao, portal hyperperfusion is, on the other hand, regarded as
106 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
central to the problem in SFS grafts, leading to decreased to patients with cirrhosis and are only rough estimates of
regeneration and increased mortality (Hessheimer et al, 2011; functional reserve. Bilirubin, albumin, international normal-
Tracy et al, 1991). Larger grafts and younger donors have ized ratio, and platelet count become abnormal only in
been recommended in patients with severe portal hyperten- advanced cirrhosis. Magnetic resonance imaging or computed
sion, as well as modulation of portal inflow. Poor hepatic tomography (CT) can measure residual LV accurately, but
venous drainage has been shown to inhibit regeneration quantitative functional testing is not as precise. Traditional
(Scatton et al, 2008), and segments with poor venous drain- techniques to measure the LV to be resected before hepatec-
age become atrophied with time. tomy can lead to inaccurate estimates of functional residual
As in liver resection, female gender may have a positive effect liver (FRL) volumes because of the presence of dilated bile
on regeneration of partial grafts in murine models (Yokoyama ducts, multiple tumors, undetected lesions, compromised LV
et al, 2007). Estrogen may be responsible for the better toler- due to cholestasis or previous chemotherapy, cholangitis, vas-
ance to various stresses due to a reduced inflammatory response cular obstruction, steatosis or cirrhosis, or segmental atrophy
and a reduced oxygen radical production, leading to improved and/or hypertrophy from tumor growth (Azoulay et al, 2000;
hepatic regeneration. However, also in transplantation, there is Kubota et al, 1997). Accurate preoperative assessment by CT
no clinical evidence that supports the results of these experi- volumetry is necessary as significant interpatient variation
mental studies. exists in hepatic volumes. In living-donor liver transplantation,
total liver volume (TLV) and FRL can be used to predict
EXPERIMENTAL STRATEGIES TO PROMOTE postresection function because the donor liver is normal.
LIVER REGENERATION However, the TLV of the recipient’s diseased liver is not a
useful index of function. Values calculated from graft weight-
Although there has yet to be developed any reliable interven- to-recipient body weight ratio (GRBWR), or standardized LV
tion to improve liver regeneration in the clinical realm, based on recipient BSA are used to predict minimum adequate
numerous approaches have been successful in the experimen- graft volume (Higashiyama et al, 1993; Vauthey et al, 2000).
tal setting. After major hepatectomy or in the situation of a In segmental graft liver transplantation, a GRBWR greater
SFS liver graft in liver transplantation, usually a robust than 0.8% or a graft-to-weight ratio (graft weight divided by
priming reaction by highly elevated levels of IL-6 and TNF-α standard liver weight of recipient) greater than 40% is recom-
is present, but induction of cell-cycle progression fails (Debo- mended to achieve graft and patient survival of greater than
nera et al, 2004). In an animal model, this problem could be 90% (Lo et al, 1999). In comparison, extended resection of
overcome by a single injection of HB-EGF (Mitchell et al, 80% of functional parenchyma can be performed in the
2005). Another strategy that may be useful in a SFS situation absence of chronic liver disease for hepatobiliary malignancies
is blockage of the receptor for advanced glycation end prod- (Abdalla et al, 2002). Recommended minimal functional
ucts (RAGE). Blockage of RAGE greatly improved survival remnant LV following extended hepatectomy is greater than
after an 85% hepatectomy in a rat model by increasing TNF 25% in a normal liver and greater than 40% in an “injured”
and IL-6 production and enhanced expression of the antiin- liver, with moderate to severe steatosis, cholestasis, fibrosis,
flammatory cytokine IL-10 (Cataldegirmen et al, 2005). cirrhosis, or following chemotherapy (Shoup et al, 2003).
Recently, the role of TGF-β as the most potent growth inhibi- Quantitative liver function tests measure the liver’s ability to
tory polypeptide currently known was assessed in a model of metabolize or extract test compounds and can identify patients
SFS liver transplantation. After SFS liver transplantation, a with impaired function at earlier stages of disease but have
sharp rise in TGF-β1 was found, forming a heteromeric limited application in predicting a liver’s ability to regenerate
receptor complex. Phosphorylation of this complex activates after major resection. Indocyanine green clearance (ICG) is
proteins of the Smad family, particularly Smad2 and Smad3 regarded as an accurate assessment of functional reserve and
(Lonn et al, 2009). Activated Smad2 and Smad3 form a can help predict mortality (Lau et al, 1997), but more is being
complex with Smad4, move into the nucleus and activate learned about measuring hepatic function in diseased livers
target genes expressing regulatory proteins and exerting its using quantitative functional testing, such as methionine
inhibitory effect on hepatocyte proliferation. Smad7, an inhibi- breath tests, cholate clearance, liver single-photon emission
tory Smad, associates stably with the TGF-β receptor complex CT scans, and liver scintigraphy and phosphorus-31 magnetic
and was shown to inhibit the TGF-β–dependent cell-cycle resonance spectroscopy (Corbin et al, 2002). When compared
arrest (Zhong et al, 2010). Therefore anti–TGF-β therapy with ICG and CT volumetric data, hepatobiliary scintigraphy
holds promise as a new strategy to improve regeneration of is a reproducible accurate tool to assess functional liver uptake
SFS grafts in clinical practice. and excretion, preoperative liver function reserve, and remnant
liver function, and it allows monitoring of postoperative liver
CLINICAL IMPLICATIONS function regeneration (Dinant et al, 2007). Assessment of
future remnant volume distinguishes those who will most
When to Stimulate Liver Regeneration Preoperatively likely benefit from preoperative liver enhancement techniques
The assessment of hepatic function before resection is diffi- PVE or hepatic artery embolization.
cult, but we do know that the risk for perioperative complica- For living donors, a remnant of at least 30% is recom-
tions increases when the remnant LV is too small, particularly mended to maintain the highest level of donor safety. The
in diseased livers (Yigitler et al, 2003). Hepatic function A2ALL study investigated quantitative liver function in detail
seems to recover quickly after resection but is difficult to in a series of living donors and found significant alterations in
measure. Conventional clinical blood tests and liver biopsy are function in the early days after donation and some subsequent
inadequate measures of hepatic function. The Child-Pugh clinical findings of elevated portal pressure, such as low platelets
classification classification and MELD score apply primarily and higher spleen size (Emond et al, 2015; Everson et al, 2013;
Chapter 6 Liver regeneration: mechanisms and clinical relevance 107
Trotter et al, 2011). If this will affect donors long term is still (Selzner et al, 1999). The first clinical attempt to minimize
unknown. ischemic injury during liver resection was performed by inter-
rupting long ischemic intervals with multiple short periods of
The Use of Portal Vein Embolization reperfusion (Makuuchi et al, 1987). The protective effect of
to Promote Regeneration IPC involves many different mechanisms, including inhibition
The selective embolization techniques increase tolerance to of apoptosis and preservation of cellular ATP content in patients
major hepatic resection by reducing the LV requiring resection undergoing major liver resection. (Clavien et al, 2003; Rudiger
and inducing hypertrophy of the FLR to approximate target et al, 2002). A recent cDNA microarray study in humans
limits in patients with large tumors or abnormal liver function. demonstrated that IPC triggers the overexpression of IL-1Ra,
Criteria for selection of patients for PVE before major hepatec- iNOS, and Bcl-2, which counteracts the ischemia-induced
tomy are FLR size; factors compromising liver function, includ- proinflammatory and proapoptotic activation (Barrier et al,
ing previous chemotherapy, hepatitis, and cirrhosis; 2005). IPC has also been described as promoting liver regen-
and the planned complexity of the procedure (Abdalla et al, eration via the upregulation of cytokines such as TNF-α and
2001; Yigitler et al, 2003). It is recommended when predicted IL-6, various heat-shock proteins, and the downregulation of
FLR is less than 20% to 25% in a normal liver and less than TGF-β (Gomez et al, 2007). Ischemic preconditioning by 10
40% in a liver with compromised function (Hemming et al, minutes of portal triad inflow occlusion and 10 minutes of
2003). Stimulation by PVE increases circulating IL-6 and reperfusion was shown to be effective both in liver resection,
TNF-α (Feingold et al, 1988; Koga & Ogasawara, 1991), with particularly in patients with mild to moderate steatosis (Clavien
activation of the mitogenic cascade, similar to PHx. In fact, et al, 2003), and in liver transplantation (Franchello et al, 2009;
marginal contralateral regeneration less than 5% after PVE is Jassem et al, 2009). There was no difference in protective
a strong predictor of liver failure after subsequent liver resection potential between intermittent clamping (15 minutes ischemia
(Ribero et al, 2007). A significant increase in DNA synthesis and 5 minutes reperfusion) and ischemic precondition with
and mRNA expression of HGF has been observed in the subsequent inflow occlusion for a maximum of 75 minutes,
nonligated lobe (Uemura et al, 2000), whereas HGF expression except for patients older than 65 years, who benefited more
is only slightly elevated, and negative regulators of hepatocyte from intermittent clamping to attenuate liver injury. Pharma-
proliferation, such as TGF-β and IL-1β, are strongly expressed cologic induction of heat-shock proteins could play a beneficial
in the shrinking ligated lobe. It is important to keep in mind role in the recovery of liver function after hepatectomy, but
that these factors also may promote tumor outgrowth in the clinical trials have to be awaited.
FLR, and continuation of chemotherapy during PVE for malig-
nant conditions should be considered (Covey et al, 2008;
Regenerative Potential of the Liver
Pamecha et al, 2009). After Chemotherapy
As discussed before, an increasing number of patients with
Associating Liver Partition With Portal Vein Ligation tumors undergo extensive chemotherapy with multiple drugs
for Staged Hepatectomy (ALPPS) before surgery. The complication rate and mortality after major
In 2012, a radical new surgical procedure was introduced to liver resection is increased in those patients, compared with
stimulate liver regeneration in patients with a small future patients not receiving these drugs (Fernandez et al, 2005;
remnant liver (Schnitzbauer et al, 2012). In this two-step Vauthey et al, 2006). The deleterious effect of chemotherapy
approach, the liver parenchyma is transected between segments on regeneration seems to increase with the total number of
II/III and IV, with concomitant ligation of the right portal vein. cycles given and shows a sharp rise after 5 courses (Karoui
One week to 10 days later, impressive hypertrophy of the left et al, 2006). Therefore we advocate no more than six cycles of
lateral segments has occurred with a median volume increase FOLFOX/FOLFIRI (5-FU, leukovorin, oxaliplatin/irinotecan)–
of 74% (range, 21% to 192%) (Schlegel et al, 2014), and in a containing chemotherapy before liver resection, with a 3-week
second stage, an extended right hemihepatectomy can be per- interval in between. The anti-VEGF monoclonal bevacizumab
formed. The procedure was initially hampered by high mortality has a long half-life and theoretically should be stopped 6 to 8
(11% up to 19%) and high morbidity (as high as 40%) (de weeks before surgery, necessitating close collaboration with the
Santibanes & Clavien, 2012; Schadde et al, 2015), but with medical oncologist in the timing of surgery. Results from PVE
increasing experience and better patient selection, better results before major liver resection under continuous bevacizumab,
are gained without perioperative mortality (Hernandez- however, showed no deterioration in increase in FLR volume
Alejandro et al, 2014). 4 weeks after PVE (Zorzi et al, 2008). Recently, significantly
Although ALPPS seems a promising technique to boost impaired hypertrophy was reported in the same situation (Aus-
regeneration in selected patients, many recommend consider- silhou et al, 2009), but this may also be attributed to extensive
ation of alternative approaches, such as adequate portal and concomitant chemotherapy (Vauthey & Zorzi, 2009). The
hepatic venous embolizations, before an all-operative approach optimal window between the completion of bevacizumab and
is attempted (Vauthey & Mise, 2014). surgery therefore remains uncertain (Clavien et al, 2007).
Ischemic Preconditioning (IPC)
NEW HORIZONS AND FUTURE PERSPECTIVES
to Stimulate Regeneration
Liver resection, transplantation, and trauma can result in pro- Therapeutic Use of Stem Cells
longed deprivation of tissue oxygen, converting cellular metabo- In addition to hepatocyte proliferation and hepatic progenitor
lism to anaerobic pathways. Reperfusion and, consequently, the cells in liver regeneration, bone marrow (BM)-derived cells
restoration of oxygen delivery lead to liver injury. This phenom- have the ability to engraft as hepatocytes (Alison et al, 2009;
enon is known as I/R injury, which impairs liver regeneration Duncan et al, 2009; Friedman & Krause, 2009). Adult BM
108 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
includes two well-defined populations of stem cells: hematopoi- In the context of disease, infusion of (BM) MSC has shown
etic stem cells (HSC), which give rise to all mature lineages of some beneficial effects in patients with liver failure (Peng et al,
blood and mesenchymal stem cells (MSC), which can differen- 2011). In chronic liver failure, some Phase I trials involving the
tiate into bone, cartilage, muscle, and fat. injection of autologous BM cells to cirrhotic patients have
Evidence for BM-to-hepatocyte transition has been demon- reported modest improvements in clinical scores (reviewed in
strated by analyzing liver samples after male-to-female BM Houlihan & Newsome, 2008; Lin et al, 2008). However, the
transplantation in rodents and humans (Alison et al, 2000; BM may also harbor cells with fibrogenic potential, which
Lagasse et al, 2000; Oertel & Shafritz, 2008; Theise et al, contribute significantly to end-stage liver fibrosis (Forbes et al,
2000). However, the extent to which this occurs and the mecha- 2004; Russo et al, 2006). Therefore MSC therapy is sometimes
nisms are still under debate (Fausto, 2004; Oertel et al, 2008). referred to as a two-edged sword, and concerns were raised
Estimates of repopulation by hematopoietic stem cells vary about MSCs promoting liver cirrhosis by differentiation into
from 0.01% to as high as 40% but are often overestimated (Hall myofibroblasts, which are involved in the fibrotic response (di
et al, 2012). Bonzo et al, 2008). The latest publications in this field indicate
In the discussion about the mechanism whereby the hema- that the use of MSCs is safe and has a beneficial effect on liver
topoietic stem cells acquire a hepatocyte phenotype, both fibrosis (Chang et al, 2009; Li et al, 2012; Pan et al, 2014;
fusion of stem cells and hepatocytes (Vassilopoulos et al, Roderfeld et al, 2010; Zhao et al, 2009). Thus MSC-mediated
2003; Wang et al, 2003) and transdifferentiation of stem cells liver therapy is a promising field, which significantly improves
into hepatocytes have been proven (Harris et al, 2004; Jang liver function and increases animal survival in experimental
et al, 2004). The highest levels of BM-derived hepatocytes liver injury models. Its role in liver regeneration after surgery
were found in humans with severe liver disease, suggesting remains to be determined.
that tissue damage may promote engraftment as hepatocytes.
The major fraction of mobilized BM stem cells expresses the Decellularized Hepatic Matrix and Hepatic
chemokine receptor CXCR4. At the same time, the mRNA Tissue Engineering
level of its ligand (SDF-1) is increased in the damaged liver
tissue. These results provide a clue that the CXCR4/SDF-1 Due to the shortage of organs for transplant, research on
interaction may be important for the mobilization of progeni- alternate modalities, such as hepatic tissue engineering, has
tor stem cells from BM to the damaged liver (Khurana & gained momentum. The applications of such engineered organs
Mukhopadhyay, 2007). Clinically, the release of adult stem could not just be seen in the setting of transplantation but also
cells from BM was demonstrated after partial liver resection as support of failing liver function after large resections.
for benign and malignant conditions (De Silvestro et al, 2004; An innovative advance in this field has been the realization
Gehling et al, 2005), and BM-derived stem cells increased the of an important role of ECM in maintenance of differentiated
regeneration of contralateral liver after clinical PVE 2.5 fold hepatocyte phenotype. Recently, strategies were developed to
(am Esch et al, 2005). derive intact ECM from a liver by using a decellularization
Additional studies report that MSCs also promote liver process (Fig. 6.7).
repair in cases of liver damage (Duncan et al, 2009). MSCs, This strategy is based upon removal of cells from an organ,
isolated from human umbilical cords (Yan et al, 2009), adipose leaving a complex mixture of structural and functional proteins
tissue (Banas et al, 2008), bone marrow (Kuo et al, 2008), or that constitute the ECM (Caralt et al, 2014), which is then
rat bone marrow (Abdel Aziz et al, 2007) improved liver func-
tion of rodents undergoing acute liver damage (e.g., CCl4
injections).
The therapeutic effects of MSCs or MSC-derived hepato-
cytes in liver injury can be explained by three primary mecha-
nisms. First, MSCs generate cells that function as normal
hepatocytes, after fusing with metabolically defective hepato-
cytes (Kallis et al, 2007; Lagasse et al, 2000; Wang et al, 2003).
The second mechanism is soluble factors secreted by MSCs in
response to acute damage. Infusion of human MSC-conditioned
medium into rats treated with D-galactosamine (i.e., acute liver
damage) improved liver function after 24 hours (Parekkadan
et al, 2007; van Poll et al, 2008), with a 90% decrease in
apoptosis and a threefold increase in the number of proliferat-
ing hepatocytes. The same was shown after 70% hepatectomy,
with upregulated hepatic gene expression of cytokines and
growth factors relevant for cell proliferation, angiogenesis, and
antiinflammatory responses (Fouraschen et al, 2012).
Finally, the paracrine effects of MSCs may be exerted
by sharing of shed microvesicles (MVs) (Herrera et al, 2010).
Intercellular exchange of protein and RNA-containing mic- FIGURE 6.7 Decellularized liver scaffold. A pig liver was treated with
roparticles is an increasingly important mode of cell-cell 4% Triton X-100 and 0.1% ammonia for approximately 16 hours at a
communication, and MSCs may redirect the behavior of dif- low flow rate of 60 mL/min. Vascular structures such as the vena cava
ferentiated hepatic cells by horizontal transfer of mRNA shuttled retain their strength, whereas the liver extracellular matrix is totally dis-
by MVs (Deregibus et al, 2007; Ratajczak et al, 2006). posed of all cell types.
Chapter 6 Liver regeneration: mechanisms and clinical relevance 109
reseeded with an appropriate population of cells (Sabetkish significant reduction of hepatic steatosis, which was associated
et al, 2014; Zhou et al, 2014) and connected to the bloodstream with reduced cholesterol synthesis rates and stimulation of
and biliary system. Using the whole-organ acellular matrix as hepatic fatty-acid oxidation. The clinical relevance of miRNAs
a three-dimensional scaffold for seeding hepatocyte-like cells, a was shown in differences in spontaneous recovery from acute
fully functional transplantable bioengineered liver graft may liver failure. Patients with spontaneous recovery from acute
become a reality. liver failure showed significantly higher serum levels of miR-122
One of the major remaining obstacles toward clinical appli- and liver tissue levels compared with nonrecovered patients,
cation is now to choose a cell source for liver repopulation. So with strong downregulation of miRNA target genes that impair
far, adult primary hepatocytes have been the primary choice, liver regeneration, including heme oxygenase-1; programmed
but scarcity of high-quality human hepatocytes limits tissue cell death 4; and the CDK inhibitors p21, p27, and p57 (John
engineering applications. et al, 2014). Besides upregulation of miR-122 and miR-21 after
With the advent of technologies enabling reprogramming of partial liver resection, other miRs are downregulated: miR-22a,
adult somatic cells to a pluripotent state (induced pluripotent miR-26a, miR-30b, miR378, Let-7f, and Let-7g. Inhibition of
stem cell, iPS), it may now become possible to generate the miR33 improves liver regeneration after PHx in mice, indicat-
large numbers of inducible human hepatocytes (iHeps), needed ing miRNAs as critical regulators of hepatocyte proliferation
to recellularize a liver bioscaffold (Berger et al, 2015; Hay et al, during liver regeneration (Bandiera et al, 2015; Chen et al,
2008a, 2008b; Huang et al, 2011; Sekiya & Suzuki, 2011; 2011; Cirera-Salinas et al, 2012; Song et al, 2010). Also in liver
Sullivan et al, 2009; Yu et al, 2013). transplantation, distinct patterns of successful and failed regen-
There is, however, concern about the plasticity of these cells eration could be discerned, with inhibition of miRNAs 150,
to form bile ducts, a main hurdle to usefulness in clinically 663, and 503 being associated with successful regeneration
transplantable liver matrix engineering. A solution to this (Salehi et al, 2013).
problem may come from recently discovered bipotential liver In a murine model of hepatectomy in increasing age,
organoids (Huch et al, 2015). These cells are positive for Lgr5, upregulated miRNAs may contribute to the aging-related
the receptor for the Wnt agonist R-spondin. They are able decline in oxidative defense by targeting various classes of
to differentiate into both hepatocytes and cholangiocytes, glutathione-S-transferases (Maes et al, 2008). Antagonizing
as precursors of bile ducts, depending on culture media these miRNAs may reverse the decline of regeneration and
composition. oxidative defense mechanisms in aging liver.
The intricate spatiotemporal environment of a decellularized
liver matrix, with additional use of nonparenchymal cells of the SUMMARY
liver, may provide the ideal niche for functional differentiation
of such organoids. This is truly an evolving and timely field with In the last century, knowledge about liver regeneration has
much ongoing research in which knowledge of liver regenera- rapidly evolved from a truly mythical black box event into
tion is essential. growing understanding of the pathways involved in this amazing
complex multistep process. Much was learned about the
The Role of miRNA in Liver Regeneration dynamics and redundant intracellular signaling pathways of
A family of tiny regulatory RNAs, known as microRNAs liver regeneration, but less is still known about the exact signals
(miRNAs), was found to have profound roles in the control of that initiate and stop liver regeneration. Our advanced knowl-
diverse aspects of hepatic function and dysfunction, including edge on liver regeneration and prevention of liver failure led to
hepatocyte growth, stress response, metabolism, viral infection safer extreme liver resections for benign and malignant diseases
and proliferation, gene expression, and maintenance of hepatic and the use of living-liver donors in liver transplantation.
phenotype (Ambros, 2004; Elmen et al, 2008). miRNAs are Despite our better understanding, there has been little
small endogenous noncoding RNAs that posttranscriptionally structured advancement in therapeutic options in case of liver
repress the expression of protein-coding genes by base-pairing failure due to insufficient liver regeneration. New challenges lie
with the 39 untranslated regions of the target mRNAs (Bartel, ahead in the use of therapeutic strategies to enhance liver
2004; Grimson et al, 2007). regeneration in patients in whom normal regeneration fails and
In 2002, miR-122 was identified as an abundant miRNA in thus push the possibilities of liver resection to the next level.
the liver (Lagos-Quintana et al, 2002) and characterized as the Furthermore, while promoting liver cell proliferation, we must
most frequent miRNA isolated in the adult liver (Chang et al, be very cautious not to stimulate tumor growth in patients with
2004). Using distinct protocols to silence miR-122, evidence primary or metastatic liver tumors as a consequence of our
for the overall importance of miR-122 in the regulation of liver therapy.
metabolism was found (Esau et al, 2006; Krutzfeldt et al,
2005). Silencing miR-122 in high-fat–fed mice resulted in a References are available at expertconsult.com.
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CHAPTER 7
Liver fibrogenesis: mechanisms and
clinical relevance
Diana Vetter and Scott L. Friedman
Liver fibrosis represents a scarring response to either acute or Remarkably, as many as 45% of all deaths are related to some
chronic liver injury. Following acute liver injury, parenchymal kind of fibrosis (Wynn, 2008), stressing the importance of this
cells regenerate to successfully preserve hepatocellular mass response and explaining the growing interest in this field of
and function. This acute process is associated with an inflam- research. For decades, fibrosis was considered an irreversible
matory and fibrogenic response but with limited deposition of disease that progresses to cirrhosis with a greater risk for hepa-
extracellular matrix (ECM). In contrast, prolonged liver injury tocellular carcinoma and with development of liver failure. This
leads to sustained production of growth factors, proteolytic meant that the only potential treatment for liver fibrosis was
enzymes, angiogenic factors, and fibrogenic cytokines. These liver transplantation once cirrhosis was present.
events culminate in the accumulation of extracellular matrix, Research during the past 35 years has yielded increasing
forming septa that coalesce into broad bands of scar tissue insight into the cellular and molecular mechanisms of this
encircling nodules of hepatocytes and leading to altered micro- disease, uncovering an orchestrated pathophysiology, and iden-
vascular structure (Friedman, 2004; Lee et al, 2015) (Fig. 7.1). tifying the hepatic stellate cell (HSC) as the central cell type in
This late stage of fibrosis, termed cirrhosis, ultimately impairs fibrogenesis (Friedman et al, 1985) and, most important,
liver function and leads to portal hypertension and its revealing the potential reversibility of the disease and discovery
complications. of potential therapeutic targets.
Typically, progression of fibrosis to cirrhosis evolves for
decades before clinical events ensue, but disease may progress MOLECULAR AND CELLULAR MECHANISMS
more rapidly following repeated episodes of severe acute alco- OF FIBROSIS
holic hepatitis, subfulminant hepatitis (especially due to drug
toxicity), and fibrosing cholestasis in patients with hepatitis C The anatomic arrangement of the parenchymal and nonparen-
virus (HCV) reinfection following liver transplantation. In chymal cells of the liver contributes to its unique role as an
addition, there have been reports of rapidly progressive acute immune organ and helps explain how the liver responds to an
HCV with fibrosis in men coinfected with human immunode- insult. The liver is composed primarily of epithelial cells (hepa-
ficiency virus (HIV) (Fierer et al, 2008). tocytes and cholangiocytes), as well as resident nonparenchy-
Genetic and environmental factors also influence the course mal cells that include hepatic macrophages (Kupffer cells),
of the disease. For example, polymorphisms in a number of sinusoidal endothelium, and HSCs. In addition to Kupffer
candidate genes involving the inflammatory (e.g., Toll-like cells, a growing list of specialized immune cells have been
receptor 4 [TLR4] [Guo et al, 2009]) or the immune (Powell characterized, including dendritic cells, natural killer (NK)
et al, 2000) response may influence the progression of liver cells, and natural killer T (NKT) cells, emphasizing that the
fibrosis in humans. In HCV, the development of a seven-gene liver represents a key organ in the regulation of innate immunity
signature has good prognostic value in assessing the risk (Crispe, 2014; Gao & Radaeva, 2013) (see Chapter 10).
for cirrhosis development (Huang et al, 2007) and has been The liver capsule extends as septa into the liver, delineating
further validated in two separate cohorts (Pradat et al, 2010; hepatic lobules that form the structural units of the liver. The
Trepo et al, 2011). However, with the development of highly lobule forms a hexagonal structure with portal triads (including
effective and well-tolerated therapies for HCV, this kind of branches of the hepatic portal vein, the hepatic artery, and the
genetic test has diminishing utility for HCV disease, because bile duct) localized in the periphery of the lobule, and with a
fibrosis progression risk is unlikely to influence the decision portal vein branch in the center (see Fig. 7.1). Hepatocyte plates
whether to treat the infection, as eventually most patients will radiate outward from the central vein and are separated from
probably be treated. Unfortunately, the development of a each other by sinusoids. The latter form the connecting element
similar genetic risk score for nonalcoholic fatty liver disease between the branches of the hepatic portal veins and hepatic
(NAFLD) has been elusive, possibly because the disease is arteries with the central vein. Kupffer cells, NK cells, NKT
more heterogeneous. cells, and dendritic cells, all of which are important components
The main etiologies of liver fibrosis in Western countries are of the innate immune system, reside in the hepatic sinusoids.
chonic HCV and hepatitis B virus (HBV) infection, alcohol The subendothelial space between the sinusoidal endothelium
abuse, and nonalcoholic steatohepatitis (NASH) (see Chapters and hepatocytes is also termed the space of Disse. Thus the
70 and 71). As a generalized tissue response to chronic injury, HSCs, which lie in the space of Disse, have direct contact with
fibrosis also occurs in many other organs (heart, lung, kidneys) endothelial cells and hepatocytes. Sinusoidal endothelial cells
and typically represents the result of an ongoing inflammation. are highly fenestrated, which allows unimpeded flow of plasma
110
Chapter 7 Liver fibrogenesis: mechanisms and clinical relevance 111
Normal liver
Portal triad
Bile duct
Hepatocytes
HSC
Hepatic
arteriole
Fibrotic liver
Increase in fibril-forming
collagen in space of Disse
FIGURE 7.1. Matrix and cellular alteration in hepatic fibrosis. Normal liver parenchyma contains epithelial cells (hepatocytes) and nonparen-
chymal cells: fenestrated sinusoidal endothelium, hepatic stellate cells (HSCs), and Kupffer cells (KCs). A, Sinusoids are separated from hepatocytes
by a low-density basement membrane–like matrix confined to the space of Disse, which ensures metabolic exchange. Upon injury, the HSCs become
activated and secrete large amounts of extracellular matrix (ECM), resulting in progressive thickening of the septa. B, Deposition of ECM in the space
of Disse leads to the loss of both endothelial fenestrations and hepatocyte microvilli, which results in both the impairment of normal bidirectional
metabolic exchange between portal venous flow and hepatocytes and the development of portal hypertension. (From Hernandez-Gea V, Friedman
SL: Pathogenesis of liver fibrosis, Annu Rev Pathol 6:425–456, 2011.)
112 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
from sinusoidal blood into the space of Disse. Through this factor kappa B (NF-κB) in Kupffer cells, which leads to
arrangement, hepatocytes and HSCs are exposed directly to increased tumor necrosis factor-α (TNF-α) production (see
plasma derived largely from venous blood draining the Fig. 7.2). TNF-α in turn induces neutrophil infiltration and
intestine. stimulates mitochondrial oxidant production in hepatocytes,
which are then sensitized to undergo apoptosis. Furthermore,
Common Triggers of Hepatic Fibrogenesis ROS and acetaldehyde, the main degradation product of
Ongoing insult to the liver will lead to an increased inflamma- alcohol, both activate HSCs and stimulate inflammatory signals
tory state with activation of hepatic stellate cells, which ulti- (Maher et al, 1994). Interestingly, many of the same gut defects
mately tilts the profibrotic and antifibrotic balance toward in alcoholic liver disease are now also implicated in NASH, with
fibrosis. Viral infection, reactive oxygen species (ROS), and bile additional focus on the nature of the microbiome as well as the
acids are among the most common stress signals for the liver integrity of the gut mucosa as determinants of fatty liver disease
(Fig. 7.2). An in vitro study further suggests that free fatty acids (De Minicis et al, 2014; Dumas et al, 2014; Fouts et al, 2012).
promote fibrogenesis by indirect activation of HSCs (Wobser In HCV infection, the virus escapes the immune response
et al, 2009), which may be relevant to the pathogenesis of fatty and infects hepatocytes (Wang et al, 2013). This causes oxida-
liver disease. tive stress, again leading to recruitment of inflammatory cells
In alcoholic liver disease, ethanol decreases gut motility, and HSC activation. HSCs can also be directly activated either
increases epithelial permeability, and promotes overgrowth by HCV through membrane receptors (Mazzocca et al, 2005;
of gram-negative bacteria. Consequently, lipopolysaccharide Schulze-Krebs et al, 2005), or by HBV (Martin-Vilchez et al,
(LPS) concentration is elevated in portal blood, through the 2008) (see Chapter 70).
TLR4 signaling complex, to generate ROS via reduced nico- Bile acids are hepatotoxic agents and typically target hepa-
tinamide adenine dinucleotide phosphate (NADPH) oxidase tocytes but may also injure biliary epithelium (Higuchi &
(Paik et al, 2003; Roh & Seki, 2013; Vazquez-Torres et al, Gores, 2003). In addition to their potential role in provoking
2004; Zhang et al, 2012). Oxidants then upregulate nuclear damage, there is an increasing appreciation for the role of bile
Small intestine
Gram-neg.
bacteria↑
Kupffer cells (macrophages)
Inflammatory TNF-α
cytokines Neutrophils
ROS
Alcohol Mito. oxidant Apoptosis qHSCs
production
NASH
ROS
HCV Oxidative Sensitized to
stress↑ apoptosis NADPH
HBV aHSCs Proliferation
FXR Contractility
Free fatty acids Fibrogenesis
Bile acids via EGFR Altered matrix
degradation
HSC chemotaxis
Infammatory
signaling
Myofibroblasts
FIGURE 7.2. Pathways of cellular injury and fibrosis. This diagram depicts the key pathways of cellular injury and fibrosis. The main causes of
chronic liver injury are alcohol, nonalcoholic steatohepatitis (NASH), viral infection, and injury from bile acids in cholestatic conditions. All factors
activate hepatic stellate cells (HSCs), which is a key event in liver fibrogenesis. Alcohol can promote gram-negative bacterial overgrowth of the small
intestine and/or reduced gut integrity, thereby increasing lipopolysaccharide (LPS) in the portal blood. LPS activates Kupffer cells (hepatic macro-
phages), which increase the mitochondrial oxidant production in hepatocytes by way of tumor necrosis factor-α (TNF-α), thereby sensitizing them
to apoptosis. Kupffer cells also promote local accumulation of T cells and neutrophils, which, along with apoptotic hepatocytes, stimulate the activa-
tion of HSCs. Damage to hepatocytes by NASH or infection with hepatitis B or C viruses (HBV, HCV) promotes oxidative stress, further sensitizing
hepatocytes to apoptosis. Free fatty acids also increase the intracellular oxidative stress of hepatocytes. Bile acids inhibit activation of HSCs via a
farnesoid X receptor (FXR) pathway. aHSCs, Activated HSCs; EGFR, endothelial growth factor receptor; ERK-1, extracellular signal-regulated kinase-
1; mito., mitochondrial; NADPH, reduced nicotinamide adenine dinucleotide phosphate; qHSCs, quiescent HSCs; ROS, reactive oxygen species;
TNF-α, tumor necrosis factor-α.
Chapter 7 Liver fibrogenesis: mechanisms and clinical relevance 113
acids as ligands for nuclear receptors, in particular the farnesoid lung, bone marrow, and pancreas, among others (Iwaisako
X receptor (FXR), which drives an entire cellular program that et al, 2014; Lua et al, 2014). The relative importance of each
can alter hepatocellular metabolism and bile secretion and fibrogenic cell type in liver fibrogenesis may depend on the
composition (Adorini et al, 2012). Remarkably, the therapeutic origin of the liver injury. Recent fate-tracing studies using
benefit of vertical sleeve gastrectomy has also been ascribed to genetically altered reporter mice implicate stellate cells as the
FXR signaling in an animal model, raising the possibility that dominant source of MFBs (Mederacke et al, 2013) in paren-
intestinal FXR alone may be sufficient to drive weight loss and chymal liver disease; however, some contribution from biliary
improved metabolic parameters in NASH (Ryan et al, 2014). portal fibroblasts is important in cholestatic liver disease
Oxidant stress, mediated by ROS, is a common mediator of (Perepelyuk et al, 2013; Wells, 2014).
injury in many liver diseases in which damaged hepatocytes HSC activation can be divided conceptually into two phases.
become apoptotic or necrotic, thereby releasing ROS (Nieto First there is initiation, with early changes in gene expression
et al, 2002) and NADPH oxidase, which both activate HSCs and phenotype, resulting from paracrine stimulation, primarily
(Canbay et al, 2004). Injured hepatocytes also release inflam- due to changes in surrounding ECM, as well as exposure to
matory cytokines and soluble factors that activate Kupffer cells lipid peroxides and products of damaged hepatocytes. Next
and stimulate the recruitment of activated T cells. This inflam- there is perpetuation, which results from the effects of these
matory milieu further stimulates the activation of resident stimuli on maintaining the activated phenotype and generating
HSCs. Bile acids also directly stimulate proliferation of HSCs fibrosis. Within the nucleus, a growing number of transcription
by activating the epidermal growth factor receptor (Svegliati- factors regulate HSC activation, including peroxisome prolif-
Baroni et al, 2005). In contrast to hepatocytes, HSCs are pro- erator–activated receptors (PPARs), retinoid receptors, liver X
tected from bile acid–induced apoptosis by excluding bile acids receptor, REV-ERBα, NF-κB, FXR, GATA4, vitamin D recep-
(Svegliati-Baroni et al, 2005). tor, JunD, Kruppel-like factor 6, and FOXF1 (Lee et al, 2015;
NAFLD is increasingly prevalent due to increased rates of Mann & Mann, 2009). A number of general and cell type–
childhood and adult obesity in the United States and Western specific membrane receptors and signaling pathways also
Europe (see Chapter 71). In fact, the percentage of liver trans- control HSC biology, including receptor tyrosine kinases, che-
plantations performed for this indication is rapidly rising, which mokine receptors, and integrins (Lee et al, 2015). In addition
is likely to accelerate further as more viral hepatitis patients are to these novel pathways, there has been substantial progress in
effectively cured with antivirals, combined with a growing prev- understanding how epigenetics contributes to stellate cell
alence of obesity (Charlton, 2013). NAFLD can progress to biology and fibrosis through both histone modifications and the
NASH, with consequent fibrosis and cirrhosis (Loomba & contribution of microRNAs (Lee et al, 2015; Mann, 2014).
Sanyal, 2013; Michelotti et al, 2013; Noureddin et al, 2013; As noted above, portal fibroblasts (Beaussier et al, 2007;
Singh et al, 2014). The pathogenesis is not fully understood. Ramadori & Saile, 2004), and bone marrow–derived MFBs
However, multiple convergent pathologies are increasingly (Russo et al, 2006) have also been identified as collagen-
implicated, including insulin resistance, oxidant stress, altered producing cells in the injured liver. Although earlier studies
adipokine balance, lipotoxicity, effects of the microbiome, and implicated epithelial-mesenchymal transition as a source of
enhanced inflammation, among others (De Minicis et al, 2014; fibrogenic cells (Rygiel et al, 2008), more recent findings
Tacke & Yoneyama, 2013; Wree et al, 2013). strongly refute its importance in liver (Chu et al, 2011).
Senescent/Inactivated/
Quiescent Activated
Apoptotic
Inactivated
Apoptotic
Organ Phenotype
FIGURE 7.3. Functions, features and phenotypes of hepatic stellate cells in normal and diseased liver. Hepatic stellate cells may exist as
several different phenotypes with distinct molecular and cellular functions and features, each of which contributes significantly to liver homeostasis
and disease. Quiescent stellate cells are critical to the normal metabolic functioning of the liver. Liver injury provokes transdifferentiation of quiescent
stellate cells to their activated phenotype, leading to metabolic reprogramming, increased autophagy to fuel the metabolic demands, amplification
of parenchymal injury, and the development of “classic” phenotypic features of activated hepatic stellate cells/myofibroblasts. Through these changes,
activated stellate cells drive the fibrotic response to injury and the development of cirrhosis. As liver injury subsides, activated stellate cells can be
eliminated by one of three pathways: apoptosis, senescence, or reversion to an inactivated phenotype. Senescent stellate cells are more likely to be
cleared by natural killer (NK)-cell–mediated cell death, whereas inactivated stellate cells remain “primed” to respond to further liver injury. This reduc-
tion in the number of activated stellate cells contributes to the regression of fibrosis or cirrhosis and repair of the liver in most, but not all, patients.
The relative contribution of these three pathways of stellate cell clearance to fibrosis regression is not yet clear. ECM, Extracellular matrix; HSCs,
hepatic stellate cells. (From Lee YM, et al: Pathobiology of liver fibrosis—a translational success story, Gut 64:830–841, 2015.)
the collagen type 1 messenger RNA (mRNA) (Tsukada et al, Marra, 2010). All pathways downstream of the βPDGF-β
2005). Local activation of TGF-β1 at the cell surface by inte- receptor, the key receptor isoform in HSCs, promote prolifera-
grins has led to the prospect of antagonizing integrins as an tion. First, c-Jun N-terminal kinase is stimulated through
antifibrotic therapy (Henderson et al, 2013). In addition to MAPK (Schwabe et al, 2001); second, PDGF receptor stimu-
TGF-β1, CTGF (Lipson et al, 2012), and Hedgehog signaling lates the RAS/RAF complex, followed by mitogen-induced
have also been implicated as important fibrogenic mediators in extracellular kinase and extracellular signal-regulated kinase
liver injury and repair (Michelotti et al, 2013; Xie et al, 2013). engagement (Schwabe et al, 2001); third, activation of the
PI3K pathway, leading to AKT (Protein kinase B) activation
Proliferation and phosphorylation of the 70S6 kinase (Reif et al, 2003).
The predominant stimulus to MFB proliferation is the mitogen
platelet-derived growth factor (PDGF) (Borkham-Kamphorst Immunoregulation
et al, 2004), in addition to other mitogens, including epidermal The liver is a microenvironment of diminished immunogenicity,
growth factor, VEGF, and fibroblast growth factor (Mann & which is necessary to cope with the high exposure of antigens
Chapter 7 Liver fibrogenesis: mechanisms and clinical relevance 115
from the portal vein (Crispe, 2003) (see Chapter 10). This
feature also accounts for the tolerance of liver transplantation Vasoregulation
across ABO barriers and may contribute to the chronic nature MFBs play an important role in the regulation of sinusoidal
of HBV or HCV, in which the virus persists despite the develop- blood flow and may contribute to portal hypertension that is
ment of an immune response. Upon entry of the antigen to the characteristic of advanced liver disease (see Chapters 76 and
sinusoid, classic antigen-presenting cells (Kupffer cells, den- 79,). The release of endothelin-1 (ET-1) can stimulate their
dritic cells) are first encountered. Subsequently, HSCs in the contraction through the endothelin type A (ETA) receptor
space of Disse may contact antigens. Indeed, HSCs display a (Khimji & Rockey, 2011), thereby promoting tissue contrac-
wide range of immunoregulatory functions and are an essential tion, increasing portal resistance, and generating portal hyper-
part of the local immunogenicity (Crispe, 2014; Gao & Radaeva, tension. On the other hand, MFBs and endothelial cells also
2013; Gao & Xu, 2014; Jiang et al, 2013; Kubes & Mehal 2012; secrete nitric oxide (NO), which is the physiologic antagonist
Watanabe et al, 2009). of ET-1.
Hepatic MFBs produce a range of proinflammatory and
antiinflammatory cytokines (see Chapter 11) and recruit Structural Features of Hepatic Fibrogenesis
lymphocytes through secretion of chemokines (monocyte che- In hepatic fibrosis, the total amount of collagen is increased up
moattractant protein-1, interleukin-8 [IL-8], C-C chemokine to sixfold, whereas the parenchymal mass (e.g., hepatocytes) is
21 [CCL21], regulated on activation, normal T-cell expressed progressively diminished. The composition of the ECM changes
and secreted, C-C chemokine receptor 5 [CCR5]) (Gao & Xu, with progression of disease (see Fig. 7.1). Collagen type IV in
2014; Marra & Tacke, 2014), thus amplifying the inflammatory the space of Disse is replaced by interstitial collagens, type I and
response. However, upon activation they exert a profound III. Additionally, the discontinuous basal membrane beneath
immunosuppressive activity by inducing T-cell apoptosis (Yu the sinusoidal endothelial cells is replaced by a continuous base-
et al, 2004). In the setting of liver transplantation, MFB- ment membrane, and sinusoidal fenestrations are reduced. This
induced T-cell apoptosis via programmed death ligand-1 (Yu decreased porosity (also known as “capillarization”), combined
et al, 2004) may enable local immunotolerance of the liver. In with perisinusoidal fibrosis, scar contraction, and formation of
liver fibrosis, MFBs may further regulate the contribution of intrahepatic shunts, contribute to increased hepatic venous
lymphocytes to the course of hepatic fibrosis by ingesting dis- pressure and portal hypertension. Fibrillar collagens that are
ease-associated lymphocytes (Muhanna et al, 2008). produced by MFBs also interact with MFBs via discoidin
The interaction between HSCs and immune cells is bidirec- domain receptors and integrins (Olaso et al, 2001), thereby
tional. T cells activate HSCs by interferon-γ (IFN-γ), which inhibiting apoptosis and increasing MFB proliferation.
upregulates both stimulatory (CD80, CD86, CD54) and inhib- With the maturation of the fibrotic scar, not only is the
itory (B7-H1) surface molecules, and enhances both inflamma- amount of collagen increased, but the scar also becomes
tory and suppressive cytokines. However, the inhibitory increasingly insoluble through chemical cross-linking by lysyl
molecules are thought to override the stimulatory counterparts, oxidase 2 (LOXL2), tissue transglutaminase, and a disintegrin
resulting in immunosuppression. Lymphocytes can also mediate and metalloproteinase with thrombospondin-type repeats
hepatic fibrosis by activating HSCs. CD8-positive T lympho- metalloproteinase with thrombosponin type I motif (ADAMTS2)
cytes are more fibrogenic toward stellate cells than CD4 T (Kesteloot et al, 2007). Indeed, stellate cells are an important
lymphocytes (Safadi et al, 2004). This may explain, in part, source of these cross-linking enzymes (Perepelyuk et al, 2013).
why patients coinfected with HIV and HCV have accelerated Cross-linking makes the fibrous septa progressively resistant to
fibrosis, as their CD4:CD8 cell ratios are reduced. Of the CD4- proteolysis by matrix metalloproteinases (MMPs). The long-
positive T lymphocytes, previously called T-helper cells, the standing clinical dogma that the slower the pace of injury, the
humoral immunity mediated by T-helper 2 cells (Th2) is pro- less reversible the scar, is supported by animal studies in which
fibrogenic in liver injury, whereas the cell-mediated immunity even advanced fibrosis of short duration is reversible. Thus the
by the Th1 cells via IFN-γ, TNF-α, and IL-2 is antifibrogenic reversibility of a scar may be limited primarily by the extent of
(Shi et al, 1997). collagen cross-linking. Clinically, increased septal thickness and
HSCs can also function as antigen-presenting cells (Winau smaller nodule size, both of which reflect more advanced stages
et al, 2007). They can interact with bacterial LPSs directly via of fibrosis, are significant predictors of worse clinical outcomes
TLR4, which amplifies their activation. TLR4 signaling leads (Nagula et al, 2006). Efforts to therapeutically increase the
to downregulation of a TGF-β pseudoreceptor, BMP (bone solubility of collagen have shown that an antibody to LOXL2
morphogenic protein) and activin membrane-bound inhibitor, has marked antifibrotic effects in animal models of fibrosis in
which thereby amplifies fibrogenic activity of MFBs (Seki & liver and other organs (Barry-Hamilton et al, 2010), which has
Brenner, 2008). Signaling through TLR4 may be elicited not led to its use in ongoing clinical trials in fibrosis and cancer
only by exogenous ligands, including LPS, but also by endog- (Nishioka et al, 2012).
enous ligands, including high-mobility group box 1 protein
(Pradere et al, 2010; Roh & Seki, 2013; Wang et al, 2013). The Regulation of Collagen Deposition and Degradation
discovery of endogenous ligands for TLR4 has been part of a The deposition and degradation of collagen are tightly regulated.
larger appreciation that many cells, including HSCs, possess MMPs are the key enzymes that degrade fibrillar collagens
intracellular machinery known as the inflammasome, which (collagen types I and III) and noncollagenous ECM substrates
transduces signals arising from cellular damage (Henao-Mejia (Iredale et al, 2013). The tissue inhibitor metalloproteinases
et al, 2012; Kubes & Mehal, 2012; Vandanmagsar et al, 2011; (TIMPs) are their major antagonists by inactivating proteases
Wree et al, 2014). The role of the inflammasome is especially and by inhibiting MFB apoptosis (Murphy et al, 2002).
pertinent to understanding the pathogenesis of inflammation Both decreased levels of interstitial collagenases and increased
and fibrosis in NAFLD and NASH. levels of MMP inhibitors in liver injury create an imbalance that
116 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
favors reduced degradation of fibrillar collagens in hepatic fibro- including two stages of cirrhosis (“incomplete”and “complete”
sis.The interstitial collagenases MMP-1, MMP-8, and MMP-13 cirrhosis) (Ishak et al, 1995). The METAVIR score (an acronym
in humans and MMP-13 in rodents unwind the triple-helical derived from a French Investigator group) is a simple, widely
collagen type I, which is the principal collagen in the fibrotic applied five-stage scoring system (METAVIR Cooperative
liver, so that each α-chain is presented to the active site of the Study Group, 1994; Poynard et al, 1997) that is the most com-
enzyme that cleaves the collagen (Iredale et al, 2013). Other monly used worldwide. It incorporates the fibrosis scores F0 to
MMPs (e.g., MMP-2) cannot unwind the triple-helical collagen F4, and the activity scores A0 to A3, which assess the amount
and thus cannot degrade intact collagen type I alone. In early of necroinflammation. Specifically, F0 = no fibrosis, F1 = fibro-
liver injury, MMP-2 degrades the low-density basement mem- sis without septa, F2 = few septa, F3 = numerous septa without
brane present in the subendothelial space (Zhou et al, 2004). cirrhosis, and F4 = cirrhosis; further, A0 = no necroinflamma-
Its replacement with fibril-forming matrix impairs hepatocyte tory activity, A1 = mild necroinflammatory activity, A2 =
differentiation and function. During progressive fibrosis, expres- moderate necroinflammatory activity, and A3 = severe necro-
sion of MMP-1 (humans) or MMP-13 (rodents) is decreased, inflammatory activity.
and MMP-2 expression increases (Milani et al, 1994; Preaux For NAFLD, a separate scoring system for grading inflam-
et al, 1999). In parallel, the expression of tissue inhibitor mation and staging fibrosis has been widely adopted (Brunt
metalloproteinases (TIMP)-1 and TIMP-2, which inhibit the et al, 2011; Kleiner et al, 2005; Sanyal et al, 2011), which
collagen-degrading MMPs, is increased (Murphy et al, 2002; captures key histologic features of disease progression that are
Ramachandran & Iredale, 2009). distinct from viral liver disease (see Chapter 71). Specifically,
Hepatic macrophages are increasingly recognized as the key NAFLD and NASH, as well as alcoholic liver disease, are pri-
cellular determinant of matrix degradation, with some contri- marily centrilolobular rather than the periportal distribution
bution by dendritic and other inflammatory cells (Jiao et al, typical of viral liver diseases. The NAFLD Kleiner stages are
2012; Mitchell et al, 2009; Tacke & Zimmermann, 2014). In stage 0 = no fibrosis, stage 1 = perisinusoidal or periportal
mouse models, macrophages augment fibrogenesis during pro- fibrosis (1a: mild, zone 3; 1b: moderate, zone 3; 1c: portal/
gression of liver fibrosis, whereas during resolution, they hasten periportal), stage 2 = periportal and perisinusoidal fibrosis,
matrix degradation through increased production of MMP-13 stage 3 = bridging fibrosis, and stage 4 = cirrhosis.
(Fallowfield et al, 2007). More important, there is substantial There are other scoring systems specifically developed for
heterogeneity of macrophages in liver injury and resolution to different etiologies of liver fibrosis. For example, Ludwig and
account for these divergent activities, with a subset known as coworkers proposed a four-stage system to describe fibrosis for
Ly6c-lo cells implicated in degrading matrix during fibrosis both primary biliary cirrhosis (Ludwig et al, 1978) and scleros-
regression (Pellicoro et al, 2014; Ramachandran & Iredale, ing cholangitis (Ludwig et al, 1981).
2012; Ramachandran et al, 2012). Despite these major For fibrosis staging, there is increasing reliance on absolute
advances in identifying the key fibrolytic cell in liver fibrosis quantification of collagen in liver biopsy samples as assessed by
regression, it is not clear which is the major interstitial collage- computerized morphometry, instead of using a discontinuous
nase in fibrosis regression, because MMP-1 is only expressed scoring system composed of discrete stages. Indeed, collagen
at low levels in liver. proportionate area assessment is far more predictive of clinical
outcomes, even in NASH, and therefore its use is rapidly
DIAGNOSIS AND CLINICAL MONITORING gaining popularity, especially as an end point in clinical trials
OF HEPATIC FIBROSIS (Calvaruso et al, 2009; Huang et al, 2014; Manousou et al,
2013).
Many patients with chronic liver disease may initially be seen There is a great need for reliable, quantitative noninvasive
with late-stage fibrosis, because earlier stages are often asymp- diagnostics for fibrosis, and recent studies indicate steady
tomatic. Thus clinicians must have a high index of suspicion progress. Cross-sectional imaging studies such as computed
for occult fibrosis, especially in patients with unexplained eleva- tomography (CT) and magnetic resonance imaging (MRI) can
tions of liver enzymes, splenic enlargement, stigmata of liver demonstrate features of advanced liver disease, such as nodu-
disease, and/or laboratory or imaging findings suggestive of larity and signs of portal hypertension (splenomegaly, enlarged
portal hypertension (see Chapter 79). caudate lobe, esophageal varices). Diffusion-weighted MRI
When chronic liver disease is suspected, the liver biopsy measures the apparent diffusion coefficient of water, a param-
remains the gold standard for diagnosing and staging of liver eter that depends upon tissue structure. It has compared favor-
fibrosis. However, it is an invasive procedure with risk of ably to other noninvasive measures for determining advanced
adverse events and, equally important, a high likelihood of fibrosis (Murphy et al, 2015). More recent advances in MR
sampling (Bedossa et al, 2003; Ratziu et al, 2005) and inter- methods include MR elastography (Loomba et al, 2014), MR
pathologist and intrapathologist variability (Bedossa et al, fat fraction, and other related technologies (Banerjee et al,
2003). At least one third of biopsies may differ by one fibrosis 2014; Noureddin et al, 2013b & 2013a; Tang et al, 2014).
stage between the right side and left side hepatic lobes in HCV There are also efforts to develop newer MR probes that will
(Regev et al, 2002) and NAFLD (Ratziu et al, 2005). Shorter enable quantification of total liver collagen or elastin content
biopsies are associated with an increase in reported diagnoses (Ehling et al, 2013; Fuchs et al, 2013).
of mild and moderate fibrosis at the cost of more severe fibrosis, Biochemical parameters associated with hepatocyte injury
representing an understaging of fibrosis (Bedossa et al, 2003). (aspartate aminotransferase [AST], alanine aminotransferase
There are several commonly used histologic staging systems [ALT]), cholestatic liver injury (bilirubin, alkaline phospha-
for fibrosis (see Chapter 76). The Histology Activity Index tase), impaired liver synthetic function (apolipoproteins, cho-
score reported by Knodell includes three stages (Knodell et al, lesterol, coagulation factors, α2-macroglobulin, hyaluronic
1981), whereas the Ishak score differentiates six stages, acid, albumin, globulins), or impaired hepatic clearance of
Chapter 7 Liver fibrogenesis: mechanisms and clinical relevance 117
endogenous or exogenous substances from the circulation (bili- to liver biopsies that were staged according to the Kleiner score
rubin, bile acid, caffeine, lidocaine metabolites, bromsulpha- (Adams & Angulo, 2007; Angulo et al, 2007). If ELF was used
lein, methacetin, indocyanine green, cholate, or ammonia) to delineate any fibrosis (using thresholds with a sensitivity and
(Everson et al, 2012) can provide information on the presence specificity of 90%, respectively), the authors concluded that
and cause of the disease. These tests all assess impaired liver liver biopsy could have been avoided in 48% of the patients.
function in fibrosis and may prove to be more quantitative and
sensitive than tests of liver injury or morphology. Indeed, pul-
Cytokines and Chemokines Associated
monary function tests (e.g., spirometry) have been a mainstay with Hepatic Fibrosis
of clinical assessment in lung disease rather than tissue analysis Of the cytokines and chemokines that are associated with
of lung for decades. Continued progress in using functional hepatic fibrosis, TGF-β1 is the dominant stimulus to the pro-
rather than structural assessment of liver disease is expected. duction of ECM by HSCs. Hepatic mRNA levels of TGF-β1
are increased in chronic liver disease in association with
Biochemical Tests increases in mRNA levels of type I collagen (Houglum et al,
A more direct approach incorporates serum molecules associ- 1994). In HCV-related chronic liver disease, serum TGF-β
ated with fibrosis, including those involved in deposition or levels correlate with the Knodell fibrosis score, but not with
degradation of ECM, as well as specific fibrogenic cytokines clinical, biochemical, or virologic parameters (Nelson et al,
associated with fibrosis. A number of combination serum tests 1997). Interestingly, TGF-β levels also decreased in a group of
have been evaluated for predicting fibrosis stage and outcomes, HCV patients with histologic decreases in necroinflammation
with improving sensitivity and specificity. To date, no single in the absence of changes in fibrosis following IFN treatment
molecule, but rather combinations of different components, (Roulot et al, 1995). Thus TGF-β serum levels not only cor-
demonstrate the best sensitivity and negative predictive values relate with fibrosis scores but may also indicate necroinflam-
to exclude significant fibrosis. mation. PDGF is upregulated following liver injury, and the
The most studied combination serum tests are the AST-to- amount of PDGF correlates with the severity of fibrosis (Yoshida
platelet ratio index (Wai et al, 2003), the Fibrosis-4 index et al, 2014).
(Sterling et al, 2006), the Forns test (Forns et al, 2002), and
the proprietary FibroTest (FT; Biopredictiv, Paris) (Imbert- Proteomics and Glycomics
Bismut et al, 2001). Newer proprietary biomarker scores Proteomics and glycomics are promising new technologies suit-
include the HepaScore (Quest Diagnostics, Madison, NJ) able as noninvasive diagnostic methods. Patterns of proteins or
(Leroy et al, 2014) and the FibroMeter (Cales et al, 2005). All glycoproteins can be assessed by mass spectroscopy of serum
these biochemical tests range from sufficient to excellent in samples (Miller et al, 2014; Paulo et al, 2013; Rodriguez-
ruling out significant fibrosis (F3 to F4) when the proper cutoff Suarez et al, 2012). Profiles of serum protein N-glycans were
value is chosen, but they are less useful in distinguishing mild found to have similar AUROC values to the FT for the diag-
from moderate fibrosis. The sensitivities of the tests vary based nosis of compensated cirrhosis. The combination with the FT
on the etiology of the liver disease. Further difficulties of these was able to increase the sensitivity and specificity of the test
tests are the absence of an ideal gold standard, in view of the (Callewaert et al, 2004).
liver biopsy’s significant sampling variability and interlabora-
tory differences (Gressner et al, 2009). The lack of a true gold Stiffness Assessments
standard means that the utility of serum tests can never be fairly An alternative approach to fibrosis assessment is the measure-
evaluated when compared to biopsy (Mehta et al, 2009). ment of liver stiffness using a number of devices, the first of
Overall, these serum markers’ performances are approxi- which, Fibroscan (FS; Echosens), uses vibration-controlled
mately comparable (Castera et al, 2013). Although it is unlikely transient elastography. Although FS was the first to assess stiff-
that these alone will suffice in assessing short-term disease ness clinically, other technologies are now also available for this
progression in clinical trials of antifibrotic drugs or in manage- purpose, including acoustic radiation force impulse imaging
ment of chronic liver diseases, they do predict long-term out- (Lupsor et al, 2009; Rifai et al, 2011) and shear wave elastog-
comes and therefore may have some utility in the future (Mayo raphy (Ferraioli et al, 2012). As noted above, stiffness can also
et al, 2008; Ngo et al, 2006). be assessed by MR elastography, which has the advantage of
assessing the entire liver (Loomba et al, 2014). However, there
Serum Assays of Extracellular Matrix Molecules is far more experience and published data assessing FS than
Serum assays have been developed that measure circulating the other technologies.
molecules involved either in the deposition of ECM or its deg- For FS, the stiffer the liver tissue, the faster a wave propa-
radation, as well as cytokines involved in fibrogenesis. Among gates. Results are expressed in kilopascals (kPa) (Kettaneh
the better-validated of these tests is the enhanced liver fibrosis et al, 2007; Sandrin et al, 2003). With the FS, the virtual cyl-
(ELF) panel (Parkes et al, 2011). This test incorporates inder of tissue that is assessed is at least 200 times larger than
markers of ECM turnover (TIMP-1, hyaluronic acid, and a biopsy sample and therefore is far more representative of the
amino-terminal peptide of procollagen III [P3NP]). The ELF hepatic parenchyma. Thus the FS may provide a more accurate
test was better at identifying minimal, moderate or severe fibro- and reproducible picture of cirrhosis than liver biopsy. There
sis than a clinical-biochemical panel (age, body mass index, is also potential value of the FS in early stages of disease, where
presence of diabetes or impaired fasting glucose, AST : ALT fibrosis may be unevenly distributed and thus underestimated
ratio, platelets, and albumin), and the combination of both by liver biopsy. Furthermore, FS has very low interobserver
scores showed further improved area under the receiver operat- variability. However, its accuracy is limited in patients with
ing characteristic curve (AUROC) values in the subset of obesity, ascites, or acute hepatitis. FS has been evaluated exten-
patients with an altered clinical-biochemical panel, in reference sively (Alkhouri et al, 2013; Castera et al, 2013) and is licensed
118 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
in several European and Asian countries, and in the United clinical use, but dozens are currently in clincal trials. Thus
States and Canada. meaningful success seems imminent.
It is important to remember that stiffness can arise from
edema or inflammation, not only fibrosis, and thus interpreta- Reversibility of Fibrosis: “Point of No Return”
tion of the results in the proper clinical context is essential The concept of fibrosis as an irreversible and constantly pro-
because acute hepatitis can yield stiffness values comparable to gressing state is no longer considered accurate. Liver fibrosis of
cirrhosis. Also the ability to perform the test and the accuracy different etiologies is usually reversible by removing the
of data may be reduced in obese patients, although newer causative agent (Friedman & Bansal, 2006). For example, a
probes may overcome this problem. When the FS has been decrease in the viral load of HBV patients, clearance of HCV
combined with the FT in HCV patients, both tests agreed in with pegylated IFN and ribavirin or direct-acting antivirals
70% to 80% of subjects, with increasing concordance in higher (D’Ambrosio et al, 2012; Marcellin et al, 2013) (but not main-
stages of liver fibrosis. Compared with the liver biopsy, results tenance IFN monotherapy [Di Bisceglie et al, 2008]); cessation
were confirmed in 84% to 94% of cases, with a tendency of of ethanol intake; weight loss or bariatric surgery in patients
FS/FT to underestimate fibrosis (Castera et al, 2005). More with NASH (Lassailly et al, 2014; Tai et al, 2012); and decrease
recent studies are focused on assessing its accuracy in NAFLD in iron or copper, or immunosuppressive therapy in autoim-
and NASH (Alkhouri et al, 2013; Kumar et al, 2013). To assist mune diseases have been shown experimentally and clinically
in this effort, an additional technology has been added to FS, to limit fibrosis progression, and to even regress cirrhosis in
called controlled attenuation parameter, which can estimate some patients. In fact, removing the causative agent is still the
liver fat content (de Ledinghen et al, 2012). most effective antifibrotic therapy.
In patients with more advanced disease, assessment of vas- Although fibrosis, inflammation, and bile duct proliferation
cular changes can be highly predictive of outcomes. Specifi- decrease when the damaging stimulus is withdrawn, regenera-
cally, the measure of the pressure gradient across the liver, or tive nodules may become autonomous and grow progressively.
hepatic venous pressure gradient (HVPG), is highly predictive This raises a key question of whether a point of no return exists,
of clinical deterioration (Ripoll et al, 2007). Although invasive, wherein even complete clearance of the underlying disease will
this technique is increasingly incorporated into clincal trials, no longer yield an improvement in cirrhosis. Increased cross-
but efforts are underway to develop noninvasive imaging linking of the collagen fibrils during time makes the fibrous
approaches that can capture the same information as HVPG septa progressively resistant to proteolysis by metalloprotein-
without the need for hepatic catheterization. ases, and hypoxia stimulates secretion of proangiogenic factors
In aggregate, all these noninvasive approaches can accurately by HSCs, such as VEGF and angiopoietin-1, which induce
distinguish between patients with little or no fibrosis and those proliferation and motility (Nakamura et al, 2007). However,
with advanced disease, but these approaches are less reliable at antagonism of VEGF, in particular, may be deleterious, as it
discriminating intermediate stages of fibrosis. They show a high also plays a role in restoration of liver architecture after cessa-
level of variability due to interlaboratory differences, but on the tion of experimental liver injury (Yang et al, 2014). Overall, as
other hand, the patients at risk for false-positive results are well many as 70% of patients with cirrhosis will have regression of
defined. Although the combination of FT, ActiTest (Biopredic- fibrosis once the primary etiology is mitigated, but in those
tiv), and FS, or the ELF panel, in NAFLD patients seem to be whom disease progresses thereafter, there may be a positive
good noninvasive alternatives to liver biopsy, their value in feedback loop between angiogenesis and fibrogenesis, which
individual patient management during time needs to be estab- persists even when the primary etiology is cleared, leading to
lished. These tests may even be superior to liver biopsy at cor- sustained abnormalities of the intrahepatic vasculature.
rectly staging and grading fibrosis (Poynard et al, 2004).
Despite its limitations, to date no single test can match the Prevention of Hepatocyte Apoptosis in Liver Injury
overall information from liver biopsy histology (inflammation, Apoptosis of hepatocytes during liver injury is a proinflamma-
fibrosis, steatosis, architecture). The role of noninvasive alter- tory event associated with Kupffer cell and HSC activation
natives so far lies in improving the fibrosis staging and grading (Canbay et al, 2004). Thus agents have been developed to
made from liver biopsies and, second, in reducing the number minimize apoptotic death of hepatocytes in chronic liver injury
of liver biopsies by screening patients with abnormal liver tests, by inhibiting the caspases that contribute to the apoptotic
to identify patients with a higher probability of liver fibrosis who cascade. In the surgical setting, reduced hepatocyte damage is
need further evaluation or therapy. There is legitimate hope for pursued by decreasing the time of vascular occlusion (Pringle
prognostic value of noninvasive tests and that disease progres- maneuver) during resection or shortening the ischemia-
sion or response to therapy can be assessed by combinations of reperfusion time in transplantsurgery. Experimental approaches
tests that assess serum markers, liver function, vascular changes, to reduce ischemia-reperfusion injury, (e.g., intermittent clamp-
as well as histology. This, however, remains to be clarified by ing or drugs) merit continued development to preserve hepa-
longitudinal studies. tocyte integrity.
Caspase Inhibitors
THERAPEUTIC STRATEGIES
Apoptosis is a functional antagonist to mitosis. Together they
The elucidation of pathways of hepatic fibrogenesis has pro- regulate homeostatic cell turnover. The two main pathways of
vided a rational framework for developing antifibrotic therapies apoptosis are the extrinsic pathway, which is death ligand–
in chronic liver disease (Fig. 7.4). Methods to attack several death receptor–mediated and is dependent on caspase-8, and
points are under development, and it may ultimately be advan- the intrinsic pathway, which is regulated by BCL2-induced
tageous to combine more than one therapy for maximal effi- mitochondrial dysfunction and downstream activation of
cacy. To date, no antifibrotic therapy has been approved for caspase-9 and its effector caspases: 3, 6, and 7. Pan-caspase
Chapter 7 Liver fibrogenesis: mechanisms and clinical relevance 119
Normal Cirrhotic
liver liver
Liver Injury
FIGURE 7.4. Mechanisms by which antifibrotic therapies may lead to fibrosis regression. 1. Disease-specific therapies that control or cure
the underlying disease are still the most effective antifibrotic approach. 2. Targeting receptor-ligand interactions with either established or experimental
drugs to reduce hepatic stellate cell (HSC) activation will attenuate fibrosis development, with multiple potential strategies under development. 3.
Inhibition of the most potent of the profibrogenic pathways, for example, preventing activation of latent TGF-β, or blocking the activity of CTGF, are
among the more promising antifibrotic strategies. 4. Resolution of fibrosis can be promoted by enhancing the apoptosis of activated hepatic stellate
cells either with drugs or through the activity of either NK cells or fibrolytic macrophages, and by increasing degradation of extracellular matrix, or
by preventing its cross-linking with antagonists to LOXL2. ACE-I, angiotensin converting enzyme-I inhibitor; CB1R; cannabinoid receptor type 1;
CTGF, connective tissue growth factor; ET-1, endothelin 1; FXR, farnesoid X receptor; HBV, HCV, hepatitis B and C virus, respectively; LOXL2, lysyl
oxidase 2; mAb, monoclonal antibody; NASH, nonalcoholic steatohepatitis ; NF-κB, nuclear factor kappa B; NK, natural killer; PPAR, peroxisome
proliferator–activated receptor; SVR, sustained virologic response; TGF-β, transforming growth factor-β; TIMP, tissue inhibitor of metalloproteinase;
UDCA, ursodeoxycholic acid. (From Lee YM, et al: Pathobiology of liver fibrosis—a translational success story, Gut 64:830–841, 2015.)
inhibitors are being used to assess the therapeutic effect of the drug should be antiinflammatory. In the 2 weeks of treat-
apoptosis inhibition. In preclinical studies, the pan-caspase ment, AST and ALT levels were significantly reduced in the
inhibitor Z-VAD-FMK was able to reduce mortality in rats with subset of patients with HCV as their underlying disease, without
acute hepatic failure after major hepatic resection (Yoshida affecting the HCV mRNA levels. No adverse events occurred
et al, 2007). Other caspase inhibitors have reduced ischemia- (Pockros et al, 2007). More recent trials of this agent are
reperfusion injury in rodents, decreased fibrogenesis in mice ongoing in different liver diseases. Caspase inhibitors thus far
after bile duct ligation (Canbay et al, 2004), and also decreased are considered safe, as animals with genetic deletions of death
fibrogenesis in a methionine/choline-deficient (MCD) diet– receptors do not show increased spontaneous tumors. None-
induced NASH mouse model. In the latter, hepatic steatosis theless, the potential emergence of tumors following long-term
and fibrogenesis was improved, however, without improvement administration remains a lingering concern.
of liver injury (Witek et al, 2009).
There are currently clinical trials using a pan-caspase inhibi-
Inhibition of Hepatic Stellate Cells Activation
tor for patients with liver disease of different etiologies. This or Inactivation of Myofibroblasts
agent, Emricasan (formerly called IDN-6556), however, also Oxidant stress in the form of ROS released by injured hepato-
inhibits caspase-1, which has an inflammatory effect, and thus cytes through the action of NADPH represents a major
120 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
fibrogenic stimulus. Thus antioxidants including vitamin E Affecting the phosphorylation of CCAAT/enhancer-binding
(Sanyal et al, 2010), silymarin, CYP2E1 inhibitors (Nieto et al, protein (CEBP-B) may lead to caspase activation and enhanced
2002), phosphocholine, cysteamine (Dohil et al, 2011) or HSC apoptosis. CEBP-B is a transcription factor predomi-
S-adenosyl-L-methionine may benefit fibrosis, particularly in nantly expressed in adipose, hepatic, and immune tissue. When
patients with alcohol-induced liver disease and NASH, in which CEBP-B is phosphorylated by ribosomal S-6 kinase (RSK), this
oxidant stress plays an especially important role. In principle, leads to activation of caspase-8, which leads to MFB apoptosis
antioxidants should be efficacious in inflammatory liver disease. (Buck & Chojkier, 2007). Thus activating RSK or caspase-8
However, efforts to establish the activity of antioxidants are directly will lead to MFB apoptosis.
confounded by the uneven quality of commercially available There are also receptor-ligand–mediated pathways of MFB
products, especially as these compounds are typically available apoptosis that are potential therapeutic targets. For example,
over-the-counter and their potency is not monitored. activation of the cannabinoid 1 (CB1) receptor leads to
Given their widespread use in diabetes, PPARγ agonists have increased collagen deposition and protects MFB from apopto-
been tested in clinical trials both in NASH and HCV (Belfort sis, whereas the CB2 receptor is proapoptotic via induction of
et al, 2006), but their activity is modest and is associated with intracellular oxidative stress. Correspondingly, CB1 knockout
unwanted weight gain, especially in patients with NASH mice or CB1 antagonist–treated mice (Teixeira-Clerc et al,
(Sanyal et al, 2010). PPARγ nuclear receptors are expressed 2006), as well as CB2 receptor–stimulated mice, (Munoz-
in HSCs, and PPARγ overexpression can regress MFBs to Luque et al, 2008) display less fibrosis and more MFB apop-
their quiescent state experimentally (Hazra et al, 2004). With tosis than control mice after CCl4 or thioacetamide (TAA)
improved formulation, PPARγ ligands may overcome some of treatment, or bile duct ligation (BDL), and CB2 knockout mice
their unwanted adverse effects in clinical trials and merit further show increased CCl4-induced fibrosis (Julien et al, 2005).
evaluation. Whereas trials of a systemic CB1 receptor antagonist for obesity
WNT signaling has been implicated in pulmonary and renal and NASH were discontinued because of central nervous
fibrosis and has also been reported to promote hepatic fibrosis system (CNS) effects, a new generation of peripheral CB1
by enhancing HSC activation and survival. This suggests that antagonists that do not enter the CNS are under development
WNT antagonism may be a useful target in liver fibrosis and could have a major role as an antifibrotic strategy.
(Boulter et al, 2012; Ren et al, 2013; Zhu et al, 2012), but no NK cells directly interact with the retinoic acid early-1
trials have been conducted, in part because of the complexity (RAE-1) ligand expressed by early activated MFBs and can
of WNT signaling and its divergent activities. lead to apoptosis (Radaeva et al, 2006). This effect is lost,
however, in mature MFBs as these cells lose RAE-1 expression
Induction of Myofibroblast Apoptosis (Radaeva et al, 2007), thereby limiting the potential of thera-
Because the natural resolution of fibrosis leads to apoptosis and peutic NK-cell–mediated MFB death in advanced fibrosis (Gao
clearance of MFBs, approaches that exploit these native path- & Radaeva, 2013).
ways of resolution merit attention. In addition to apoptosis, The adipokines adiponectin and leptin are natural counter-
activated HSCs/MFBs can also revert to an inactivated state, regulators. Leptin is produced by MFBs that contribute to their
driven in part by PPARγ signaling (Kisseleva et al, 2012; activation (Ikejima et al, 2002; Marra, 2002) and has a profi-
Troeger et al, 2012). brogenic effect on MFBs in hepatic injury (Saxena et al, 2002).
One approach to driving MFB apoptosis is TIMP antagonism. In contrast, adiponectin promotes MFB apoptosis (Ding et al,
Because TIMP is antiapoptotic and blocks matrix proteases, 2005) and inhibits liver fibrogenesis in vitro and in vivo
reduced expression or neutralization favors clearance of MFBs (Kamada et al, 2003). Adiponectin may become a useful anti-
through increased apoptosis and enhanced breakdown of scar fibrotic agent, particularly in NASH.
(Iredale et al, 1998). The translation of this approach to humans
will be challenging, however, as human cells appear to have more
Blocking Myofibroblast–Extracellular
enhanced antiapoptotic activity through increased expression of Matrix Interactions
the antiapoptotic protein BCL-2 (Novo et al, 2006). The ECM and MFBs interact in a positive feedback mecha-
NF-κB is a nuclear transcription factor that inhibits apop- nism that could be amenable to therapeutic antagonism. MFBs
tosis of MFBs. Thus any compound that inhibits NF-κB merits interact with ECM via α/β-integrins (Zhou et al, 2004), thereby
evaluation, in particular through the antagonism of JunD decreasing apoptosis and increasing proliferation of MFBs.
(Smart et al, 2006). An example of NF-κB antagonism is bort- This leads to increased collagen type I deposition, which further
ezomib, a proteosomal inhibitor that prolongs the half-life of promotes survival of fibrogenic MFBs (Issa et al, 2003). Thus
inhibitor of kappa B-α (IκB-α), a naturally occurring cytosolic blocking the MFB-ECM interaction could lead to increased
inhibitor of NF-κB (Elsharkawy et al, 2005), preventing it from MFB apoptosis. This has been confirmed by α3β2-integrin
translocating to the nucleus and acting as a transcription factor. disruption with echistatin, neutralizing antibodies, or siRNA
Related compounds, including gliotoxin or sulfalazine, exert (Zhou et al, 2004). Similar studies exploring antagonism of
similar effects by regulating transcription of NF-κB. For integrin α5β6 are ongoing. Related to this has been the pro-
example, treatment of rodents with the NF-κB inhibitor glio- posal to block integrins as a means of attenuating TGF-β acti-
toxin, which with the help of targeting technologies specifically vation (Henderson et al, 2013); such efforts are in preclinical
targets MFBs, selectively induced MFB apoptosis, and acceler- development but have great promise for human studies.
ated regression of fibrosis in experimental liver injury (Douglass
et al, 2008). Further, an NF-κB decoy increased TNF-α– Antagonizing Compounds That Mediate Inflammation
induced MFB apoptosis and decreased carbon tetrachloride As inflammation precedes and stimulates liver fibrosis, the
(CCl4)-induced fibrosis in comparison with the control group use of antiinflammatory drugs has been proposed. A number
(Son et al, 2007). of agents have antiinflammatory activity. For example,
Chapter 7 Liver fibrogenesis: mechanisms and clinical relevance 121
corticosteroids have been used for decades to treat autoimmune chronic hepatic inflammation. The concern regarding use of
hepatitis. Pentoxifylline may exert its antifibrotic activity by TGF-β blocking agents has further increased due to the first
downregulating TGF-β1 and CTGF signaling (Raetsch et al, clinical study using CAT-192, a recombinant human antibody
2002). However, pentoxifylline can upregulate TIMP-1, that neutralizes TGF-β in patients with cutaneous systemic
thereby reducing its antifibrotic effect. It also inhibits NF-κB sclerosis, in which a significant increase in morbidity and mor-
in Kupffer cells, thereby reducing TNF-α production, the tality was shown, with no evidence of a therapeutic effect
impact of which is uncertain. Recent clinical studies of pentox- (Denton et al, 2007; Yingling et al, 2004). Based on growing
fylline in alcoholic liver disease have shown negative results, concerns about systemic TGF-β neutralization, current efforts
and thus there is waning enthusiasm for this agent (Park et al, are directed at local inhibition of TGF-β at the cell surface,
2014). primarily by blocking integrins that participate in cell surface
A more rational antiinflammatory strategy may be the antag- TGF-β activation, as described above.
onism of chemokines because they are increasingly implicated To antagonize PDGF, administration of a PDGF kinase
in human liver disease (Marra and Tacke, 2014). Small-mole- inhibitor with an HSC-selective carrier (mannose-6-phosphate
cule antagonists of chemokine receptors are well tolerated and modified human serum albumin) significantly reduced BDL-
currently in clinical trials based on promising studies in animals induced fibrosis (Gonzalo et al, 2007). Imatinib mesylate
and humans (Ochoa-Callejero et al, 2013). (Gleevec), a clinically used PDGF receptor tyrosine kinase
The renin-angiotensin system may also amplify inflamma- inhibitor, also attenuates proliferation and migration and fibro-
tion and has assumed major importance in the understanding sis in animal models (Gordon & Spiera, 2011; Kim et al, 2012;
of hepatic fibrosis. Angiotensin II is a vasoconstrictive peptide Kuo et al, 2012; Yoshiji et al, 2005), and newer drugs, such as
that is expressed by activated HSC in chronically injured livers nilotinib, show promise as well (Liu et al, 2011). Sorafenib, a
(Bataller et al, 2003b; Paizis et al, 2002). It induces hepatic multikinase inhibitor approved for treatment of liver cancer,
inflammation and stimulates fibrogenic actions of HSCs, also shows antifibrotic activity in animal models (Hong et al,
including cell proliferation, cell migration, secretion of proin- 2013), attesting to the contribution of receptor tyrosine kinases
flammatory cytokines, and collagen synthesis (Bataller et al, such as PGDF-R in fibrosis as well as cancer. However,
2000; Bataller et al, 2003a & 2003c). Inhibitors of this system sorafenib has adverse effects (e.g., rash, diarrhea, hand-foot
have been in clinical use for antihypertensive therapy for a syndrome), which may be acceptable to patients with cancer
substantial time, which makes their use in humans attractive. but will not be acceptable to asymptomatic patients with fibrotic
Preliminary studies in patients with chronic HCV and NASH liver disease. Thus better-tolerated kinase inhibitors are an
suggest a positive effect on fibrosis progression by administering appealing class of antifibrotic compounds.
blocking agents (Colmenero et al, 2009; Oakley et al, 2009; Apart from blocking HSC-stimulating factors, activating
Yokohama et al, 2004). HSC inhibitory factors is yet another possibility. Hepatocyte
Ursodeoxycholic acid (UDCA) has a beneficial effect on growth factor (HGF) inhibits HSC activation, decreases TGF-
fibrosis in primary biliary cirrhosis. Similarly, a nitric oxide– β, and increases HSC apoptosis (Kim et al, 2005). However,
releasing derivative of UDCA reduces inflammation, fibrosis, potential procarcinogenic effects are probable and would limit
and portal pressure in an animal model (Fiorucci et al, 2003). its therapeutic use. Clinical trials with HGF deletion variants
Interestingly, UDCA also activates the pregnane X receptor, and HGF mimetics are underway.
which has antifibrotic properties (Beuers et al, 2009). In rodents, the blockade of the ETA receptor, which leads
More recently, ligands for FXR, another nuclear receptor, to vasocontriction or scar-contraction upon binding of ET-1,
have been developed, which are also antifibrotic in animal and the administration of vasodilators (prostaglandin E2 and
models and in a Phase 2 clinical trial in NASH (Neuschwander- NO donors) have antifibrotic qualities (Feng et al, 2009;
Tetri et al, 2014; Zhang et al, 2009). Larger Phase III trials of Rockey, 2013). At one point, ET receptor blockade was highly
this agent are planned. attractive; however, clinical trials of these drugs for other indi-
cations demonstrated unacceptable liver toxicity (Kenna et al,
Selectively Antagonizing Pathways of Hepatic Stellate 2015), and thus their development was halted until safety con-
Cell Activation cerns can be more thoroughly addressed.
Fibrogenic, proliferative, proangiogenic, vasoconstrictive, and Bone marrow–derived mesenchymal stem cells have an
proinflammatory mediators work synergistically toward hepatic antifibrotic effect—on the one hand, increasing HSC apopto-
fibrogenesis in the setting of chronic liver injury. Thus efforts sis through secretion of HGF, and, on the other hand,
are underway to antagonize the specific mediators driving these by decreasing proliferation of HSCs through release of
pathways. IL-10 and TNF-α upon stimulation by IL-6 from hepatic
Multiple approaches have been directed toward blocking the MFBs (Parekkadan et al, 2007a; & 2007b). This makes stem
profibrogenic TGF-β signaling pathway. The effects of soluble cell therapy an interesting direction for fibrosis therapies.
TGF-β receptor type II (George et al, 1999), TGF-β blocking However, bone marrow–derived mesenchymal stem cells also
antibodies, TGF-β antisense oligonucleotides, or agents that contribute to scar-forming MFBs in various organs, including
interfere with TGF-β downstream signal transduction have the liver (Russo et al, 2006). A key problem with autologous
been assessed experimentally (see Fig. 7.4). Systemically block- and stem cell and bone marrow therapies to date has been
ing the TGF pathway has theoretical limitations, however, their incomplete characterization, such that the exact compo-
because apart from stimulating wound healing and fibrosis, sition of cells being transplanted is not standardized (Moore
TGF-β is also a central inhibitor of uncontrolled inflammation et al, 2014). Therefore a key goal of future studies is to
and essential in inducing epithelial differentiation and in trig- understand and fully control the cellular composition of such
gering apoptosis. This raises safety concerns for the general and therapies to ensure that their effects are predictable and
long-term use of TGF-β inhibition, especially in patients with reproducible.
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2014.
CHAPTER 8
Bile secretion and pathophysiology of biliary
tract obstruction
Henry Anthony Pitt and Attila Nakeeb
123
124 PART 1 LIVER, BILIARY AND PANCREATIC ANATOMY AND PHYSIOLOGY
acids are synthesized from cholesterol via two main pathways: mediated by sodium-dependent and sodium-independent
a classic pathway leads to the formation of cholic acid, and an mechanisms. The sodium-dependent pathway accounts for
alternative pathway results in the synthesis of chenodeoxycholic more than 80% of taurocholate uptake but less than 50% of
acid. The classic pathway is the predominant mode of bile acid cholate uptake (Meier & Stieger, 2002). In recent years, a
synthesis in humans. As a result, 60% to 70% of the bile acid number of transport proteins have been identified that play a
pool consists of cholic acid and its metabolite deoxycholic acid, key role in this process (Fig. 8.1). The bile salt transporter
with chenodeoxycholic acid occurring less commonly in human is termed the sodium-taurocholate cotransporting polypeptide
bile (Holm et al, 2013; Kullak-Ublick et al, 2004). (NTCP), and is exclusively expressed in the liver and located
In plasma, bile acids circulate bound to either albumin or in the basolateral membrane of the hepatocyte. Sodium-
lipoproteins. In the space of Disse within the liver, bile salt independent hepatic uptake of bile acids is mediated primarily
uptake into the hepatocytes is very efficient. This process is by a family of transporters termed the organic anion transporting
polypeptides (OATPs). In contrast to NTCP, these transporters
have a broader substrate affinity and transport a variety of
TABLE 8.1 Composition of Hepatic and Gallbladder Bile organic anions, including the bile salts. OATP-C is the major
Characteristics* Hepatic Bile Gallbladder Bile sodium-independent bile salt uptake system, but OATP-A
also takes up bile acids, and OATP-8 mediates taurocholate
Sodium 160 270
uptake.
Potassium 5 10
Intracellular bile acid transport occurs within a matter of
Chloride 90 15 seconds. Two mechanisms may be responsible for bile acid
Bicarbonate 45 10 transcellular movement: One involves transfer of bile acids
Calcium 4 25 from the basolateral membrane to the canalicular membrane
Magnesium 2 4 via bile acid–binding proteins (Crawford, 1996); the other
Bilirubin 1.5 15 moves cellular bile salts through vesicular transport. In con-
Proteins 150 200 trast, the transport of bile salts across the canalicular membrane
Bile acids 50 150 of hepatocytes represents the rate-limiting step in the overall
Phospholipids 8 40 secretion of bile salts from the blood into bile.
Cholesterol 4 18 Bile salt concentrations are 1000-fold greater within the
canaliculi than in the hepatocytes. This gradient necessitates an
Total solids — 125
active transport mechanism, which is an adenosine triphos-
pH 7.8 7.2
phate (ATP)-dependent process. The ATP-binding cassette
Significant ranges may be seen.
transporter ABCB 11 (formerly known as the bile salt export
*All determinations are milliequivalents per liter, except for pH. pump [BSEP]) plays a key role in this process (Henkel et al,
Hepatocyte Hepatocyte
Bile Canaliculus
Bile Salt ??Biliary Lipid Uptake
Uptake BSEP MDR3
NTCP BS and Intracellular Transport??
HBAB BL BL
BS BS
Na+ BS
MDR1 OATP-A
D/OA
??Bile Salt Intracellular Transport?? Bile D/OA
BRCP
D/OA
BS B
OATPs MRP2 MRP2 OATP-C
BS B, D/OA
BS B
Vesicles
ER/Golgi ER
2013). The ABC transporters mediate the transport of metabo- HEPATIC BILE
lites, peptides, fatty acids, cholesterol, and lipids in the liver, Micelles
intestines, pancreas, lungs, kidneys, brain, and in macrophages. Unilamellar vesicle
Although ABCB 11 is the major transporter for monovalent (phospholipid-rich)
bile salts into the canaliculus, MDR-related protein-2 (MRP2),
a member of the multidrug-resistant protein family, also trans-
ports sulfated and glucuronidated bile salts into the canaliculus.
MRP2 also mediates the export of multiple other organic
anions, including conjugated bilirubin, leukotrienes, glutathi-
one disulfide, chemotherapeutic agents, uricosurics, antibiotics, – H2O
GALLBLADDER
toxins, and heavy metals (Gerk & Vore, 2002).
BILE
Recent studies suggest that bile acids are signaling molecules
that regulate lipid, glucose, and energy metabolism (Li &
Chang, 2015). This function of bile acids is mediated primarily
by the nuclear receptor farnesoid X receptor (FXR) and the Unilamellar vesicle
G-protein–coupled receptor TGR5. Bile acids in the small and (cholesterol-enriched)
large intestine regulate the gut microbiome, incretin secretion,
and fibroblast growth factors 15 and 19 (FGF15/FGF19) pro- Fusion
duction. These FGFs, in turn, modulate lipid, glucose, and
energy metabolism and may play a role in the rapid improve-
ment in glycemic control after gastric bypass surgery. In addi- Large, cholesterol-rich
tion, FXR and TGR5 receptors exist in other tissues, such as multilamellar vesicles
the heart and the kidneys, and therefore may help to explain
the dysfunction that occurs in these organs with biliary obstruc-
tion (Swann et al, 2011).
Obstructive jaundice
↓ Clearance of Endotoxemia
cardiotoxins?
Cardiovascular
system
Renal system Coagulation system
↓ LV ↓ Plasma ↓ Peripheral
function volume resistance
Renal impairment or
acute renal failure
FIGURE 8.4. Obstructive jaundice leads to renal impairment or acute kidney injury. ANP, Atrial natriuretic peptide; LV, left ventricular.
absorption of endotoxins and inhibit anaerobic bacterial growth. degradation product levels before surgery are at increased risk
Endotoxin also causes renal vasoconstriction and redistribution for hemorrhagic complications. In addition to problems with
of renal blood flow away from the cortex, and disturbances in endotoxemia, patients with coexisting cirrhosis often have addi-
coagulation that include the activation of complement, macro- tional problems related to thrombocytopenia from hypersplen-
phages, leukocytes, and platelets (Hunt et al, 1982). As a ism and fibrinolysis. Portal hypertension in patients with
result, glomerular and peritubular fibrin is deposited. This cirrhosis also exacerbates these coagulation disorders.
factor, in combination with reduced renal cortical blood flow,
results in the tubular and cortical necrosis observed in jaun- Immune System
diced patients with renal failure. Surgery in patients with jaundice is associated with a higher
rate of postoperative septic complications compared with those
Coagulation without jaundice, due in large measure to defects in cellular
Disturbances of blood coagulation are commonly present in immunity that make them more prone to infection (see Chap-
jaundiced patients. The most frequently observed abnormality ters 10 and 12). Cainzos and colleagues (1992) have demon-
is prolongation of the prothrombin time. This problem results strated an association between jaundice and altered delayed-type
from impaired vitamin K absorption from the gut, secondary hypersensitivity. Only 16% of 118 patients with jaundice were
to a lack of intestinal bile. This coagulopathy is usually revers- immunocompetent, compared with 76% of 59 healthy con-
ible with parenteral administration of vitamin K. Decreased bile trols, when tested with a panel of seven skin antigens. Several
levels in the small intestine may result in diminished absorption authors have shown impaired T-cell proliferation (Thompson
of other fat-soluble vitamins and fats, which results in weight et al, 1990), decreased neutrophil chemotaxis (Andy et al,
loss and loss of calcium. This latter factor, as well as the earlier- 1992), defective bacterial phagocytosis (Scott-Conner et al,
mentioned increase in circulating endotoxin, may further con- 1993), and suppression of natural killer–cell activity (Lane
tribute to clotting abnormalities. et al, 1996) following bile duct ligation in animals. As men-
In experimental animals, endotoxin affects metabolism of tioned earlier, the ability of the reticuloendothelial system, spe-
factors XI and XII and causes platelet and direct endothelial cifically Kupffer cells, to clear bacteria and endotoxin from the
damage (Hunt et al, 1982). Moreover, endotoxin release in circulation also is reduced in obstructive jaundice. Studies in
patients with jaundice results in a low-grade, disseminated humans also have demonstrated decreased T-lymphocyte pro-
intravascular coagulation with increased fibrin degradation liferation (Fan et al, 1994), decreased expression of adhesion
products. Hunt and colleagues have shown that patients molecules (Plusa e al, 1996), and altered monocyte functions
with jaundice with circulating endotoxin or increased fibrin (Lago et al, 2006).
130 PART 1 LIVER, BILIARY AND PANCREATIC ANATOMY AND PHYSIOLOGY
The absence of bile from the intestinal tract also plays a with extrahepatic bile duct obstruction and 123 nonjaundiced
role in the infectious complications seen in patients with control patients undergoing cholecystectomy. The patients with
obstructive jaundice. Bacterial translocation from the gut is jaundice had only 11% of the skin propylhydroxylase activity
increased in the setting of bile duct obstruction (Deitch et al, of the controls. In the subgroup of patients with jaundice sec-
1990). Obstruction causes a disruption of the enterohepatic ondary to malignancy, propylhydroxylase activity was less than
circulation and results in loss of the emulsifying antiendotoxin 7% of controls. With relief of obstruction, the activity increased
effect of bile acids; therefore a larger pool of endotoxin is to 22% of controls. Interestingly, in patients with jaundice
available within the intestine for absorption into the portal secondary to benign obstruction, the activity increased to 100%
circulation. The combination of reduced or absent bile in of controls.
the intestine and impaired cellular immunity and reticuloen-
dothelial cell function appears to be a major factor contribut- Other Factors
ing to more frequent infective complications in the jaundiced Other problems that face patients with jaundice are anorexia,
patient. weight loss, and malnutrition. Appetite is adversely influenced
Acute cholangitis is a bacterial infection of the biliary ductal by the lack of bile salts in the intestinal tract. In addition,
system, and it varies in severity from mild and self-limited to patients with pancreatic or periampullary malignant lesions
severe and life threatening (see Chapter 43). The clinical triad may have partial duodenal obstruction or abnormal gastric
associated with cholangitis—fever, jaundice, and pain—was emptying, in some cases secondary to tumor infiltration of the
first described in 1877 by Charcot. Cholangitis results from a celiac nerve plexus. Patients with pancreatic or ampullary
combination of two factors: significant bacterial concentrations tumors also may have pancreatic endocrine and exocrine insuf-
in the bile and biliary obstruction. Although bile from the gall- ficiency. This latter problem may further compound other
bladder and bile ducts is usually sterile, in the presence of nutritional defects that, in turn, may exacerbate the immune
common bile duct stones or other obstructing pathology, the deficits of the patient with jaundice.
incidence of positive cultures increases; likewise, instrumenta- Several recent observations suggest that the many physio-
tion of the biliary tree also greatly increases rates of bile colo- logic derangements induced by obstructive jaundice take a long
nization. The most common organisms recovered from the bile time to reverse. For example, Koyama and colleagues (1981)
in patients with cholangitis include Escherichia coli, Klebsiella have shown that hepatic mitochondrial function does not return
pneumonia, the enterococci, and Bacteroides fragilis (Thompson to normal even 7 weeks after relief of obstruction. This same
et al, 1990a). However, even in the presence of high biliary prolonged effect of obstructive jaundice has been noted with
bacterial concentrations, clinical cholangitis and bacteremia lymphocyte, polymorphonuclear, and Kupffer cell function.
will not develop, unless obstruction causes elevated intraductal Therefore even patients who have had temporary relief of
pressures (Lipsett & Pitt, 1993). biliary obstruction via percutaneous or endoscopic stents are
Normal biliary pressures range from 7 to 14 cm H2O. In the likely to remain at risk for significant complications following
presence of bacteribilia and normal biliary pressures, hepatic surgery because derangements in hepatic function are likely still
venous blood and perihepatic lymph are sterile. However, with present at the time of operation. Moreover, a recent analysis by
partial or complete biliary obstruction, intrabiliary pressures Strasberg and colleagues (2014) suggests that preoperative
rise to 20 to 30 cm H2O, and organisms rapidly appear in both jaundice may adversely affect long-term survival in patients
the blood and lymph. The fever and chills associated with with resected pancreatic cancer.
cholangitis are the result of systemic bacteremia caused by
cholangiovenous and cholangiolymphatic reflux. Management
The most common causes of biliary obstruction are choledo- Historically, the only option for the relief of obstructive
cholithiasis (see Chapter 36), benign strictures (see Chapter jaundice was operative intervention; however, with the develop-
42), biliary-enteric anastomotic strictures (see Chapters 31), ment of therapeutic techniques such as percutaneous (see
and periampullary or proximal biliary cancers (see Chapters 49 Chapters 30 and 52) and endoscopic stenting (see Chapter 29),
to 51 and 59). Before 1980, choledocholithiasis was the cause balloon dilation, and endoscopic sphincterotomy, many non-
of approximately 80% of the reported cases of cholangitis. In operative options for the relief of obstructive jaundice are now
recent years, however, malignant strictures have become a fre- available. The surgeon must determine the safest and most
quent cause, especially after the placement of biliary stents. effective therapy for each individual patient and must ade-
Endoscopic cholangiography, percutaneous transhepatic chol- quately prepare each patient for surgery or nonoperative thera-
angiography, and stent placement via either the endoscopic or peutic intervention.
percutaneous route are all known to cause bacteremia, and Patients with obstructive jaundice and those with hepatocel-
these procedures are frequently performed in patients with a lular disease severe enough to cause jaundice are prone to
presumptive diagnosis of malignant obstruction. many secondary problems. Patients with jaundice are at
increased risk for the development of kidney injury, gastroin-
Wound Healing testinal bleeding, infections, and wound complications (see
Delayed wound healing and a high incidence of wound dehis- earlier section on Pathophysiology). Cardiac, pulmonary, and
cence and incisional hernia have been observed in patients with renal function must be considered in every patient undergoing
jaundice undergoing surgery. Patients with obstructive jaundice major abdominal surgery. In addition, special attention must
have decreased activity of the enzyme propylhydroxylase in be focused on the patient with jaundice’s nutritional status,
their skin. Propylhydroxylase is necessary for the incorporation coagulability, immune function, and presence or absence of
of the amino acid proline into collagen, and its activity has been biliary sepsis. Complications related to portal hypertension,
used as a measure of collagen synthesis. Grande and colleagues such as ascites, varices, and encephalopathy, may also develop
(1990) measured skin propylhydroxylase activity in 95 patients in patients with chronic liver disease and cirrhosis, and these
Chapter 8 Bile secretion and pathophysiology of biliary tract obstruction 131
abnormalities may require specific treatment (see Chapters 76 which should include biliary drainage in patients with cholan-
and 79 to 82). gitis in addition to systemic antibiotics.
In cirrhotic patients, clotting abnormalities are often multi-
Cardiopulmonary factorial and include thrombocytopenia secondary to hyper-
In assessing cardiopulmonary status, the patient’s age, history splenism, prolongation of PT and partial thromboplastin time
of recent myocardial infarction, and the presence of congestive (PTT), and fibrinolysis. Vitamin K should be administered if
heart failure, significant valvular heart disease, or a disturbance the PT is prolonged. If no effect is seen and/or if the PTT is
of normal cardiac rhythm all have been correlated with increased also prolonged, fresh frozen plasma should be given. Throm-
operative risk (Goldman et al, 1977). In addition, patients with bocytopenia usually can be managed by intraoperative platelet
severe pulmonary disease may not be candidates for extensive infusions. If the patient has a shortened clot lysis time and
abdominal surgery. hypofibrinogenemia, ε-aminocaproic acid may be indicated.
Renal Pruritus
Patients with jaundice especially those with cirrhosis and chol- Pruritus is often a distressing problem in the jaundiced patient.
angitis, are at increased risk for renal insufficiency. The main- The exact cause of pruritus remains obscure, but increased
tenance of adequate blood volume and the correction of circulating levels of bile salts, histamines, and central nervous
dehydration are extremely important if renal complications are system opiate receptors have been implicated. In some patients,
to be avoided. Fluid management can be quite complex in relief from itching can be obtained by bile salt–binding agents,
patients with jaundice, because both excess and insufficient such as cholestyramine. Various sedatives and antihistamines
fluids may be problematic. Therefore selected patients may also can provide relief of itching in jaundiced patients. However,
benefit from invasive hemodynamic monitoring with central relief of biliary obstruction remains the most effective method
venous catheters and, less commonly, pulmonary artery cath- for managing pruritus, and improvement can occur rapidly
eters, to assist in assessing intravascular volume. after stent placement, although occasionally can take a week
Certain oral bile salts have been shown to be efficacious in or so.
preventing the development of postoperative kidney injury. In
a study by Cahill (1983) 54% of 24 patients with jaundice not Cholangitis
given oral bile salts before surgery were found to have systemic Biliary sepsis also has been identified as a major risk in jaun-
endotoxemia, which was associated with renal impairment in diced patients (see Chapter 43). Cholangitis occurs when
two thirds of the cases. In comparison, none of the 8 patients partial or complete obstruction of the bile duct exists, resulting
with jaundice given 500 mg of sodium deoxycholate every 8 in increased intraluminal pressure and infected bile proximal to
hours for 48 hours before surgery had portal or systemic endo- the obstruction. Patients with cholangitis may present with
toxemia. Moreover, none of these eight patients had evidence right upper quadrant abdominal pain, fever, and/or jaundice
of renal impairment. (Charcot’s triad). Patients with “toxic” cholangitis—Charcot’s
triad plus shock and mental confusion (Reynold’s pentad)—
Nutrition have significant mortality with appropriate antibiotic therapy
Malnutrition is a significant risk factor for surgery in the setting alone and therefore require emergent biliary decompression.
of obstructive jaundice (see Chapter 26). Halliday and col- Gigot and colleagues (1989) identified seven prognostic
leagues (1988) noted that patients who died in the postopera- factors that are indications for urgent biliary decompression:
tive period following surgery for obstructive jaundice had a (1) acute kidney injury, (2) liver abscess, (3) cirrhosis, (4) high
significant reduction in body weight, midarm circumference, malignant stricture, (5) percutaneous transhepatic cholangiog-
total body potassium, and reactivity to skin test antigens prior raphy, (6) female gender, and (7) advanced age. However,
to operation. In a study from Italy (Foschi et al, 1986), enteral emergent surgical treatment is associated with significant mor-
hyperalimentation was found to significantly decrease operative bidity and mortality; therefore both percutaneous and endo-
morbidity and mortality in a group of patients treated with 20 scopic biliary drainage have been proposed as effective therapy
days of preoperative percutaneous biliary drainage. Although for the 5% to 10% of patients with cholangitis who are unre-
most patients with benign biliary problems are adequately sponsive to conservative therapy. Lai and colleagues (1992)
nourished, various degrees of malnutrition are frequently have shown, in a series of 82 patients with severe acute chol-
present in patients with malignant obstruction. Therefore angitis, that endoscopic drainage is associated with a lower
patients with malignant obstructive jaundice should be evalu- morbidity (34% vs. 66%) and mortality (10% vs. 32%) than
ated for evidence of malnutrition and have nutritional support operative drainage. A more complete discussion of the bacteri-
instituted if necessary. ology and antibiotic management of patients with cholangitis
can be found in Chapters 12 and 43.
Coagulation
Patients with obstructive jaundice, cholangitis, or cirrhosis all Preoperative Drainage
are prone to excessive intraoperative bleeding. The most The preoperative relief of jaundice and the reversal of its sys-
common clotting defect in patients with obstructive jaundice is temic effects by either endoscopic or transhepatic biliary
prolongation of the prothrombin time (PT), which is usually decompression has been proposed as a method to decrease the
reversible by the administration of parenteral vitamin K. risk of surgery in jaundiced patients. However, several prospec-
Patients with severe jaundice and/or cholangitis also may tive randomized studies have shown that the routine use of
develop disseminated intravascular coagulation (DIC), which preoperative biliary drainage (PBD) does not reduce operative
may require infusion of platelets and fresh frozen plasma. morbidity or mortality in patients with obstructive jaundice
Reversal of DIC also requires control of the underlying sepsis, (Hatfield et al, 1982; Lai et al, 1994; McPherson et al, 1984;
132 PART 1 LIVER, BILIARY AND PANCREATIC ANATOMY AND PHYSIOLOGY
Pitt et al, 1985; van der Gaag et al, 2010, Wig et al, 1999) patients with periampullary malignancy. Patients with proximal
(Table 8.3). In addition, meta-analyses also concluded that biliary obstruction undergoing major hepatic resection repre-
preoperative biliary drainage increased (P < .001), rather than sent an entirely different subgroup, but a multicenter European
decreased, overall complications from surgery and the drainage study suggests that those requiring right hepatectomy benefit
procedure and provided no benefit in terms of reduced mortal- from preoperative drainage of the future liver remnant (see
ity or decreased hospital stay (Fang et al, 2013, Sewnath et al, Chapters 51 and 103B and C). Preoperatively placed transhe-
2002). In fact, several retrospective studies have documented patic catheters also may be of value in the operating room
a higher incidence of infectious complications (wound infec- during difficult biliary dissections in patients with proximal
tion, pancreatic fistula) and even mortality in patients undergo- biliary tumors or strictures, and they may aid in the placement
ing pancreatic or biliary tract resection after preoperative biliary of long-term transhepatic stents. Finally, preoperative drainage
decompression (Sewnath et al, 2002; Sohn et al, 2000). is required in patients receiving neoadjuvant therapy. In these
A criticism of some of the prospective studies is that the patients, metal stents have fewer problems with cholangitis at
duration of preoperative drainage (10 to 18 days) may have no additional cost (Walter et al, 2015).
been inadequate to reverse the multiple metabolic and immu-
nologic abnormalities associated with severe obstructive jaun- SUMMARY
dice. Both animal and human studies demonstrate that the
recovery of various metabolic and immune functions requires Over the past few decades, tremendous strides have been made
at least 6 weeks to pass after the relief of biliary obstruction in our understanding of bile secretion and our ability to care
(Clements et al, 1993; Kennedy et al, 1994; Thompson et al, for the jaundiced patient. Clinicians now have a better under-
1990b). Similarly, animal studies strongly suggest that return standing of normal bile salt, biliary lipid, and bilirubin physiol-
of bile to the intestinal tract has significant advantages over ogy and can classify the diseases that cause jaundice as defects
external biliary drainage (Roughneen et al, 1986). in normal metabolism. Similarly, investigators have elucidated
Although the data suggest that routine PBD may be of the multiple pathophysiologic effects of jaundice that explain
limited benefit, PBD may have some value in selected patients why jaundiced patients are at risk for increased perioperative
with advanced malnutrition, biliary sepsis, and hilar malignan- morbidity and mortality.
cies that require liver resection (Farges et al, 2013). Regarding
the latter, most of the published data regarding PBD focus on References are available at expertconsult.com.
Chapter 8 Bile secretion and pathophysiology of biliary tract obstruction 132.e1
OVERVIEW
transforming growth factor-β (TGF-β), promote cholangiocyte
Primary liver cancers are among the most rapidly evolving growth along with accrual of molecular aberrations. Impaired
malignant tumors worldwide. An underlying chronic inflamma- deoxyribonuclease (DNA) damage repair (DDR) and tumor
tory liver disease, which precedes liver cancer development for suppressor genes, as well as activation of protooncogenes, cause
several decades and creates a protooncogenic microenviron- malignant transformation together with a deregulated plethora
ment, frequently impairs progress in therapeutic approaches. of key signaling pathways, for instance, cyclooxygenase-2
Depending on the cellular target of malignant transformation, (COX2), phosphatidylinositol-3-kinase (PI3K)/AKT/mTOR,
a large spectrum of molecular and morphologic patterns is (PI3K: Phosphoinositide 3-kinase; AKT: v-akt murine thymoma
observed. As such, it is crucial to advance our existing under- viral oncogene homolog 1/Protein kinase B; mTOR: Mechanis-
standing of the molecular pathogenesis, particularly the genomic tic Target of Rapamycin) epidermal growth factor receptor
heterogeneity of these malignancies, to improve current clinical (EGFR), ERB-B2 receptor tyrosine-kinase receptor (ERBB2),
strategies and patient outcome. This has been achieved for RAS/RAF/mitogen-activated protein kinase (MAPK), hepato-
other cancers, such as breast carcinoma, facilitated by the delin- cyte growth factor, Janus activating kinase/signal transducer and
eation of patient subsets and individualization for precision activator of transcription (JAK/STAT), IL-6, and vascular
therapies. In hepatobiliary cancers, many questions persist as endothelial growth factor (VEGF) (Andersen, 2015; Andersen
to the evolutionary process and cellular origin of the initial & Thorgeirsson, 2014; Marquardt & Andersen, 2014). Interac-
transforming incident, the context of tumor plasticity, and the tion between the epithelial and stromal compartments contrib-
causative features driving the disease. Next-generation sequenc- utes to uncontrolled proliferation, survival, angiogenesis,
ing (NGS) and other novel molecular as well as cytologic/ invasion, and metastasis.
histologic techniques have begun to underline the persistent Many studies have evaluated the role of single genes in CCA
alterations, which may trigger the inherited drug resistance (a (particularly using immunohistochemical techniques), includ-
hallmark of liver, biliary tract, and pancreatic tumors), metas- ing their potential impact in prognosis and as diagnostic markers
tasis, and disease recurrence. However, a complex issue remains (Andersen, 2015; Andersen & Thorgeirsson, 2014; Sia et al,
for interpreting the heterogeneous pool of co-occurring aberra- 2013b). Recent integrative genomics approaches (microarray-
tions in the tumor genotype, in which chromosomal proximity based studies) have broadly assessed molecular factors in CCA
to a causal aberration likely influences, for example, the thera- (Andersen et al, 2012; Oishi et al, 2012; Sia et al, 2013a; Wang
peutic response. In this chapter, we will present a comprehen- et al, 2013). A 238-gene signature was shown to have clinical
sive overview of the molecular achievements that currently are relevance correlating with a high-risk group of patients and
advancing the characterization of hepatobiliary cancers. We will predicted overall and recurrence-free survival (Andersen et al,
focus on biliary tract cancer, that is, cholangiocarcinoma 2012). This prognostic gene signature included 36 independent
(CCA), a broadly treatment-refractory tumor type whose survival genes, which mostly are cholangio specific and repre-
molecular pathogenesis is very poorly understood (see also sent the β-catenin/myelocytomatosis, tumor necrosis factor,
Chapters 9B, 9C, and 9D). We will discuss how genomic and vascular endothelial growth factor receptor (VEGFR)/
achievements can be applied clinically to advance diagnosis and ERBB pathways.
therapy, as well as ultimately improve patient outcome.
Chromosomal Aberrations
MOLECULAR ALTERATIONS IN Several comparative genomic hybridization (array CGH)
CHOLANGIOCARCINOMA studies have been used to examine the chromosomal imbalance
of hepatobiliary tumors. A meta-analysis of five studies ana-
The pathogenesis of CCA is a multistep process (Andersen, lyzed 98 intrahepatic CCA (iCCA) cases and identified common
2015) that often originates in a state of chronic biliary inflamma- chromosomal gains at 1q, 5p, 7p, 8q, 17q, and 20q, as well as
tion and, consequently, biliary damage (cholestasis) triggered by losses at 1p, 4q, 8p, 9p, 17p, and 18q (Andersen & Thorgeirs-
external stimuli. Obstruction of the bile acid results in aberrant son, 2012). McKay and colleagues (2011) analyzed 32 patients
cytokine signaling and promotes cholangiocyte proliferation (7 iCCAs, 13 perihilar cholangiocarcinomas [pCCA] and 12
though the activation of growth factors. Release of proinflam- distal cholangiocarcinomas [dCCA], and they found common
matory mediators, for instance, interleukin-6 (IL-6) and gains among the CCA subtypes at 16q, 17p, 17q, 19p, and
133
134 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
19q. Interestingly, these chromosomal regions encode two (19%), and PBRM1 (polybromo 1) (17%) (Jiao et al, 2013).
important genes: ERBB2/HER2 (chr17q12) and MAP2K2/ Interestingly, the authors determined that 47% of iCCA cases
MEK2 (chr19p13) in the development of hepatobiliary tumors have somatic alterations in at least one chromatin-modifying
and represent favorite drug targets in many clinical trials. In gene, which is not mutually exclusive, and further suggests a
other diseases, single nucleotide polymorphisms (SNPs) have continuum of epigenetic changes. As such, patients with a
been implicated as diagnostic and prognostic markers. Large- mutated IDH gene were found to have a significantly reduced
scale genome-wide association studies in CCA are limited; 3 year survival rate of 33% compared with 81% for patients
however, several such projects have been completed both with wild-type IDH status. These patients, including patients
in hepatocellular carcinoma (HCC) (Li et al, 2012b) and with mutations in chromatin-remodeling factors, may, as a
pancreatic cancer, for instance, the PanScan consortium result of their tumor genotype, experience an altered sensitivity
(Amundadottir et al, 2009; Petersen et al, 2010). Using SNP to drugs, for instance, demethylating agents and histone deacet-
arrays, Sia and colleagues (2013a) analyzed 149 iCCA cases ylase inhibitors.
and identified several focal copy number alterations, including In a recent study that focused on patients with Chinese eth-
gains at 1q and 7p as well as losses at 3p, 4q, 6q, 8p, 9p, 9q, nicity, the authors sequenced the complete exome of seven
13q, 14q, 17p, and 21q. In all, these data show common iCCAs and their surrounding nontumoral tissues (Gao et al,
genetic trends, such as gains on the chromosomal arms 1q and 2014). Interestingly, these patients were all selected as treat-
7p, as well as a tendency for a structural overlap with HCC, ment naïve and, besides, diagnosed without any background
with a gain at 1q, 8q, 11q, and 17q and a loss at 4q, 8p, 13q, liver or biliary diseases. The study showed a range of 7 to 192
and 17p (Andersen & Thorgeirsson, 2012; Marquardt & mutations per tumor, which is comparable to other current
Andersen, 2012). studies. However, the authors found a prevalence of transver-
sions (A : C or G :T variants) compared with transitions (A : G
Detection of Somatic Mutations Following the Era of or C :T variants) at a ratio of 3.7 : 1, including a predominant
Deep Sequencing change of G/C nucleotides. Interestingly, transversions are also
In CCA, deep-sequencing approaches were first used to most frequently described in HCC (Guichard et al, 2012;
describe the genetic variants of liver fluke-related tumors (Ong Huang et al, 2011), suggesting a common origin of at least a
et al, 2012). The authors performed whole-exome sequencing subset of primary liver tumors. A key finding in this study, which
of eight fluke-related tumors and the matched normal tissues. included a prevalence screening of 124 tumors, was a high
They validated their results using Sanger sequencing for a total incidence of activating somatic mutations in the gene for protein
of 206 somatic mutations, affecting 187 genes. The average tyrosine phosphatase nonreceptor type 3 (PTPN3) (41%) (Gao
number of nonsynonymous (protein-altering) variants was 26 et al, 2014), associated with increased expression of the PTPN3
per tumor, ranging from 19 to 34. The predominant somatic protein and disease recurrence. Recurrent alterations were
substitution was a C : G > T : A transition (COSMIC database: found in nine members (PTPRB, PTPRQ, PTPRS, PTPRZ1,
333/545, 61% of cases). Frequent somatic mutations were SBF1, SBF2, MTMR3, and EYA1) of the PTP family, which
found in genes such as TP53 (44.4%), KRAS (16.7%), and increased the overall mutational frequency to 51.6%, and
SMAD4 (16.7%). Additionally, alterations in 10 previously making the PTP family the most affected pathway in iCCA.
unrecognized genes included inactivating mutations in MLL3, Recently, Morris and colleagues (2011) showed that a deletion
ROBO2, RNF43, and PEG3, as well as activating mutations in in protein tyrosine phosphatase receptor type S (PTPRS) led to
the GNAS oncogene. These genes are involved in histone mod- the activation of EGFR and PI3K, two pathways often deregu-
ification, genomic instability, and G protein–coupled signaling. lated in iCCA, implying that the PTP family may represent an
Analysis of 15 non–fluke-associated CCAs (10 iCCAs and 5 important therapeutic target (Table 9A.1).
extrahepatic CCAs) showed, when compared with fluke-related Direct analysis of targeted regions, hot-spot mutations, or
CCA, a distinct genetic pattern that correlated with this panels of cancer-related genes are likely more relevant for
regional-specific risk factor (Chan-On et al, 2013). The study implementation to the clinic. A recent target-specific exome
also included a prevalence screen of 108 CCAs associated with sequencing approach (hybridization-capture libraries) was used
fluke infestation and 101 cases of non–fluke-related etiology. to evaluate 182 cancer-related genes from 28 formalin-fixed
The mean somatic mutational rate of non–fluke-infested CCA iCCA cases (Ross et al, 2014). This study concluded that
was 16 per tumor (range, 1 to 62), a significantly lower muta- actionable genomic aberrations were found in two thirds of the
tional burden compared with fluke-infested tumors, with an examined tumors, suggesting that there is, in at least 67% of
average of 26 somatic variants. In part, this may explain the patients, a potential for genomics-driven approaches to either
elevated risk of disease caused by the parasitic infection. Impor- individualize or influence clinical decision making. Moreover,
tantly, Chan-On and colleagues (2013) identified a significant a NGS-based analysis of 75 CCA cases performed in hot-spot
degree of variation in chromatin-modifying genes, such as regions, representing 236 genes, classified the identified altera-
BAP1 (BRCA1-associated protein 1) (10%) and ARID1A (AT- tions into a few select cellular pathways, including MAPK
rich interaction domain 1A) (10%), as well as confirmed the (35% to 55%), mechanistic target of rapamycin (mTOR) (25%
presence of key somatic mutations in the genes IDH1 (isocitrate to 40%), DNA repair (16% to 45%), chromatin remodeling
dehydrogenase 1) and IDH2. Besides these genetic variants, (15% to 33%), and fibroblast growth factor (5% to 13%) sig-
recurrent mutations were identified in genes AGPAT6, ATP10A, naling (Churi et al, 2014). Interestingly, patients enrolled in
BRPF3, CCT8L2, GPR112, HMCN1, and LRRIQ1. Analysis this study were referred to best-fit clinical trials based on the
of an additional 32 iCCAs, with a mean variant rate of 39 genetic aberrations, including seven cases with wild-type KRAS
somatic mutations per genome (range, 13 to 300), identified (sustained stable disease on erlotinib), one patient with a KRAS
inactivating mutations in multiple chromatin-remodeling mutation (sustained stable disease on pazopanib and tra-
factors, with a high prevalence in BAP1 (25%), ARID1A metinib), two patients with B-Raf proto-oncogene, serine/
Chapter 9A Advances in the molecular characterization of liver tumors 135
TABLE 9A.1 Key Somatic Variants in Liver, Biliary, and Pancreatic Tumors
Target Genes CCA HCC PDAC||
Telomere Maintainence
TERT promoter nr 20%-60% nr
WNT/β-Catenin
CTNNB1, AXIN1/2, APC 0% 2%-35% 9%
Cell Cycle and DNA Repair
TP53 7%-36% 18%-35% 41%-85%
CKN2A/B, CDKs, RB1, ATM 4%-7% 4%-12% 3%-25%
IRF2 0% 0%-5% nr
Apoptosis
TNFRSF10A/B, TRADD, CASP, XIAP, 0%-21% 8%-20% nr
MCL1*
Chromatin-Remodeling Factors
ARID1A 10%-36% 10%-16% 0%-9%
ARID2 nr 2%-18% nr
BAP1 11%-20% nr 4%-25%
MLLs 0%-17% 1%-8% 8%-9%
PBRM1 0%-13% 0%-3.5% 0%-2%
PI3K/mTOR/RAS Pathway
ERBB1-3 0%-25% 0%-10% nr
KRAS 0%-40% 0%-1.5% 90%-100%
NRAS 7%-17% nr nr
HRAS nr 0%-1% nr
RPS6KA3 nr 0%-9% nr
PIK3CA, PIK3C2G 4%-17% 0%-2% 0%-2%
PTEN 7%-11% 0%-2% 0%-9%
TSC1 0%-4% 0%-1% 0%-9%
Epigenetics
IDH1, IDH2, IDH3A 0%-36% 0%-1% nr
Protein Tyrosine Phosphatase
PTPN family 41%-52% nr 0%-2%
FGF Pathway
FGF19 nr 4%-15% nr
FGFR2 0%-14% 0%-2% nr
FGFR2 fusion gene products† 50% nr nr
JAK/STAT Pathway‡
JAK1 nr 0%-9% 0%-17%
IL6R nr 0%-26% nr
IL6ST nr 2%-3% nr
Oxidative Stress Response
NRF2 nr 0%-8% nr
KEAP1 nr 0%-6% nr
TGF-β/SMAD Pathway
TGF-β, TGFBR1/2 0%-4% 0%-1% 0%-6%
§
SMAD4 0%-17% 0%-1% 20%-27%
*Gene amplification found in iCCA.
†
FGFR2 gene fusions with BICC1, KIAA1598, AHCYL1, MGEA5 in iCCA etc.
‡
No somatic variants were reported in iCCA; however, the pathway is commonly activated in more than 50% of iCCA cases.
§
SMAD4 mutations reported in iCCA associated with liver fluke infestation.
||
Overlap of somatic mutations observed in pancreatic cancer with hepatobiliary tumors. Key mutations in PDACs are KRAS, TP53, and SMAD4).
CCA, Cholangiocarcinoma; HCC, hepatocellular carcinoma; iCCA, intrahepatic cholangiocarcinoma; nr, somatic mutation not reported; PDACs, pancreatic ductal adenocarcinomas.
136 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
threonine kinase (BRAF) mutations (reached a partial response 2011). A genome-wide analysis of 28 CCA, which utilized the
on a BRAF inhibitor) and one patient received a c-MET inhibi- Illumina 27K methylation array (Illumina, San Diego), identi-
tor and experienced a significant metabolic response according fied a total of 1610 differentially expressed CpG sites compared
to the fluorodeoxyglucose/positron-emission tomography scan. with adjacent normal tissue (Sriraksa et al, 2013). These CpG
In contrast, two patients with ERBB2 mutations who were loci involved 603 hypermethylated genes, including the homeo-
treated with either trastuzumab or lapatinib experienced no box (HOX) genes and targets of the polycomb repressive
drug efficacy. The limited drug effect may suggest the need for complex 2 (PRC2), EED, and SUZ12, as well as histone meth-
combinatorial therapy to achieve a successful response, inhibit- ylation. In a comprehensive genome-wide analysis of differen-
ing signaling pathways downstream of the primary target, such tially methylated regions (DMRs), Goeppert and colleagues
as the MAPK, PI3K/AKT/mTOR, or prostaglandin E2 (PGE2)/ (2014) evaluated 10 iCCAs and 8 extrahepatic CCAs. Interest-
COX2 pathways. ingly, the authors found a significant enrichment of genes
involved in WNT, TGFb, PI3K, MAPK, and NOTCH signal-
Translocations ing, key pathways commonly altered in iCCA.
Recent NGS data have shown a high prevalence of FGFR2 gene Frequent mutations have been shown in both IDH1 and
fusions reported in CCA, including FGFR2-BICC1 (2/4) (Wu IDH2 (Borger et al, 2012; Wang et al, 2013). Mutations in
et al, 2013), FGFR2-KIAA1598 (1/28) (Ross et al, 2014), IDH are associated with hypermethylation enriched in CpG
FGFR2-TACC3 (1/28) (Ross et al, 2014), FGFR2-AHCYL1 promoter shores, which suggests a global deregulation within
(7/66) (Arai et al, 2014), and FGFR2-MGEA5 (1/6) (Borad the transcriptional program (Wang et al, 2013). In support,
et al, 2014; Graham et al, 2014). Interestingly, Borad and IDH1 was recently emphasized as an epigenetic rheostat that,
colleagues (2014) identified FGFR2 gene fusions in 50% when mutated, was proposed to reshape the genomic landscape
(3/6) of iCCA cases. This is currently the only study to include with a global consequence on the transcriptional machinery,
both transcriptome (RNAseq) and whole-genome sequencing triggering an altered state in the cellular process of differentia-
of tumors from the same patient. Arai and colleagues (2014) tion (Turcan et al, 2012). Importantly, mutations in IDH were
concluded from a cohort of more than 100 CCAs that the recently shown to cause the deregulation of hepatocyte nuclear
FGFR2 rearrangements occurred in approximately 14% (9/66) factor 4a (HNF4a), blocking hepatocytic differentiation and
intrahepatic cases. Interestingly, FGFR2 leads to the activation thus promoting bile duct cancer (Saha et al, 2014).
of MAPK, a pathway activated in the majority of CCA cases. The contribution of chronic liver inflammation alongside an
These data underscore the need to evaluate the efficacy of aberrant epigenetic landscape provides survival signals to the
FGFR inhibitors, such as BGJ398 and PD173074, in CCA. tumor. The cyclin-dependent kinase inhibitor p16 is frequently
Importantly, it was shown that FGFR2 translocations can be silenced by epigenetic modifications and was proposed as a
detected by fluorescence in situ hybridization (FISH) (Graham prognostic marker in patients with primary sclerosing cholan-
et al, 2014), making it a possible diagnostic tool. gitis (Ahrendt et al, 1999), suggesting that this change is an
early event in the malignant process. Also, inflammatory signals,
CONSEQUENCE OF EPIGENETIC ALTERATIONS for instance, v-akt murine thymoma viral oncogene homolog 1/
Protein kinase B (AKT), can trigger the release of cytokines
An aberrant epigenome is a common hallmark of human through the JAK/STAT pathway and promote tumorigenesis
cancers, including the molecular pathogenesis of hepatobiliary (Isomoto et al, 2005; Kobayashi et al, 2005). In fact, the sup-
tumors. Epigenetic mechanisms involved in gene regulation pressor of cytokine signaling 3 (SOCS3), which is silenced by
include histone modification, DNA methylation, and noncod- promoter hypermethylation, is a common target in CCA
ing RNAs. There is limited information related to the impact (Isomoto et al, 2007). Reduced expression of SOCS3 results
of altered histone modifications in the transformation of chol- in activation of IL-6/STAT3 signaling and a subsequent auto-
angiocytes as well as the response of CCA to epigenetic-based crine feedback loop, as well as paracrine signaling within the
therapies. However, in the past few years, NGS studies have tumor microenvironment.
highlighted the likely importance of chromatin-remodeling
factors as well as IDH in hepatobiliary cancer development. Alterations in the Noncoding RNA Landscape
MicroRNAs (miRs) function as critical rheostats of the genome,
Aberrant DNA Cytosine-Guanine Dinucleotide regulating key properties such as cell survival, autophagy, stem-
(CpG) Methylation ness, and response to therapy.A number of studies have inves-
Promoter hypermethylation has been shown in numerous tigated the biologic significance and aberrant expression of
important cancer-associated genes in CCA (Isomoto, 2009; miRs in CCA cell lines (Braconi et al, 2010; Meng et al, 2006;
Sandhu et al, 2008). Epigenetic silencing of tumor suppressor Meng et al, 2008; Mott et al, 2007), demonstrating a link
genes, such as p16INK4a/CDKN2A (17% to 83%), SOCS3 between tumor growth, response to therapy, and expression of
(62%), RASSF1A (31% to 69%), p15 (54%), CDH1 (17% to inflammatory cytokines. Kawahigashi and colleagues (2009)
49%), hMLH1 (19% to 45%), APC (27% to 47%), p14ARF provided the first comprehensive profile of differentially
(19% to 30%), and GSTP1 (15% to 31%) are among some of expressed miRs in iCCA-derived cells (HuCCT1 and MEC)
the most frequent events. compared with normal bile duct epithelial cells (HIBEpiC). A
Studies of DNA methylation have been restricted to select unique 27-miR signature was identified, which included down-
candidate gene approaches. A recent study analyzed 26 selected regulation of 8 miRs (i.e., miR22, miR125a, miR127, miR199a,
genes in 102 liver fluke-related iCCAs and found a unique miR199a*, miR214, miR376a, and miR424) specific to the
promoter hypermethylation of DcR1/Dicer1 and the gene normal bile duct epithelium. (If a microRNA from each arm
encoding: opioid binding protein/cell adhesion molecule-like [-3p or 5p] of the same pre-miRNA hairpin exists in uneven
(OPCML), compared with adjacent tissue (Sriraksa et al, amounts, the least abundant miR is denoted with an asterisk.)
Chapter 9A Advances in the molecular characterization of liver tumors 137
In two recent studies, miRs were profiled in iCCA (Chen et al, on chromosomes, and as such, further assist in the cytologic
2009; Selaru et al, 2009). Selaru and colleagues (2009) showed diagnosis by increasing the overall sensitivity (Barr Fritcher
that the expression level of miR21 could distinguish iCCA from et al, 2014). FISH utilizes fluorescently labeled probes that
normal bile ducts. Also, increasing expression of miR21 cor- bind to a complementary specimen DNA and can be visualized
related with a decreased expression of programmed cell death using a fluorescence microscope. FISH probes can be designed
4 and tissue inhibitor of metalloproteinase 3, suggesting that to specifically demonstrate chromosomal aberrations, such as
miR21 may act as an oncomir. This miR was also found to loss or gain of chromosomes, which indicates potential malig-
regulate phosphatase and tensin homolog-dependent activation nant transformation. In addition, FISH probes can be locus
of PI3K signaling, which affects the chemosensitivity of CCA specific and applied to detect structural variation, such as chro-
(Meng et al, 2006). Another study found a cluster of 38 miRs mosomal amplifications (e.g., HER2 or MET) or translocations
differentially expressed in 27 iCCAs, compared with 10 normal (e.g., anaplastic lymphoma kinase–echinoderm microtubule-
cholangiocytes (Chen et al, 2009). Interestingly, hierarchical associated protein-like 4 or FGFR2). In principle, FISH probes
clustering grouped the clinical samples into two clusters, dis- can be randomly assorted and are only limited by the number
tinguishing the patients according to the level of the CA19-9 of fluorescent signals. Studies evaluating the efficacy of FISH
antigen. This marker is a serum-secreted mucin-type glycopro- analysis in cytopathologic diagnosis have mainly been focused
tein commonly used as a predictor for CCA and shown to be on the UroVysion FISH method (Abbott Molecular, Des
associated with poor prognosis after surgical resection (Huang Plaines, IL). This commercial assay was initially developed for
et al, 2004). In addition, the status of vascular invasion was diagnosis of bladder cancer and contains probes directed
significantly correlated with the patient stratification. Recently, against chromosome 3, 7, and 17, as well as a locus-specific
miR200c was found in iCCA shown to prevent epithelial-to- probe for 9p21 (the INK4 locus, where the genes encoding
mesenchymal transition (EMT) (Oishi et al, 2012). Integrative p16/14 and p15 reside). Several publications have demon-
analysis of miR and gene expression profiles linked miR200c strated that the specificity of FISH in the diagnosis of CCA is
to the expression of neural cell adhesion molecule 1 (NCAM1), the same as that of routine cytology, whereas its sensitivity is
a marker of the hepatic stemlike phenotype. Another microRNA significantly higher (Barr Fritcher et al, 2014; Vasilieva et al,
(miR204) was found in Chinese iCCAs and shown to play a 2012). Because the ancillary UroVysion FISH technique was
critical role in controlling EMT by regulating the expression of not developed directly for CCA, it may be worthwhile to design
Slug, as well as E-cadherin and vimentin (Qiu et al, 2013). an assay that takes into account genetic aberrations more per-
Similarly, inhibition of miR214 was shown to promote EMT tinent to CCA, which likely would increase the sensitivity of
in iCCA cell lines (Huh28 and HuCCT1) by directly targeting the cytopathologic diagnosis. Moreover, FISH analysis can be
Twist (Li et al, 2012a). Further studies of “miR-to-gene” regu- combined, for instance, with measurement of the CA19-9
lation are warranted to determine the contribution of miRs in serum level or analysis of mutations in KRAS, to increase
EMT and iCCA development, their predictive and prognostic accuracy in the diagnosis of CCA (Barr Fritcher et al, 2013;
significance, as well as potential in therapeutics. Kipp et al, 2010). Other techniques involve analysis of cells
obtained from ERCP to measure the DNA content by flow
FUTURE DIRECTIONS FOR MOLECULAR cytometry. In addition, digital imaging analysis has been
ANALYSIS OF CCA described and gives a qualitative account of the cellular con-
stituents using spectroscopic data (Rumalla et al, 2001; Ryan
Molecular analysis of CCA is currently not performed routinely and Baldauf, 1994). However, both of these techniques are
in the diagnosis and clinical management of CCA patients experimental but warrant further evaluation to support their
(Bridgewater et al, 2014). However, we may predict that the value in assisting cytopathologic diagnosis.
growing knowledge of the underlying molecular pathogenesis Similar to supporting the diagnosis of CCA, no molecular
of CCA in the near future will have broad implications in clini- analysis is currently performed with the aim to direct manage-
cal practice and therapeutics. ment of CCA patients, whereas genomics in lung or colon
The diagnosis of CCA may be supported by ancillary molec- cancer routinely is performed to reveal predictive markers in
ular analysis, in particular on cytologic specimens. CCA tends the guidance of targeted therapy. However, it is likely just a
to grow longitudinally along the bile duct system, and therefore question of time before molecular aberrations in drugable path-
it is often difficult to obtain a representative biopsy. As a result, ways, such as KRAS, MAPK/MEK, ERBBs, IL-6/STAT3,
cytologic brushings obtained during endoscopic retrograde IDH1/2, FGFR2, and MET, will be routinely tested in the
cholangiopancreatography (ERCP) is the method of choice in clinic; however, it remains unclear if proteomic profiles as mea-
the evaluation of biliary strictures under suspicion of malig- sured by matrix-assisted laser desorption/ionization imaging
nancy. These specimens are rated by a cytopathologist as (1) mass spectrometry will play a role in patient management in
benign or negative for malignancy, (2) equivocal, or (3) positive the near future (Le Faouder et al, 2014).
for malignancy. However, cytopathologic evaluation of biliary
cells to diagnose a CCA has poor clinical sensitivity, which is IMPLEMENTATION OF NEXT-GENERATION
typically below 50% (Barr Fritcher et al, 2014). In contrast, the SEQUENCING TO THE CLINIC
specificity is nearly 100%. The low sensitivity of cytology using
ERCP brushings can be explained by sampling errors and cyto- The inception of NGS technologies and the accompanying
logic interpretation, which can be difficult, particularly in the opportunities have not only generated great opportunities but
background of chronic inflammation and if only a few tumor also considerable challenges for translational applications in
cells are present in the specimen. cancer research. Besides the associated costs, the amount of
FISH is a cytogenetic technique that can be used to detect generated data and depths of analyses currently exceed the
and localize the presence or absence of specific DNA sequences mainstream ability to interpret and subsequently transform the
138 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
data into useful clinical information (Stadler et al, 2014). culprit cannot necessarily be assumed in hepatobiliary cancers.
Further, application of these technologies for translational This is a concern for future clinical trial designs. Thus, very
applications requires both training and interaction in multidis- large cohorts are required to obtain a sufficient amount of
ciplinary teams consisting of not only health care providers but material for identification and treatment of patients who share
also scientific specialists, such as molecular biologists and bio- a similar molecular profile.
informaticians, as well as patients themselves. The difficulty of During the past decade, a detailed map has been generated
establishing ethically and clinically valid standards for the of the structural variation in the human cancer genome. This
appropriate use of the NGS technology and integration in our map delineates how tumors in general may develop as the
diagnostic pipeline remain a major question and burden consequence of intragenic mutations in roughly 140 genes
(McCarthy et al, 2013). that belong to 12 distinct signaling pathways with common
In primary liver cancer, several problems unique to the cellular processes (cell fate, cell survival, and genome mainte-
disease have to be overcome for successful implementation of nance). Alterations in this framework are major genetic
genomics into clinical routine. First, the application of transla- drivers that promote cellular transformation (Vogelstein et al,
tional genomics requires availability of well-preserved speci- 2013). In the clinic, these genes may represent a tailored
mens in addition to routine pathology, which highlights the NGS panel for routine mutational profiling, which may be
need for mandatory biopsies and, consequently, adaptation of offered as a sensitive diagnostic test and guidance for thera-
current guidelines. Further, molecular and cellular (e.g., peutic decisions.
stromal infiltration) tumor heterogeneity as well as resistance In the past few years, technical progress has greatly advanced
to current treatment modalities might require sequential analy- our understanding of hepatocarcinogenesis by increasing our
sis of the respective genomic landscape to successfully guide knowledge of the molecular complexity and intratumoral het-
individual treatment decisions. The underlying liver disease, as erogeneity. To achieve a paradigm shift toward precision medi-
well as the cellular diversity, might require additional sampling cine in the management of hepatobiliary cancers, multicenter
of the noncancerous microenvironment, which further compli- consortia and international collaborations are crucial for future
cates analysis and, at the end, decisions. success. Given the failure of recent phase 3 trials (Worns and
The spectrum of molecular alterations is highly dependent Galle, 2014), gastroenterology and hepatology will need to
on the ethnicity, etiology, and regional background of the liver reach the “NGS-age.”
disease. As a consequence, significant molecular heterogeneity
is increasingly recognized, corroborating that a clear oncogene References are available at expertconsult.com.
Chapter 9A Advances in the molecular characterization of liver tumors 138.e1
Sriraksa R, et al: Aberrant DNA methylation at genes associated with Vogelstein B, et al: Cancer genome landscapes, Science 339:1546–
a stem cell-like phenotype in cholangiocarcinoma tumors, Cancer 1558, 2013.
Prev Res (Phila) 6:1348–1355, 2013. Wang P, et al: Mutations in isocitrate dehydrogenase 1 and 2 occur
Sriraksa R, et al: CpG-island methylation study of liver fluke-related frequently in intrahepatic cholangiocarcinomas and share hyper-
cholangiocarcinoma, Br J Cancer 104:1313–1318, 2011. methylation targets with glioblastomas, Oncogene 32:3091–3100,
Stadler ZK, et al: Cancer genomics and inherited risk, J Clin Oncol 2013.
32:687–698, 2014. Worns MA, Galle PR: HCC therapies-lessons learned, Nat Rev Gas-
Turcan S, et al: IDH1 mutation is sufficient to establish the glioma troenterol Hepatol 11:447–452, 2014.
hypermethylator phenotype, Nature 483:479–483, 2012. Wu YM, et al: Identification of targetable FGFR gene fusions in diverse
Vasilieva LE, et al: Modern diagnostic approaches to cholangiocarci- cancers, Cancer Discov 3:636–647, 2013.
noma, Hepatobiliary Pancreat Dis Int 11:349–359, 2012.
CHAPTER 9B
Molecular pathology of pancreatic cancer and
premalignant tumors
Jaclyn F. Hechtman and Christine Iacobuzio-Donahue
139
140 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
with other pancreatic carcinomas of the ductal type, and have adenocarcinomas (Adsay et al, 2001) and (2) IPMNs have a
a 5 year survival of 60% (Maire et al, 2002). propensity to be multifocal lesions; therefore patients who
PanINs and IPMNs show some overlapping features. For undergo partial pancreatectomy and are left with a remnant
example, both are inherently intraductal lesions composed pre- pancreas need to be followed for life, even when the lesion
dominantly of columnar, mucin-producing cells that may grow originally resected was a noninvasive IPMN (Sohn et al,
in a flat configuration or may produce papillae; these lesions 2004).20
show a range of cytologic and architectural atypia and can give Genetic analyses of IPMNs have disclosed abnormalities in
rise to invasive adenocarcinomas of the pancreas (Fig. 9B.4E). many of the same genes altered in conventional ductal adeno-
An important feature that distinguishes the two lesions is carcinoma, including mutations in the KRAS2, TP53, and
that PanINs are microscopic lesions and IPMNs are macro- CDKN2A genes, although the frequency and stage of neoplastic
scopic. Nevertheless, recognition of an IPMN and its distinc- progression at which these alterations occur in IPMNs differ
tion from a PanIN lesion is important for two reasons: (1) from PanINs (Hruban et al, 2004; Sessa et al, 1994). For
IPMN-associated colloid carcinomas have a significantly better example, contrary to PanINs, IPMNs harbor KRAS mutations
prognosis than either PanIN- or IPMN-associated tubular in only half of analyzed cases (Amato et al, 2014). Moreover,
abnormalities in SMAD4, which are present in 30% of PanIN-3
and 55% of PDA, are rare in IPMNs (Iacobuzio-Donahue et al,
2000). IPMNs may also contain genetic alterations of genes
1st era 2nd era
that are specific to this form of neoplasia. Activating mutations
in GNAS have been found in more than 70% of IPMNs, and
1988 1994 1996 2000 2005 2010
a subset show genetic inactivation of RNF43 (Amato et al,
2014). Interestingly, correlations between phenotypic differen-
tiation of IPMNs (described later) and mutations have been
identified: GNAS mutations are more common in gastric and
KRAS DPC4 FANC gene
p53 intestinal-type IMPNs than in pancreaticobiliary-type IPMNs,
mutations inactivation mutations
whereas KRAS mutations are more common in gastric and
p16 inactivation Sporadic and familial Pancreatic
pancreatic genome carcinoma pancreaticobiliary type IPMNs (Amato et al, 2014). Molecular
BRAC2 inactivation surveyed sequenced testing of pancreatic cyst fluid for GNAS and KRAS mutations
FIGURE 9B.1. Genetic landmark discoveries in pancreatic cancer may help support a diagnosis of IPMN and distinguish it from
research. The first era is highlighted by the discovery of tumor suppres- other cystic lesions, including neuroendocrine tumors with
sor genes such as DPC4 and loss of p16. The second era is highlighted cystic degeneration, benign pseudocysts, and solid and cystic
by genomic profiling of discovery and validating sets of isolated and pseudopapillary neoplasms. However, a negative result does not
purified tumors from pancreatic cancer patients. rule out mucinous cystic neoplasm (Singhi et al, 2014).
Discovery of core
signaling pathways
disrupted in PDA
Validation studies:
Functional work
Immunohistochemistry on
clinical specimens
FIGURE 9B.2. Simplified flowchart of genetic discoveries performed in the two eras of genetic research. In the first era (left), resected
pancreatic cancers were xenografted, and genomic DNA was isolated for genetic analysis of a region or putative tumor suppressor or oncogene. In
the second era (right), combining advances in equipment and techniques and high-throughput sequencing allowed a genomic survey of the pancreatic
cancer genome. LOH, Loss of heterozygosity; PDA, pancreatic ductal carcinoma; SAGE, serial analysis of gene expression.
Chapter 9B Molecular pathology of pancreatic cancer and premalignant tumors 141
Surgery Surgery
Gemcitabine
Another distinction between PanINs and IPMNs relates to telomeric abnormalities, and epigenetic silencing by methyla-
the expression of the caudal differentiation factor CDX2, a tion of defined promoter DNA sequences. An individual pan-
marker of intestinal differentiation. Most IPMNs express creatic tumor contains on average 63 genetic alterations,
CDX2, in particular IPMNs associated with an invasive colloid primarily point mutations. Only a small subset of these muta-
carcinoma, whereas this is uncommon both in PanINs and in tions is required for tumorigenesis (Jones et al, 2008).
the subset of IPMNs that give rise to invasive cancers resem- The field of analyzing the genetics of pancreatic cancer can
bling ductal adenocarcinomas (Adsay et al, 2004). CDX2 be broken down chronologically (see Fig. 9B.1). First, land-
expression in IPMNs is generally associated with expression of mark studies starting in the late 1980s and spanning nearly two
MUC2, an intestinal epithelial apomucin, whereas the absence decades are highlighted by the discovery of KRAS activation,
of CDX2 expression usually is associated with expression of SMAD4 and BRCA2 mutations, and CDKN2A silencing (see
MUC1, a biliary apomucin, and concomitant lack of expression Figs. 9B.1 and 9B.2, left). Some of these discoveries spurred
of MUC2. These findings have suggested that there may be new lines of investigation in the field of pancreatic cancer as
two divergent pathways of carcinogenesis within the pancreatic well as specific classification of PDA subtypes (Iacobuzio-
ducts (Adsay et al, 2002). The first is a so-called intestinal Donahue et al, 2009). More recently, with the help of advanced
pathway that gives rise to CDX2- and MUC2-expressing DNA sequencing technology, investigators have been able to
IPMNs that progress to the better-prognosis colloid carcino- sequence the entire genomes of various pancreatic cancer sub-
mas. The second is a pancreatobiliary pathway that gives rise types (see Figs. 9B.1 and 9B.2, right).
to CDX2-negative, MUC2-negative, MUC1-expressing PanINs
and a subset of IPMNs, both of which can progress to the Copy-Number Aberrations
poorer-prognosis conventional ductal adenocarcinomas. Although now considered primitive, valuable cytogenetic analy-
sis performed more than a decade ago found that chromosomal
aberrations occur in virtually every pancreatic cancer. Cytoge-
GENETICS OF PANCREATIC DUCTAL netic analyses of pancreatic cancers have shown multiple,
ADENOCARCINOMA nonrandom numeric and structural changes (Griffin et al,
1995; Sirivatanauksorn et al, 2001). The most common
Genomic (DNA) Alterations in Pancreatic Cancer numeric abnormalities include losses of chromosomes 6, 12,
The multitude of genetic abnormalities in pancreatic cancer 13, and 18 and gains of chromosomes 7 and 20. Structural
have many characteristics similar to other solid tumors; thus abnormalities (intrachromosomal break points) frequently
they include point mutations in critical genes, chromosomal involve 1p and 1q, 3p, 4q, 6q, 7q, 17p, 11p, 11q, 15q, 16q,
(copy number) aberrations, mitochondrial DNA mutations, and 19q (Rigaud et al, 2000). The technical limitations of
142 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
A B
C D
E
FIGURE 9B.4. Pathologic features of precursor lesions of pancreatic ductal adenocarcioma (PDA). A, Pancreatic intraepithelial neoplasia
(PanIN). PanIN-1, flat lesion composed of columnar cells with basally located benign-appearing nuclei and supranuclear mucin. B, PanIN2 showing
mild cytologic and architectural atypia, including crowding, nuclear enlargement, and tufting. C, PanIN-3 showing complex papillary architecture with
budding of epithelial cells into lumen and severe cytologic atypia of lining cells. D, Intraductal papillary mucinous neoplasm (IPMN) with low-grade
dysplasia showing well-formed papillae lined by mucin-containing cells. D, IPMN with high-grade dysplasia with complex branching papillae and cells
showing marked cytologic atypia. E, Invasive, moderately differentiated PDA forming angular abortive glands and invading perineural spaces.
Chapter 9B Molecular pathology of pancreatic cancer and premalignant tumors 143
Hereditary breast/ BRCA1 BRCA2 NCCN test criteria require BRCA1: 2.26-fold* Cross-linking chemotherapeutics
ovarian cancer personal or family BRCA2: 3- to 9-fold† (mitomycin C, cisplatin,
syndrome (HBOCS) history of breast and chorambucil, melphalan) PARP
ovarian cancer inhibitors
Peutz-Jeghers STK11 (LKB1) Diagnosis of index case 132-fold; lifetime risk Reports of a PJS- associated cancer
syndrome (PJS) is generally based on ~36%§ with loss of the wild-type STK11
clinical findings/ allele, together with a germline
working definition‡ mutation in the other allele
Some sporadic PDAs exhibit somatic
mutations of STK11||
Hereditary pancreatitis PRSS1, Testing guidelines are 50- to 67-fold; Tumor susceptibility is presumably due
SPINK1, based on symptoms lifetime risk 44%a,b to mitogenic stimulation and clonal
CFTR, CTRC with or without family outgrowth of PDA cells as part of
history of pancreatitis¶ the normal healing responses that
occur subsequent to repeated
rounds of tissue destructionb
FAMM melanoma CDKN2A Documented patients/ 13- to 39-fold† Somatic p16 alterations were identified
syndrome families with multiple in 80% of PDAsc
melanomas
HNPCC-Lynch MLH1, MSH2, Bethesda Guidelines† MSI-H pancreatic cancer may have a
syndrome MSH6, PMS2 (tumor MSI/IHC) and better prognosis after resection,
Amsterdam Clinical possibly because of intensive
Criteria II (germline immunoreaction to the tumord
studies)
Familial adenomatous APC APC is considered in Relative risk 4.46e Some theorize that pancreaticobiliary
polyposis (FAP) individuals with ≥20 Lifetime risk ~2%f secretions affect the development of
colon adenomas adenomas and cancer in this areag
Cystic fibrosis (CF) CFTR Genotyping identifies Relative risk 5.3i Modifier genes or environmental
patients with class IV factors may also be important in
and V mutations, stratifying risk (e.g., mucin genes
which are likely to are found in both CF and PDA)j
represent those with a
functioning pancreash
*From Thompson D, et al: Cancer incidence in BRCA1 mutation carriers, J Natl Cancer Inst 94(18):1358–1365, 2002.
†
From Brand RE, et al: Advances in counseling and surveillance of patients at risk for pancreatic cancer, Gut 56(10):1460–1469, 2007.
‡
From Giardiello FM, et al: Increased risk of cancer in the Peutz-Jeghers syndrome, N Engl J Med 316(24):1511–1514, 1987.
§
From Giardiello FM, et al: Very high risk of cancer in familial Peutz-Jeghers syndrome, Gastroenterology 119(6):1447–1453, 2000.
||
From Su GH, et al: Germline and somatic mutations of the STK11/LKB1 Peutz-Jehgers gene in pancreatic and biliary cancers, Am J Pathol 154(6):1835–1840, 1999.
¶
From Ellis et al: Genetic testing for hereditary pancreatitis: guidelines for indications, counseling, consent, and privacy issues, Pancreatology 1(5):405–415, 2001.
a
From Lowenfels AB, et al: Hereditary pancreatitis and the risk of pancreatic cancer: International Hereditary Pancreatitis Study Group, J Natl Cancer Inst 89(6):442–446, 1997.
b
From Howes N, et al: Clinical and genetic characteristics of hereditary pancreatitis in Europe, Clin Gastroenterol Hepatol 2(3):252–261, 2004.
c
From Rozenblum E, et al: Tumor-suppressive pathways in pancreatic carcinoma, Cancer Res 57(9):1731–1734, 1997.
d
From Nakata B, et al: Prognostic value of microstaellite instability in resectable pancreatic cancer, Clin Cancer Res 8(8):2536–2540, 2002.
e
From Giardiello FM, et al: Increased risk of thyroid and pancreatic carcinoma in familial adenomatous polyposis, Gut 34(10):1394–1396, 1993.
f
From Burt RW: Colon cancer screening, Gastroenterology 119(3):837–853, 2000.
g
From Wallace MH, et al: Upper gastrointestinal disease in patients with familial adenomatous polyposis, Br J Sur 85(6):742–750, 1998.
h
From Krysa J, et al: Pancreas and cystic fibrosis: the implications of increased survival in cystic fibrosis, Pancreatology 7(5-6):447–450, 2007.
i
From Maisonneuve P, et al: Risk of pancreatic cancer in patients with cystic fibrosis, Gut 56(9):1327–1378, 2007.
j
From Singh AP, et al: MUC4 expression is regulated by cystic fibrosis transmembrane conductance regulator in pancreatic adenocarcinoma cells via transcriptional and post-transcriptional mechanisms,
Oncogene 26(1):30–41, 2007.
FAMM, familial multiple mole; HNPCC, hereditary nonpolyposis colorectal cancer; IHC, immunohistochemical; MIS-H, microsatellite instability, high frequency; MSI, microsatellite instability; NCCN, National
Comprehensive Cancer Network; PARP, poly (ADP-ribose) polymerase; PDA, pancreatic ductal adenocarcinoma.
Modified from Showalter SI, et al: Identifying pancreatic cancer patients for targeted treatment: The challenges and limitations of the current selection process and vision for the future, Expert Opin Drug
Deliv 7(3):1–12, 2010.
Table 9B.1; see Familial Pancreatic Cancer section) (van der defects in other FANC genes yet to be thoroughly investigated
Heijden et al, 2004). Unlike most in vivo experiments, xeno- (i.e., FANCA) are the direct cause of some familial and spo-
grafted mice with isogenic cell lines (FANCC deficient and radic PDAs.
proficient) experienced regression of tumor after a single dose
of the available mitomycin C intrastrand cross-linking drug Oncogenes
(van der Heijden et al, 2005). Although other mutations in the Perhaps the best evidence that KRAS activation is an early and
Fanconi complementation group have not yet been described, important event in tumorigenesis that comes from decades of
other than FANN, FANCC, and FANCG, and the frequency research on pancreatic cancer. The KRAS oncogene on chromo-
of these mutations in PDA appear to be low, it is likely that some 12p is the most commonly altered oncogene, with as many
Chapter 9B Molecular pathology of pancreatic cancer and premalignant tumors 145
as 90% of pancreatic cancers containing mutations on codons gene in approximately 30% of pancreatic cancers, which offers
12, 13, and 61 (Caldas et al, 1994b). Activating mutations potential therapeutic benefit because targeted therapies have
impair the intrinsic guanosine triphosphate (GTP)ase activity of been developed that specifically inhibit the growth of MTAP-
the KRAS gene product, resulting in a protein that is constitu- deficient cells (Chen et al, 1996).
tively active in intracellular signal transduction. KRAS mutation As many as 80% of pancreatic cancers contain an inactiva-
happens early in the pathway to oncogenesis, with approximately tion of the TP53 gene on chromosome 17p. Such inactivation
30% of PanIN-1 lesions harboring KRAS mutations (Hruban most often occurs via intragenic mutation combined with loss
et al, 2000; Moskaluk et al, 1997). The first mouse model of of the second allele, although homozygous deletions also occur
pancreatic cancer was generated by constitutive overexpression in some PDAs. The TP53 (p53) protein leads to cell-cycle
of mutant KRAS2 in murine pancreatic ductal epithelium, arrest and activates apoptosis in the presence of DNA damage.
underscoring its importance in pancreatic oncogenesis (Hingo- It is believed that loss of TP53 function allows cells to survive
rani et al, 2003). This model was further developed into a power- and divide, despite the presence of damaged DNA, leading to
ful and useful preclinical model for PDA progression (Hingorani accumulation of additional genetic abnormalities and, eventu-
et al, 2005). Several good sources on mouse modeling and pan- ally, to neoplasia. Nuclear overexpression of the TP53 protein
creatic cancer have been published (Frese et al, 2007; Karreth does not correlate well with mutation status. By immunohisto-
et al, 2009; Olive et al, 2006; Tuveson et al, 2005). chemistry, TP53 accumulation is seen only in the advanced
Rarely, pancreatic cancers with wild-type KRAS genes PanIN-3 lesions, consistent with TP53 being a “late” genetic
harbor point mutations of BRAF, another gene in the event in pancreatic cancer progression (Maitra et al, 2003).
RAS/RAF/mitogen-activated protein kinase (MAPK) signaling PDA cells with a mutant TP53 have been shown to have a
pathway, thereby explaining why mutations of these genes greater propensity for metastases (Morton et al, 2010). Of
occur in mutually exclusive patterns in pancreatic cancer note, in an experimental model, the BRCA2 gene could not be
(Calhoun et al, 2003). This highlights the importance of iden- artificially disrupted in cancer cells with intact wild-type TP53
tifying different molecular targets that lead to similar pathways status (Gallmeier et al, 2007; Hucl et al, 2008).
in pancreatic cancer development and of finding a drug that Inactivation of the SMAD4 gene on chromosome 18q21
can target one pathway, not one gene. Studies have shown that occurs in 55% of pancreatic cancers by homozygous deletions
targeting KRAS may have potential in modulating angiogenesis (30%) or by intragenic mutations and loss of the second allele
in tumorigenesis. Matsuo and colleagues (2009) showed that (25%). Loss of SMAD4 function interferes with intracellular
oncogenic overexpression of KRAS increases production of signaling cascades downstream of the TGF family of cell surface
angiogenesis, promoting CXC chemokines and vascular endo- receptors, leading to decreased growth inhibition and uncon-
thelial growth factor (VEGF) from human pancreatic duct epi- trolled proliferation. Although SMAD4 alterations are most
thelial cells. This upregulation acts through the MAPK pathway common in PDA, they are also frequently seen in other carci-
and c-JUN signaling (Matsuo et al, 2009). KRAS mutation has nomas, occurring in approximately 15% of colorectal carci-
been shown to be associated with increased VEGFA expression noma and 10% of gastric carcinoma (Cerami et al, 2012).
and poorer prognosis in pancreatic carcinoma (Ikeda et al, Similar to TP53, loss of SMAD4 function is a late genetic event
2001). Yet to date, targeting KRAS activation in PDA patients in pancreatic carcinoma progression, with loss of SMAD4 seen
has shown no success. Perhaps KRAS activation is a critical only in a few PanIN-3 lesions (Maitra et al, 2003). Examination
early event in pancreatic tumorigenesis, but once cells become of resected tumor specimens found that SMAD4 inactivation
malignant, there is no need for constitutive KRAS activation, portends a poorer prognosis and greater potential to metasta-
or for oncogenic addiction, for that matter. size (Blackford et al, 2009; Iacobuzio-Donahue et al, 2009).
Other oncogenes implicated in pancreatic cancers include Moreover, in a study of PDA patients who underwent autopsy,
MYC and EGFR, which can be mutated (GNAS) or amplified loss of SMAD4 was highly correlated with extensive metastatic
(MYC) in various subsets of cancers. Overexpression of MYC burden. Identification of downstream targets might allow res-
transcripts occurs in approximately 50% to 60% of pancreatic toration of SMAD4-dependent signaling in pancreatic cancer,
cancers and has been shown to cooperate with KRAS (Aguirre yielding an improved prognosis (Cao et al, 2008).
et al, 2004; Han et al, 2002; Stellas et al, 2014). Several tumor-suppressor genes are inactivated in smaller
numbers (5% to 10%) of pancreatic cancers, including STK11
Tumor Suppressor Genes (chromosome 19p) (Sahin et al, 2003), TGFBR1 (chromo-
CDKN2A, on chromosome 9p, is the most commonly inacti- some 9q), TGFBR2 (chromosome 3p), RB1 (chromosome
vated gene in pancreatic cancers, occurring in 90% of patients 13q) (Jaeger et al, 1997), and MAP2K4 (chromosome 17p) (Su
(Caldas et al, 1994a; Schutte et al, 1997). CDKN2A belongs et al, 1998). MAP2K4 function has been explored in a number
to the cyclin-dependent kinase inhibitor family and inhibits of models, yet the main reason for its loss in pancreatic cancer
cell-cycle progression through the G1-S checkpoint mediated is still unknown (Cunningham et al, 2006).
by cyclin-dependent kinases such as CDK4 and CDK6. Homo- Separately, DNA-level abnormalities in the switch/sucrose
zygous deletions (40%), intragenic mutation with loss of the nonfermentable (SWI/SNF) complex gene member AT-rich
second allele (40%), and epigenetic silencing by promoter interaction domain 1A (ARID1A) have been reported in approx-
methylation (10% to 15%) all contribute to gene inactivation. imately 14% of PDAs in provisional TCGA data, mostly gene
Loss of CDKN2A function occurs throughout the process of deletions and truncating mutations, whereas another 6% of PDA
oncogenesis, with lesions appearing in different PanINs: 30% have decreased messenger RNA (mRNA) ARID1A levels
of PanIN-1A and PanIN-1B, 55% of PanIN-2, and 71% of without corresponding DNA abnormality, suggesting an epigen-
PanIN-3 lesions show loss of nuclear p16 protein expression etic aberration (Biankin et al, 2012; Cerami et al, 2012).
(Wilentz et al, 1998). The CDKN2A homozygous deletions ARID1A and other SWI/SNF members remodel chromatin,
encompass the methylthioadenosine phosphorylase (MTAP) thus controlling the transcription and expression of various
146 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
genes. Abnormalities in ARID1A have been associated with mutations and allelic loss, it has become apparent since the
upregulation of the phosphoinositide-3-kinase (PI3K) pathway 1990s that epigenetic mechanisms of silencing are probably as
as well as sensitivity to PI3K and AKT inhibition (Samartzis important in terms of frequency and prevalence in many cancers
et al, 2014). (Baylin et al, 2000). Epigenetic silencing occurs predominantly
Mixed-lineage leukemia 3 (MLL3 or KMT2C) is a gene through hypermethylation of so-called CpG islands in the pro-
involved in histone methylation and transcriptional coactiva- moter region of tumor suppressor genes, leading to transcrip-
tion. It functions as a tumor suppressor and is recurrently tional abrogation. In cancers, preferential hypermethylation of
mutated in approximately 18% of pancreatic carcinoma, with the promoter occurs in the neoplastic cells with consequent
the most common mutation type being truncating mutations downregulation of gene expression, but this does not occur in
(frameshift and nonsense mutations) (Biankin et al, 2012; the corresponding normal counterpart. Epigenetic silencing is
Cerami et al, 2012). seen frequently in pancreatic cancers and tends to involve genes
that function in tumor suppression or in critical homeostatic
Other Caretaker Genes pathways (e.g., CDKN2A, E-cadherin, retinoic acid β, osteo-
In addition to classic oncogenes or tumor suppressor genes, nectin, SOCS1) or in both (Sato et al, 2003a; Ueki et al, 2000).
caretaker genes (beyond Fanconi anemia–related genes) have Aberrant methylation of genes is also found in precursor
been shown to play a role in oncogenesis. In theory, caretaker lesions of pancreatic cancers and tends to occur in intermedi-
genes do not influence cell growth and proliferation directly but ate- or late-stage lesions (PanIN-2 and PanIN-3) (Fukushima
rather prevent the accumulation of DNA damage and cumula- et al, 2002). Although there has been extensive work on the role
tive mutations within key exonic sequences that make up the of promoter hypermethylation in the pathogenesis of cancers,
human genome. Loss of function of the DNA damage repair more recent data suggest that promoter hypomethylation in
genes (MLH1, hMSH2) occurs in a small subset of pancreatic candidate genes also may be important in cancer development
cancers in the familial setting, but has been reported to occur and progression. Genes showing preferential hypomethylation
in approximately 17% of sporadic, nonfamilial cases (Borelli in pancreatic cancers—SERPINB5, S100P, MSLN, PSCA, and
et al, 2014; Ghimenti et al, 1999; Nakata et al, 2002). Histo- CLDN4—are usually overexpressed in the cancers compared
logically, these microsatellite instability (MSI) cancers com- with healthy pancreas, suggesting that epigenetic mechanisms
prise poorly differentiated cancers with a syncytial growth can affect gene expression in either direction (Sato et al, 2003b).
pattern, expanding tumor margins, extensive necrosis, and Aberrant epigenetic silencing by promoter methylation also
intratumoral lymphocytic infiltrates. This uncommon variant has been reported in IPMNs, including methylation of the
has been termed medullary cancer to distinguish it from the more SOCS1 and CDKN2A genes (Sato et al, 2002). Global analyses
common PDAC (Wilentz et al, 2000b). Although findings in of gene expression in IPMNs have revealed the overexpression
colon cancer have attempted to correlate MSI status with of LCN2, LGALS3, CTSE, CLDN4, and three members of the
response to 5-fluorouracil, other studies have questioned these trefoil factor family, TFF1, TFF2, and TFF3 (Sato et al, 2004a;
claims (Brody et al, 2009a). Terris et al, 2002). These global analyses also have shown that
CLDN4, CXCR4, S100A4, and MSLN all are expressed at
Telomere Length Abnormalities significantly higher levels in invasive IPMNs than in noninva-
Telomeres are hexameric repeats of the sequence TTAGGG at sive IPMNs, suggesting that these proteins may contribute to
the ends of chromosome arms that confer stability to chromo- the process of invasion (Sato et al, 2004b).
somes during cell division and prevent the ends from becoming
“promiscuous” (Gisselsson, 2003). In other words, intact telo-
mere structure guards against chromosomal fusion and thus
Core Signaling Pathways Disrupted in
may prevent chromosomal instability (Greenberg et al, 2005; Pancreatic Cancer
Raynaud et al, 2008). In fact, telomeric dysfunction has been The modern era of molecular biology has progressed to allow
hypothesized to be one of the more important gateways of high-throughput surveying of the pancreatic cancer genome
chromosomal instability, a signature of most solid cancers char- (see Figs. 9B.1 and 9B.2, right), bringing some clarity to our
acterized by aneuploidy and extensive chromosomal rearrange- understanding of the interactions of molecular pathways in
ments. The development of direct visualization of in situ tumorigenesis. This high-throughput analysis revealed that
telomere length was a breakthrough for understanding telomere pancreatic cancers contain an average of 63 genes that are
length abnormalities and cancer development (Meeker et al, genetically altered (Jones et al, 2008). In this work, Jones and
2004). A study by van Heek and colleagues (2002) showed colleagues used a combination of modern molecular techniques
that telomere length abnormalities are one of the earliest to report that 67% to 100% of all pancreatic cancer genomes
demonstrable genetic aberrations in pancreatic cancer, with surveyed had a genetic abnormality in 12 core signaling path-
greater than 90% of the lowest-grade PanIN lesions showing ways and processes. These pathways, confirmed by later studies
marked shortening of telomeres, compared with normal duct as well, include apoptosis, DNA damage control, regulation
epithelium (van Heek et al, 2002). It has been hypothesized of G1-to-S phase transition, Hedgehog signaling, hemophilic
that intact telomeres may serve as “caretakers” in the pancreatic cell adhesion, integrin signaling, c-JUN N-terminal kinase sig-
ducts and that the loss of telomeres in PanIN lesions sets the naling, KRAS signaling, regulation of invasion, small GTPase-
stage for progressive accumulation of chromosomal abnormali- dependent signaling (other than KRAS), TGFB signaling, and
ties, eventually culminating in neoplasia. WNT/NOTCH signaling (Biankin et al, 2012; Jones et al,
2008).
Alternative Genetic Silencing: Epigenetic Abnormalities Recently, genetic aberrations in the axon guidance pathway
Although the classic two-hit hypothesis postulated that tumor genes have been identified in genes in the SLIT/ROBO pathway
suppressor gene silencing occurs by a combination of intragenic (mutations and deletions in SLIT, ROBO1, and ROBO2),
Chapter 9B Molecular pathology of pancreatic cancer and premalignant tumors 147
ephrins (EPHA5 and EPHA7), and class 3 semaphorins (ampli- Identification of mutations in the FANC-BRCA pathway in
fications and mutations in SEMA3A and SEMA3E) (Biankin familial cancers has the potential to shed light on the treatment
et al, 2012). These genes have been implicated in cell growth, of sporadic cancers as well. It has been suggested that perhaps
metastasis, and invasion (Mehlen et al, 2011), overlapping with as many as 25% of sporadic breast and ovarian cancers manifest
some of the pathways listed in the previous paragraph. a BRCA-like phenotype. (Turner et al, 2004). The data have
Unlike certain subtypes of leukemia that are driven by single been derived from BRCA1, FANCC, FANCG, and FANCF
“targetable” oncogenes, we have learned that pancreatic cancers methylation studies (Turner et al, 2004). Further studies are
result from genetic alterations of large numbers of genes that warranted, but future banking of sporadic pancreatic cancers
function through a distinct number of pathways. The study by to study all of the tumor characteristics—posttranscriptional
Jones and colleagues (2008) suggests that it may be beneficial modification, polymorphisms, CGH analysis—along with thor-
to target the physiologic effects of disrupted pathways rather ough analysis of family history may reveal a “BRCAness”
than individual target genes. In fact, targeting multiple path- among certain sporadic pancreatic tumors, aiding in the per-
ways or multiple points in the pathway may be in line with the sonalization of therapy (Martin et al, 2010). Focused DNA-
early preclinical and clinical success stories of the concept of repair microarray analysis may also shed light on other cancer
“synthetic lethality” (Ashworth, 2008). susceptibility genes.
Of note, a recent report demonstrated that PALB2, formerly
FAMILIAL PANCREATIC CANCER known as FANCN, is a gene inherited in a mutant form that
produces a stop codon in a small percentage of familial PDAs.
Approximately 10% of pancreatic cancers show familial aggrega- This gene was discovered to be mutated in 3 of 96 familial
tion (Petersen et al, 2003). The presence of two first-degree pancreatic cancers, each producing a different stop codon
family members with pancreatic cancer confers a 6- to 18-fold (Jones et al, 2009). Truncating mutations in PALB2 were not
increased risk of the disease in other first-degree relatives. This found in any of the 1084 patients of similar ethnicity used as a
risk is increased 32- to 57-fold in families with three or more control cohort in a similar study, thus ruling out a polymorphic
first-degree relatives with pancreatic cancer (Klein et al, 2004; sequence variant. This information suggests that next to
Tersmette et al, 2001). Only a minority of these familial cancers BRCA2, PALB2 is the second most commonly mutated gene
is caused by a recognized cancer syndrome associated with in hereditary pancreatic cancer (Jones et al, 2009). Thus most
germline mutations in known genes. Included in Table 9B.1 are familial pancreatic cancers have no known genetic bases at this
possible “targeted therapies” for the genes and disorders germane time, although many believe an autosomal dominant inheri-
to pancreatic cancer.Thus this table underscores the significance tance of a rare mutant allele is the most likely cause of these
for understanding the inherited lesion that may have contributed cancers. Of apparently “sporadic” (nonfamilial) pancreatic
to the pancreatic cancers found in these families. cancer patients, 7% harbor germline mutations in the BRCA2
For example, as mentioned earlier in this chapter, Fanconi gene, and this low-penetrance pattern is peculiar to cancers
anemia is characterized as a rare, autosomally recessive cancer arising in the Ashkenazi Jewish population (Goggins et al,
syndrome that results initially from a mutation in one of the 1996). Perhaps no single gene is responsible for the other
multiple FANC/BRCA complementation groups in the FANC/ familial forms of PDA, carcinogenesis of which may be the best
BRCA pathway (Mathew, 2006). One gene in this pathway, example that core pathways collaborate with the environment
BRCA2, is associated with a greatly increased risk of cancer (Yeo et al, 2009); thus no single gene from one pathway will
when deleted via a biallelic mutation. The BRCA genes play a prove to be disrupted in the complex process of tumorigenesis
critical role in DNA repair via RAD51 repair pathways (Gud- in this familial form of pancreatic cancer.
mundsdottir et al, 2006). Loss of functional BRCA1 and Several other known genetic syndromes associated with
BRCA2 conveys chromosomal instability to cells by impairing PDA exist, including familial atypical mole and multiple mela-
the critical function of DNA double-stranded break repair noma syndrome (FAMM) and Peutz-Jeghers syndrome (PJS).
(Ashworth, 2008). It has been well established that DNA dam- FAMM results from the microdeletion of CDKN2 on chromo-
aging agents such as mitomycin C or cisplatin effectively kill some 9p21.3, particularly p16INK4a (Gruis et al, 1995; Ranade
cells with loss of BRCA2 or related genes (see Fig. 9B.5) et al, 1995). As a result, CDK4/6 function is uninhibited.
(Hussain et al, 2004). FAMM kindred have also been reported to harbor CDK4 muta-
Currently, poly (adenosine diphosphate-ribose) polymerase tions that prevent CDKN2 binding, as opposed to CDKN2
(PARP) inhibitors have similar promising results as intrastrand microdeletions, in some cases (Zuo et al, 1996). Patients with
cross-linking agents in early-phase trials in other cancer types FAMM have an approximately 80% lifetime risk of melanoma
(ovarian, breast) (Farmer et al, 2005). Certainly, pancreatic and a 20% lifetime risk of PDA (Rustgi et al, 2014). PJS is an
cancer is a logical tumor system in which to test novel PARP autosomal dominant syndrome caused by mutations of the
inhibitors in combination with other DNA-damaging agents. tumor suppressor STK11 (LKB1). This syndrome is best
Targeting the FANC-BRCA pathway with PARP inhibitors known for polyps throughout the small and large intestine with
similarly has been shown to lead to synthetic lethality, creating an arborizing pattern of musculature, and these patients develop
a convenient and fortuitous therapeutic window (Ashworth, various types of carcinoma, including PDA. PDA develops in
2008). The makeup of this therapeutic window relies on the approximately one fourth of patients with PJS by age 75 years
fact that healthy cells will have an intact DNA repair mecha- (Korsse et al, 2013).
nism and thus will be capable of managing and repairing Another condition that may progress to PDA is hereditary
the damage put forth by a DNA-damaging agent. In contrast, pancreatitis. These patients carry germline mutations in the
the tumor will be unable to repair such damage due to loss PRSS1 gene, which encodes cationic trypsinogen. Multiple
of a key aspect of this repair mechanism (i.e., BRCA2; see mutations have been described; the original was R117H, which
Fig. 9B.5). resulted in the elimination of a hydrolysis site in trypsin and an
148 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
inability to inactivate trypsin (Whitcomb et al, 1996). Patients (Lopez de Silanes et al, 2005). It is has been shown that during
with hereditary pancreatitis are at a 35-fold relative risk for times of certain cellular stressors—brought on by agents such
PDA by age 75 years. Diet modification, including lowering as ultraviolet C (UVC) irradiation, heat shock, hypoxia, tamox-
triglyceride intake, as well as abstaining from smoking or drink- ifen (Hostetter et al, 2008), and actinomycin D—HuR can
ing, are advised to decrease the risk of progression to chronic bind to certain apoptotic or survival mRNA transcripts by
pancreatitis. binding to AU-rich elements in the 3′ untranslated region
(UTR) of these mRNAs. In regard to tumorigenesis, HuR has
TRANSCRIPTOMIC (RNA) ABNORMALITIES IN been shown to bind to and stabilize proteins such as p21, p53,
PANCREATIC CANCER and cyclin A (Gorospe, 2003). For instance, Gorospe and col-
leagues (2003) showed that HuR can enhance translation of
Several studies have analyzed pancreatic cancers and compared proteins such as p53 under stress from UVC irradiation. Thus
their gene expression profile with healthy pancreas tissue to HuR’s role in cellular stress and damage gives it a likely pivotal
identify differentially overexpressed and underexpressed genes role in both the tumorigenesis process and in the acute cellular
(Argani et al, 2001a; Crnogorac-Jurcevic et al, 2001; Geng response to chemotherapy in pancreatic cancer cells.
et al, 1998; Iacobuzio-Donahue et al, 2002, 2003a, 2003b; In vitro and in vivo studies have shown that PDAs with HuR
Ryu et al, 2001, 2002). A comprehensive analysis of pancreatic overexpression were dramatically sensitive to gemcitabine, the
cancer using high-density oligonucleotide microarrays identi- standard chemotherapeutic treatment for pancreatic cancer,
fied 217 genes as overexpressed threefold or greater in cancers when compared with a control group (Constantino et al, 2009;
versus healthy tissue (Iacobuzio-Donahue et al, 2003a). Six Richards et al, 2010). Patients who had low cytoplasmic HuR
genes—keratin 19, retinoic acid–induced 3, secretory leukocyte levels had a sevenfold increase in mortality compared with
protease inhibitor, stratifin, tetraspan 1, and transglutaminase patients who had elevated cytoplasmic HuR levels (Fig. 9B.6)
2—were found to be overexpressed in pancreatic cancer by (Constantino et al, 2009).
three platforms: oligonucleotide, cDNA microarrays, and serial
analysis of gene expression (SAGE). The future role of one or MicroRNAs
all of these six genes in early detection or therapy remains to MicroRNAs (miRNAs) are defined as short, noncoding regions
be elucidated. of RNA sequences (22 nucleotides) that can potently regulate
The identification of differentially expressed genes not only gene expression patterns; miRNAs have been shown to regulate
serves the further understanding of the basic biology of pancre- a number of disease- and developmental-related genes, and
atic cancers, it also provides a fertile ground to identify markers they are tissue specific in expression (Rosenfeld et al, 2008).
for early diagnosis, imaging, and novel therapeutic strategies. These miRNA-specific attributes make them putative, power-
Mesothelin (MSLN) was identified by SAGE as a gene over- ful, and unique candidate biomarkers (Mardin et al, 2009).
expressed in pancreatic cancers, and it was confirmed by immu- Discovering the presence of miRNAs in pancreatic cancer may
nohistochemistry to be restricted to the neoplastic epithelium be extremely valuable, although understanding the significance
(Argani et al, 2001b). This identification led to the develop- of these miRNAs may be more difficult and tedious, as miRNAs
ment of a pancreatic cancer vaccine targeted to the mesothelin have been shown to distinguish between various disease states
antigen and the development of antimesothelin antibody- and tissues, including pancreatitis, PDA, IPMN, and healthy
conjugated immunotoxins (Thomas et al, 2004). Phase 1 clini-
cal trials showed that investigated antimesothelin drugs are well
1.0 Cytoplasmic HuR
tolerated, and patients with advanced cancers often achieve
stable disease on antimesothelin therapy (Hassan et al, 2007; High
Hassan et al, 2010). In 2013, the U.S. Food and Drug Admin- + Low
0.8
istration (FDA) granted the antimesothelin drug CRS-207
approval for use in combination therapy with GVAX, a drug + ++ + ++ + +
Proportion alive
Posttranscriptional Regulation
0.4
In recent years, strong evidence has shown that posttranscrip-
tional regulation of genes can directly affect both the tumori-
genesis process (Lopez de Silanes et al, 2003, 2005) and cancer 0.2 +
cell susceptibility to chemotherapy (Brody et al, 2009a; Con- ++
stantino et al, 2009; Gorospe, 2003). Posttranscriptional gene
regulation can have the same effect on gene expression as a 0.0
genetic mutation or methylation of a promoter. One potent 0 200 400 600 800 1000 1200 1400
mechanism of posttranscriptional regulation involves RNA- Days postsurgery
binding proteins. One such RNA-binding protein that has been
FIGURE 9B.6. Tumor human antigen R (HuR) cytoplasmic status can
shown to be important in a number of tumor systems is Hu
stratify pancreatic cancer patients treated with standard-of-care chemo-
antigen R (HuR), a ubiquitously expressed member of the HU therapy (gemcitabine) into two groups: responders (high cytoplasmic
family that mediates cellular response to stress and DNA HuR) versus nonresponders (low cytoplasmic HuR). (From Costantino
damage by posttranscriptional regulation (Hinman et al, 2008). CL, et al: The role of HuR in gemcitabine efficacy in pancreatic cancer:
Elevated HuR cytoplasmic expression is detected in tumors HuR up-regulates the expression of the gemcitabine metabolizing
with poor pathologic features and poor predicted outcomes enzyme deoxycytidine kinase, Cancer Res 69(11):4567–4572, 2009.)
Chapter 9B Molecular pathology of pancreatic cancer and premalignant tumors 149
specimens (Mardin et al, 2009). Further, it has been shown rarely (approximately 3%) harbor TP53 mutations. Instead, the
that a miRNA molecular signature can stratify long- and short- sporadic forms of this tumor frequently harbor death domain–
term survivors (Bloomston et al, 2007). associated protein/gene (DAXX)/alpha-thalassemia X-linked
mental retardation protein/gene (ATRX) mutations (43%) or
multiple endocrine neoplasia type 1 (MEN1) mutations (44%)
MOLECULAR GENETICS OF OTHER (Jiao et al, 2011).
PANCREATIC NEOPLASMS In addition to sporadic forms, pancreatic neuroendocrine
tumors are also seen as a component of various inherited tumor
Acinar Cell Carcinoma syndromes associated with germline mutations, including
Unlike PDA, acinar cell carcinomas (ACC) activating muta- MEN1, due to mutations that cause loss of function of the
tions in KRAS are uncommon (Chmielecki et al, 2014). MEN1 and VHL genes in MEN and von Hippel Lindau syn-
Whole-exome sequencing of 17 ACCs revealed hot-spot–acti- dromes, respectively (Charlesworth et al, 2012; Thakker,
vating mutations, including GNAS p.R201C in two tumors and 2014). PanNETs occurring in association with these syndromes
BRAF p.V600E in one tumor, as well as mutations in tumor are thought to follow a less aggressive course more often.
suppressors, including SMAD4, TP53, retinoblastoma 1 (RB1),
phosphatase and tensin homolog (PTEN), and ARID1A (Jiao FINAL THOUGHTS AND PERSPECTIVES
et al, 2014). In addition to point mutations and indels, SND1-
BRAF fusions were identified in 6 of 44 (14%) either pure or We are currently at an interesting and critical time in studying
mixed differentiation acinar cell carcinomas. Transfectants the molecular aspects of pancreatic cancer. The research com-
expressing this fusion have shown increased MAPK pathway munity has incredible resources at its disposal, ranging from
activity as well as sensitivity to the MAP/extracellular signal- patient databases to complex sequencing equipment. This
regulated protein kinase (ERK) kinase (MEK) inhibitor tra- coming of age of pancreatic cancer research must include sur-
metinib (Chmielecki et al, 2014). Epigenetic changes have also geons, pathologists, molecular biologists, and medical oncolo-
been identified, including microsatellite instability in 10% to gists collaborating toward ultimately better and more personalized
20% of ACCs (Jiao et al, 2014; Liu et al, 2014). patient care. Current research will also need to provide better
early detection markers so that physicians can have more oppor-
Pancreatic Neuroendocrine Tumors tunities to prevent cancer from forming, instead of attempting
Pancreatic neuroendocrine tumors (PanNETs) also have differ- to cure it before it is too late.
ent molecular profiles than either PDAs or ACCs. PanNETs
lack KRAS, SMAD4, and CDKN2A mutations, and only very References are available at expertconsult.com.
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support MKK4 as a genetically targeted tumor suppressor gene, CDK4 in familial melanoma, Nat Genet 12(1):97–99, 1996.
Cancer Res 58(11):2339–2342, 1998.
Terris B, et al: Characterization of gene expression profiles in intra-
ductal papillary-mucinous tumors of the pancreas, Am J Pathol
160(5):1745–1754, 2002.
CHAPTER 9C
Molecular pathogenesis of biliary tract cancer
Jason K. Sicklick and Paul T. Fanta
BILIARY TRACT CANCERS Study Group of Japan, 2000). Intrahepatic tumors have been
subcategorized by their growth characteristics into three groups,
Cholangiocarcinoma (CC), or biliary tract adenocarcinoma, is namely, mass-forming, periductal-infiltrating, or intraductal-
the sixth leading gastrointestinal tumor in the Western world. growing types (Liver Cancer Study Group of Japan, 2000).
First described by Durand-Fardel in 1840 (Olnes & Erlich, Until recently, International Classification of Disease (ICD)
2004), this malignancy arises within cholangiocytes of the codes combined IHCC with hepatocellular carcinoma under
biliary tree. As a result, tumors may occur within the liver (i.e., the code for primary liver tumor (Khan et al, 2002a, 2002b).
intrahepatic cholangiocarcinoma [IHCC]), within the extrahe- But these are clearly different entities, and the second and third
patic biliary tree (i.e., extrahepatic cholangiocarcinoma editions of the International Classification of Diseases for
[EHCC]), or within the gallbladder (i.e., gallbladder cancer Oncology (ICD-O-2/3) have attempted to correct for this issue.
[GBCA]). Together, these biliary tract cancers constitute a rare However, in ICD-O-2, Klatskin tumors were assigned a unique
set of malignancies with poor prognoses. Patients diagnosed histology code, but this was cross-referenced to the topography
with these tumors often are seen late in their clinical course, code for intrahepatic rather than extrahepatic tumors. Under
and chemotherapeutic regimens lack significant response rates. the third ICD-O-3 edition, Klatskin tumors are cross-
As a result, in patients with advanced disease treatment goals referenced to either location (Khan et al, 2012). In addition to
are often palliative in nature (Ishak et al, 1994) (see Chapters the aforementioned coding issues, many tumors previously
47, 49, 50, and 51). Due to the rarity of these entities, as referred to as liver adenocarcinoma of unknown primary site were
well as their common cell of origin, treatment for all three likely unrecognized IHCCs. Together, these changes in ICD-
tumor types has been identical. However, with fairly recent classification have influenced observed changes in the incidence
developments in next-generation sequencing (NGS) and other rates of IHCC and EHC.
molecular techniques, differentiation among these tumor types
can be refined into distinct diseases with unique genetic signa- EPIDEMIOLOGY
tures. Examination of these molecular signatures may be impor-
tant in clinical trial design using drugs targeting specific Although rare, CC has a distinctly higher incidence in certain
pathways. demographic groups and geographic regions (see Chapters 50,
51, and 59). The peak incidence of CC is the seventh decade
CLASSIFICATION of life, with a slightly higher male predilection (Olnes & Erlich,
2004). The annual reported incidences of IHCC and EHCC
The vast majority of biliary tracts tumors are adenocarcinomas in the United States are each approximately 0.6 to 1.0 cases
(Nakeeb et al, 1996), and they most often arise at or near the per 100,000 people (Welzel et al, 2006), with an estimated
hepatic duct confluence. The latter fall under the general cate- 5800 new cases each year. Interestingly, U.S. Surveillance, Epi-
gory of EHCCs (see Chapter 51), which are now further subclas- demiology, and End Results (SEER) data suggest that age-
sified in the current American Joint Committee on Cancer standardized incidence rates (ASIR) for IHCC gradually rose
seventh edition (Edge, 2010) and National Comprehensive from 0.59 per 100,000 people in 1990 to 0.91 in 2001 (Khan
Cancer Network (NCCN) guidelines as perihilar cholangiocarci- et al, 2012). This was followed by a sharp fall before plateauing
noma, or Klatskin tumors, after the Yale University pathologist at 0.60 per 100,000 people in 2007. The ASIR for EHCC
who was one of the first to report a series of patients with this remained relatively stable at approximately 0.80 per 100,000
condition, and distal cholangiocarcinoma (Benson et al, 2014). people until 2001. It then began increasing to 0.97 per 100,000
Bismuth (1992) further categorized perihilar cholangiocarcino- people in 2007. These trends coincide with a switch from
mas by their precise location with reference to the biliary bifurca- ICD-O-2 to ICD-O-3 in 2001. Therefore, although the inci-
tion and the hepatic lobar ducts. This classification is most useful dence of EHCC has remained constant, the incidence of IHCC
for descriptive purposes and for operative planning. In contrast has increased in the United States.
to the perihilar tumors, the distal cholangiocarcinomas account Outside of the United States, CC incidence rates vary mark-
for a relatively small fraction of all bile duct tumors, and midbile edly, presumably reflecting differences in infectious causes, envi-
duct tumors are even rarer (see Chapter 59). Finally, less com- ronmental risk factors (i.e., sedentary lifestyles, alcohol,
monly seen than the aforementioned is disease that has diffuse smoking, and diet) exposure to toxic chemicals, and genomics.
involvement of the entire biliary tree. The highest disease incidence rates are in northeast Thailand
Cholangiocarcinoma may also arise from the intrahepatic (96/100,000 men), where it occurs approximately 100 times
bile ducts, giving rise to the subgroup known as intrahepatic or more often than in the West. For uncertain reasons, epidemio-
peripheral cholangiocarcinoma (see Chapter 50) (Liver Cancer logic studies have shown that the mortality of intrahepatic
150
Chapter 9C Molecular pathogenesis of biliary tract cancer 151
biliary tract neoplasms is rising globally, but those of extrahe- IHCC, the authors concluded that these conditions might
patic tumors are static or falling. Examination of the World explain the divergent incidence trends of IHCC and EHCC.
Health Organization mortality data for the United States, These data also support an earlier report by Palmer and col-
United Kingdom, France, Italy, Japan, and Australia from 1979 leagues who performed a literature review and meta-analysis of
to 1998 (Ishak et al, 1994) demonstrates that mortality rates for case-control studies on IHCC, demonstrating that major risk
IHCC were increased in both sexes in all countries except factors for this cancer include cirrhosis, chronic hepatitis B and
among Japanese women. More recently, a U.S. study examined C, alcohol use, diabetes, and obesity (Palmer et al, 2012).
trends in IHCC incidence using data from the SEER program, Based upon the aforementioned predisposing factors, a
which represents greater than 10% of the total United States common theme of chronic biliary epithelial inflammation
population. Data from 1976 to 2000 were analyzed by age, sex, appears to be a predisposing factor for the development of
and ethnicity. The incidence of IHCC increased by 165%, from biliary tract cancers. Primary sclerosing cholangitis (PSC; see
0.32 per 100,000 (1975 to 1979) to 0.85 per 100,000 Chapter 41) is the most common condition predisposing to
(1995 to 1999). This increase was reflected in all groups but was CC, with rates of 8% to 40% reported in patients with PSC
highest in black men (139%), followed by white men (124%) (Khan et al, 2002a). Compared with sporadic cases, PSC
and white women (111%). The increased incidence may be patients tend to be seen with CC earlier in life (e.g., most com-
attributable, in part, to increased detection (Olnes & Erlich, monly in the 30- to 50-year-old age groups) (Bergquist et al,
2004). However, increased detection of a tumor is usually asso- 1998; Pitt et al, 1995). Experimental and epidemiologic data
ciated with an increase in the proportion of patients with early- also suggest a pathogenic association between CC and liver
stage disease or smaller tumors. But the rise in intrahepatic fluke infestation, especially Opisthorcis viverrini and, less defini-
cancers was not associated with a significant change in the pro- tively, Clonorchis sinensis (see Chapter 45) (Watanapa, 1996).
portion of early-stage cancers, histologically confirmed tumors, Congenital abnormalities of the biliary tree, congenital hepatic
or smaller lesions (Broome et al, 1996). Furthermore, the inci- fibrosis, and choledochal cysts (cystic dilatations of the bile
dence did not seem to be plateauing, as would be expected ducts), also carry a 15% risk of malignant change after the
if the increase were due to an improvement in diagnostic modal- second decade of life, with an average age of onset at 34 years
ities, such as magnetic resonance imaging and computed (see Chapter 46) (Scott et al, 1980). Furthermore, with
tomography (Khan et al, 2002a; Shaib & El-Serag, 2004; Taylor- untreated choledochal cysts the risk increases to 28% (Lipsett
Robinson et al, 2001). Conversely, the incidence of EHCC has et al, 1994; Ohtsuka et al, 2001). Biliary stasis, reflux of pan-
shown no such change and may be declining. According to creatic juice, activation of bile acids (van Mil et al, 2001), and
SEER data, U.S. age-standardized mortality rates for extrahe- deconjugation of carcinogens are also speculated as mechanistic
patic tumors fell from 0.6 per 100,000 in 1979 to 0.3 per drivers of carcinogenesis related to the theme of chronic inflam-
100,000 in 1998; and age-standardized incidence rates decreased mation. Finally, biliary adenomas and papillomatosis have been
from 1.08 per 100,000 to 0.82 per 100,000 in the same period. associated with the development of CC.
Despite improved imaging modalities, most patients are seen
with unresectable disease and typically die within 12 months of Biology of Clinical Risk Factors
diagnosis. In addition to a lack of highly efficacious systemic Several underlying mechanisms play a role in the induction of
therapies, sepsis from cholangitis, frequently related to inter- chronic biliary inflammation and cholestasis.
ventions performed for biliary obstruction and progressive liver
failure, contribute to the high mortality (Shaib & El-Serag, Bile Content and Deconjugation of Xenobiotics
2004). Although biliary tract tumors remain relatively rare, Polymorphisms in bile salt transporter proteins (i.e., BSEP,
there has been increased interest in studying the biology of ATP8B1, and ABCB4) can lead to unstable bile content and
these diseases in recent years (Khan et al, 2002a; Patel, 2001, deconjugation of environmental toxins (i.e., xenobiotics) previ-
2002; Taylor-Robinson et al, 2001). ously conjugated in the liver (Jacquemin, 2001; Meier et al,
2004; Thompson & Strautnieks, 2001). In the background of
CHRONIC BILIARY INFLAMMATION AND congenital bile duct abnormalities, this process increases the
CHOLESTASIS risk of CC (Kubo et al, 1995). Individuals who are heterozy-
gous for bile salt transporter polymorphisms are thought to
Clinical Risk Factors have an increased predisposition to CC as adults, following
Reported risk factors for biliary tract cancers comprise a diverse exposure to cofactors that result in chronic inflammation in the
group of conditions that include infectious causes, congenital biliary tree (Kubo et al, 1995).
conditions, inflammatory diseases, drugs, environmental expo-
sures, and toxins (Patel, 2014). In a study of the SEER data- DNA Mutagens
base, Welzel and colleagues found that in addition to established Promutagenic deoxyribonuclease (DNA) adducts have been
risk factors (e.g., choledochal cysts and cholangitis), biliary identified in CC tissue, indicating exposure to DNA-damaging
cirrhosis, cholelithiasis, hepatolithiasis, alcoholic liver disease, agents (Khan et al, 2003). Thorotrast, a radiologic contrast
nonspecific cirrhosis, diabetes, thyrotoxicosis and chronic pan- agent banned in the 1960s, has been strongly associated with
creatitis, obesity, chronic nonalcoholic fatty liver disease the development of CC many years after exposure and may
(NAFLD), hepatitis B virus infection, hepatitis C virus (HCV) increase the risk of cholangiocarcinogenesis 300-fold (Hardell
infection, human immunodeficiency virus infection, and et al, 1984; Sahani et al, 2003; Shaib & El-Serag, 2004). Expo-
smoking were associated with the development of these tumors sures to byproducts from the rubber and chemical industries,
(Welzel et al, 2006). Given that three of these factors (i.e., HCV including dioxins and nitrosamines (Sorensen et al, 1998), as
infection, chronic NAFLD, and obesity) have increased in inci- well as those from alcohol and smoking (Chalasani et al, 2000),
dence in the United States and were only associated with have been implicated.
152 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Tumor-Stromal Interactions
Hedgehog (Hh) PDGF
Notch PLK
the interaction between environmental factors and host genetic glycosylase (NEIL)1 genes encode DNA glycosylases involved
factors. Most of the putative environmental risk factors for CC in repair of oxidative base damage, and mutations in these genes
result in chronic biliary inflammation leading to repair mecha- are associated with CC.
nisms and, ultimately, carcinogenesis.
Conceptually, exposure to an inflammatory stimulus would Activation-Induced Cytidine Deaminase
not have the same effect on each cell due to changes in perfu- Other work has also suggested that chronic inflammation can
sion (e.g., centrilobular versus periportal), as well as differen- play a critical role leading up to cholangiocarcinogenesis.
tial levels of cytochrome P450 expression, exposure to bile salt Komori and colleagues (2008) found that the proinflammatory
concentrations, and exposure to inflammatory components cytokine-induced aberrant production of activation-induced
(e.g., cytokines and immune surveillance cellular components, cytidine deaminase (AID), a member of the DNA/RNA-editing
such as Kupffer cells and hepatic stellate cells) (see Chapters 7 enzyme family, might link bile duct inflammation to an
and 10). Based on this, the concept of heterogeneity can be enhanced genetic susceptibility to mutagenesis that leads to
inferred where distinctive clonal populations may arise based CC. Ectopic AID production is induced in response to tumor
upon differential response to stimuli. In this section, we review necrosis factor-α (TNF-α) stimulation via a nuclear factor
the underlying host factors associated with bile tract cancers. kappa B (NF-κB)–dependent pathway. Aberrant expression of
AID in biliary cells results in the generation of somatic muta-
Genetic Polymorphism at Cytochrome P450 tions in tumor-related genes, including tumor protein 53
Genetic polymorphisms exist in the cytochrome (CYP) P450 (TP53), c–myelocytomatosis viral oncogene (c-MYC), and the
enzyme complex, a large family of constitutive and inducible promoter region of the cyclin-dependent kinase inhibitor A
enzymes that play a central role in the oxidative metabolism of (CDKN2A) sequences. In human tissue specimens, reverse
both environmental toxins and endogenous compounds. These transcription polymerase chain reaction analyses revealed that
polymorphisms play a critical role in how endogenous and AID was significantly increased in 28 of 30 CC tissues (93%),
exogenous toxins are biotransformed by the liver. Similar to whereas only trace amounts of AID were detected in the normal
many other cancers, which rely upon a sequence of chronic liver. Immunohistochemistry showed that all of the CC tissue
injury and repair, the development of CC may be partially regu- samples examined showed overproduction of endogenous AID
lated by the host ability to respond toxic insults. protein in cancer cells. Moreover, immunostaining for AID was
Several CYPs are involved in metabolism of oxysterols, detectable in 16 of 20 bile epithelia in PSC.
which are cholesterol oxidation products whose expression may
be dysregulated in inflammation-related diseases, including Human CYP1A2 and Arylamine N-Acteyltransferases
cancer. A recent study focused on CYP39A1, which can metab- (NAT1 and NAT2)
olize 24-hydroxycholesterol and plays an important role in the The CYP1A2, NAT1, and NAT2 genes have been shown to
inflammatory response and oxidative stress (Khenjanta et al, be potential modifiers of an individual’s susceptibility to
2014). Immunohistochemistry showed that 70% of CC patients certain types of cancers. Prawan and colleagues (2005) evalu-
had low CYP39A1 expression, which correlated with metasta- ated the relationship between CYP1A2, NAT1, and NAT2
sis. In the setting of Opisthorchis-associated CC, the expression polymorphisms in Thai patients with CC. A total of 216 CC
and function of CYP2A6 and CYP2E1 were altered in the livers patients and 233 control subjects were genotyped using PCR.
of 13 patients (Yongvanit et al, 2012). This report provides Two CYP1A2 alleles (CYP1A2*1A wild type and *1F), six
evidence that enhanced CYP2A6 activity and diminished NAT1 alleles (NAT1*4 wild type, *3, *10, *11, *14A, and
CYP2E1 activity may be involved in the progression of CC. *14B), and seven NAT2 alleles (NAT2*4 wild type, *5, *6A,
Finally, recent molecular profiling of EHCC specimens dem- *6B, *7A, *7B, and *13), were analyzed. The CYP1A2*1A/*1A
onstrated significant enrichment of CYP-metabolic pathways, genotype conferred a decreased risk of the cancer (adjusted
including transcription factors such as glutathione-S-transfer- odds ratio [OR], 0.28; 95% confidence interval [CI], 0.08 to
ase α1 (GSTA1) and GSTA3, which may cause abnormal gene 0.94), compared with CYP1A2*1F/1*F. Frequency distribu-
expression and tumorigenesis through CYP450-metabolic tions of rapid NAT2*13 and two slow alleles, *6B and *7A,
pathways (Qi et al, 2014). Therefore differential CYP activity were associated with lower CC risk. This study suggests that
may be involved in the initiation and/or progression of disease the NAT2 polymorphism might be a modifier of individual
via modulation of chronic inflammation, viral hepatitis, para- risk of CC.
sitic infestation, and recurrent cholangitis (Khan et al, 2005).
Trefoil Factor Family
MRP2/ABCC2 Trefoil factor family 1 (TFF1) is critical for mucosal protection
Hoblinger and colleagues (2009) reported that multidrug and tumor suppression in the stomach. To examine its role in
resistance–associated protein 2 (MRP2/ABCC2) is one of the cholangiocarcinogenesis, specimens with varying degrees of
adenosine triphosphate-binding cassette (ABC) transporters dysplasia were examined. These included IHCC as a result of
expressed on the apical membrane of hepatocytes and cholan- hepatolithiasis, biliary epithelial dysplasia with hepatolithiasis,
giocytes. ABCC2 plays an important role in the biliary clear- hepatolithiasis without dysplasia or carcinoma, IHCC without
ance of endogenous and exogenous toxic compounds. The hepatolithiasis, and control normal livers (Sasaki et al, 2003).
ABCC2 variant c.3972C>T in exon 28 has been shown to be TFF1 expression in the biliary epithelium was increased in
associated with the risk of carcinogenesis. hepatolithiasis compared with control livers (P < .01). In biliary
epithelial dysplasia and noninvasive IHCC with hepatolithiasis,
MUTYH and NEIL1 TFF1 was extensively expressed, and MUC5AC gastric mucin
Forsbring and colleagues (2009) recently found that the human was usually colocalized with TFF1. However, TFF1 expression
mutY DNA glycosylase (h-MUTYH) and Nei-like DNA was significantly decreased in invasive IHCC, despite preserved
154 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Mitogenic Factors
Identification of these mitogenic stimuli with resultant increases
in DNA, RNA, protein synthesis, as well as increases in immune Extrahepatic
modulation, have been implicated in the carcinogenesis of FIGURE 9C.2. Common gene expression alterations in biliary tract
biliary tract tumors. The liver fluke Opisthorchis viverrini can cancers. A Venn diagram is used to depict the relationship of transcrip-
generate mitogenic substances, such as glutathione-S-transfer- tional changes among biliary cancer subtypes. There were 165 common
ase (GST), which act as a secretory product that may play an genes with significantly altered expression in intrahepatic cholangiocar-
important role in promoting the genesis of CC. GST has a cinoma, extrahepatic cholangiocarcinoma, and gallbladder cancer.
proliferative function on NIH-3T3 murine fibroblasts and
MMNK1 nontumorigenic human bile duct epithelial cells in a
dose-dependent manner with subsequent in vitro activation of Malignant Transformation
both phospho-AKT (v-akt murine thymoma viral oncogene Gene Expression Analysis
homolog 1) (pAKT) and phospho-ERK (extracellular signal- In 2009, Miller and colleagues (2009) investigated the molecular
regulated kinase) (pERK) (Daorueang et al, 2012). Other alterations in carcinomas of the biliary tree, including IHCC,
mitogens can activate these pathways. Recombinant human EHCC, and GBCA, using frozen specimens from patients who
TFF2 can stimulate proliferation and trigger phosphorylation underwent surgical resection. Unsupervised hierarchical cluster-
of epidermal growth factor receptor (EGFR) with downstream ing analysis revealed that cancers from these different sites did
ERK activation, displaying potential mitogenic impact in CC not cluster separately, implying that there was no difference in
via EGFR/mitogen-activated protein kinase (MAPK) activation the global gene expression patterns between the biliary cancer
(Kosriwong et al, 2011). Moreover, TFF family members have subgroups. Although the individual cancer subtypes did not
been assessed as potential biomarkers in CC. Gene copy cluster separately, unique patterns of differential gene expression
number, messenger ribonucleic acide (mRNA) levels, and were observed when compared with normal biliary epithelium.
protein expression were evaluated in bile duct epithelium biop- The relationship between gene transcriptional changes among
sies collected from individuals with CC, precancerous bile duct the three biliary cancer subtypes is depicted in a Venn diagram
dysplasia, and from disease-free control participants. The (Fig. 9C.2). Overall, 165 probe sets were commonly differen-
TFF1, TFF2, and TFF3 mRNA levels were significantly tially expressed in all three cancer subtypes. Selected commonly
increased in CC tissue. differentially expressed genes are listed in Table 9C.1.
In healthy tissues, cellular senescence results in irreversible
growth arrest. However, this is prevented in malignant cells by Copy-Number Alterations
maintenance of chromosomal length via telomerase activity. The same study (Miller et al, 2009) also investigated alterations
This is observed in CC cells but not in normal cholangiocytes. in gene copy number using array-based comparative genome
Data would suggest that interleukin-6 (IL-6) is partially respon- hybridization (aCGH) analysis. Considerable heterogeneity
sible for this because it acts as an autocrine promoter of CC was observed in the extent of chromosomal instability between
growth. IL-6 stimulation leads to enhanced telomerase, patients, even within the same subtype (i.e., IHCC, EHCC,
decreased cellular senescence, and thereby increased CC and GBCA). For example, some patients had alterations in
growth (Yamagiwa et al, 2006). Moreover, in conjunction with nearly every chromosomal arm, and other patients with the
hepatocyte growth factor (HGF), IL-6 increases CC cell growth same diagnosis had few structural chromosomal changes.
in vitro, as well as induces a rapid release of prostaglandin Despite the heterogeneity, segments of chromosomes 3p, 6q,
synthesis, followed by downstream signal transduction via 8p, 9p, and 14q were commonly lost across all three biliary
MAPKs, protein kinase C, and calmodulin (Wu et al, 2002). cancers subtypes. Commonly amplified chromosomal regions
Taken together, these, and probably other mitogens, drive the across the three subtypes include segments of 1q, 3q, 5p, 7p,
proliferation of CC. 7q, 8q, and 20q. Based upon the expression analysis data and
Chapter 9C Molecular pathogenesis of biliary tract cancer 155
TABLE 9C.1 Top 10 Genes with Significantly Altered Expression in Gallbladder Cancer (GB), Intrahepatic Cholangiocarcinoma (Intra), and
Extrahepatic Cholangiocarcinoma (Extra) Along with the Fold Change (Δ) in Expression in Each Cancer Subtype
Chromosomal
Δ GB Δ Intra Δ Extra Gene Gene Title Location Functional Pathway
aCGH data, this work suggested that these three biliary tract 130 site-specific gene mutations. Mutations were identified
tumors were fairly similar in their molecular signature. within several of these genes, including KRAS (35%), TP53
However, a more recent study demonstrated that even within (22%), phosphatidylinositol-4,5-bisphosphate-3-kinase cata-
IHCC, there are distinct patterns. They analyzed 149 formalin- lytic subunit alpha (PIK3CA, 10%), B-Raf protooncogene
fixed IHCC cases by single nucleotide polymorphism array, and (BRAF, 7%), adenomatosis polyposis coli (APC, 6%), neuro-
identified several similar and different copy-number alterations blastoma RAS viral oncogene (NRAS,3%), isocitrate dehydro-
(CNAs), including gains at 1q and 7p as well as losses at 3p, genase 1 (IDH1,2%), v-AKT murine thymoma viral oncogene
4q, 6q, 8p, 9p, 9q, 13q, 14q, 17p, and 21q (Sia D. et al, 2013). homolog 1 (AKT1, 1%), β1-catenin (CTNNB1, 1%), and phos-
Although gains in chromosomal arms 1q and 7p seem frequent, phatase and tensin (PTEN, 1%). Although IDH1 mutations
there are clear discrepancies between studies where DNA copy- were rare in other common gastrointestinal malignancies, they
number gains range from 0% to 73% (Endo et al, 2002; Sirica, were identified in three tumors (25%) of an initial series of 12
2008; Sirica et al, 2002). biliary tract carcinomas. To better define both IDH1 and IDH2
mutations, an additional 75 bile duct cancers, making 87 total
Pre–Next-Generation Sequencing tumors (IHCC [N = 40], EHCC [N = 22], and GBCA [N =
With the revolutionary changes that are occurring in genomics, 25)] were examined (Table 9C.2).
the cost, sequencing time, and analysis time of NGS has sig- Combining these cohorts of biliary tract cancers, mutations
nificantly decreased during the last several years. Whole-exome in IDH1 and IDH2 were found in 10.3% of cases. On subset
sequencing and targeted sequencing of several hundred cancer- analysis (Table 9C.3), only IHCC (9/40, 23%) had IDH1
specific genes has provided significant insight and a deeper (20%) or IDH2 (3%) mutations, whereas none were identified
understanding of oncogenes and tumor-suppressor genes in EHCC or GBCA. Therefore IDH1 mutations were defined
involved in biliary tract carcinogenesis. In the era preceding as a molecular feature of IHCC, as well as suggested as a
NGS, several studies showed abnormal expression of the potential therapeutic target specific to IHCC. In contrast,
Kirsten rat sarcoma (KRAS) oncogene in 21% to 100% of KRAS (23%) and TP53 (14%) predominated in EHCC,
cases, as well as alteration in the TP53 tumor-suppressor gene whereas PIK3CA (12%) mutations were the most common in
in up to 37% of archival CC specimens (Isa et al, 2002). These GBCA. For the first time, this study defined a specific genetic
genetic alterations were associated with a more aggressive phe- abnormality in this lethal cancer that represented a potentially
notype in biliary tract tumors (Isa et al, 2002). KRAS and TP53 new target for therapy. Because the original publications were
mutations were also been identified in bile and pancreatic juice unable to molecularly distinguish IHCC, EHCC, and GBCA,
of affected patients (Isa et al, 2002; Itoi et al, 1999), but neither this study represented a paradigm shift in which we now rec-
KRAS nor TP53 mutational analysis were shown to be superior ognize that a subset of genes are frequently and specifically
to conventional cytopathology in the diagnosis of pancreatico- altered in each subtype of biliary tract cancer.
biliary tumors. However, combined pathologic analysis and Since this publication in 2012, several additional studies
mutation analysis increased diagnostic sensitivity (Aishima have been reported using whole-exome sequencing analysis. In
et al, 2002; Isa et al, 2002; Itoi et al, 1999). a U.S. study of 32 IHCCs, the investigators identified frequent
inactivating mutations in multiple chromatin-remodeling genes,
Post–Next-Generation Sequencing including BRCA1-associated protein 1 (BAP1, 17.5%), AT-rich
Compared with older studies, which relied upon sequencing interaction domain 1A (ARID1A, 15.0%), and polybromo 1
one gene a time, more recent studies have capitalized upon (PBRM1, 17.5%) (see Table 9C.2) (Jiao et al, 2013). Similar
NGS to narrowly or broadly characterize tumors. In 2012, to the earlier report, they also identified frequent mutations at
Borger and colleagues studied 287 tumors from gastrointestinal previously reported hot spots in the IDH1 (10%) and IDH2
cancer patients, including biliary tract, colorectal, gastroesoph- (5%) genes encoding metabolic enzymes. However, in contrast
ageal, hepatic, pancreatic, and small intestine carcinomas to the earlier study, TP53 (20%) was the most frequently altered
(Borger et al, 2012). They evaluated 15 known cancer genes for gene in the nine GBCA specimens studied.
156 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
TABLE 9C.3 Most Common Somatic Mutations by Biliary Tract TABLE 9C.4 Most Common Somatic Mutations and
Tumor Subtype Immunohistochemical Changes by Biliary Tract Tumor Subtype
IHCC (N = 40) EHCC (N = 22) GBCA (N = 25) IHCC EHCC GBCA
Gene Sequencing (N = 120) (N = 25) (N = 64)
AKT1 3% 0% 0%
APC 0% 0% 4% IDH1 14% 0% 1.5%
BRAF 3% 0% 0% KRAS 17% 28% 13%
CTNNB1 0% 0% 4% TP53 8% 44% 41%
IDH1 20% 0% 0% IHCC EHCC GBCA
IDH2 3% 0% 0% Immunohistochemistry (IHC) (N = 434) (N = 126) (N = 244)
KRAS 5% 23% 4%
ERBB2 overexpression 1.5% 18% 15%
NRAS 5% 0% 4%
PBRM1 loss 21% 15% 53%
PIK3CA 0% 0% 12%
EHCC, Extrahepatic cholangiocarcinoma; ERBB2, ERB-B2 receptor tyrosine kinase 2; GBCA,
PTEN 3% 0% 0%
gallbladder carcinoma; IDH1, isocitrate dehydrogenase 1; IHCC, intrahepatic cholangiocarcinoma;
TP53 5% 14% 4% KRAS, Kirsten rat sarcoma; PBRM1, polybromo 1.
AKT1, v-AKT murine thymoma viral oncogene homolog 1; APC, APC, adenomatosis polyposis coli; From Holcombe RF, et al: Tumor profiling of biliary tract carcinomas to reveal distinct molecular
BRAF, B-Raf protooncogene; CTNNB1, β1-catenin; IDH1/2, isocitrate dehydrogenase 1/2; KRAS, alterations and potential therapeutic targets, J Clin Oncol 33(Suppl 3):abstr 285, 2015.
Kirsten rat sarcoma; NRAS, neuroblastoma RAS viral (v-ras) oncogene homolog; PIK3CA,
phosphatidylinositol-4,5-bisphosphate-3-kinase catalytic subunit alpha; PTEN, phosphatase and
tensin; TP53, tumor protein 53. With the evolution of personalized medicine, many more
From Borger DR, et al: Frequent mutation of isocitrate dehydrogenase (IDH)1 and IDH2 in patients are having molecular analyses performed on their
cholangiocarcinoma identified through broad-based tumor genotyping, Oncologist 17:72–79, 2012. tumors. Two large studies analyzing biliary tract carcinomas
that utilized different molecular platforms were recently pre-
sented (Holcombe et al, 2015; Ross et al, 2015). Together,
In a separate study from Singapore, Chan-On and col- these studies provide further insight into the distinct molecular
leagues (2013) profiled 209 CCs from Asia and Europe, includ- alterations identified in each subtype (Tables 9C.4 and 9C.5).
ing 108 cases caused by infection with the liver fluke O. viverrini, In the first study, 815 cases (IHCC (N = 434), EHCC [N =
as well as 101 cases caused by non–Opisthorchis-related etiolo- 126], GBCA [N = 244], and not otherwise specified [N = 11])
gies. Whole-exome sequencing (IHCC [N = 10] and EHCC [N were evaluated using a commercial multiplatform profiling
= 5]) identified recurrent somatic mutations in BAP1 (26.7%) service (Caris Life Sciences, Phoenix, AZ) (Holcombe et al,
and ARID1A (26.7%), as well as frequent mutations in IDH1 2015). Testing included sequencing (Sanger sequencing and
(20%), KRAS (20%), and TP53 (20%). Compared with intra- NGS) and protein expression analysis (immunohistochemistry,
hepatic non–Opisthorchis-related tumors, the fluke-related IHC). In this analysis, 24 of 47 genes tested had mutations,
IHCC had higher rates of TP53 (50%) and KRAS (37.5%) with the highest rates in TP53 (28%), KRAS (18%), IDH1
mutations. On the other hand, they had lower ARID1A (12.5%) (9%), and SMAD4 (6%). Breast cancer 1/2 (BRCA1/2) muta-
mutations and no mutations in BAP1 or IDH1. This study cor- tions were seen in 3 of 41 (7.3%) and 5 of 40 (12.5%) cases,
roborated the finding of frequent somatic alterations in specific respectively. On analysis of individual tumor types (see Table
genes identified in the U.S. study, as well as demonstrated that 9C.4), IDH1 (14%) mutations remained a molecular feature of
different causative etiologies are associated with distinct sets of IHCC, whereas KRAS (28%) and TP53 (44%) predominated
somatic mutations (e.g., BAP1, IDH1, KRAS, TP53) within the in EHCC. Additionally, TP53 (41%) mutations were the
same tumor type. most common in GBCA. Mutually exclusive protein loss of
Chapter 9C Molecular pathogenesis of biliary tract cancer 157
expression (Stutes et al, 2007). Several miRs, including onco- as well as promote angiogenesis by regulating the expression of
genic miRNAs (e.g., miR-214 and miR-21) that regulate secreted pro-angiogenic proteins (Marti et al, 2015). Moreover,
PTEN-dependent activation of phosphatidylinositol-3-kinase nuclear YAP expression was shown to represent a biomarker of
(PI3K) signaling (He et al, 2013; Kawahigashi et al, 2009), as response to FGFR-directed therapy (Rizvi et al, 2016). Overall,
well as miRs associated with aberrant signaling pathways (e.g., these developmental signaling pathways appear to be important
HGF/MET and IL-6), and stem cell traits (e.g., miR-200c), in disease progression, whereas cross talk between these path-
have been reported. Others have described the regulation of ways needs further investigation.
epithelial-to-mesenchymal transition (EMT)–related genes,
including neural cell adhesion molecule 1, Slug/E-cadherin/ Epidermal Growth Factor Receptor
vimentin, and Twist, by miR-200c, miR-204, and miR214, Although somatic mutations in EGFR family members are rare,
respectively (Li et al, 2012; Oishi et al, 2012; Qiu et al, 2013). overexpression of the receptors occurs in 10% to 32% of CCs.
Comparison of CC lines with cholangiocytes also revealed Furthermore, aberrant phosphorylation of EGFR activates
downregulation of eight miRs (e.g., miR22, miR125a, miR127, MAPK, and p38 signaling can increase cyclooxygenase-2
miR199a, miR199a*, miR214, miR376a, and miR424). (COX-2). In turn, this can inhibit apoptosis while enhancing
Although, the exact role of each miR as either onco-miRs or tumor growth. However, although in vitro EGFR inhibition
prognostic markers remains to be determined, they appear to with erlotinib has been shown to CC cell proliferation, in vivo
be serving important roles in the genesis of biliary cancers. dual blockage of EGFR and ERBB1/ERBB2 with lapatinib is
necessary.
Tumor Growth and Metastasis
Dysregulated Signaling Pathways Hepatocyte Growth Factor (HGF)/MET
The progression and metastasis of biliary tract tumors appear The HGF/MET pathway is rarely mutated in biliary tract
to be driven by a variety of cellular signaling pathways involved tumors, but amplification of MET, the HGF receptor, has been
in responses to embryonic/stem cell signaling pathways (e.g., reported in IHCC. In turn, HGF/MET can activate many
Wnt, Hh, Notch, Hippo), growth factors (e.g., EGF, HGF/ pathways, including MAPK, PI3K, and STAT, as well as has
MET, VEGF), intracellular signal transduction (e.g., KRAS/ to stimulate migration and invasion in CC cells.
MAPK), cytokine signaling (e.g., IL-6/STAT), and cell-cycle
progression (e.g., polo-like kinases [PLKs]) (Sia et al, 2013). Vascular Endothelial Growth Factor and Angiogenic Signaling
VEGF is a signal protein produced by cells that stimulates
Embryonic Signaling angiogenesis. Alterations occur in almost half of IHCCs and
It is increasingly recognized that embryonic signaling pathways correlate with a poor prognosis. Although the application of
are important in the genesis of numerous types of malignancies. targeted therapies such as sorafenib, which targets wild-type
The Hedgehog (Hh), Notch, Wnt/β-catenin, and Hippo signal- BRAF and vascular endothelial growth factor receptor
ing pathways are important regulators of proliferation, survival, (VEGFR), has been studied, the preclinical data have been
self-renewal, and development in embryos and cancers in disappointing in CC models.
adults. The Hh pathway was initially reported be overexpressed
in CC (Berman et al, 2003). Hh has been also shown to regu- IL-6/JAK/STAT Cytokine Signaling
late tumor-stromal interactions in the liver that stimulate the IL-6 is an inflammatory cytokine that is overexpressed in CC
proliferation, migration, and invasion of CC cells (Kim et al, and regulates growth via either autocrine or paracrine mecha-
2014). Hh also directly regulates the viability of CC (El Khatib nisms. The overexpression of IL-6 observed in CC may result
M et al, 2013). Similarly, the Notch pathway has been shown from epigenetic silencing of SOCS-3 (Isomoto et al, 2007).
to regulate cell proliferation, migration, invasion, as well as Binding of IL-6 to its receptor (gp130) results in heterodimer-
EMT while working in concert with TP53 to regulate cell ization with the Janus kinases (JAK1, JAK2, or TYK2). In turn,
viability (El Khatib et al, 2013). Aberrant expression of Notch this drives, activation of STAT3 (i.e., the JAK/STAT pathway)
receptors 1 and 3 play a role during cancer progression, and and/or the MAPK pathway. In turn, IL-6 can regulate the
the Notch pathway protein DLL4 correlates with poor survival methylation of growth factor receptors, telomerase activity, and
in EHCC and GBCA (Yoon et al, 2011). The Wnt/β-catenin miRNA expression (Meng et al, 2008; Wehbe et al, 2006). As
pathway may also be of importance, although genomic muta- a result, inhibiting IL-6 signaling has been proposed as a novel
tions in genes, including APC, are rare. Thus the Wnt/β-catenin therapeutic target (Braconi et al, 2010).
pathway may not be as critical as other pathways in biliary tract
tumors. Finally, the Hippo signaling pathway is a tumor sup- Polo-Like Kinases
pressor pathway in which deletion of the macrophage- The PLKs are a family of serine/threonine kinases involved in
stimulating 1/2(MST1/2) gene was recently shown to cause key regulatory processes, including cell-cycle progression (G2/M
hepatocellular carcinoma (HCC) (Zhou et al, 2009). Inactiva- transition) and cytokinesis. Targeting PLK-1 has been shown to
tion of MST1/2 resulted in activation of the yes-associated increase the efficacy of 5-fluorouracil (Thrum et al, 2011),
protein 1 (YAP1) oncogene and resistance to FAS receptor whereas PLK-2 is a mediator of Hh signaling in CC (Fingas
(FasR)-induced apoptosis. FasR is also known as apoptosis et al, 2013). Currently, PLK inhibitors are in development.
antigen 1 (APO-1), cluster of differentiation 95 (CD95),
or tumor necrosis factor receptor superfamily member 6 Epithelial-to-Mesenchymal Transition
(TNFRSF6). Furthermore, overexpression of YAP1-mediated Epithelial-to-mesenchymal transitions (EMT), mesenchymal-
activation of Notch and Wnt signaling induced the expression to-epithelial transitions (MET), and, epithelial-mesenchymal
of downstream Notch targets. More recently, YAP was shown interactions (EMI) are often lumped together under the term
to regulate proliferation and anti-apoptotic mechanisms in CC, EMT (Sicklick, 2013). However, in the former phenomenon,
Chapter 9C Molecular pathogenesis of biliary tract cancer 159
epithelial cells lose their polarity and cell-cell adhesion, while the proliferation and activation of CC cells and HSC expression
gaining migratory and invasive properties to become mesenchy- of the angiotensin II type 1 (AT1) receptor in autocrine and
mal. This is thought to be involved in the initiation of metasta- paracrine fashions, respectively (Okamoto et al, 2010). In vitro,
sis. As discussed above, miR200c was determined to prevent CC cell migration and survival are also modulated by the cross-
EMT (Oishi et al, 2012), whereas miR204 regulated genes talk between stromal cell–derived factor-1 (SDF-1) produced
associated with EMT (Zha et al, 2014), and miR214 inhibition by HSC and CC cells bearing the SDF-1 receptor, CXCR-4
was found to promote EMT (Li et al, 2012). Further studies (C-X-C chemokine receptor type 4) (Gentilini et al, 2012).
of miR gene regulation are warranted to determine the contri- Interestingly, Ang II also enhances EMT through the interac-
bution of miRs in biliary carcinogenesis, prognosis, and tion between activated HSC and the SDF-1/CXCR4 axis
therapeutics. (Okamoto et al, 2012). In addition, IL-1β produced by HSC
induces the expression of CXCL5 (C-X-C motif chemokine 5)
Tumor-Stromal Interactions in CC cells. In tumors, CXCL5 expression correlates with a
Hepatic stellate cells (HSCs) are stromal cells in the benign worse overall survival after curative hepatic resection (Okabe
hepatic parenchyma that possess both neural and myofibro et al, 2012). Taken together, the regulation of paracrine tumor-
blastic features (see Chapter 7). HSCs are the major cell stromal pathways may be a useful target in controlling IHCC
type involved in hepatic fibrosis and cirrhosis. In addition, progression.
portal myofibroblasts can contribute to hepatic fibrosis. It is
increasingly realized that tumor-stromal interactions play posi- SUMMARY
tive and negative roles in hepatic carcinogenesis and fibrosis
(Fingas et al, 2011; Kim et al, 2014; Magistri et al, 2014). In the last decade, we have gained significant insight into the
Because CC is a very desmoplastic tumor (Kajiyama et al, environmental risk factors, genomic alterations, tumor hetero-
1999), and the microenvironment is a key component of the geneity, and epithelial-mesenchymal interaction/transitions
tumor development and progression, these interactions are associated with the development of biliary tract adenocarcino-
most relevant to IHCC. As a result, the hepatic stromal com- mas. Presented is a comprehensive review of the molecular
partment is increasingly recognized in the pathogenesis of pathogenesis of CC, which relies upon the underlying themes
IHCC (Andersen et al, 2012; Chuaysri et al, 2009; Massani of chronic inflammation to the biliary epithelium, host-mediated
et al, 2013). response, and subsequent development of the malignant phe-
Several pathways appear to regulate this process. For notype. Many new candidates for targeted therapy based on
instance, the Hh pathway regulates HSC (Sicklick et al, 2005). molecular analyses have emerged, including the MET, EGFR,
In turn, HSCs stimulate the proliferation, migration, and inva- ERBB2, FGFR, JAK/STAT, RAS/RAF/MAPK, PI3K/AKT/
sion of CC cells, as well as promote angiogenesis through Hh mTOR, Wnt/Hh/Notch/Hippo, and IDH pathways. Data has
pathway activation. This renders CC cells more susceptible also emerged on the role of epigenetics and miRs, providing
to necrosis by Hh inhibition (Kim et al, 2014). Moreover, the potential for further studies in these areas. Identifying and
myofibroblast-derived platelet-derived growth factor-BB pro- cataloging somatic alterations and associating these alterations
tects CC cells from TRAIL (TNF-α–related apoptosis-inducing with clinical outcomes may assist in the development novel
ligand) cytotoxicity by a Hh-dependent process (Fingas et al, therapeutic interventions, enhancing early diagnosis, identify-
2011). Finally, expression of the Hh target gene, osteopontin, ing at-risk individuals, and ultimately improving survival in
is an independent predictor of survival in IHCC patients these devastating malignancies.
(Sulpice et al, 2013).
In addition, other mechanisms are emerging in this cross- References are available at expertconsult.com.
talk. Angiotensin II (Ang II) produced in IHCC tissue regulates
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CHAPTER 9D
Molecular biology of liver carcinogenesis
and hepatitis
Masafumi Shimoda and Jack R. Wands
OVERVIEW OF MOLECULAR ETIOLOGY are most prevalent include West and Central Africa and East
and Southeast Asia, with China alone accounting for more than
Recent advances in molecular genetics have emphasized the 50% of the world cases (Ferlay et al, 2015). It is noteworthy
multistep process of tumorigenesis. It is evident that cancer is that HBV is highly endemic in these areas, with the exception
a genetic disease involving aberrant chromosome rearrange- of Japan, where HCV is more prevalent. Oceania, North and
ments, genetic mutations, and epigenetic silencing of tumor South America, and Northern and Eastern Europe are low-rate
suppressor genes (Farazi & DePinho, 2006). Independent of areas.
the etiology, hepatocellular carcinoma (HCC; see Chapter 91) Trends in HCC incidence are likely to be different in regions
generally develops where sustained hepatocyte turnover occurs of high and low persistence of HBV and HCV infection
in the setting of injury-inflammation-regeneration, which leads (El-Serag & Rudolph, 2007). Comparative studies performed
to the accumulation of chromosomal aberrations. In this between 1977 and 1982 and between 1993 and 1997 show that
context, monoclonal populations of hepatocytes become pre- the incidence of HCC in Hong Kong, Shanghai, Singapore, and
neoplastic and, following additional genomic alterations, change Japan has begun to decrease (Parkin et al, 2002). The fall in
into dysplastic cells and eventually HCC (Thorgeirsson & incidence is apparently due to vaccination against HBV, which
Grisham, 2002). Accumulated genetic alterations in preneo- has been accomplished in greater than 80% of newborns
plastic lesions and HCC result in the activation, as well as (Chang et al, 2009), because chronic HBV infection in those
inactivation, of many growth factor signal transduction path- countries is usually acquired through mother-to-newborn or
ways involved in hepatic transformation. It is believed that sibling-to-sibling transmission at a young age. In contrast, the
increased hepatocyte turnover associated with chronic liver incidence of HCC has rapidly increased in some countries, such
injury may be a major feature of hepatic oncogenesis. However, as Australia, the United States, and the United Kingdom, as a
another central question is whether hepatitis viruses, the leading result of chronic HCV infection. For example, HCC is the
cause of HCC worldwide, directly contribute to the develop- fastest growing cause of cancer-related deaths in the United
ment of this disease. Accumulating evidence suggests that States. The annual incidence of liver cancer increased from 2.6
chronic hepatitis B (HBV) and hepatitis C virus (HCV) infec- per 100,000 population for the years 1978 to 1980 to 8 per
tion play a direct role in the molecular pathogenesis of HCC 100,000 in 2010, of which at least 3 of 4 cases are accounted
through specific viral–cellular protein interactions (Branda & for by HCC (El-Serag & Kanwal, 2014). Reasons for this
Wands, 2006; see Chapter 70). increased incidence are not entirely clear but may reflect a
greater prevalence and role of persistent HCV infection
EPIDEMIOLOGY (McGlynn et al, 2001).
Age-specific rates of HCC peak at 75 years and older in most
Primary liver cancer is the fifth most common cancer in men regions of the world (El-Serag & Rudolph, 2007). With the
and the ninth most common in women worldwide. It is esti- exception of Africa, the peak incidence in women occurs 5 years
mated that 782,000 new patients with the disease were diag- later than that found in men. In the United States, recent trends
nosed in 2012 (Ferlay et al, 2015). The 5-year survival rate is have revealed a peak incidence shifting toward a relatively
less than 15% in developed countries, and the United States younger age group (El-Serag & Kanwal, 2014).
has a survival rate of 16.6%, making liver cancer the second Significant gender and ethnic variation in incidence, as well
most fatal tumor after pancreatic cancer (SEER Cancer Statis- as mortality from HCC, has also been found; male rates are
tics Factsheets 2007-2011). Presumably because of its poor nearly triple that of females (Ferlay et al, 2015). The most likely
prognosis, liver cancer is the second leading cause of cancer explanation for gender variation is that men have more risk
death in men and the sixth among women in the world. It is factors, such as exposure to hepatitis virus infection, excessive
estimated that about 745,000 individuals worldwide died from alcohol intake, smoking, and increased iron stores in the liver
this disease in 2012 (Ferlay et al, 2015). (El-Serag & Rudolph, 2007). In addition, androgen receptor
Primary liver cancers consist of numbers of histologically accelerates the progression of HCC through interaction with
distinct types of tumors that arise from hepatocytes, biliary the HBV genome (Ma et al, 2008; Wu et al, 2010). The inci-
epithelial cells, and fibroblasts. The most common is HCC, dence of HCC also varies with race and ethnicity in the same
which accounts for 70% to 85% of all hepatic tumors (Perz area. In the United States, the incidence and subsequent mor-
et al, 2006). Approximately 80% of HCC worldwide is caused tality rates from HCC are two times greater in Asians than
by chronic infection with HBV or HCV or both. The HCC African Americans, which are two times greater than those
burden is unevenly distributed worldwide; areas where tumors found in whites (El-Serag & Rudolph, 2007). These variations
160
Chapter 9D Molecular biology of liver carcinogenesis and hepatitis 161
are explained in part by the accumulation of major risk factors contaminate corn, rice, and peanuts in China and sub-Saharan
in each ethnic group. Africa. High rates of dietary exposure to AFB1 increase the risk
of HCC 4-fold. When people with chronic HBV infection are
RISK FACTORS exposed to AFB1, the relative risk for HCC dramatically
increases to about 60-fold (Kew, 2003). This synergistic effect
Unlike most malignancies, HCC has well-established extrinsic between AFB1 exposure and chronic HBV infection is an
risk factors that account for at least 80% of tumors, namely important observation because in some regions of the world,
chronic infection with HBV or HCV (see Chapter 70). Key AFB1 exposure and chronic HBV infection rates are high.
epidemiologic aspects of HBV- and HCV-induced HCC are Excessive ethanol consumption (>50 to 70 g/day) is another
summarized in Table 9D.1. Chronic HBV infection is the well-defined risk factor for HCC. In the United States, ethanol-
leading cause of HCC, and it has been estimated that there are induced HCC accounted for more than 20% of HCC patients
350 to 400 million HBV carriers, which account for 5% of the between 1996 and 1999 (Davila et al, 2004). Donato and col-
global population. About 59% of HCC patients in developing leagues (2002) showed a linear increase of a relative risk for
countries and 23% of HCC patients in developed countries are HCC by 5-fold when 60 to 140 g/day alcohol is taken. The
chronically infected with HBV (American Cancer Society, 5-year cumulative HCC incidence in alcoholic cirrhosis without
2011). Reported relative risks of HCC among HBV carriers HBV and HCV infection is 8% (Fattovich et al, 2004); however,
range between 5-fold and 100-fold compared with the general it is unlikely that ethanol itself has a direct carcinogenic effect.
uninfected population. This wide range of the estimated values Rather, excessive ethanol ingestion indirectly affects hepatocar-
is caused by the dependence of the relative risk on multiple cinogenesis through the promotion of cirrhosis. Indeed, greater
factors, including HBV load, presence of cirrhosis, and expo- than 80% of HCC tumors found in alcoholics develop in the
sure to aflatoxin B1 (AFB1) (El-Serag, 2012). The 5-year background of a cirrhotic liver. A synergistic effect between
cumulative incidence rates of HCC from HBV-related cirrhosis heavy alcohol consumption and hepatitis virus infection is
are 17% in highly endemic areas and 10% in Europe and the observed in several studies. The relative risk of HCC attribut-
United States (Fattovich et al, 2008). In addition, approxi- able to heavy alcohol consumption alone was only 2.4-fold,
mately 70% to 90% of HBV-related HCC develops in patients whereas in combination with chronic HCV infection, it
with cirrhosis. increased to 50-fold (Hassan et al, 2002). Others have reported
Chronic HCV infection is the second leading cause of HCC. that the concomitant HCV infection in alcoholics increases the
The estimated number of HCV carriers worldwide is 180 risk for HCC 2-fold, whereas HBV infection moderately
million, which accounts for 2% of the global population. increases this risk 1.2- to 1.5-fold (Donato et al, 2002; Jee et al,
Approximately 33% of HCC tumors in developing countries 2004).
and 20% of HCC in developed countries are attributable to Growing evidence now suggests that metabolic dysfunction,
persistent HCV infection (American Cancer Society, 2011). including obesity, diabetes, and nonalcoholic fatty liver disease
According to cross-sectional and case-control studies, HCC (NAFLD), are important risk factors for HCC, especially in
risk is increased 15- to 20-fold in HCV-infected persons com- developed countries (see Chapter 71). Several large cohort
pared with the HCV-negative population (El-Serag, 2012). The studies revealed that obesity is a definitive risk factor for HCC
5-year cumulative incidence of HCC with HCV-related cir- with the 1.5- to 4-fold increased risk. Men are more susceptible
rhosis in developed countries is 17%, with an exception for to obesity-associated HCC than women. Diabetes mellitus also
Japan, where the 5-year cumulative incidence is 30% (Fattovich has established as a moderately strong risk factor for HCC, with
et al, 2004). The high incidence of HCV-related HCC in Japan a two- to four-times higher risk (El-Serag & Rudolph, 2007;
may be due to the prevalence of HCV genotype 1b. AFB1 Starley et al, 2010). More recently, nonalcoholic steatohepatitis
is produced by Aspergillus flavus and related fungi that (NASH), the more aggressive form of NAFLD, is considered
to be a cause of a large proportion of cryptogenic cirrhosis,
which is liable for these patients to develop HCC. However,
TABLE 9D.1 Comparison of Epidemiologic Features between the overall incidence of HCC in patients with NAFLD is much
HBV- and HCV-Induced HCC lower than in patients with well-established etiologies (Starley
HBV HCV et al, 2010).
Other risk factors for HCC include hemochromatosis and
Virus carriers (% of 350-400 million 180 million (2%) hepatic porphyria. It should be noted that daily coffee intake
global population) (5%) reduces the incidence of HCC between 25% and 75% in the
Highly prevalent Asia, sub-Saharan Africa, South and general population in a dose-dependent manner (Inoue et al,
areas Africa, Melanesia, East Asia, South
Micronesia America
2005). This effect may be attributable to the inhibition of trans-
forming growth factor-β (TGF-β) signaling by methylxanthine
Relative risk of HCC 5- to 100-fold* 15- to 20-fold
caffeine, which reduces liver fibrosis (Gressner, 2009).
5-year cumulative 10% (Europe and 17% (Europe and
incidence rates United States) United States)
of HCC from 17% (East Asia) 30% (Japan) GENETIC AND EPIGENETIC ALTERATIONS
cirrhosis
HBV, Hepatitis B virus; HCC, hepatocellular carcinoma; HCV, hepatitis C virus.
Chronic inflammation accompanied by sustained cycles of
injury and regeneration of hepatocytes over 20 to 40 years
*Depends on multiple factors including HBV load, presence of cirrhosis, and exposure to
aflatoxin B1. promotes the development of liver fibrosis, cirrhosis, and even-
From El-Serag HB, Kanwal F: Epidemiology of hepatocellular carcinoma in the United States: Where
tually HCC (Fig. 9D.1A) (see Chapter 7). Pathologically, HCC
are we? Where do we go? Hepatology 60:1767–1775, 2014; and El-Serag HB: Epidemiology of occurs early within cirrhotic nodules, which can form in areas
viral hepatitis and hepatocellular carcinoma, Gastroenterology 142:1264–1273, 2012. of adenomatous hyperplasia or dysplasia. These cells eventually
162 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Cirrhotic nodule
Hyperplasia
Dysplasia
Malignant
Normal liver Chronic hepatitis Cirrhosis transformation Hepatocellular carcinoma
Telomere shortening
Chromosome instability
β-Catenin mutation
A Loss of p53
Injury
Inflammation Hypermethylations
Regeneration
B Hepatocellular carcinoma
FIGURE 9D.1. A, Diagram showing progression of liver disease and genetic events accompanied by chronic inflammation. B, Common mechanisms
underlying hepatocarcinogenesis. A number of factors contribute to chromosome instability and other genetic alterations, which lead to the formation
of hepatocellular carcinoma.
Chapter 9D Molecular biology of liver carcinogenesis and hepatitis 163
become more atypical, and the malignant transformation from investigations performed in TERC knockout mice (Farazi
process becomes complete (Theise et al, 2002). Hepatocellular et al, 2003). This study indicates that telomerase reactivation
carcinoma is like other malignancies and represents a DNA occurred and appeared to be necessary for late-stage tumor
disease with accumulation of many alterations in oncogenes progression; thus the reactivated telomerase enzyme maintains
and tumor suppressor genes. The accumulation of genetic aber- the shortened telomere length in these tumor cells and prevents
rations that induces cellular transformation may take 20 to 40 them from undergoing apoptosis.
years, suggesting that liver carcinogenesis involves a multistep DNA damage-response pathways are safeguards that regu-
process. late cell-cycle checkpoints and prevent DNA-damaged cells
Cirrhosis may represent end-stage liver disease as a result of from further proliferation. Several studies report that the func-
persistent HBV or HCV infection. Because 80% to 90% of tions of key regulatory molecules, including p53, mouse double-
HCC tumors originate from cirrhotic liver, it is evident that minute 2 (MDM2), retinoblasoma 1 (RB1), p16INK4a (/also
continuous rounds of cellular injury, followed by regeneration known as CDKN2A [cyclin-dependent kinase inhibitor 2A],
in the milieu of chronic inflammation, fundamentally contrib- and gankyrin, were impaired in human HCC. The p53 protein,
utes to the oncogenic processes. The sustained cycles of injury encoded by the transforming protein 53 (TP53) gene, is a
and repair increase the chance of genomic alteration. Further- master molecule that maintains genome integrity by inducing
more, the host inflammatory response to viral infection, includ- cell-cycle arrest, followed by activation of DNA repair systems.
ing activation of stellate cells, causes the release of When excessive DNA damage occurs, p53 initiates apoptosis.
proinflammatory cytokines, which accelerate hepatic carcino- TP53 is one of the most mutated genes in HCC, and the muta-
genesis by augmenting oxidative stress and DNA damage tions often result in loss of function. The frequency ranges
(Bataller & Brenner, 2005; Giannelli et al, 2005; Ogata et al, between 11% and 35%, depending on regions (Tornesello et al,
2006). Continuous rounds of this process in the presence of 2013). The regional difference in the frequency is attributable,
inflammation not only increase the chance of genomic altera- in part, if not completely, to a specific mutation caused by
tions but also produce chromosome instability. For example, AFB1 exposure. TP53 missense mutations in codon 249
hyperploidy has been observed in 43% of dysplastic peritu- (R249S) were found in more than 50% of AFB1-related HCC
moral regions and in about 50% of HCC tumors (Laurent-Puig (Gouas et al, 2009), and it was the main cause of AFB1-induced
& Zucman-Rossi, 2006). Molecular mechanisms underlying liver cancer (Bressac et al, 1991). Therefore TP53 mutations in
such genomic instability include telomerase dysfunction, defec- HCC can be frequently found in Africa and Asia where people
tive segregation of chromosomes, and an impaired DNA are exposed to a high level of AFB1. Other mutations of TP53
damage response (Fig. 9D.1B). are found in 20% to 40% of HCC without molecular evidence
Recent advances in genome-wide analysis, including whole- of AFB1 exposure (El-Serag & Rudolph, 2007). The aberration
genome sequencing and DNA array technologies, have pro- of the p53 pathway can be caused by molecules that inappro-
vided more detailed information on the alterations of oncogenic priately regulate p53 functions. MDM2 is an E3 ubiquitin
or tumor suppressive genes. These sophisticated studies drew ligase targeting tumor suppressor proteins, including p53 and
an important conclusion that HCC does not have a clear addic- RB1. Strikingly, gankyrin (encoded by PSMD10), which pro-
tion to a specific gene, and that genomic alterations in HCC motes such protein degradation by MDM2, was overexpressed
are quite extensive. Accordingly, development of molecularly in 100% (n = 34) of human HCC (Higashitsuji et al, 2000,
targeted therapy for HCC will be challenging. Nevertheless, 2005). More recently, genome-wide copy number variation
several frequently mutated genes were found in HCC genomes, analysis identified interferon regulatory factor 2 (IRF2) as a
including those for telomerase reverse transcriptase (TERT), novel tumor suppressor gene in HCC that activates the p53
p53, and β-catenin. pathway, and showed that IRF2 loss-of-function mutations
Telomere shortening is a key feature of chronic liver disease were frequently and exclusively found in HBV-related HCC
that allows sustained proliferation of hepatocytes (Urabe et al, (Guichard et al, 2012). The CDKN2A gene encodes for two
1996). In human HCC, telomere shortening has been shown splice-variant products, including p16INK4a and p14ARF,
to have a positive correlation with increased chromosome which positively regulate the p53 and RB1 signaling pathways.
instability—chromosomal gains, losses, and translocations—by The expression of the CDKN2A gene was suppressed in 30%
promoting chromosomal fusions (Plentz et al, 2004). A study to 70% of human HCC as a result of methylation of the pro-
of telomerase-deficient mice reveals that telomere dysfunction moter region (Jin et al, 2000; Liew et al, 1999; Matsuda et al,
initiates tumor formation (Farazi et al, 2003). It is noteworthy 1999; Weihrauch et al, 2001). Loss of heterogeneity (LOH) of
that 90% of human HCCs show robust activation of telomerase chromosome 9p, where CDKN2A is located, was found in 15%
(Lee et al, 2004; Nagao et al, 1999; Shimojima et al, 2004). In to 20% of tumors (Boige et al, 1997; Laurent-Puig et al, 2001;
some HBV-induced HCC tumors, the viral genome was found Nagai et al, 1997). Interestingly, CDKN2A deletion rarely
to be integrated into the TERT locus, which results in increased occurs in HCC when TP53 is also mutated (Tannapfel et al,
expression of telomerase (Ferber et al, 2003; Fujimoto et al, 2001). Taken together, impairment of the p53 and RB1 path-
2012; Murakami et al, 2005). More recently, direct sequencing ways is a common genetic feature of HCC.
of the TERT promoter region revealed that 59% of HCCs had The canonical WNT (wingless type) pathway plays a central
recurrent somatic mutations, which may result in the activation role in the development of many cancer types and is a key regu-
of TERT (Nault et al, 2013). Other findings related to telom- lator of the signal is β-catenin, which is encoded by the CTNNB1
erase biology indicate amplification of telomerase RNA com- gene. CTNNB1 is the most frequently mutated gene in HCC,
ponent gene (TERC) mRNA and allelic loss of chromosome ranging from 20% to 40% (Cieply et al, 2009; Tornesello et al,
10p, where a putative telomerase inhibitor resides (Nishimoto 2013). The activating mutations frequently occur in exon 3,
et al, 2001; Takeo et al, 2001). Such telomerase reactivation which result in the nuclear accumulation of β-catenin, thereby
and telomere shortening in HCC cells may be explained in part inducing WNT-responsive gene expression. Indeed, nuclear
164 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
accumulation of β-catenin in HCC cells and in clinical HCC because of chromosomal gains and losses and by point muta-
samples is associated with a more aggressive phenotype and tions in the genes. However, recent studies have revealed that
with poor prognosis of HCC patients (Inagawa et al, 2002). epigenetic mechanisms—such as DNA methylation and short,
Another frequently mutated gene in the canonical WNT noncoding RNA (21 to 23 nucleotides) species, or microRNA
pathway is AXIN1, a gene encoding a cytoplasmic protein that (miRNA)—also contribute to aberrant expression of oncogenes
negatively regulates WNT signaling. AXIN1 mutations are and tumor suppressor genes. In human HCC, aberrant DNA
found in 6.8% to 15.2% of HCC (Guichard et al, 2012; Satoh methylation patterns have been detected (Kanai et al, 1999;
et al, 2000). Loss-of-function mutations of AXIN1 lead to a Thorgeirsson & Grisham, 2002; Yu et al, 2003). More impor-
decrease in degradation of β-catenin and to nuclear localization tant, hypermethylation has been observed at the earliest stages
of this protein. of HCC development, and the extent of hypermethylation
Epigenetic regulation of the genome is a fundamental deter- tends to increase with tumor progression (Lee et al, 2003).
minant of global gene expression. Epigenetic regulators have Specific gene targets for hypermethylation include CDKN2A,
come to be recognized as tumor suppressors because next- PTGS2, CDH1, PYCARD, GADD45B, and DLC1. Among
generation sequencing of cancer genomes has defined frequent these genetic elements, it has been shown that CDKN2A,
mutations in epigenetic regulators, including chromatin remod- GADD45B, and PTGS2 expression were directly affected by
eling proteins and histone-modification proteins. In HCC, the methylation, using human HCC cell lines (Higgs et al, 2010;
AT-rich interactive domain (ARID) family, including ARID1A, Liew et al, 1999; Matsuda et al, 1999; Murata et al, 2004).
ARID1B, and ARID2, was found to be mutated in 6% to 17% In addition, miRNA contributes to messenger (mRNA)
of HCC genomes (Fujimoto et al, 2012; Guichard et al, 2012; instability by hybridizing with its complementary target
Li et al, 2011). Through the interaction with the switch/sucrose sequence, followed by mRNA degradation, so that a protein
nonfermentable (SWI/SNF) chromatin-remodeling complex, cannot be generated. Several studies reveal aberrant expression
ARID family proteins bind transcription factors and recruit the of some miRNAs in human HCCs compared with the adjacent,
remodeling activity to a specific gene. Mechanisms underlying nontumorous counterparts. For example, miR-21 was expressed
tumor development by loss-of-function mutations of ARID in human HCC; it targets the phosphatase and tensin (PTEN)
family genes are not known in detail, but it is highly likely that tumor suppressor gene (Meng et al, 2007). MicroRNA-122,
ARID mutations are associated with tumor proliferation, dedif- which targets the cyclin G1 cell-cycle regulator (Gramantieri
ferentiation, and inhibition of apoptosis (Wu & Roberts, 2013). et al, 2007), is abundant in normal hepatocytes and is essential
MLL and MLL3 are histone methyltransferases that positively for homeostasis of hepatocytes. Its implication in hepatocar-
regulate gene transcription. MLL gene translocations are fre- cinogenesis was revealed by using knockout mice and clinical
quently found in infant leukemia, but the significance of loss- samples (Kojima et al, 2011; Tsai et al, 2012). More recently,
of-function mutations of MLL family in HCC remains to be evidence was presented that links aberrant expression of miRNA
determined (Nakagawa & Shibata, 2013). Key genetic altera- to the multistep process of hepatocarcinogenesis. The expres-
tions in HCC are summarized in Table 9D.2. sion of miR-26a was diminished in murine and human tumors,
It is evident that the expression and function of oncogenes resulting in enhanced activity of cyclin D2 and E2 to promote
and tumor suppressor genes are affected by copy number cell proliferation. Moreover, when exogenous miR-26a was
overexpressed in mice prone to form multiple HCCs, substan-
tial protection from disease progression was observed, indicat-
TABLE 9D.2 Genetic Alterations Frequently Found in HCC ing a possible therapeutic approach for this disease (Kota et al,
Gene Symbol Genetic Alteration Frequency (%) 2009). These findings indicate that epigenetic and posttran-
scriptional regulation of gene expression plays an important
Telomere Maintenance role in hepatic oncogenesis.
TERT Promoter activation 20-60
WNT/β-Catenin
SIGNAL TRANSDUCTION PATHWAYS
CTNNB1 Gain-of-function mutation 20-40
AXIN1 Loss-of-function mutation 3-16 Genetic alterations of oncogenes and tumor suppressor genes
Cell Cycle impinge on a wide variety of signal transduction pathways
TP53 Loss-of-function mutation 11-35 involved in proliferation and tumor cell viability. Although the
spectrum of affected signal transduction pathways in HCC cells
CDKN2A Loss of heterozygosity 15-20
Promoter inactivation 30-70 is more heterogeneous compared with that of affected signals
Proliferation in other tumor types, key pathways are commonly dysregulated
in human HCC, such as the WNT/β-catenin, erythroblastosis
IRF2 Loss-of-function mutation 5
(ERB)-B receptor tyrosine kinase (ERBB)/extracellular signal-
IGF2R Allelic loss 0-13
regulated protein kinase (ERK)/phosphatidylinositol-3-kinase
Epigenetic Modifier
(PI3K), and insulin-like growth factor (IGF)/insulin receptor
ARID1A Loss-of-function mutation 10-17 substrate (IRS)/ERK/PI3K cascades (Fig. 9D.2).
ARID1B Loss-of-function mutation 7 The WNT/β-catenin pathway regulates cell proliferation,
ARID2 Loss-of-function mutation 6-16 motility, and differentiation. WNT proteins are ligands that
MLL3 Loss-of-function mutation 4 bind to Frizzled (FZD) cell-surface receptors to stabilize
HCC, Hepatocellular carcinoma. β-catenin in the cytoplasm, followed by translocation to the
From Ding J, Wang H: Multiple interactive factors in hepatocarcinogenesis, Cancer Lett
nucleus, where it upregulates WNT-responsive genes (Thomp-
346:17–23, 2014; and Marquardt JU, Thorgeirsson SS: SnapShot: hepatocellular carcinoma, son & Monga, 2007). In the absence of WNT signaling, the
Cancer Cell 25:550, 2014. amount of cytosolic β-catenin is low as a result of proteolytic
Chapter 9D Molecular biology of liver carcinogenesis and hepatitis 165
IGF
LRP-5/6
LRP-5/6
TGF-α
WNT
Receptor
ERBB
FZD FZD
Cytoplasm
DVL DVL DVL
IGF-1R
AXIN IRS
AXIN
GRB2
APC P
GSK-3β β-Catenin SOS
P RAS-
β-Catenin PI3K AKT
GTP
β-Catenin IKK
β-Catenin
P RAF
β-Catenin
β-Catenin P GSK-3β
β-Catenin MEK mTOR
Proteasomal degradation ERK
Nucleus
degradation produced by the action of glycogen synthetase immunohistochemical staining (Fujito et al, 2004; Inagawa
kinase-3β (GSK-3β)/ adenomatosis polyposis coli (APC)/ et al, 2002; Ishizaki et al, 2004; Mao et al, 2001; Wong et al,
AXIN kinase destruction complex. However, when WNT 2001). These findings suggest that nuclear accumulation of
ligands bind to the Frizzled/ low density lipoprotein receptor- β-catenin is an excellent biomarker for activation of WNT sig-
related protein-5/6 (LRP-5/6)/Dishevelled (DVL) receptor naling in HCC. More important, β-catenin activation occurs at
complex, phosphorylation of β-catenin by GSK-3β is inhibited an earlier stage of the oncogenic process in dysplastic cells,
to allow its accumulation in the cytoplasm. The β-catenin suggesting that the WNT/β-catenin cascade is directly involved
molecules are then transported into the nucleus and bind to in tumor formation (Calvisi et al, 2001, 2004; de la Coste et al,
T-cell factor (TCF)/leukocyte enhancer factor (LEF) tran- 1998; Merle et al, 2004; Thorgeirsson & Grisham, 2002).
scription factors; this complex acts as transcriptional regula- The other cell-surface molecules that play a major role in
tors. Finally, the TCF/LEF/β-catenin complex promotes the activation of WNT/β-catenin signaling are called FZD
activation of target genes, including cyclin D1 (CCND1), receptors FZD. There are 10 FZD receptors (FZD1 to FZD10)
myelocytomatosis viral oncogene (MYC), prostaglandin- in humans. Indeed, studies reveal that 23% to 59% of HBV-
endoperoxide synthase 2 (PTGS2), and JUN, which leads to related HCCs overexpress the FZD7. Through the interaction
proliferation of HCC cells. with a FZD-ligand WNT3, overexpressed FZD7 leads to the
As discussed above, gain-of-function mutations of CTNNB1 activation of this pathway in human tumors and HCC cell lines
or loss-of-function mutations of AXIN1 result in the nuclear (Kim et al, 2008; Pez et al, 2013). The functional consequences
accumulation of β-catenin. The frequency of β-catenin nuclear of FZD7 overexpression were enhanced cell motility and inva-
accumulation varies between 17% and 75%, as determined by sion. In murine HCC models, overexpression of FZD7 occurred
166 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
in dysplastic nodules and HCC tissue but not in normal liver IGF-binding proteins (IGFBPs). IGF-2R is a decoy receptor
(Merle et al, 2004, 2005). These findings illustrate that FZD7 to which IGF-2 exclusively binds, but no activation of down-
overexpression was a common event during hepatic oncogen- stream molecules occurs. IGFBP-3, a predominant form of
esis and that it promotes tumor cell motility and invasion. IGFBPs, is a neutralizing peptide that binds to circulating
Receptor tyrosine kinases (RTKs) and subsequent signal IGF-1 and IGF-2 (Pollak, 2008).
transduction, including the mitogen-activated protein kinase Many lines of evidence have established that dysregulation
(MAPK) pathway and the phosphatidylinositol-3-kinase of IGF pathway is involved in the malignant transformation,
(PI3K)/AKT pathway, play a central role in tumor cell prolif- cancer development, and even resistance to anticancer agents.
eration and survival. The ERBB family (especially ERBB1), The same is true for HCC. Comprehensive analysis of 104
MET proto-oncogene, IGF-1 receptor (IGF-1R) are the RTKs HCC cases revealed that IGF pathway activation, namely the
frequently activated in HCC cells. The ERBB family consists presence of phosphorylated IGF-1R, was found in 21% of the
of four RTKs, including ERBB1/EGFR/HER1, ERBB2/HER2/ cases (Tovar et al, 2010). Overexpression of IGF-2, downregu-
NEU, ERBB3/HER3, and ERBB4/HER4 (Yarden & Sli- lation of IGFBP-3, or allelic losses of IGF2R, which all lead to
wkowski, 2001). When ligands bind to the ERBB1 receptor, the activation of the pathway, was found in 25% of the cases.
autophosphorylation occurs that leads to an association with Another report showed that the IGF-2 ligand was overex-
the growth factor receptor–bound protein 2 (GRB2) adaptor pressed in 16% to 40% of tumors, as well as in dysplastic tissue,
molecule and PI3K. When phosphorylated ERBB1 binds to suggesting that IGF-2 may act by autocrine and/or paracrine
GRB2, the complex activates the RAS (rat sarcoma) oncopro- mechanisms (Breuhahn et al, 2006). IRS adaptor molecules are
tein, resulting in enhancement of RAF serine/threonine kinase also important in HCC development. IRS-1 is overexpressed
activity. Activated RAF kinase triggers MEK/ERK kinases, as in the majority of human HCCs (Cantarini et al, 2006; Nishi-
well as ERK, which translocates to the nucleus and upregulates yama & Wands, 1992); overexpression was associated with
the transcription of oncogenes such as FBJ murine osteosar- increased tumor size and progression via activation of the
coma viral oncogene homolog (FOS), JUN, and MYC. When MEK/ERK cascade, which promotes cell proliferation (Tanaka
phosphorylated ERBB1 binds to PI3K, ERBB1 activates PI3K et al, 1997). Constitutive MEK/ERK pathway activation may
and the downstream AKT kinase. AKT phosphorylates a also occur via downregulation of a RAF kinase inhibitor protein
number of important molecules, including mechanistic target (RKIP); this event promotes HCC cell proliferation and migra-
of rapamycin (mTOR), GSK-3β, and inhibitor of kappa B tion (Lee et al, 2006). Indeed, downregulation of RKIP was
kinase (IKK) to promote proliferation and viability of tumor found in 90% of human HCC and suggests that it plays a role
cells. as a tumor suppressor protein in this disease. IRS-2 has also
It has been established that ERBB1 and ERBB3 were over- been found to be overexpressed in the majority of human
expressed in 68% and 84% of HCC, respectively, which cor- tumors and in HCC cell lines (Boissan et al, 2005). The finding
relates with a more clinically aggressive phenotype (Ito et al, of IGF signaling in HCC has led to the development of several
2001a). Ligands for ERBB include epidermal growth factor monoclonal antibodies that bind and neutralize the IGF-1
(EGF), TGF-α, heparin-binding EGF (HB-EGF), amphiregu- receptor and of small molecules that antagonize IGF-1R as a
lin, β-cellurin, and epiregulin. In this regard, TGF-α and potential therapeutic approach; such agents are undergoing
HB-EGF proteins may play a role in the pathogenesis of HCC. preclinical and early-phase clinical trials for solid tumors and
TGF-α was frequently upregulated at an earlier stage of tumor HCC (Pollak, 2008).
formation (Schaff et al, 1994; Yeh et al, 1987; Zhang et al, The angiogenic pathway is an emerging and promising
2004). In murine models, HCC develops in TGF-α–overex- molecular target in HCC because HCC is usually a highly
pressing transgenic mice, whereas TGF-α–knockout mice were vascular tumor. Angiogenesis is a complex process regulated by
resistant to chemically induced hepatic neoplasms, indicating many factors, such as vascular endothelial growth factor
that TGF-α upregulation was closely linked to the oncogenic (VEGF), platelet-derived growth factor (PDGF), and basic
process (Jhappan et al, 1990; Russell et al, 1996). HB-EGF fibroblast growth factor (bFGF). VEGF and its receptors
protein was a potent mitogen for hepatocytes, detected in 59% VEGF-R1, -2, and -3 are overexpressed in HCC, and overex-
to 100% of HCC (Inui et al, 1994). Moreover, overexpression pression of VEGF is associated with poor prognosis (Dhar
of HB-EGF was found at an earlier stage of HCC with mod- et al, 2002; Tseng et al, 2008). PDGF recruits pericytes and
erately or well-differentiated features (Ito et al, 2001b), suggest- smooth muscle cells around new vessels, which are important
ing that HB-EGF is an important ligand in initiation of this components of arteries. bFGF is involved in endothelial cell
disease. As a consequence, MAPK activity is increased in HCC migration, capillary branching, and the activity of proteases,
compared with adjacent nontumorous tissues (Osada et al, essential for angiogenesis as well. These growth factors bind
2005; Schmidt et al, 1997). and stimulate their corresponding receptors on angiogenic
The IGF signaling cascade is a well-defined pathway that cells, and activate the subsequent signal pathways including
regulates energy metabolism and cell growth. It consists of MAPK, PI3K/AKT, SRC, and phospholipase C (PLC)-γ path-
ligands, receptors, adaptors, and subsequent MAPK and PI3K/ ways. Sorafenib is a small-molecule multikinase inhibitor that
AKT pathways. The ligands are IGF-1, IGF-2, and insulin as inactivates VEGF receptors, PDGF receptors, v-Kit Hardy-
well. The activation of this pathway begins when the ligands Zuckerman 4 feline sarcoma viral oncogene homolog (KIT),
bind to receptors, including IGF-1R homodimers and heterodi- and B-Raf proto-oncogene (BRAF) (Wilhelm et al, 2006). It is
mers consisting of IGF-1R and insulin receptors, resulting in the first drug proven to be effective in advanced HCC (Llovet
the activation of their kinase domain. Activated receptors then et al, 2008). Thus the antiangiogenic approach may become a
phosphorylate adaptor proteins such as IRS-1 and IRS-2, mainstream of the systemic treatment of HCC, and in fact,
which are able to trigger the MAPK and PI3K/AKT signaling many clinical trials for use of such agents are currently
cascades. Negative regulators of this pathway are IGF-2R and underway.
Chapter 9D Molecular biology of liver carcinogenesis and hepatitis 167
P Core
HBV genome
~ 3.2 kb
DNA
PreS/S
(+) strand
(-) strand X
Lipid bilayer
Nucleocapsid
A PreC/core B
HBV
Cell injury
and increased cell
turnover
Recycling
Cytoplasm
Transcription
cccDNA
Repair
Nucleus
Viral integration
with cellular DNA
C
FIGURE 9D.3. A, Structure of the hepatitis B virus (HBV) DNA genome, showing the four open reading frames involved in generation of preC/core,
preS/S, P, and X proteins. B, Structure of infectious HBV particle, showing the nucleocapsid containing an HBV genome and polymerase (P) and
an envelope derived from the lipid bilayer, where preS/S proteins are embedded. C, Life cycle of HBV, showing viral entry through receptors, followed
by uncoating and translocation of HBV DNA to the nucleus, where it is repaired to generate a covalently closed circular DNA (cccDNA) form that
serves as the template for transcription of the pregenomic and other viral mRNA necessary for replication. (From Wands JR: Prevention of hepatocel-
lular carcinoma, N Engl J Med 351:1567–1570, 2004. Copyright © 2004 with permission from Massachusetts Medical Society. All rights reserved.)
Chapter 9D Molecular biology of liver carcinogenesis and hepatitis 169
JAK STAT
HBx Enhanced
IRS proliferation
p53
Mitochondria RAS RAF MEK ERK
P13K
AKT
Impaired p53
DNA repair RNA pol II
systems HBx complex Modulated
transcription
HBx
Transcr.
DNA factor
Cytoplasm Nucleus
HBV genome
Insertional mutagenesis
and chromosome instability
FIGURE 9D.4. Characteristics of the HBx protein and its involvement in tumor formation. HBx plays a crucial role in hepatitis B virus (HBV)-induced
carcinogenesis. HBx is located in the cytoplasm and activates cellular signaling cascades. This viral nonstructural protein also inhibits p53-mediated
apoptosis. Nuclear HBx modulates a set of transcription factors through interaction with a RNA polymerase complex. The HBV genome integrates
into the host genome during persistent viral infection and promotes chromosome instability. AKT, v-Akt murine thymoma viral oncogene homolog;
ERK, extracellular signal-regulated protein kinase; HBx, hepatitis B virus X protein; IRS, insulin receptor substrate; JAK, Janus activating kinase; MEK,
mitogen-activated protein kinase; PI3K, phosphatidylinositol-3-kinase; PYK, proline-rich tyrosine kinase; RAF, Raf-1 proto-oncogene; RAS, rat
sarcoma (oncoprotein); SRC, sarcoma; STAT, signal-transducer and activator of transcription; transcr., transcription.
IRS-1/MEK/ERK cascade (Longato et al, 2009). In addition, expression has been shown to block p53-mediated apoptosis,
nuclear HBx has been reported to act as a transcriptional coact- and it provides a clonal selective advantage to HBV-infected
ivator, although it does not directly bind to DNA. Growth hepatocytes (Elmore et al, 1997; Huo et al, 2001; Wang et al,
molecules known to be influenced by HBx expression include 1995).
cyclic adenosine monophosphate (cAMP) response element– Interestingly, HBx can trigger the release of calcium ion
binding protein (CREB), activating transcription factor 2 from mitochondria, leading to the enhanced replication of HBV
(ATF2), activating enhancer binding protein 2 (AP-2), and DNA through interaction with a proline-rich tyrosine kinase 2
CREB-binding protein/p300 (Bouchard & Schneider, 2004). (PYK2) and SRC kinase (Bouchard et al, 2001). Calcium
Several reports indicate an interaction between HBx and release and localization of HBx in mitochondrial membranes
p53 tumor suppressor protein. In this context, HBx binds cause oxidative stress, in which reactive oxygen species (ROS)
to p53 and may suppress its functions. For example, HBx are produced (Bouchard et al, 2003; Yang & Bouchard, 2012).
binds to p53 in the nucleus and inhibits expression of p53 ROS directly damage DNA, leading to aberrant DNA replica-
responsive genes. Nuclear HBx also alters the association of tion. HBx also influences the androgen signaling pathway,
p53 with transcription factors, such as excision repair cross- which may explain, in part, the known male predominance of
complementation group 3 (ERCC3) and transcription factor HBV-induced HCC (Chiu et al, 2007). Taken together, these
IIH (TFIIH), which are involved in nucleotide excision repair findings indicate that HBx plays a complex and pleiotropic role
(Jia et al, 1999; Wang et al, 1994, 1995). Moreover, HBx in the multistep process of tumor development.
170 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Evidence has been accumulating that the risk of HCC is HEPATITIS C VIRUS
substantially increased by viral factors, such as the level of
HBV replication produced by naturally occurring mutations in HCV is a member of the Flaviviridae family and is the only
the core and precore promoter regions (Baptista et al, 1999; member of the genus Hepacivirus (Tellinghuisen & Rice, 2002).
Kao et al, 2003; Kuang et al, 2004). A high viral replication The HCV genome consists of a single positive-strand RNA of
phenotype places the infected liver at greater risk for transfor- approximately 9.6 kb in length (Fig. 9D.5A). HCV RNA con-
mation, as shown in Figure 9D.3C. Finally, with the develop- tains a large (approximately 9.0 kb) ORF in which structural and
ment of diagnostic techniques sensitive enough to detect very nonstructural coding regions are located near the 5′ and 3′ ends
low levels of serum HBV DNA (<100 copies/mL), it has of the viral genome, respectively. Both 5′ and 3′ untranslated
become increasingly apparent that many patients with chronic (UTR) domains have been found to be essential for viral RNA
HCV infection also are infected with low levels of HBV. In replication. Translation of the HCV RNA can be initiated by an
this setting, HBV maintains its oncogenic properties, and evi- internal ribosome entry site (IRES) located in the 5′ UTR. The
dence has accumulated that occult HBV infection, defined as single ORF encodes for a polyprotein precursor, consisting of
less than 10,000 virions per mL of serum, may be associated about 3000 amino acids; it is cleaved into 10 smaller proteins by
with chronic hepatitis and cirrhosis of heretofore unknown the action of several proteases derived from both host and virus.
origin (Wands, 2004). These 10 viral-related molecules include three structural (core
5´ UTR 3´ UTR
Core E1 E2 p7 NS2 NS3 NS4A NS4B NS5A NS5B
IRES
Attachment
HCV particle
Hepatocyte
Receptor Release
Replication
Lipid
Entry droplet
(endocytosis)
n
tio
Assembly
sla
an
Tr
Ribosome
HCV
polyprotein
[C], E1, and E2) and 7 nonstructural (NS; p7, NS2, NS3, NS4A, a complex and initiate replication of the RNA genome in col-
NS4B, NS5A, NS5B) proteins. The core forms a nucleocapsid laboration with some host proteins. Viral particles are assem-
that contains the HCV genome. The nucleocapsid is covered by bled from the structural proteins, and the RNA genome
an envelope composed of a lipid bilayer, in which the two struc- becomes encased between membranes derived from lipid drop-
tural proteins E1 and E2 are embedded. The function of p7 is lets and the ER. Assembled particles are delivered to the plasma
not well understood, but it appears to be a transmembrane membrane and released into the blood by exocytosis. Impor-
protein with ion channel activity. NS2 is a metalloprotease that tantly, the entire process related to HCV replication is restricted
cleaves between NS2 and NS3. The NS3 is a serine protease that to the cytoplasm; unlike HBV, the viral RNA does not form a
produces NS4A, NS4B, NS5A, and NS5B viral proteins; it also DNA intermediate, and thus the HCV genome does not inte-
has RNA helicase and nucleoside triphosphatase (NTPase) grate into the host’s cellular DNA.
activity. NS4A acts as a cofactor for NS3 activity, and NS4B is The evolution of chronic hepatitis to cirrhosis during per-
an integral membrane protein located on the cytoplasmic side sistent HCV infection may be mediated by the host immune
of endoplasmic reticulum (ER); it has been implicated in the response directed against epitopes that reside on the various
assembly of replicase complex. The NS5A protein is believed to viral proteins. Chronic HCV infection may develop as a result
act as a component of RNA replicase complex, and it plays a role of immune evasion as a function of quasi-species formation
in evasion of the host’s cellular immune response. The NS5B is during active viral replication. The RNA polymerase of HCV
an RNA-dependent RNA polymerase essential for the replica- lacks proofreading capacity and contributes to rapid diversifi-
tion of the HCV genome. cation of the viral population; therefore mutant HCV can
The life cycle of HCV consists of at least six different stages: escape from the adaptive immune response because of selec-
attachment/entry, translation, processing, genome replication, assem- tion pressure (Rehermann & Nascimbeni, 2005). Moreover,
bly, and release into the circulation (Fig. 9D.5B). HCV particles several viral proteins, including NS3 and NS5A, may contrib-
attach to the hepatocyte cell-surface membrane and enter the ute to viral persistence as a result of attenuation of cellular
cell via key proteins such as CD81, SR-BI, claudin-1, and interferon activity, which appears essential for virus elimina-
occludin. After entry into the hepatocyte, the nucleocapsid is tion (Foy et al, 2003; Polyak et al, 2001). These immune-
delivered to the cytoplasm, and the HCV RNA is released and evasion mechanisms promote chronicity of HCV infection,
immediately translated. The large polyprotein is processed on which promotes hepatic inflammation, cirrhosis, and HCC
the cytoplasmic side of the ER, and nonstructural proteins form (Fig. 9D.6).
Stellate cell
TGF-β
Promotion of
fibrosis
GSK-3β
p21WAF1
Hepatocyte
FIGURE 9D.6. Pathogenic role of hepatitis C virus (HCV) proteins. This diagram illustrates how HCV proteins, including core, NS3, NS5A, and
NS5B, may modulate cellular function. Such proteins promote hepatocarcinogenesis in diverse ways via activation of signaling pathways and stellate
cells, and they suppress immune responses to the virus and generate oxidative stress in the liver. AKT, v-Akt murine thymoma viral oncogene homolog;
CDK2, cyclin-dependent kinase 2; ERK, extracellular signal-regulated protein kinase; GRB2, growth factor receptor-bound protein 2; GSK-3β, gly-
cogen synthetase kinase-3β; MEK, mitogen-activated protein kinase; NS, nonstructural; PI3K, phosphatidylinositol-3-kinase; pol, polymerase; TGF-β,
transforming growth factor-β; WNT, wingless type.
172 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
At least four HCV proteins, including core, NS3, NS5A, transgenic mice (Moriya et al, 1998). Moreover, iron loading
and NS5B, have been proposed to have cellular transforming in transgenic mice expressing the full-length HCV genome
activity both in vitro and in vivo as depicted in Figure 9D.6. promotes HCC formation, again implicating chronic oxidative
Transgenic mice overexpressing HCV core in the liver have stress in the pathogenesis of HCV-mediated HCC (Furutani
been shown to develop steatosis as well as HCC (Moriya et al, et al, 2006). The mechanisms underlying oxidative stress–
1998). In addition, the core protein has been shown to have induced hepatocarcinogenesis involve increased chromosome
transforming potential in vitro (Ray et al, 1996). HCV core instability and mutations in the host cellular DNA produced by
binds numerous cellular proteins and modulates the RAF/ the action of ROS (Machida et al, 2006; Naganuma et al,
MEK /ERK signal transduction pathway (Levrero, 2006). The 2004). Moreover, HCV directly induces lipid accumulation in
core protein also augments the TGF-β pathway by upregulating hepatocytes as a result of ER stress, because viral replication
TGF-β expression in hepatic stellate cells to promote fibrosis occurs on the ER membranes, where the core impedes ER
(Bataller et al, 2004). Enhanced proliferation of HCC cells has functions (Lonard et al, 2004). Hepatic steatosis induced by
been demonstrated by overexpression of the HCV core protein HCV infection promotes oxidative stress and ROS production
in vitro. This phenomenon was due to upregulation of WNT1 (Koike, 2005). Collectively, many of the HCV proteins are
expression, suggesting a functional link between HCV core believed to contribute to hepatocyte transformation during per-
expression during active viral replication and subsequent activa- sistent viral infection through stimulation of cell proliferation,
tion of the WNT/β-catenin signaling cascade (Fukutomi et al, increased cell survival, induction of genomic instability, and
2005). promotion of immune evasion.
NS3 has been shown to complex with the wild-type p53
protein (Ishido & Hotta, 1998). By modulating the activity of FUTURE DIRECTIONS
p53, NS3 inhibits transcription of the leucine carboxyl methyl-
transferase 2 (LCMT2) gene, which encodes a cell-cycle regula- In the postgenomic era, comprehensive examination of tumors
tor, p21WAF1/CIP1. In addition, it has been found to repress via next-generation sequencing and microarray technologies
LCMT2 promoter activity in a dose-dependent manner and makes it highly likely that molecular genetic changes evolving
stimulates cell growth (Kwun et al, 2001). from normal liver to dysplasia to HCC will be more precisely
The NS5A protein may act as a transcriptional modulator defined. Moreover, rapid advances in epigenetics analysis,
through interactions with other cellular proteins, such as GRB2, miRNA function, and cancer stem cell biology will greatly
p53, p21WAF1/CIP1, and CDK2. The functional conse- enhance our understanding of the molecular pathogenesis of
quences have been inhibition of hepatocyte apoptosis, leading HCC. Traditional anticancer drugs, which target the DNA
to persistent HCV infection (Reyes, 2002). One potential replication machinery, have marginal therapeutic effect on
mechanism by which NS5A may be able to exert an effect on HCC growth, and new molecular targets will need to be
gene expression and cellular growth is through functional asso- defined. To date, unlike other cancer types, including breast,
ciations with p53 and TATA box–binding proteins (TBPs). In colon, and lung, most clinical trials of molecularly targeted
addition, NS5A can bind directly to the p85 regulatory subunit therapeutics against HCC, except for sorafenib, have not
of PI3K and phosphorylate AKT, resulting in activation of yielded expected results (see Chapter 101). Reasons for failure
pro–cell survival signals (Street et al, 2004). More recently, it are heterogeneous, but we should learn from each trial and
has been observed that NS5A-mediated activation of PI3K further deepen the understanding of altered properties of
resulted in the stabilization and accumulation of β-catenin in tumor cells (Llovet & Hemandez-Gea, 2014). Such investiga-
the cytoplasm and nucleus through inactivation of GSK-3β tions emphasize the importance of unraveling the molecular
(Milward et al, 2010; Street et al, 2005). mechanisms of liver carcinogenesis, which may ultimately
Another possible pathway activated in HCV-induced HCC result in “personalized” medical approaches for this devastat-
involves oxidative stress generated by increased production of ing disease.
ROS during persistent viral infection. Indeed, ROS production
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CHAPTER 10
Liver immunology
Steven C. Katz, Zubin M. Bamboat, Venu G. Pillarisetty, and Ronald P. DeMatteo
173
174 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
B
PMN
B
MAC B B
NK DC CD4 CD4
CD4
CD4
CD4 CD4
MAC
PMN
CD8
CD8 CD8
DC
CD8
CD8 CD8
FIGURE 10.1 Innate and adaptive immunity. A, Innate immunity includes the body’s initial defenses against infection. It includes certain comple-
ment proteins, epithelial barriers, natural killer (NK) cells, neutrophils (polymorphonuclear [PMN]), phagocytes such as macrophages (MACs), and
antigen-presenting cells such as dendritic cells (DCs). Innate immune cells may directly kill tumor or infected cells, and then present antigen to adap-
tive immune cells. B, In contrast, adaptive immunity refers to the precisely targeted immune mechanisms that occur later in the immune response.
The adaptive immune system has B-cell–mediated humoral (dissolved) and T-cell–mediated cellular components. The innate and adaptive immune
systems overlap extensively, communicating by direct cellular contact or cytokine secretion. B-cell secretion of antibodies functions to block infections
and trigger the destruction of pathogenic organisms. T-cell–mediated immunity occurs after antigen presentation and leads to direct cellular lysis by
CD8 T cells with support from the CD4 arm.
parenchymal cells and resident immune cells of the liver. The release large amounts of soluble MHC class I molecules that
microanatomic and rheologic features of the hepatic sinusoids potentially could function to neutralize cytolytic T cells. KCs
facilitate highly efficient antigen presentation and interactions and NK T cells have been implicated as important in the devel-
among immune cells. opment of hepatic tolerance, because the depletion of either
has been associated with a loss of oral tolerance. Liver DCs and
Tolerance and Immunosuppression T cells also have been suggested to play a role in liver tolerance
One of the most intriguing aspects of liver immunology is the because, as a group, they have been shown to be less immuno-
strong tendency to develop tolerance to orally ingested antigens genic than their counterparts from lymphoid organs, such as
and liver allografts. From a teleologic perspective, tolerance to the spleen and peripheral blood (Bamboat et al, 2009a; Katz
oral antigens is clearly advantageous. In experimental animal et al, 2005). LSECs have been found to promote tolerance, and
models and clinical liver transplantation studies, a greater pro- hepatic B cells are suppressed in certain models (Thorn et al,
pensity for graft acceptance has been noted compared with 2014). Controversy exists, however, as to whether these differ-
transplantation of other solid organs. A liver transplant protects ences are developmental, due to conditioning within the liver
a kidney allograft transplanted simultaneously from the same or as a result of chemotactic signals in the liver that attract a
donor (Creput et al, 2003). Unfortunately, primary and meta- unique population of cells. It is likely that both intrinsic differ-
static tumors in the liver exploit intrahepatic immunosuppres- ences in liver immune cells and environmental factors are criti-
sion to evade destruction by the immune system. A deeper cal in defining the nature of liver immunology.
understanding of liver tolerance may support therapeutic inter-
ventions to stimulate immunity for cancer or control liver LIVER IMMUNE CELLS
immune cell function for inflammatory conditions.
Multiple competing theories to explain the cause of liver Although the liver performs myriad nonlymphoid functions, it
tolerance have been advanced. One postulate is that, as in contains numerous nonparenchymal cells (NPCs), one quarter
central thymic tolerance, clonal deletion of antigen-specific T of which are leukocytes. The composition of the intrahepatic
cells occurs in the liver. Another theory is that liver allografts leukocyte population is markedly different from that seen in
Chapter 10 Liver immunology 175
Effector function
Treg
Tolerance CD8
Immunity CD4
Proinflammatory
-γ Intracellular pathogens
IFN Treg
CD8 T
GF- Antiinflammatory
β, IL
-1 0 Tolerance CD8 Intrahepatic tumor
Treg
PD-1
IFN-γ Proinflammatory PD-L1
Th1 Intracellular pathogens CD4
CD8
Naïve T TNF, IL-1
or B cell CD8
2 Th2
IL-4 Allergy, asthma CD8
APC IL-5, 13 Helminth infections CD4
CD8
1 IL-17 Extracellular pathogens
Th17
TNF, IL-21 Autoimmunity Treg
CD4
Signal 3 CD4
Treg IL-10 Immunosuppression
CD4
TGF-β Tolerance
IL-10 Antibody production FIGURE 10.3 The balance between tolerance and immunity in the
Bcell Autoimmune disease
TGF-β, IFN liver. The liver exhibits a fine balance between the induction of tolerance
FIGURE 10.2 Antigen-presenting cell (APC) instruction of T and and excessive immune responses. Examples of the liver as a tolerogenic
B cells. Signals 1 (antigen presentation), 2 (costimulation), and 3 (cyto- organ include its role in oral tolerance, chronic hepatitis infection, and
kine production) between APCs and naïve T or B cells govern the transplantation. In addition, the liver is among the most common sites
subsequent adaptive immune response. Naïve CD4+ T cells can differ- of distant metastatic disease in patients with cancer. In contrast, the liver
entiate into four types of T cells—Th1, Th2, Th17, and Treg—each with is also the site of many autoimmune diseases, such as autoimmune
a distinct cytokine profile and specific effector function. In turn, pro- hepatitis, primary sclerosing cholangitis, and primary biliary cirrhosis.
grammed CD4+ T cells modulate CD8+ T cells that can differentiate into Immune responses to intrahepatic antigens occur when effector CD4+
either cytotoxic or regulatory cells capable of killing foreign pathogens and CD8+ T cells are not suppressed by regulatory T cells (Treg) or
or suppressing immune responses, respectively. B cells can also dif- immunoinhibitory pathways such as the programmed death-1/pro-
ferentiate into cytokine and antibody-producing cells, which play a role grammed death ligand-1 (PD-1/PD-L1) axis (left). In contrast, when
in responses against tumors, pathogens, and autoimmune diseases. Tregs expand or immunoinhibitory pathways are upregulated, tolerance
APCs, Antigen-presenting cells; IFN-γ, interferon-γ; IL, interleukin; TGF- occurs (right). Hepatocytes may also present antigens and express
β, transforming growth factor-β; TNF, tumor necrosis factor. immunomodulatory molecules. (From Saied A, et al: Immunotherapy for
solid tumors—a review for surgeons, J Surg Res 187:525–535, 2014.)
other organs (Fig. 10.5). The liver contains most of the cellular
components of innate and adaptive immunity. Importantly,
liver immune cells demonstrate unique functional properties Dendritic Cells
that tend to promote a tolerogenic milieu. Substantial hetero- DCs are a heterogeneous population of leukocytes that are
geneity among liver immune cells precludes simple generaliza- primarily responsible for the capture of antigens in the periph-
tions concerning their function. The pleiotropic roles attributed ery and subsequent presentation to immune effector cells. DCs
to liver immune cells are likely to be highly contextual, render- are now recognized as the most potent APCs of the immune
ing their study both fascinating and challenging. system. Murine DCs are typically isolated based on their high
expression of the integrin CD11c. Immature DCs are special-
Antigen-Presenting Cells ized to capture antigens and then migrate to lymph nodes,
Experimental and clinical observations that antigens passing where they can interact with T cells. After an encounter with
through the liver can lead to tolerance make the understanding a pathogenic stimulus, such as bacterial lipopolysaccharide,
of intrahepatic antigen presentation particularly relevant (Li DCs undergo phenotypic and functional changes, whereby
et al, 2004). APCs play a crucial role in driving adaptive their ability to capture antigens is diminished, but they increase
immune responses and bridging innate to adaptive immunity. their expression of MHC class II and T cell costimulatory
DCs, LSECs, KCs, and hepatic B cells all play a role in antigen molecules. Costimulatory molecule expression is essential in
presentation within the liver. The context in which an APC facilitating antigen presentation and efficient T-cell activation.
presents an antigen can dramatically alter the response of Inflammatory conditions often promote a process of matura-
antigen-specific T cells. Specifically, when antigen presentation tion, whereby DCs increase expression of MHC and costimula-
occurs in conjunction with the appropriate costimulatory mol- tory molecules, enabling efficient antigen presentation and
ecules, T cells proliferate and develop an immunogenic pheno- T-cell activation. However, liver DC phenotype and function
typic and functional profile (Fig. 10.6). In contrast, antigens is somewhat unique, as we discuss later.
presented in the absence of costimulation or presence of immu- The body of literature addressing the function of DCs grown
noinhibitory signals lead to anergy or activation-induced T-cell in vitro from murine bone marrow progenitors or human
death, two of the mechanisms of peripheral tolerance induction peripheral blood mononuclear cells is vast. DCs isolated directly
and maintenance. from the spleen, lymph nodes, or thymus also have been well
176 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Central
vein Kupffer cell
A
To gain a better understanding of liver DCs as they function
in situ, recent focus has been on freshly isolated liver DCs. In
our initial studies, we expanded the number of liver DCs to
facilitate their isolation. Because granulocyte-macrophage
LSEC Hepatocyte
colony-stimulatory factor (GM-CSF) had been used to grow
DC progenitors in culture from liver nonparenchymal cells, and
because we had previously shown that in vivo GM-CSF over-
Space of Disse Hepatic expression increases the number of myeloid DCs in the spleen
sinusoid
Kupffer Lymphocyte (Miller et al, 2002a), we suspected that it might expand liver
cell Immature DCs as well. We found that overexpression of GM-CSF using
DC
an adenoviral vector led to a dramatic increase in the number
of highly immunostimulatory liver DCs (Pillarisetty et al,
2003). We also showed that a large proportion of the cells
recruited to the liver by GM-CSF were DC precursor cells that
Blood from develop into CD11c+ DCs in culture, which suggests that DC
portal vein
Blood to development can occur in the liver. We used immunohisto-
central vein
chemistry to locate both types of recruited cells. The liver DCs
Lymph drains from space of Disse and enters were concentrated around the central veins, whereas the DC
lymphatic capillaries in the portal area
precursors were distributed diffusely throughout the liver
B parenchyma.
Our experience with expanding liver DCs sheds light on in
situ liver DC development. We found that compared with the
relatively well-studied DCs from the spleen, CD11c+ liver DCs
were immature and only weakly immunostimulatory (Pillari-
setty et al, 2004). In contrast to spleen DCs, liver DCs are
heterogeneous in their expression of MHC class II and costim-
ulatory molecules. Myeloid (CD11b+) and lymphoid (CD8α+)
liver DCs, which each comprise approximately 10% of the total
population of DCs in the liver, were as able to activate T cells,
as were their splenic counterparts. The bulk of the remaining
cells, which had low-to-no expression of CD11b and CD8α,
were poor T-cell stimulators. This study showed that the pres-
ence of these atypical DCs accounted for the weakly activating
nature of liver DCs on the whole. More recently, we discovered
that the CD11chi subset of DCs within the liver is required for
effective presentation of soluble protein (Plitas et al, 2008).
Using a transgenic mouse in which CD11chi DCs can be
depleted selectively, we found that activation of antigen-specific
C
CD8+ T cells in the liver only occurred in the presence of
CD11chi DCs.
Our investigation into liver DCs has now been extended into
humans. We found that freshly isolated DCs from human liver
studied. In contrast, because of the rarity of DCs in the liver, exhibit tolerogenic properties when compared with autologous
few studies have shown the phenotype or function of liver DCs. blood DCs. Human liver DCs are weaker stimulators of T cells
Initial studies showed that liver DC progenitors are relatively and produce the antiinflammatory cytokine interleukin-10 (IL-
immature with poor immunostimulatory ability that can 10), which induces the differentiation of naïve CD4+ T cells
promote immunologic tolerance (Lau & Thomson, 2003; Lu into regulatory T cells with suppressive function (Fig. 10.7;
et al, 1994, 2001). Bamboat et al, 2009a).
Chapter 10 Liver immunology 177
4%
2%
6%
5%
5%
LSEC
DC
3% Kupffer
T Cells
NKT Cells
B Cells
NK Cells
75%
LSEC
T CELL KC
DC
B
FIGURE 10.5 Liver immune cell composition. A, After mechanical and enzymatic digestion of freshly harvested murine liver specimens, hepa-
tocytes were removed by centrifugation. Flow cytometry analysis was then performed on hepatic nonparenchymal cells (NPCs). Liver sinusoidal
endothelial cells (LSECs) constitute most (~75%) of the liver NPCs. Liver leukocytes contain a particularly high proportion of natural killer T (NKT)
cells and Kupffer cells. Liver dendritic cells (DC) are unique in their subset composition and function. B, LSECs line the hepatic sinusoidal spaces,
where liver T cells, KCs, and DCs interact to orchestrate immune responses.
Kupffer Cells Techniques that allow the more precise delineation of cel-
Liver macrophages, referred to as Kupffer cells, have long been lular subtypes have stimulated reassessment of previously held
believed to be the primary phagocytic cells of the liver. KCs notions concerning KCs and other immune cells. Specifically,
represent the largest pool of macrophages in the body, derived the advent of flow cytometry has allowed us to define cells by
from monocytic precursors in the blood. They are typically their surface marker expression, rather than simply by size or
found in the hepatic sinusoids; however, they also can migrate other crude physical characteristics shared by many cell types.
through the space of Disse to interact with hepatocytes (see Fig. This point is illustrated by the fact that many liver DCs express
10.4). KCs have been thought to play a major role in antigen the cell-surface marker CD11b, which has been used to define
presentation and have been implicated in portal venous toler- KCs in the liver. Much of the antigen-presenting ability previ-
ance. Evidence also suggests that KCs may regulate T-cell ously attributed to KCs may be a result of DC function. KCs
responses to antigens and induce immune tolerance to liver and MDSCs also have similar cell-surface marker expression.
allografts (Sun et al, 2003). The lack of consistent definitions of cells by surface marker
178 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
**
**
** **
3000 Sham 5000 *
Sham
I/R
ALT (IU/L)
2000
3000
1500
2000
1000
500 1000
0 0
WT WT TLR9–/–TLR9–/– Treatment PBS DT PBS DT
A Isotype 1A8 Isotype 1A8 B Donor cells PBS PBS cDCs cDCs
CCR2-mediated
Liver cDC Inflammatory recruitment
Monocyte
TLR9
↓TNF
↑TNF
TLR9 ↑ALT
↑ROS
C
FIGURE 10.7 The role of Toll-like receptor 9 (TLR9) in neutrophils and dendritic cells (DCs) during liver ischemia/reperfusion (I/R). A,
Wild-type (WT) and TLR9−/− mice were depleted of neutrophils using an antibody (1A8) or isotype control (Isotype). Mice then underwent sham lapa-
rotomy (Sham) or 1 hour of segmental ischemia, followed by 12 hours of reperfusion (I/R). Serum alanine aminotransferase (ALT) was then measured.
B, Conventional DCs (cDCs) were depleted selectively in transgenic mice via a single injection of diphtheria toxin (DT). Control mice were injected
with phosphate-buffered saline (PBS). Twelve hours later, mice were injected intravenously with cDCs or PBS just prior to sham or I/R. Serum ALT
was measured 12 hours later. C, After segmental liver I/R (70% ischemia), the resultant hepatocyte death causes release of host DNA, which activates
cDCs and neutrophils via TLR9. cDCs produce interleukin-10 (IL-10), which suppresses the function of inflammatory monocytes. As a result, less
inflammatory cytokines (tumor necrosis factor [TNF], IL-6) and reactive oxygen species (ROS) are produced, causing less liver injury. In contrast,
neutrophil TLR9 activation causes an increase in TNF and ROS production, which increases ALT. *P < .05; **P < .01; CCR2, C-C chemokine recep-
tor. (A, From Wiley InterScience. Bamboat ZM, et al: Toll-like receptor 9 inhibition confers protection from liver ischemia-reperfusion injury, Hepatology
51:621–632, 2009; B and C, modified from the American Society for Clinical Investigation. Bamboat ZM, et al: Conventional dendritic cells reduce
ischemia/reperfusion injury in mice via IL-10, J Clin Invest 120:559–569, 2010.)
dysfunction is reversible, which points to potential therapeutic immunosuppressive properties as well (Katz et al, 2005). The
opportunities. high proportion of γδ T cells in the liver suggests that they have
an important immunologic role, but further investigation is
γδ T Cells required. As with most lymphocyte populations, heterogeneity
The γδ T-cell receptor is relatively invariant, and can recognize among liver γδ T cells precludes simple generalizations con-
multiple nonpeptide antigens without the need for MHC pre- cerning their functions.
sentation. γδ T cells represent 10% of liver T cells, whereas
they comprise only a small proportion (< 5%) of T cells in the Natural Killer T Cells
blood or lymphoid organs. γδ T cells also are abundant at other NKT cells share characteristics of conventional T cells and NK
environmental interfaces, including the skin and mucosal sur- cells and are defined by the presence of several T-cell and NK
faces. Through secretion of activating and modulatory cyto- cell-surface markers. Most NKT cells react against glycolipid
kines, γδ T cells help orchestrate early responses to atypical antigens in the context of CD1d, which is a MHC class I–like
bacterial and viral pathogens. γδ T cells can also promote anti- glycoprotein. CD1d is expressed on APCs and hepatocytes.
tumor immunity through their early secretion of interferon-γ NKT express invariant T-cell receptor chains that are con-
(IFN-γ) (Gao et al, 2003). A study from our group focused on served across species, suggesting an important role for NKT
liver γδT cells and demonstrated that this cell type has cells in the innate immune response to pathogens. Activated
180 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
NKT cells are capable of producing IFN-γ and IL-4, which are T-cell activity that can be usurped by tumors to induce T-cell
the prototypical Th1 and Th2 cytokines, respectively. suppression (see Fig. 10.6). CTLA-4 is expressed on acti-
NKT cells constitute a relatively large proportion of T cells vated T cells and constitutively on Tregs, and blocking the
found in the liver compared with other organs. In addition, an activity of CTLA-4 enables T-cell functional rescue. Like
expansion of NKT cells is seen in the liver in several models of CTLA-4, PD-1 is a coinhibitory receptor but with distinct
liver injury, such as partial hepatectomy. NKT cells have been biologic properties. PD-1 has two known ligands: programmed
shown to play a role in the mechanisms of inflammatory dis- death ligand-1 (PD-L1) and PD-L2. Many tumors and sup-
eases and clearance of infection in the liver. Depletion of NKT pressive immune cells express PD-L1, and PD-1 engagement
cells has been shown to abrogate the effects of experimentally by PD-L1 results in T-cell functional exhaustion (Curiel et al,
induced hepatitis in a mouse model, and mice lacking NKT 2003). Exhausted T cells have a markedly diminished capac-
cells are susceptible to viral and bacterial infections. NKT cells ity for cytokine production, proliferation, and tumor lysis.
are now also thought to play a part in tumor surveillance in the Although blockade of CTLA-4 or PD-1 may result in autoim-
liver. Data from murine primary and metastatic tumor models mune or inflammatory toxicity, targeting PD-1 in the liver
have shown that NKT cells can mediate tumor rejection, in may be associated with protection of normal parenchyma. In
part because of their ability to secrete IFN-γ (Teng et al, 2007). an animal model, we have recently demonstrated that PD-1
Work in other murine models suggests that liver NKTs have blockade can resuscitate T cells within the liver while actually
the capacity to suppress T-cell proliferation and hence contrib- minimizing inflammatory injury to normal parenchyma (Licata
ute to the immunosuppressive nature of the intrahepatic space et al, 2013).
(Katz et al, 2005). Tregs are a subset of CD4 T cells and mediate tolerance by
suppressing antigen-specific T cells (Shevach, 2002). Differen-
Natural Killer Cells tiation of Tregs is programmed by the FOXP3 transcription
NK cells are innate responders and, unlike T cells, do not factor, which is also useful for identifying Tregs experimentally.
possess specific antigen receptors. By expressing a variety of Immunosuppression by Tregs is mediated through numerous
activating and inhibitory receptors, NK cells can bind ligands mechanisms, including secretion of tolerogenic cytokines and
on their target cells. The resulting activation of NK cells causes expression of PD-L1. MDSCs work in concert with Tregs in
the release of lytic granules, or cytokines such as IFN-γ, which promoting an immunosuppressive environment. MDSCs are a
kill the infected host of tumor cell in an MHC-unrestricted heterogeneous group of cells derived from a myeloid lineage
fashion. NK cells are a major component of murine and human pathway. Phenotypically, MDSCs have features of immature
liver lymphocytes (see Fig. 10.5) and mediate inflammatory neutrophils, monocytes, or NK cells. MDSCs express PD-L1
reactions seen in viral and autoimmune hepatitis. Bulk human and also promote T-cell suppression through production of
liver NK cells possess weaker lytic capabilities when compared suppressive cytokines and enzymes. Tregs and MDSCs are
with autologous blood NK cells (Burt et al, 2009) because the likely both important contributors to baseline liver tolerance
liver has a greater proportion of NK-cell subtypes with weaker and suppression of immune responses to intrahepatic infection
cytolytic function when compared with blood NK cells. or cancer.
B Cells
CYTOKINES
B cells, along with T cells, mediate adaptive immune responses.
B cells are responsible for humoral immunity through antibody Cytokines (see Chapter 11) are small proteins that enable com-
production. B cells may also function as APCs under certain munication among immune cells, providing signals that govern
conditions. Although hepatic B cells have received very little and shape responses to tumor or pathogen. Cytokines can be
attention, they make up a significant proportion of liver lym- roughly divided into two categories, those of innate and those
phocytes. They play prominent roles in viral and autoimmune of adaptive immunity (Table 10.1). Cytokines also can be dis-
disease affecting the liver (Novobrantseva et al, 2005). In con- tinguished based on whether they are inflammatory or antiin-
trast, the contribution of hepatic B cells to the biology of liver flammatory. However, individual cytokine function is highly
tumors is poorly defined. Our group has recently reported that contextual, depending on environmental cues and target cell
MDSCs in the liver suppress hepatic B cells through downregu- features. Although hundreds of cytokines have been described,
lation of CD80, which is a costimulatory molecule involved in we limit our discussion here to a select few that have been
T-cell activation (Thorn, 2014). This may be a mechanism shown to be produced in, and have important effects on, the
through which hepatic B-cell function is altered to contribute liver.
toward intrahepatic tolerance. Further work is required to
develop our understanding of how hepatic B cells are affected Tumor Necrosis Factor-α
by the liver microenvironment and in turn influence intrahe- Tumor necrosis factor-α (TNF)-α was originally isolated from
patic diseases. animals treated with lipopolysaccharide, and its name is derived
from the fact that it was found to lyse tumors in vitro and in
IMMUNOINHIBITORY PATHWAYS AND vivo. TNF-α is one of the most important inflammatory cyto-
SUPPRESSOR CELLS kines. It directly regulates innate immunity and often has sys-
temic effects. TNF-α is primarily produced by macrophages in
Suppressive or coinhibitory signaling pathways are important response to lipopolysaccharide from gram-negative bacteria. It
mediators of intrahepatic tolerance. The immunoinhibitory also is secreted by T cells, mast cells, DCs, and NK cells.
receptors receiving the most attention in laboratories and clin- TNF-α has consistently been found to play a pathogenic role
ical trials are CTLA-4 and PD-1 (Brahmer et al, 2012; Finn, in acute liver failure in multiple animal models and in humans.
2008). The PD-1 and CTLA-4 axes are pivotal regulators of TNF receptors are present on most cell types, and the TNF
Chapter 10 Liver immunology 181
Innate Immunity
TNF-α Macrophages, T cells, DCs Endothelial cells: activation
Neutrophils: activation
Hypothalamus: fever
Liver: synthesis of acute-phase proteins
Muscle and fat: catabolism
Multiple cell types: apoptosis
IL-1 Macrophages, endothelial cells Endothelial cells: activation
Hypothalamus: fever
Liver: synthesis of acute-phase proteins
Chemokines Macrophages, endothelial cells, T Leukocytes: chemotaxis, activation, migration into tissues
cells, fibroblasts, platelets
IL-12 Macrophages, DCs, NK DCs T cells: Th1 differentiation
NK DCs, NK cells, and T cells: IFN-γsynthesis, increased cytologic activity
IFN-α, IFN-β IFN-α: macrophages, plasmacytoid All cells: antiviral state, increased inhibition of IL-12 production and
DCs IFN-β: fibroblasts expression of costimulatory and MHC class II molecules
IL-10 Macrophages, T cells (mainly Th2) Macrophages, DCs: inhibition of IL-12 production and expression of
costimulatory and MHC class II molecules
IL-6 Macrophages, DCs, endothelial Liver: synthesis of acute-phase proteins
cells, T cells
IL-15 Macrophages, others NK cells: proliferation
T cells: proliferation (memory CD8+ cells)
IL-18 Macrophages NK cells and T cells: IFN-γ synthesis
Adaptive Immunity
IL-2 T cells T cells; proliferation, increased cytokine synthesis; potentiates Fas-
mediated apoptosis
IL-4 CD4+ T cells (Th2), mast cells B cells: isotype switching to IgE
T cells: Th2 differentiation, proliferation
NK DCs and NK cells: increased IFN-γ production
IL-5 CD4+ T cells (Th2) Eosinophils: activation, increased production
IFN-γ CD8+ T cells (Th1), NK DCs, NK Macrophages: activation
cells
B cells: isotype switching to opsonizing and complement-fixing IgG
subclasses
T cells: Th1 differentiation
Various cells: increased MHC class I and II expression, increased antigen
processing and presentation to T cells
TGF-β T cells (regulatory), macrophages, T cells: inhibition of proliferation and effector functions
other cell types
B cells: inhibition of proliferation; IgA production
Macrophages: inhibition
Lymphotoxin T cells Neutrophils: recruitment and activation
Lymphoid organogenesis
IL-13 CD4+ T cells (Th2) B cells: isotype switching to IgE
Epithelial cells: increased mucus production
Macrophages: inhibition
IL-17 CD4+ T cells (Th17) Bone marrow progenitors: neutrophil development
Fibroblasts and endothelium: IL-6 and G-CSF production
DCs, Dendritic cells; G-CSF, granulocyte colony-stimulating factor; IFN, interferon; IgA, IgG, immunoglobulin A and G, respectively; IL, interleukin; NK, natural killer; MHC, major histocompatability
complex; TGF-β, transforming growth factor-β; Th, T helper; TNF, tumor necrosis factor.
Modified from Abbas AK: Cellular and molecular immunology, Philadelphia, 2003, Saunders Elsevier.
182 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
receptor family is a large group of proteins with myriad roles crosstalk among intrahepatic immune cell subsets has greatly
in inflammation and immunity. informed our appreciation of liver disease pathogenesis. The
following sections highlight the role of the hepatic immune
Interleukin-6 system in a variety of diseases affecting the liver.
IL-6 is a pleiotropic cytokine that is highly expressed by the
liver and has effects on innate and adaptive immunity. It is Transplantation
synthesized by DCs, KCs, T cells, B cells, endothelial cells, Transplant immunology has shed significant insight into the
fibroblasts, and keratinocytes. IL-6 is produced as an early unique properties of the liver as an immunologic organ. Unlike
response to TNF-α and is thought to amplify the inflamma- other organs, the liver can be accepted across MHC barriers in
tory response in the liver through the induction of acute-phase animal models of transplantation (Qian et al, 1994). In addi-
protein production by hepatocytes. As part of its promotion of tion, systemic, donor-specific tolerance often develops in liver
the early immune response, IL-6 also stimulates the differen- allograft recipients (Kamada et al, 1981). In humans, liver
tiation of neutrophils from bone marrow precursors. In transplants confer protection from other organs from the same
coöperation with TGF-β, IL-6 promotes expansion of proin- donor (Rasmussen et al, 1995), and recipients can often be
flammatory Th17 cells. Additionally, experimental models weaned off immunosuppression altogether (Mazariegos et al,
have shown that absence of IL-6 in cultures impairs DC 1997). The unique ability of allografts to resist rejection and
T-cell stimulatory function; however, IL-6–knockout mice promote extrahepatic tolerance speaks to the immunosuppres-
have normal numbers and types of DCs in their spleens and sive properties liver immune cells.
livers (Bleier et al, 2004). IL-6 also is known to play an The development of mouse models of orthotopic liver trans-
important role in liver regeneration after trauma or hepatec- plantation has provided an opportunity to gain mechanistic
tomy. We recently found that serum IL-6 levels correlated insight into the regulation of immune responses in the liver
with activity of intrahepatic T-cell immunotherapy for liver (Qian et al, 1991). Of the factors that are thought to contribute
metastases (Saied et al, 2014). to hepatic tolerance (Box 10-1), microchimerism and induction
of activated T-cell apoptosis have been the most intensively
Type I Interferons (Interferon-α and Interferon-β) studied and widely accepted. Defined as the persistence of
Type I IFNs refers to a family of structurally similar cytokines donor cells in allograft recipients, microchimerism has been
that are crucial in the immune response to viral infection. postulated to be a prerequisite for organ allograft acceptance
IFN-α is secreted by immune cells, whereas IFN-β is secreted (Starzl et al, 1992, 1996). The high antigenic load derived from
by multiple cell types, such as fibroblasts, in response to viral the donor liver coupled with persistence of donor APCs within
infection. IFN-α was previously thought to be produced by lymphoid tissues of the recipient may provide a continuing
macrophages; however, more recent evidence has shown that source of allostimulation (Sriwatanawongsa et al, 1995; Suzuki
plasmacytoid DCs are its primary producers (Siegal et al, et al, 1988). The persistent activation of alloreactive recipient
1999). Type I IFNs have direct antiviral action by triggering T cells is thought to result in exhaustive deletion and induction
virally infected cells to produce enzymes that interfere with of systemic tolerance. The role of specific donor-derived liver
viral RNA or DNA replication. They also lead to the increased APCs, such as DCs and KCs, in contributing to chimerism-
expression of MHC class I molecules on the surface of virally induced tolerance remains unclear. Although freshly isolated
infected cells, increasing their likelihood of being killed by liver DCs have been shown to exhibit tolerogenic potential via
cytolytic CD8+ T cells. Additionally, type I IFNs inhibit cel- the production of IL-10 (Bamboat et al, 2009a), others have
lular proliferation. IFN-α has been used clinically in the treat- shown that donor-derived liver DCs prime recipient T cells to
ment of viral hepatitis and as an adjuvant therapy for differentiate into proinflammatory subtypes that promote rejec-
melanoma. tion (Bosma et al, 2010).
The immunoregulatory role of KCs has also been exten-
Type II Interferons (Interferon-γ) sively investigated. KCs have been implicated in the induction
IFN-γ is a type II IFN. It is the archetypal proinflammatory
cytokine associated with antitumor immune responses. IFN-γ
activates macrophages and plays a crucial role in bridging
innate and adaptive immunity by increasing antigen presenta- BOX 10.1 Factors Contributing to Hepatic Tolerance
tion through the MHC class I and II pathways (Schroder et al, • Immunosuppression via release of soluble MHC class I antigens
2004). It is produced by T cells, B cells, NKT cells, DCs, and • Distinct lymphocyte population with distinct functions (KCs,
macrophages. IFN-γ promotes Th1-driven cytotoxic T-cell DCs, NK, and NKT cells, LSECs)
responses, which are essential for clearance of virally infected • Constant antigen load from the portal circulation
cells or tumors. In addition, IFN-γ promotes MHC expression • Induction of activated T-cell apoptosis
• Microchimerism
on APCs and enhances NK-cell cytotoxic activity. Increases in
• Immature phenotype and tolerogenic function of resident liver
serum IFN-γ levels have been correlated with favorable clinical
APCs (DCs, KCs, LSECs)
responses to immunotherapy treatments. • Altered Th1 versus Th2 profile within the liver (favoring Th2)
• Presence of suppressor cells (Tregs and MDSCs)
IMMUNE SYSTEM IN BENIGN • Immunoinhibitory pathways (CTLA-4, PD-1)
LIVER DISEASES APCs, Antigen-presenting cells; CTLA-4, cytotoxic T-lymphocyte–associated antigen-4; DCs,
dendritic cells; KCs, Kupffer cells; LSECs, liver sinusoidal endothelial cells; MDSC, myeloid-
Intrahepatic immune cells play prominent roles in myriad derived suppressor cells; MHC, major histocompatibility complex; NK, natural killer; NKT, natural
inflammatory, infectious, and neoplastic diseases affecting the killer T cell; PD-1, programmed death-1; Treg, regulatory T cells.
liver. Our understanding of liver immune cell biology and Modified from Gershwin ME, et al: Liver immunology. Philadelphia, 2003, Hanley and Belfus.
Chapter 10 Liver immunology 183
of oral tolerance and in lymphocyte apoptosis, which has been www.who.int/mediacentre/factsheets). The cost to society is
a proposed mechanism of immunosuppression in liver trans- magnified when the increased risk for cirrhosis and liver cancer
plantation (Callery et al, 1989). More recently, KCs have been in those infected with HBV and HCV are taken into account.
shown to play a crucial role in induction of antigen-specific Immune-mediated or inflammatory destruction of liver paren-
T-cell tolerance (Breous et al, 2009) and are thought to sup- chyma is a common final pathway in viral hepatitis. The pres-
press T-cell response via the production of prostaglandins (You ence of large numbers of KCs and DCs in the liver, which
et al, 2008). Despite evidence of the tolerogenic potential of produce TNF-α in response to viral antigens, leads to high local
KCs, the use of gadolinium chloride to suppress KC function levels of inflammatory cytokines and untoward host cell damage.
has not been shown to impact survival of liver allografts in Similarly, T cells, NKT cells, and NK cells in the liver produce
mouse models of liver transplantation. The disparate findings IFN-γ, which also serves to amplify the local immune response
concerning the role of KCs in liver transplantation may reflect by activating KCs and DCs. Consistent with this, chronic active
the opposing effects of tolerogenic MDSCs and proinflamma- hepatitis is morphologically identified by piecemeal necrosis
tory macrophages, both of which share considerable phenotypic and a predominantly mononuclear cell infiltrate (Ferrari et al,
overlap with KCs. 1999).
The overall bias of intrahepatic T-cell responses toward Despite immune cell activation and inflammatory cytokine
tolerance and apoptosis might account for the survival of liver production, the host is frequently unable to clear HBV or HCV.
allografts (Crispe, 2003). Activated T cells and their subse- Therefore, to achieve successful viral control and limit collat-
quent apoptosis within the liver are thought to be another criti- eral damage, a sustained, antigen-specific immune response is
cal component in the induction of hepatic tolerance and the necessary (Gerlach et al, 1999; Maini et al, 2000). Recognition
acceptance of liver allografts. Recently, hepatic stellate cells of multiple viral epitopes by the host is also advantageous, as
(HSCs) have been found to mediate liver T-cell apoptosis via it theoretically minimizes the emergence of mutants that escape
the PD-L1/PD-1 axis (Charles et al, 2013). HSCs may also the immune system. Unfortunately, effective T-cell responses
induce expansion of Tregs as another mechanism of influencing against HBV and HCV are susceptible to suppression by the
T-cell tolerance (Dangi et al, 2012). PD-1/PD-L1 immunoinhibitory access and Treg (Fuller et al,
From a more clinical perspective, patients transplanted for 2013). The tolerogenic predisposition of the liver may suppress
end-stage liver disease secondary to hepatitis B or C often adaptive immunity to HBC and HCV, accounting in part for
experience higher viral loads after transplantation secondary to the persistence of these infections.
the antirejection immunosuppressive regimen. Recurrent viral A number of additional host parameters have been shown
disease in the transplanted liver is inevitable and is therefore in experimental models to alter the immune response to viral
one of the most common reasons for allograft failure (Brown, hepatitis infection. Age can influence the outcome of infection,
2005). Recent work using adoptive immunotherapy of donor as vertical transmission to neonates generally results in persis-
lymphocytes provides some encouraging insight into addressing tent infection throughout life. Chronic viral infection in animal
recurrent viral disease in transplant recipients. Lymphocytes models of hepatitis occurs more often when the initial insult
enriched for NK and NKT cells harvested from donor livers at fails to elicit an acute inflammatory response. In woodchucks,
the time of explantation were primed ex vivo for 2 days prior the absence of an acute infection following viral inoculation
to reinjection into allograft recipients. Hepatitis C viral loads correlated with an indolent and chronic course of disease
were found to be significantly lower at 1 month posttransplan- (Nakamura et al, 2001).
tation in patients treated with adoptive therapy versus controls Emerging research tools that will undoubtedly shed more
(Ohira et al, 2009). Using human-hepatocyte chimeric mice, light on the immune mechanisms underlying viral persistence
the authors showed that adoptive transfer of activated donor and resistance to treatment include the development of chime-
lymphocytes conferred protection via the production of IFN-γ. ric mice that are reconstituted with human hepatocytes and
Other groups have also shown that antigen-specific CD8+ T immune cells (Manz & Di Santo, 2009). The transplantation
cells are thought to be important in preventing recurrence of of human hepatocytes into immunodeficient mice will allow for
hepatitis in transplant recipients via the production of IFN-γ large-scale screening therapeutics against human hepatitis
(Jo et al, 2009). viruses. Recently, an immunocompetent humanized murine
Although the hepatic immune system has been shown to HCV infection model has been developed (Chen et al, 2014).
clearly play an important role in liver and systemic tolerance, Chimeric murine models will enable researchers to study the
definitive mechanisms in humans remain elusive. It is likely that in vivo effects of human hepatotropic viruses on human immune
multiple suppressive cell types and several overlapping immu- responses to infection for the first time.
noinhibitory pathways interact to form a network of tolerance
within the intrahepatic space. Understanding the mechanisms Autoimmune Hepatitis
controlling the tolerogenic propensity of the liver is of great Autoimmune hepatitis (AIH) is an idiopathic disorder that
significance in transplantation, as it will permit the design of leads to cirrhosis. In contrast to the preceding sections that
novel approaches to reduce immunosuppressive-related mor- highlighted disease states associated with hepatic tolerance,
bidity and mortality. AIH is a manifestation of an overactive hepatic immune
system. AIH likely reflects an imbalance between proinflam-
Hepatitis matory immune responses and immunosuppressive factors,
The viruses hepatitis B (HBV) and hepatitis C (HCV) are the latter including PD-1/PD-L1, Treg, and MDSC. It has a
noncytopathic and hepatotropic, and cause acute and chronic female predominance and is characterized by elevated levels
liver disease (see Chapter 70). The worldwide burden of disease of immunoglobulin G (IgG) autoantibodies (Obermayer-
is immense, with an estimated 500 million people infected with Straub et al, 2000). An experimental model of autoimmune
either of these two viruses (World Health Organization, http:// hepatitis is based on the treatment of mice with concanavalin
184 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
A (ConA), a plant lectin known to activate T cells in vitro. A of postoperative allograft dysfunction and morbidity (Clavien
single intravenous injection of ConA leads to severe liver et al, 1992). During liver I/R, the release of endogenous mol-
damage and is associated with the activation of CD4+ T cells ecules signal danger to the host by activating innate immune
and the production of TNF-α and IFN-γ. Further studies cells through their interaction with Toll-like receptors (TLRs)
showed that NKT cells are the most important subset of (Lotze et al, 2007). Such “danger signals,” or danger-associated
CD4+ T cells involved in mediating ConA hepatitis. The molecular patterns (DAMPs), can be classified as intracellular
importance of NKT cells in mediating autoimmune liver proteins, nucleic acids, or components of the extracellular
damage also is supported by the observation that injection of matrix that are released following host cell injury (see Fig.
α-galactosylceramide, an activator of NKT cells through 10.7). The ensuing host innate immune response results in
CD1d binding, leads to a similar form of injury as that seen untoward collateral tissue damage that culminates in hepato-
in ConA hepatitis. AIH has also been linked with dysfunction cyte death and a systemic inflammatory response. The injury
of Tregs, leading to a hyperfunctional Th17 compartment and stems from the inability of TLRs on innate immune cells to
excessive inflammation (Grant et al, 2014). The pathogenesis distinguish infectious ligands from DAMPs released by autolo-
of AIH highlights the critical importance of balance between gous tissue. The need for effective approaches to manage
proinflammatory and antiinflammatory immune processes patients with I/R-induced organ damage is highlighted by the
within the liver. fact that current treatment is merely supportive care.
Using a murine model of segmental liver I/R, we reported
Primary Biliary Cirrhosis that hepatic DCs and TLR9 play critical roles in modulating
Primary biliary cirrhosis (PBC) is an autoimmune liver disease the host immune response during liver I/R (Bamboat et al,
that leads to the destruction of intrahepatic bile ducts and 2009b). Hepatocyte DNA released during ischemia binds
subsequent cholestasis and cirrhosis (Bergasa et al, 2004; TLR9 in a variety of liver immune cells that then cause liver
Lindor et al, 2009). Most cases of PBC are associated with damage. Using TLR9-knockout mice, we found that the global
antimitochondrial (95%) and antinuclear antibodies (50%) absence of TLR9 signaling confers protection from liver I/R
antibodies directed against self-antigens. Dysregulated CD4+ injury. Interestingly, the immune effects of TLR9 activation
helper T cells and CD8+ cytotoxic T lymphocytes are thought appear to be cell specific. In neutrophils, host DNA binds TLR9
to be important in the pathogenesis of PBC. This is supported and exacerbates injury through production of inflammatory
by the findings of lymphoid infiltration of the portal tracts and cytokines and reactive oxygen species (ROS). In contrast, DCs
aberrant expression of MHC class II on biliary epithelial cells. respond to host DNA by curtailing injury via production of
Because biliary epithelial cells are the primary target of injury antiinflammatory IL-10, which confers protection by suppress-
in PBC, their expression of MHC molecules and cytokines ing the function of inflammatory monocytes that migrate to the
likely plays an important role in the pathogenesis of this disease. liver from the bone marrow (see Fig 10.7). Human liver DCs
The degree of Th17 activity within the liver of PBC patients also have a propensity to secrete large amounts of IL-10 at
has been associated with severity of disease, and IL-17 pro- baseline and after TLR activation (Bamboat et al, 2009a). T
motes excessive fibrosis (Yang et al, 2014). In addition to lymphoctes also play a role in I/R tissue injury, with Th17 cells
pathogenic T-cell function, biliary epithelial cells from patients promoting influx of neutrophils (Kono et al, 2011). Improved
with primary biliary cirrhosis attract mononuclear cells via the understanding of the complex interactions between DAMPs
chemokine CX3CL-1 and overexpress the inflammatory cyto- and PRRs on immune cells will promote the development of
kines IL-6 and TNF-α (Shimoda et al, 2010). rational, more effective approaches to limit liver I/R injury.
TNF-α, and other inflammatory cytokines. During time, IL-6 understanding the relationship between the hepatic immune
and IL-10 production increases, favoring a more antiinflamma- system and the parasite. Eggs that are laid by adult worms in
tory state that limits immune-mediated damage and promotes the portal vein become trapped within the hepatic sinusoids and
hepatocyte regeneration. Liver DCs have been reported to trigger an immune response that results in granuloma forma-
expand following PH in mouse models (Castellaneta et al, tion. The early immune response mediated by eosinophils and
2006). After PH, liver DCs produce IL-10 and promote the neutrophils is proinflammatory. Later, the cytokine profile
development of antiinflammatory T cells. These data suggest within the liver becomes antiinflammatory and continues for
that inherent tolerogenic properties of hepatic DCs may serve the course of disease, ultimately resulting in liver fibrosis (Burke
to promote hepatocyte regeneration after hepatectomy. et al, 2009). KCs, IL-4, and IL-13 are thought to play a major
Like liver I/R, PH results in the release of a variety of danger role in skewing the immune response during the course of
signals that bind PRRs on innate immune cells, triggering a schistosomiasis infection (Hayashi et al, 1999).
cascade of signaling events that modulate the rate of parenchy-
mal regeneration. Deficiency in the intracellular signaling mol- IMMUNE SYSTEM IN MALIGNANT
ecule myeloid differentiation primary response 88 (MyD88), LIVER DISEASES
which acts downstream of almost all TLRs (except TLR3),
results in poorer outcome in mouse models of PH (Seki et al, Evidence on the importance of the hepatic immune system in
2005). In contrast, the absence of TLR3, which signals in a malignancy comes from data which reveal that (1) when com-
MyD88-independent manner, or blocking signaling of another pared with autologous blood, human liver specimens from
PRR, the receptor for advanced glycation end products patients with malignancy contain a disproportionately higher
(RAGE), promotes liver regeneration and survival after massive percentage of NK cells with reduced antitumor function (Burt
hepatectomy (Cataldegirmen et al, 2005; Zorde-Khvalevsky et al, 2009) and (2) the hepatic T-cell infiltrate predicts survival
et al, 2009). These data suggest that a balance exists between following surgery in patients with metastatic colorectal liver
various TLRs and RAGE that governs the net effect of partial cancer (Katz et al, 2009). Tumor-infiltrating lymphocytes
hepatectomy. Identification of mechanisms that limit regenera- (TILs) indicate a specific host response to tumor antigens.
tion after massive injury holds the key to expanding the limits TILs may be utilized with therapeutic intent or studied for
of liver transplantation and salvaging livers and hosts over- prognostic information (Rosenberg et al, 1986). TILs have
whelmed by carcinoma and toxic insults. been demonstrated to predict outcomes in a wide variety of
solid tumors, with the magnitude of this effect being dependent
Drug-Induced Liver Disease on tumor site and disease stage (Gooden et al, 2011). An
The prevalence of liver failure as a result of drug-induced toxic- increasing number of studies have focused on TILs as predic-
ity is increasing at an alarming rate and is the most common tors of outcome for primary and metastatic liver tumors. Our
cause of acute liver failure in the developed world (Lee, 2007). evolving understanding of intrahepatic antitumor immunity
The injury is characterized by toxin-induced hepatocyte death promises to enable development of novel therapeutic approaches
and activation of the innate immune system. This triggers a using immunomodulatory agents and adoptive cell therapy.
cascade of proinflammatory signals that result in further hepa-
tocyte death and, ultimately, in liver failure. Through the use Immune Response to Primary Liver Cancer
of mouse models of acetaminophen-induced liver injury, the Hepatocellular carcinoma (HCC) is one of the most common
roles of various components of the hepatic immune system have malignant tumors worldwide. The immune response to neo-
been well characterized. LSECs are thought to mediate liver plastic cells has been shown to be a potential determinant of
injury by detecting hepatocyte DNA via TLR9, resulting in survival in HCC patients (Fu et al, 2007; Gao et al, 2007;
production of pro–IL-1 and pro–IL-18, which are cleaved into Sasaki et al, 2008). High densities of DCs, T-cell subsets, and
their active forms by an intracellular protein complex called the tumor-associated macrophages have all been reported to be
inflammasome (Imaeda et al, 2009). Widespread inflammation favorable prognostic factors in HCC (Cai et al, 2005). TIL
ensues, resulting in additional parenchymal injury. responses to HCC occur in a more complex biologic context
than metastatic tumors given the underlying inflammatory pro-
Bacterial and Parasitic Liver Disease cesses that drive HCC carcinogenesis and progression.
Intrahepatic immunosuppression not only appears to be HCC TILs have been compared with T cells in adjacent
involved in tolerance to liver allografts but may also play a role normal liver tissue, and HCC TILs reflect a more immunosup-
in the vulnerability of the liver to various bacterial and parasitic pressed state. Mathai and coworkers (2012) demonstrated that
infections (see Chapters 12, 45, 72, 73, and 74). The liver is HCC TIL populations have a higher number of Tregs com-
susceptible to pyogenic abscesses, particularly in patients with pared with normal surrounding liver. Increased ratios of Tregs
malignant biliary tract disease undergoing complex endoscopic, (FOXP3+) to total T cells (CD3+) were independently associ-
percutaneous, and surgical interventions (Mezhir et al, 2010). ated with poorer differentiation. Furthermore, high FOXP3+ to
The host response to bacteria within the liver results in forma- CD8+ TIL ratios were associated with shorter overall and
tion of an abscess in an effort to curtail the spread of infection. disease-free survival times in HCC patients on both univariate
Neutrophils are recruited to the site of infection via chemotactic and multivariate analysis (Mathai et al, 2012). Immune sup-
signals released by the invading bacteria and activation of com- pression within HCC may also be attributed to increased
plement. Neutrophils then release cytokines and reactive expression of PD-1 on TILs. As noted earlier, PD-1 is an
oxygen species that promote inflammation and kill bacteria. immunoinhibitory receptor that suppresses T-cell division and
Helminthic infections of the liver, such as schistosomiasis, cytokine production (Wu et al, 2009). PD-1 is engaged by
echinococcosis, and ascariasis have a hepatic phase in their life PD-L1, which has been detected on HCC tumor cells. The
cycles. Animal models of schistosomiasis have helped in presence of Tregs and PD-1+ TILs is reflective of an
186 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
immunosuppressive milieu, but may represent a therapeutic outcome following resection of neuroendocrine tumor liver
opportunity as anti–PD-1 antibodies are now in clinical use for metastases (Katz et al, 2010). Tumor MHC I expression has
a variety of solid tumors. also been correlated to immune infiltrates and outcome (Tur-
TIL responses have also been studied in patients with biliary cotte et al, 2014).
tract cancers. Cholangiocarcinoma (CCA) is the second most A critical finding from studies of CRLM is that although
common primary intrahepatic malignancy, and most patients patients with favorable TIL profiles are more likely to have a
are not candidates for curative surgical intervention. A study of good outcome, the majority of individuals do not demonstrate
123 patients with intrahepatic CCA who underwent curative an effective intratumoral immune response. We speculate that
surgical resection revealed that IL-17+ (Th17) and FOXP3+ immunosuppressive intrahepatic immune cells and immunoin-
(Treg) TILs were enriched predominantly within CCA tumors, hibitory pathways limit the function of effector T cells. This
whereas CD8+ TILs were most abundant at the tumor margin. presents a therapeutic opportunity to deliver effective adoptive
IL-17+ TIL counts were an independent predictor of decreased cellular immunotherapy in conjunction with suppressive
patient survival, reflecting the importance of the Th17/Treg pathway inhibition to overcome the factors curtailing endoge-
balance in liver diseases (Gu et al, 2012). Similar to HCC, nous antitumor immunity.
tumor expression of PD-L1 was correlated with CCA stage and
tumor differentiation (Ye et al, 2009). Improving our under- Immunotherapy for Liver Cancer
standing of CCA immune responses and tumor-driven immu- Although many investigators have attempted to manipulate the
nosuppression may offer insights into novel therapeutic options immune system for the treatment of cancer (Hunder et al,
and improve risk stratification. 2008), few attempts have been made to directly target intrahe-
patic immune cells. The primary goal of cancer immunother-
Immune Response to Metastatic Liver Cancer apy, particularly for liver tumors, is to deliver or induce potent
The high prevalence of metastatic disease to the liver is likely antitumor immunity while reversing intrahepatic suppression.
due to multiple factors. Evidence suggests that particular Reversal of intrahepatic tolerance has been accomplished in
characteristics of the liver immune system may play an impor- animal models by activating liver immune cells, depleting sup-
tant role in this propensity. As delineated earlier, the primary pressor cells, or blocking immunoinhibitory pathways such as
mediators of innate and adaptive immunity found in the liver, the PD-1/PD-L1 axis. We previously demonstrated the impor-
DCs, and T cells, are unique in their distribution of subtypes tance of IL-12 production by DCs in activating NK cells toward
and skew toward tolerogenic function (Katz et al, 2005; Pil- protection against tumor in a mouse melanoma liver metastasis
larisetty et al, 2004). In addition, the liver contains suppres- model (Miller et al, 2002b). Despite having less lytic potential
sive cells such as Tregs and MDSCs that may also promote than blood NK cells, we found that human liver NK cells do
the establishment of metastatic colonies within the intrahe- have the capacity to become potent antitumor cells when acti-
patic space. vated in the presence of KCs and TLR3 ligands (Burt et al,
Several studies suggest that intrahepatic adaptive immune 2009).
responses to colorectal liver metastases (CRLM) are predictive In addition to DCs, recent work on the role of peritumoral
of recurrence and death following resection. Both CD4+ and monocytes in patients with HCC has garnered much attention
CD8+ T cells are activated within CRLM, and activated CD4+ among immunologists and hepatologists alike. Activated mono-
T helper cells may promote tumor-selective activity of cytotoxic cytes in the peritumoral stroma of HCC have been shown to
CD8+ T lymphocytes (Wagner et al, 2008). Following hepatic foster a state of tolerance and promote tumor progression via
resection, patients with high numbers of CD8+ intratumoral T the expression of an immunosuppressive molecule, PD-L1
cells were more likely to survive 10 years or longer. Among (Kuang et al, 2009). In addition, tumor expression of PD-L1
patients who survived for 10 years or more, 31% had high levels was recently shown to serve as a predictor of recurrence in
of CD8 T cells. In contrast, only 8% of those who survived less patients with resected HCC (Gao et al, 2009). Blocking anti-
than 2 years had a high level of CD8+ TIL (Katz et al, 2009). bodies to molecules such as PD-1 and PD-L1 are currently
Ratios of TIL subsets have been studied as well and may approved for human use.
provide more biologic insight than individual TIL counts. In As described above, most patients fail to mount effective
patients with CRLM, high CD8+ to CD4+ TIL ratios were an antitumor immunity, likely due to the immunosuppressive
independent predictor of long-term survival following resection nature of the intrahepatic space. Genetically modified chime-
after adjusting for multiple variables, including clinical risk ric antigen receptor T cells (CAR-Ts) offer a potential solu-
score. In a more recent study, high CD4+ to CD3+ and CD8+ tion to providing effective antitumor immunity for CRLM.
to CD3+ TIL ratios were a significant correlate of improved and CAR-Ts are produced from patient autologous T cells, using
recurrence-free survival (Katz et al, 2013). a retroviral system to engineer expression of an immune
As reported in the setting of primary liver cancer, TIL ratios, receptor that is activated upon engagement of tumor antigens
including FOXP3+ Treg, are predictive of outcome following such as carcinoembryonic antigen (CEA). In our recent phase
CRLM resection. High FOXP3+ to CD4+ and FOXP3+ to I Hepatic Immunotherapy for Metastases (HITM) trial, we
CD8+ TIL ratios were independent predictors of shorter overall demonstrated the safety and encouraging signals of clinical
survival. Overall survival at 5 years for patients with a high efficacy of hepatic artery anti-CEA CAR-T infusions in
FOXP3+ to CD4+ TIL ratio was 34% compared with 51% for patients with CRLM (Saied et al, 2014). Future HITM trials
patients with a low ratio (odds ratio = 1.6; P = .03). Similarly, will combine regional CAR-T infusions with immunomodula-
5 year survival was 35% in those with a high FOXP3+ to CD8+ tory agents designed to overcome intrahepatic suppression. It
ratio compared with 46% in those with a low FOXP3+ to CD8+ is likely that innovative combinatorial immunotherapeutic
TIL ratio (hazard ratio = 1.5; P = .05) (Katz et al, 2013). approaches will achieve greater clinical success than single-
FOXP3+ TIL counts were also found to be predictors of agent strategies.
Chapter 10 Liver immunology 187
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CHAPTER 11
Cytokines in liver, biliary, and pancreatic disease
Jason Maggi and George Miller
188
Chapter 11 Cytokines in liver, biliary, and pancreatic disease 189
Although also involved in inflammation through effects on cell FIGURE 11.2 Interleukin (IL)-6 and IL-11 signaling in cancer. IL-6
differentiation, proliferation, and apoptosis, IL-6 has also been and IL-11, produced by immune cells, fibroblasts, and epithelial and
found to play an important role in other functions, including malignant cells, activate the JAK/STAT3, SHP-2-RAS-ERK, and PI3K-
AKT pathways, through which they induce cell proliferation, survival,
immune regulation and oncogenesis (Elinav et al, 2013).
EMT/invasion, metastasis, angiogenesis and inflammation. AKT, Protein
IL-6 belongs to a nine member superfamily of cytokines,
kinase B; EMT, epithelial-to-mesenchymal transition; ERK, extracellular
which includes leukemia inhibitory factor, oncostatin M, signal-regulated kinase; gp130, glycoprotein 130; JAK, Janus activating
cardiotrophin-1, neurotrophic factor, as well as IL-11. Signal kinase; PI3K, phosphatidylinositol-3-kinase; RAS, rat sarcoma (protein);
transduction for all members of this family utilizes the signal- STAT, signal transducer and activator of transcription. (From Taniguchi
transducing receptor glycoprotein 130 kDa (gp130), making K, Karin M: IL-6 and related cytokines as the critical lynchpins between
this a potential target for future therapies. Upon formation of inflammation and cancer, Semin Immunol 26:54–74, 2014.)
gp130 homodimers by ligand binding, signaling is carried
forward primarily by the Janus activating kinase/signal trans-
ducer and activator of transcription pathway. downregulating the membrane-bound FAS apoptotic signaling
IL-6 has a wide range of effects, both in the hematopoietic pathway (Schneider et al, 1998).
system and in the innate immune response. It has been dem- The function of FAS in processes separate from apoptosis
onstrated that IL-6 has a substantial role in the balance between continues to be investigated. Although FAS was thought to be
IL-17–producing T cells and regulatory T cells; IL-6 overpro- found in cells of lymphoid or myeloid lineage, it is now known
duction and upregulation of T helper (Th)17 cells is thought to be present in a wide variety of nonlymphoid cells. Soluble
to be a critical factor in development of multiple autoimmune FASL has been demonstrated to induce inflammation through
disorders (Kimura & Kishimoto, 2010). IL-6 and IL-11, with both NIK signaling as well as phosphatidylinositol-3-kinase
known effects on cell proliferation, are felt to play a crucial role (O’Reilly et al, 2009). Ligation of FAS in these cases produces
in the development of hepatocellular carcinoma (Fig. 11.2) (see chemotactic factors, such as IL-8 and monocyte chemoattrac-
Chapter 91). Current studies are underway investigating inhibi- tant protein-1, recruiting neutrophils, although not activating
tion of these cytokines in solid tumors. them. This is contrary to, and separate from, the apoptotic
properties of FAS. Nonapoptotic function becomes vitally
FAS Ligand important in liver cells, which have the highest constitutive
Identification of the FAS ligand (FASL or CD95L) through expression of FAS. It has been demonstrated in mice that FAS
expression cloning confirmed that this membrane-associated is intimately involved in liver regeneration after partial hepatec-
protein is also a member of the TNF superfamily (Suda et al, tomy (see Chapter 6), rather than apoptosis, and functions in
1993). Initially thought to function exclusively as an inducer neutrophil recruitment in viral hepatitis (Desbarats & Newell,
of apoptosis, continued study has implicated FAS as a factor 2000). FAS also plays a role in inflammatory processes of
in inflammation, carcinogenesis, and cellular proliferation intestinal epithelial cells via interaction with TLR signaling
(Peter et al, 2007). Activation of FAS has certainly been pathways. These properties of FAS more closely resemble the
proved to trigger apoptosis, observed by the presence of FASL functions of the TNF/tumor necrosis factor receptor 1 (TNFR1)
at the surface of lymphocytes and natural killer (NK) cells, system.
where it functions to promote the elimination of transformed Additionally, links between FAS and carcinogenesis con-
and infected cells. Additionally, rapidly fatal hepatitis has tinue to be explored. Studies have demonstrated increased
been observed in murine models with upregulated FAS FAS-induced production of chemotactic factors and promotion
signaling pathway (Huang et al, 1999) (see Chapters 9D of tumor invasiveness and metastasis via MAPK pathways
and 70). (Barnhart et al, 2004). Additionally, increased serum levels of
A five stage model of activation of membrane-bound FAS soluble FAS have been correlated with decreased survival in
has been proposed, detailing a rapid caspase-dependent apop- multiple tumor types (Konno et al, 2000; Ugurel et al, 2001).
tosis of FAS-bearing cells (Lee et al, 2006). FAS also exists in This supports the view that FAS ligation, in certain physiologic
a soluble form, the result of cleavage via metalloproteases. This situations, can signal not only nonapoptotic pathways, but pos-
soluble FAS has been proposed as a FAS receptor antagonist, sibly prooncogenic transmission as well.
Chapter 11 Cytokines in liver, biliary, and pancreatic disease 193
Transforming Growth Factor-β hypoalbuminemia found in patients with chronic liver disease
Transforming growth factor-β (TGF-β) is another pleiotropic and have been predictive of a negative clinical course.
cytokine involved in many aspects of cellular function, includ- Acute-phase protein production has been found to occur as
ing differentiation, migration, angiogenesis, and apoptosis two separate groups, influenced by the presence of the specific
(Massague, 2008). It is stored as an intracellular latent form cytokine and signaling mechanism. Type I proteins, such as
until it is activated by several factors, including MMPs, integ- C-reactive protein, serum amyloid A, and complement C3, are
rins, and thrombospondin 1 (Ge & Greenspan, 2006). Of sig- primarily influenced by IL-1 and TNF-α, whereas type II pro-
nificant importance to TGF-β, the downstream effects of this teins, such as fibrinogen, α1 antitrypsinase, and ceruloplasmin,
cytokine are quite context and cell dependent. The primary are primarily stimulated by IL-6 (Moshage, 1997). These pro-
signaling mechanism is through the phosphorylation of SMAD2 teins have a wide range of effects in the acute response, both
and SMAD3, allowing translocation into the nucleus and resul- proinflammatory and antiinflammatory (Table 11.3). For
tant gene activation (Shi & Massague, 2003). Additionally, example, both haptoglobin and hemopexin act as antioxidants,
activation can occur via SMAD-independent pathways, primar- protecting against reactive oxygen species, and haptoglobin aids
ily through MAPKs. in angiogenesis, critical to hepatic regeneration (Cid et al,
The function of TGF-β is often contradictory, as it can 1993) (see Chapter 6).
function to arrest growth, as well as act as a tumor promoter. Prolonged and unregulated response can result in irrevers-
The functional switch can occur at many points in the signaling ible tissue damage in the host, and counterregulatory mecha-
pathway. In the SMAD-dependent pathway, location of forma- nisms are necessary. An IL-1 receptor antagonist has been
tion of the active complex appears to play a role in conversion implicated in attenuating the acute response; studies of pre-
to oncogenic properties, as increased phosphorylation of the treatment with IL-1 receptor antagonist (IL-1ra), a recom
linker region of SMAD3, in preference to the C-terminal binantly synthesised endogenous inhibitor of IL-1, have
region, is seen in many advanced tumors (Wrighton et al, demonstrated decreased progression of inflammation. IL-6,
2009). Although less common, mutations can also play a role which is an extremely strong inflammatory stimulus early in the
in tumor development, which is seen with increased SMAD4 response, has been implicated to counteract this effect via a
inactivation in pancreatic carcinoma (Goggins et al, 1998). negative feedback loop, decreasing production of multiple pro-
Additionally, aberrant TGF-β signaling has been implicated in inflammatory cytokines (Xing et al, 1998). Additionally, activa-
the progression of hepatic fibrosis through the increased pro- tion of the hypothalamic-pituitary-adrenal axis, primarily by
duction of connective tissue growth factor by hepatic progenitor IL-1 and IL-6, induces production of steroid hormones.
cells (Gressner et al, 2002) (see Chapter 7). Increased release of glucocorticoids facilitates transport of free
amino acids to the liver, providing the substrates necessary for
Cytokines in the Liver and Pancreas Regulation of production of antiinflammatory acute-phase products.
Cytokine Expression in the Liver
Hepatic response to inflammation and parenchymal injury pro- Cytokines and the Pancreas
duces a variety of effects in the host, both locally and systemi- Defining the effects of specific cytokines in pancreatic dysfunc-
cally. Because as many as 80% of all macrophages in the body tion is complicated by the pleiotropic effect of these molecules.
are Kupffer cells, the liver has a major impact on production Pancreatic islet cells produce multiple cytokines in the well
of inflammatory mediators. Although cytokine expression in the state, regulating B-cell function and replication. Increasing
liver is low at baseline, as a nonspecific first line of defense from IL-1 levels stimulates B-cell proliferation to respond to exog-
bacterial products from the hepatic circulation, a rapid, orches- enous stressors. However, prolonged stress has been implicated
trated response is needed for host protection. in islet cell dysfunction and destruction. Mouse models have
Hepatic cytokine contribution has been demonstrated in demonstrated the role of TGF-β in the progression of type 1
human studies, where cannulation of the hepatic vein after diabetes, and elevated concentrations of this cytokine have been
intravenous endotoxin administration revealed that large implicated in increased microvascular complications in diabetic
amounts of both TNF-α and IL-6 in the systemic circulation children (Zorena et al, 2013).
were derived from the splanchnic bed (Fong et al, 1990). TGF-β has also been studied as a contributing factor in
Increasing evidence has also defined the role of hepatic stellate the development of chronic pancreatic inflammation (see
cells in recruitment and induction of infiltrating leukocytes, Chapters 54 and 55) and pancreatic adenocarcinoma (see
amplifying the inflammatory response. Infiltration of T cells Chapter 59). Elevated levels are found in patients with chronic
and NK cells can enhance production of TNF-α, FASL, and pancreatitis, correlating with progression of fibrosis and
TGF-β, as described in studies of virally induced hepatic injury insulin resistance. It has been postulated that insensitivity to
(Melhem et al, 2006). Increasing levels of these cytokines, TGF-β stimulation, with resultant elevated levels, results in a
through varied mechanisms of insult to the host, has been switch from inhibitory effects to increased proliferation of
demonstrated in both hepatic injury and regeneration. pancreatic adenocarcinomas, in concert with additional cyto-
kine influence (Table 11.4). Accordingly, elevated TGF-β1
Cytokines and the Hepatic Acute-Phase Response and TGF-β2 receptor levels have been associated with
In response to hepatic injury, release of IL-1, IL-6, and TNF-α advanced cancers, with a trend toward worse overall survival
accounts for the stimulus to upregulate production of acute- (Javle et al, 2014).
phase reactant proteins. Whereas cytokine-stimulated tran-
scription factors produce increased amounts of acute-phase Cytokines and Apoptosis
proteins, levels of constitutively active proteins, such as albumin, The process of hepatic inflammation exists to protect the hepa-
transferrin, and blood factor XII, decrease proportionately tocytes and the host from excessive injury, while promoting
(Baumann & Gauldie, 1994). These findings account for the repair of tissue damage. However, with overwhelming or
194 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
TABLE 11.3 Hepatic Acute-Phase Proteins and Their Major Biologic Functions
Acute-Phase Reactant Major Biologic Functions
Complex II
Complex I (DISC)
Procaspase-8
Liver Regeneration mice and specific cytokine inhibitors have demonstrated the
The liver possesses a unique capacity for repair after injury; it importance of TNF-α and IL-6 in the initiation phase of regen-
is the only solid organ with the ability to fully regenerate eration (Michalopoulos & DeFrances, 1997). This is supported
damaged or lost tissue (see Chapters 6, 103, and 108). This by the finding that expression of inflammatory cytokines is
ability differs significantly from other organs, which heal by scar upregulated soon after hepatic resection, with serum levels of
formation (Fausto et al, 2006). However, in certain disease TNF-α and IL-6 detectable for up to 5 days (Abshagen et al,
states, cellular damage outpaces the regenerative capacity, and 2007). Progression to the proliferative phase is primarily regu-
healthy functioning epithelial tissue is replaced by connective lated by mitogenic factors such as hepatocyte growth factor,
tissue; such is the case with hepatic fibrosis and the develop- and the termination has been associated with members of the
ment of cirrhosis. Insights into the mechanisms involved in TGF-β superfamily, such as TGF-β1, follistatin, and activin.
hepatic regeneration open the door for potential therapeutic Inhibition of these TGF-β members in combination has been
targets to prevent chronic liver diseases. demonstrated to disrupt normal cessation of the proliferative
The process of liver regeneration has been described to phase (Oe et al, 2004).
occur in three phases: (1) initiation, (2) proliferation, and (3) An increasing body of evidence suggests that TNF-α, and,
termination (Zimmermann, 2004). Studies utilizing transgenic possibly more important, signaling through TNFR1, are crucial
Chapter 11 Cytokines in liver, biliary, and pancreatic disease 197
TNF-α
FASL
Cell membrane
TNFR
TRAIL FAS FADD
FLIP Mitochondria
TRAIL-FADD
R1/R2 Smac/Diablo
Caspase-8 Omi/HtrA2
Caspase-10 Cyto c
IAPs Apoptosome
Caspase-3 BCL-2
Caspase-7 Caspase-9
p53
NF-κB/survivin-XIAP
Apoptosis
Proliferation
Nucleus
FIGURE 11.4 Regulation of apoptosis-signaling pathways. The apoptotic cell death requires the interplay of a multitude of factors. These related
factors are organized in a tight and efficient manner to mediate apoptotic signaling. Both FAS and TNF-α demonstrate significant overlap in the
apoptotic pathway via activation of caspases 3 and 8 to signal cell death. The activation of apoptosis causes cell death instantaneously unless the
cell death is inhibited by potent antiapoptotic signals. Transcription factors such as NF-κB and p53 have the ability to mediate apoptosis through
upregulation or downregulation of apoptosis-related gene expression in nuclei. BCL-2, B-cell leukemia/lymphoma (apoptosis regulator)-2; BIR, bacu-
lovirus inhibitor of apoptosis protein (IAP) repeat; FADD, FAS death domain; FLICE, FADD-like IL-1β–converting enzyme, FLIP, FLICE-inhibitory protein;
HtrA2, HtrA serine peptidase 2; IAPs, inhibitor of apoptosis proteins;NF-κB, nuclear factor κB; Smac/Diablo, second mitochondria-derived activator
of caspase/direct inhibitor of apoptosis-binding protein with low pI; TNF, tumor necrosis factor; TNFR, TNF receptor; TRAF2, TNF receptor-associated
factor 2; TRAIL, TNF-related apoptosis-inducing ligand; TRAIL-R1, TRAIL receptor-1 XIAP, X-linked inhibitor of apoptosis protein. (From Wang K, Lin
B: Inhibitor of apoptosis proteins (IAPs) as regulatory factors of hepatic apoptosis, Cell Signal 25:1970–1980, 2013.)
198 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
before partial hepatic resection in mice reduced the oxidative Nitric oxide has also been demonstrated to contribute to the
dysfunction seen after such an insult (Jin et al, 2007). Protec- integrity of the gut mucosal barrier. LPS-induced iNOS pro-
tion has also been demonstrated through IL-6–mediated cell- duction increased permeability of an experimental intestinal
cycle arrest and activation of DNA mismatch repair genes, monolayer, resulting in a 10-fold increase in bacterial transloca-
ensuring a correct course of regeneration (Tachibana et al, tion (Forsythe et al, 2002). Supporting these findings, a
2014). study of 44 cirrhotic patients demonstrated that the level of
Adequate production of IL-6 and subsequent proliferation is disease progression corresponded to an increased presence of
linked to TNF-α and TNFR1 activation. However, as discussed NO-secreting CD14+ macrophages, implicating these cells as a
previously, TNF-α can also be a potent stimulator of apoptosis. potential source of permeability increasing cytokines (Du
The decision to trigger the antiapoptotic pathway appears to be Plessis et al, 2013).
regulated by the activation of NF-κB. After inhibition of NF-κB,
administration of TNF-α to mouse livers upregulated caspases-3 Pathogenesis of Proinflammatory Cytokines
and caspase-9 and produced massive hepatocyte apoptosis (Xu Although it is impossible to establish a direct link between an
et al, 1998). Similarly, inhibition of NF-κB using an adenoviral individual cytokine and disease progression, mounting circum-
vector produced rapid onset of liver failure after partial hepatec- stantial evidence continues to demonstrate their contributions
tomy (Iimuro et al, 1998). These findings provide the link to, and potential targets for, multiple diseases.
between TNF-α signaling and IL-6 production, as well as the Deregulation of multiple cytokines has been linked to out-
necessity of NF-κB–dependent gene transcription for appropri- comes in hepatitis (see Chapters 9D and 70). Patients infected
ate induction of hepatic regeneration. with hepatitis C have demonstrated increased hepatocyte apop-
tosis (McPartland et al, 2005). TNF-α has been shown to be
PATHOGENESIS OF ENDOTOXIN AND an integral factor in the development of fulminant hepatic
CYTOKINES IN LIVER, BILIARY, AND failure in humans and mice, and elevated serum TNF-α levels
have been correlated with mortality in alcoholic hepatitis
PANCREATIC DISEASE (Rachakonda et al, 2014). Elevated TNF-α levels correlated
In patients with advanced liver disease, there is an enhanced with level of fibrosis in hepatitis B and C patients (Akcam et al,
susceptibility to systemic endotoxemia; rarely does this occur 2012), and patients infected with hepatitis C demonstrate a
in patients without advanced disease or end-organ dysfunction. correlation between increased disease severity and elevated
Elevated levels of plasma endotoxin have been found in patients levels of soluble FAS (Hayashi & Mita, 1997). Elevated soluble
with a variety of hepatic disorders, and the degree of elevation FAS and TNF-α levels corresponded with elevated alanine
has been correlated with severity of disease (Lin et al, 1995). aminotransferase levels and increased severity of disease
The concept of the passage of viable intestinal bacteria through (Raghuraman et ak, 2005). Additionally, elevated IL-6 levels
the gut mucosa into mesenteric lymph nodes and sterile tissue strongly associated with liver-related mortality in hepatitis C
has been defined as bacterial translocation (Berg & Garlington, patients (Nakagawa et al, 2015). Studies of hepatitis B–infected
1979). mice have implicated IL-6 overexpression to altered cell-cycle
Intestinal bacterial overgrowth, as has been observed in regulation and impaired hepatic regeneration (Quetier et al,
patients with advanced liver disease, has been closely linked 2013).
with development of bacterial translocation (Chang et al, 1998; However, in advanced viral hepatitis, elevated TNF-α levels
Llovet et al, 1998). However, other factors also likely contribute often do not correspond with apoptosis of infected cells and
to translocation. Structural changes of intestinal mucosa in cir- hepatic regeneration. This is presumably due to increased
rhotic patients has been observed (Norman et al, 1980), as well NF-κB activation, preventing the apoptotic functions of TNF-α
as increased permeability allowing tight junction translocation (Collins et al, 2014). The finding that administration of anti–
(Pascual et al, 2003; Zuckerman et al, 2004). Use of nonselec- TNF-α functions in an antiviral manner, upregulating apopto-
tive β-blockers to decrease portal venous pressure gradient sis of infected cells and inhibiting regeneration, supports this
resulted in decreased translocation, as well as reduced serum line of thought (Brenndorfer et al, 2010). These findings
IL-6 and LBP levels (Reiberger et al, 2013). Additionally, mul- suggest a complex interaction between these cytokines and the
tiple disease states, such as hemorrhagic shock, have been iden- ability to remove virally infected cells.
tified to produce similarly increased permeability (Kompan Similarly, in patients with alcoholic hepatitis, elevated serum
et al, 1999). levels of TNF-α and IL-6 appear to play a significant role in
Disease states and increased translocation stimulate the gut- disease severity. In patients with acute alcoholic hepatitis, levels
associated lymphoid tissue to respond with increased produc- of these cytokines were strongly associated with 180 day mor-
tion of multiple cytokines, producing an inflammatory state, tality (Rachakonda et al, 2014). Endotoxin levels are also sig-
possibly potentiating bacterial translocation. Bile duct–ligated nificantly increased in these patients compared with healthy
mice demonstrated elevated levels of TNF-α in the lamina control participants, and concentrations have been correlated
propria of the gut, as well as accelerated hepatic fibrosis (Hart- with mortality (Fujimoto et al, 2000). Elevated endotoxin
mann et al, 2012). Similarly, elevated serum TNF-α levels are levels are likely due to increased hepatic exposure to LPS prod-
also found in mesenteric lymph nodes of cirrhotic patients ucts via translocation from the gut (Pinzone et al, 2012). The
(Genesca et al, 2003), and administration of anti-TNF anti- enhanced inflammatory reaction seen is likely mediated through
bodies has been demonstrated to significantly reduce bacterial activation of Kupffer cells via the LPS/LBP pathway, providing
translocation (Frances et al, 2007). Additionally, elevation of a potential therapeutic target of therapy for alcoholic hepatitis
serum IL-6 levels has been implicated as a contributing factor (Sandahl et al, 2014).
for increased gut permeability in hemorrhagic shock models Aberrant signaling pathways have also been implicated in
(Yang et al, 2003). the progression to malignancy. Reduced FAS expression has
Chapter 11 Cytokines in liver, biliary, and pancreatic disease 199
been implicated in the loss of normal apoptotic mechanisms reperfusion. eNOS knockout mice demonstrated increased
seen with the development of hepatocellular carcinoma (Fuku- severity of hepatic injury after ischemia compared with their
zawa et al, 2001; Shin et al, 1998). IL-6 levels were found to wild-type counterparts. Additionally, TNF-α expression was
correlate with poor prognosis in hepatocellular carcinoma (Jang upregulated to a level five times that in the wild-type mice
et al, 2012; Ohishi et al, 2014). Additionally, although no (Hines et al, 2002), suggesting a protective effect from cytokine
direct link between NO and development of carcinoma has injury. This protection has demonstrated effects beyond the
been defined, in patients with hepatocellular carcinoma, ele- liver, as NO has also been shown to reduce the incidence of
vated levels of iNOS in conjunction with COX-2 expression onset of hepatopulmonary syndrome in transplanted rats (Diao
had a significant negative effect on patient survival (Rahman et al, 2012).
et al, 2002). Despite these findings, it is often difficult to establish a link
Experimental models of obstructive jaundice demonstrate between elevated levels of proinflammatory mediators and a
similar alterations in cytokine levels, and TNF-α and IL-6 have negative clinical outcome. Insight into this link comes from
been identified as the dominant cytokines (see Chapter 8). studies of patients undergoing thoracoabdominal aortic aneu-
Endotoxin-mediated stimulation of the innate immune system rysm repair; intraoperatively, supraceliac aortic clamping pro-
produced a markedly exaggerated production of TNF-α and duces a demonstrable I/R injury, reflected by enhanced release
IL-6 in common bile duct–ligated mice compared with control of proinflammatory cytokines (Welborn et al, 2000). Microar-
subjects (Badger et al, 2012; O’Neil et al, 1997). This finding ray analysis of peripheral blood leukocytes found changes in
suggests a process of sensitization of macrophages to the effects 146 genes that were correlated with progression to multiorgan
of LPS. Support for these results is demonstrated by altered dysfunction, measured at 2 and 24 hours postreperfusion.
Kupffer cell function in obstructive jaundice, with increased Forty-one genes demonstrated increased expression at 2 hours;
responsiveness to the effects of LBP (Minter et al, 2005). several of these are involved in the innate immune response
Although IL-6 levels decreased after drainage and relief of (Feezor et al, 2004). Similarly, in a study of 25 patients under-
obstruction (Akiyama et al, 1998), slower resolution of IL-6 going thoracoabdominal aortic aneurysm repair, elevated levels
elevation has been linked with lower albumin levels and of neutrophil NF-κB strongly predicted onset of multisystem
increased frequency of positive bile cultures. Although no direct organ failure and mortality (Foulds et al, 2001).
link between IL-6 levels and outcomes can be concluded, pro-
longed elevation of IL-6 after drainage has been associated with Cytokines in Hepatic Tumor Ablation
elevated mortality in malignant obstructions (Yilmaz et al, For hepatic tumors not amenable to resection, multiple ablative
2013). techniques have been developed for local control with the goal
of improving overall survival (see Chapter 98). Although the
Cytokines in Ischemia-Reperfusion Injury mechanisms of ablation differ, all techniques aim for controlled
Ischemia-reperfusion (I/R) injury continues to be an important tumor cell destruction while sparing functional remnant liver.
cause of organ dysfunction after restoration of adequate blood However, unlike resection, ablative techniques leave the remain-
flow. This type of injury is seen in a variety of surgical condi- ing debris of devitalized tumor in situ, with large amounts of
tions, including transplantation, aortic surgery, elective hepatic tumor antigen resulting in immunologic reactions and cytokine
resections, as well as trauma-related disorders. Although the alterations.
exact mechanisms of I/R injury remain unclear, considerable Radiofrequency ablation (RFA) heats intratumoral cells to
evidence exists indicating the release of several cytokines fol- a temperature of 60° C to 100° C to create a coagulative necro-
lowing an ischemic insult (Liu et al, 2000). sis (see Chapter 98B). For optimal control, a goal of a 1 cm
TNF-α appears to play a central role in I/R injury. Murine margin of tissue surrounding the tumor should be achieved
models have demonstrated a significant increase in TNF-α (Dodd et al, 2001). Although tumor size limitations of approxi-
levels after 90 minutes of ischemia, followed by 60 minutes of mately 3 cm were required to obtain an adequate treatment
reperfusion (Colletti et al, 1990). Although the exact mecha- margin (Berber et al, 2004), advances in the technology of
nism stimulating TNF-α release is not yet defined, it appears thermal delivery are expanding this limit. In a human study of
that production is significantly influenced by Kupffer cell acti- 17 RFA-treated patients, no appreciable changes in cytokines
vation. In rats, Kupffer cells isolated from the liver after I/R (TNF-α, IL-1, IL-6, IL-1R, IL-10) were noted within the 48
demonstrated a several hundred fold increase in TNF-α pro- hours following treatment; median hepatic volume treated was
duction compared with controls. Treatment with anti–TNF-α 36.8%. Additionally, stimulation with LPS of whole-blood
antibodies significantly decreased both TNF-α and IL- 6 pro- samples demonstrated retained the ability for normal cytokine
duction (Wanner et al, 1999). Mediation of the effects of production, indicating adjacent Kupffer cells are inactivated by
TNF-α occurs primarily through activation of NF-κB. Trans- coagulative necrosis (Schell et al, 2002). However, in rat
location to the nucleus and binding activity of NF-κB models of large-volume RFA, 50% to 60% liver-volume treat-
increased as much as 66% after 5 minutes of ischemia (Li ment produced a significant rise in TNF-α and IL-6 indications
et al, 1999). Additionally, inhibition of NF-κB activation has (Ng et al, 2006). This may indicate that both tumor size and
demonstrated significantly decreased hepatic apoptosis and overall liver volume treated can be limitations for effective, safe
caspase-3 activity (Giakoustidis et al, 2010). This is similar to treatment.
findings with induction of heme oxygenase-1, which functions A more recent technique for tumor ablation is irreversible
to suppress TNF-α/TNFR1-directed hepatic apoptosis (Kim electroporation (see Chapter 98C). This therapy utilizes short,
et al, 2013). intense electric fields across cell membranes, increasing perme-
NOS also appears to be a factor in hepatic ischemia- ability. This allows for ablation of large amounts of tissue
reperfusion injury. The endothelial isoform of NOS (eNOS) without thermal effect. Preliminary animal studies have dem-
has most clearly been defined as a protective molecule during onstrated elevated percentages of CD4+ T lymphocytes and
200 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
IL-10 levels compared with hepatic resection groups (Li et al, agonists are currently demonstrating promise in murine pan-
2012), opening the possibility for future adjuvant immuno- creatic carcinoma models as tumor vaccine adjuvants (Huynh
therapy. Further studies are underway to fully elucidate the et al, 2012). Given the known importance of this receptor
relationship between electroporation and the inflammatory family in cellular signaling, TLR4 is also a potential target for
response. therapy. Despite some initial success, much work remains
before TLR antagonists can be considered as therapeutic
FUTURE DIRECTIONS agents. Multiple clinical trials continue to investigate TLRs as
potential targets for therapy (Aranda et al, 2014).
With increased understanding of cytokine functions and their Although evaluated in patients for the treatment of sepsis,
role in certain molecular pathways, intensive investigation into use of antiendotoxin as a therapy to abate the inflammatory
focused targeting of these molecules has progressed greatly over response would appear to be applicable to a variety of disorders.
the past decade. Agents are currently available as both inhibi- However, results from numerous studies investigating the clini-
tors and inducers of certain cytokines for conditions such as cal utility of antiendotoxin antibodies have been disappointing.
chronic autoimmune diseases, inflammatory disorders, and Multiple possibilities exist as potential sources for this lack of
infectious complications. Additionally, inhibition of endotoxin efficacy. Variability in patient selection, timing of treatment,
and the inflammatory response continues to show progress. and nonstandardization of preparations all have been investi-
Utilizing these advances, progression to targeted cytokine gated as potential sources. Additionally, variability in lipid A
therapy and inhibition for liver, biliary, and pancreatic diseases structure among gram-negative bacteria adds to the difficulty
certainly appears to be a logical direction for future research. of developing an effective treatment. This is supported in find-
The utility of cytokine treatment for a variety of hepatic ings that predicted mortality risk appears to be species depen-
diseases has been known for some time. Pegylated IFN-α, with dent (Hurley & Opal, 2013). Despite early setbacks, further
an elimination half-life of 75 hours, has been used in combina- investigation into delivery of antiendotoxin as subunit vaccines
tion treatment of chronic hepatitis C for more than 15 years. would appear to be an attractive option, given the relative lack
This breakthrough demonstrated the applicability of cytokine of new antimicrobials coming to market (Cross, 2014).
therapy in hepatic diseases. However, due to the pleiotropic Increased success has been observed with modulators of
nature of these cytokines, inhibition or induction of individual downstream mediators of the inflammatory process, particu-
targets proves difficult as a treatment for hepatic, biliary, and larly in the treatment of rheumatoid arthritis. Currently, five
pancreatic diseases. Interactions between multiple networks TNF-blocking agents have received U.S. Food and Drug
and pathways appear to be the driving force behind disease Administration approval, with promising results. TNF-α block-
progression, rather than alterations by an individual mediator. ers infliximab (Remicade) and adalimumab (Humira) have also
However, utilizing the known effects of these cytokines to been utilized in the treatment of complicated Crohn disease.
enhance immune responses is an area of current study. Additionally, a synthetic IL-1R antagonist, anakinra (Kineret),
Cytokine-induced killer cells—autologous lymphocytes incu- is currently in use for treatment of rheumatoid arthritis.
bated with cytokines such as IL-1 and IL-2—have shown favor- As further knowledge of the mechanisms of these agents is
able effects in the treatment of hepatocellular carcinoma in gained in the future, their applicability in hepatic, biliary, and
phase 1 and 2 studies (Ma et al, 2012). Current phase 3 studies pancreatic disorders will likely become increasingly evident.
are now underway. Although the complex interactions of multiple cytokines and
Targeting of Toll-like receptors as a means to achieve anti- pathways make targeting specific actors in hepatobiliary and
neoplastic effects in patients with pancreatic ductal adenocar- pancreatic diseases quite difficult, it is exactly this complexity
cinoma is also a current area of study. Phase 1/2 trials of that provides many untapped potential opportunities for inter-
macrophage-activating lipopeptide-2, a synthetic agonist of vention in the future.
TLR2 and TLR6, have demonstrated promising results in
R2-resected tumors (Schmidt et al, 2007). TLR2 synthetic References are available at expertconsult.com.
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CHAPTER 12
Infections in hepatic, biliary, and pancreatic surgery
Nicholas Spinelli, Matthew S. Strand, and Ryan C. Fields
Infections are a significant cause of morbidity and mortality in Chapter 43, 72, and 73). These same organisms may also pass
the surgical patient. Furthermore, infectious complications through the liver to access the systemic circulation, potentially
occurring in the postoperative setting have become a topic of leading to sepsis and septic shock. These pathologic states do
scrutiny in both the medical and public arenas. This increased not normally occur in the healthy human because of defense
awareness about infections and other perioperative complica- mechanisms that exist at multiple organ-system levels. In this
tions has been driven by major quality outcome initiatives, such section, we are interested in those mechanisms specific to the
as the National Surgical Quality Improvement Program hepatobiliary system and pancreas.
(NSQIP) sponsored by the American College of Surgeons Pathogenic organisms may enter the liver by two major
(ACS) (http://site.acsnsqip.org). It is necessary for physicians pathways. The first is the portal venous system, which delivers
and other health care providers to understand the nature of blood from the GI tract. In addition to absorbed nutrients,
infection in the surgical patient and how best to prevent it. portal venous blood also contains enteric bacteria and toxins
Caring for patients with hepatobiliary and/or pancreatic that may result in illness if not appropriately cleared by the liver.
disease can be quite challenging with regard to infection, The second pathway into the liver is via retrograde entry
especially in patients undergoing major hepatic or pancreatic through the biliary system. Organisms already present within
resection after preoperative biliary instrumentation. Although the systemic circulation may also enter the liver via a third
the hepatobiliary and pancreatic (HPB) surgical subspecialty pathway—the arterial inflow. Intravenous drug use and endo-
has evolved greatly during the past several decades, the morbid- carditis are two important mechanisms by which this can occur
ity following these procedures continues to be significant. (Fig. 12.1).
Infectious complications, in particular, are an important con- Both the liver and the biliary system contain important
tributor to this morbidity. Modern 30 day surgical-site infection defense mechanisms that prevent enteric organisms from
(SSI) rates after HPB procedures can be as high as 20% to 40% establishing infection within the liver (i.e., hepatic abscess) and/
(Ceppa et al, 2013). Infection is also associated with increased or reaching the systemic circulation. Generally, defense mecha-
hospital stay, operative times, transfusions, blood loss, intensive nisms are categorized into three types: physical, chemical, and
care unit use, and readmission rates (Kent et al, 2013). In immunologic (Table 12.1). The single most important mecha-
addition to these short-term sequelae, long-term sequelae nism within the liver is the immunologic defense provided by
include possible delay in adjuvant therapy. Kupffer cells. Kupffer cells are phagocytic cells located in the
The goal of this chapter is to understand the range of infec- sinusoids of the liver. They are derived from circulating mono-
tious complications that may accompany resections of the liver, cytes and represent almost 90% of the tissue macrophages
biliary tree, and pancreas and to gain an appreciation for the present in the human body. Kupffer cells are constantly exposed
important surgery-specific risk factors for infection. We also to enteric organisms and endotoxins, leading to their activation
review potential ways of mitigating infection risk at the preop- as phagocytes. Once activated, Kupffer cells also release various
erative, operative, and postoperative levels of patient care. With cytokines, prostanoids, nitric oxide, and reactive oxygen species
a general lack of level I evidence to guide clinical decisions, that contribute to their immune function (see Chapters 7, 10,
there continues to be controversy surrounding some of these and 11). Additionally, Kupffer cells indirectly regulate the
putative risk-lowering methods. phenotype of surrounding hepatocytes, stellate cells, endothelial
We begin this chapter with a brief review of the normal host cells, and other immune cells present in the liver (Bilzer et al,
defenses preventing the entry of infectious organisms into the 2006). Without Kupffer cells, enteric organisms and their toxins
liver, biliary system, and pancreas. We then specifically define entering the liver through portal venous blood flow would freely
postoperative infection, which can be divided into SSIs and pass into the systemic circulation. Reduction of the Kupffer cell
remote-site infections. A short discussion of the general risk mass via liver resection is an important consideration when
factors for the development of SSIs and the general measures evaluating a patient’s potential for postoperative infectious
that can be used to prevent them is also warranted before morbidity.
delving into the surgery-specific risks that have been identified Portal hypertension, whether from presinusoidal, sinusoidal,
in the HPB surgery literature. or postsinusoidal causes, undermines the ability of the Kupffer
cells to clear portal venous inflow of enteric organisms and
NORMAL HOST DEFENSES toxins. Portal venous obstruction results in the shunting of
portal venous blood to the systemic venous circulation through
Bacteria that are normally present in the gastrointestinal (GI) the development of collateral pathways. Depending on the
tract can invade the liver and biliary tree directly, resulting in degree of shunting and portal hypertension, this may allow a
hepatic abscess and ascending cholangitis, respectively (see significant portion of portal venous blood to bypass Kupffer
201
202 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Exogenous nonenteric Enteric organisms also exist within the biliary system. Tight junctions prevent
organisms in the Gl tract mixing of blood and bile within the liver by forming a physical
barrier between the bile canaliculi and hepatic sinusoids. Biliary
ductule epithelial cells each contain a single cilium that helps
Hepatic artery Portal vein via Biliary system move bile toward the extrahepatic ducts (Gilroy et al, 1995;
via systemic portal venous via sphincter Itoshima et al, 1977). Mucus produced by the extrahepatic bile
circulation system of Oddi ducts prevents prolonged contact between the ductal epithelium
and bacteria. Both of these features promote forward flow of
bile out of the liver, thus preventing retrograde ascent of any
Liver bacteria that have entered the biliary system.
Bile salts are a chemical barrier to infection and have several
important properties (see Chapter 8). First, they have both
Hepatic veins bacteriostatic and bactericidal properties (Stewart et al, 1986;
Sung et al, 1993) capable of maintaining the normal balance
of intestinal flora. Second, they have a trophic effect on the
Systemic circulation intestinal epithelium, allowing it to maintain its own effective
Portosystemic barrier against bacterial translocation (Stewart et al, 1986).
shunting in
Last, bile salts have an antiendotoxin effect (Stewart et al,
portal HTN
1986).
FIGURE 12.1. There are multiple routes by which microorganisms can
The biliary system also contains immunologically active
access the liver. Exogenous bacteria present in the bloodstream from
substances that combat infection, including immunoglobulin A
intravenous drug abuse or endocarditis travel to the liver through the
hepatic arterial system, whereas enteric bacteria typically enter the liver (Emmrich et al, 1998; Scott-Conner & Grogan, 1994), fibro-
via the portal venous system or through the biliary system. These enteric nectin (Wilton et al, 1987), and complement factors (Sumiyoshi
organisms can then invade the systemic circulation if not eradicated by et al, 1997).
host defense mechanisms present in the liver. Patients with portosys- As seen in Table 12.1, the pancreas contains similar defense
temic shunting are at increased risk for enteric bacteremia because the mechanisms that prevent its invasion by enteric organisms. An
liver’s defense mechanisms are bypassed as portal blood is diverted important difference is that there are no Kupffer cell analogues
directly into the systemic circulation. GI, Gastrointestinal; HTN, in the pancreas. The reason for this lies in the fact that the
hypertension. pancreas does not represent a “window” to the systemic circula-
tion. Its venous outflow enters the portal system that ultimately
enters the liver. Thus, unlike the liver, it does not represent a
TABLE 12.1 Normal Host Defense Mechanisms in the defense against enteric microorganisms attempting to enter the
Hepatobiliary System and Pancreas systemic circulation.
Hepatobiliary Pancreas
DEFINING INFECTIOUS COMPLICATIONS
Physical Biliary sphincter Pancreatic sphincter
Hepatic tight junctions Pancreatic tight Defining postoperative infectious complications can be accom-
junctions plished by considering two broad categories of infection: SSI
Bile flow Pancreatic juice flow and remote-site infection.
Mucus Mucus
Cilia Cilia
Surgical-Site Infection
Chemical Bile salts Pancreatic fluid The Centers for Disease Control and Prevention (CDC)
Immunologic Kupffer cells — further defines SSI based on the physical level of infection
(Mangram et al, 1999). Superficial incisional SSIs involve
Immunoglobulin A Immunoglobulin A
infections of the skin and/or subcutaneous tissue, whereas deep
Fibronectin —Complement
Complement incisional SSIs refer to those infections located in the muscle/
fascial layer of the abdominal wall. Infections located within the
abdominal cavity define organ/space SSIs (Fig. 12.2). A detailed
definition of each type of SSI is included in Box 12.1. Note
cells, thus increasing the possibility of sepsis (see Fig. 12.1) (see that these definitions are also used by the American College of
Chapters 76 and 81). Surgeons in defining SSI for the NSQIP program.
The biliary system has a number of ways to prevent retro-
grade invasion into the liver by pathogenic microorganisms. Remote-Site Infections
These defense mechanisms span all categories listed earlier. Remote-site infections include those infections distant from the
From a physical barrier standpoint, the sphincter of Oddi is incision and operative field: respiratory tract infections, urinary
effective at preventing bacterial ascent into the liver. However, tract infections, and catheter-related bloodstream infections.
removal of this mechanism frequently occurs in HPB operations
and other procedures (e.g., endoscopic retrograde cholangio- GENERAL RISK FACTORS FOR THE
pancreatography with sphincterotomy and/or stenting) and is an DEVELOPMENT OF SURGICAL-SITE INFECTION
important contributor to postoperative and periprocedural
infectious morbidity. Cholangitis with septic shock is the most There are two important sources of risk regarding the develop-
serious complication. Microscopic physical defense mechanisms ment of a postoperative SSI. Both patient-specific factors and
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery 203
Reduce hemoglobin A1c levels to <7% before operation Class II data Anderson et al, 2008
Smoking cessation 30 days before operation Class II data Anderson et al, 2008; Mangram et al, 1999
Administer specialized nutritional supplements or enteral nutrition Class I and class II Anderson et al, 2008; Anonymous, 1991;
to patients at severe nutritional risk for 7-14 days preoperatively; data with Mangram et al, 1999; Weimann et al, 2006
preoperative parenteral nutrition should not be routinely used, significant
except selectively in patients with severe underlying malnutrition heterogeneity
Adequately treat preoperative infections, such as urinary tract Class II data Anderson et al, 2008; Mangram et al, 1999
infections
Decolonization of unselected patients with mupirocin is not Class I data Anderson et al, 2008; Kalmeijer et al, 2002;
currently recommended Konvalinka et al, 2006; Laupland & Conly,
2003; Mangram et al, 1999; Perl et al, 2002;
Suzuki et al, 2003
Identification and decolonization of Staphylococcus aureus carriers Limited class I data Hacek et al, 2008; Rao et al, 2008
may be a potentially useful intervention, but requires further
investigation
Preoperative showering with chlorhexidine. Not currently Class I data Anderson et al, 2008; Mangram et al, 1999;
recommended Webster & Osborne, 2007, 2012
Modified from Teresa C. Horan, Robert P. Gaynes, William J. Martone, William R. Jarvis and T. Grace Emori: CDC definitions of nosocomial surgical site infections: a modification of CDC definitions of
surgical wound infections, Infection Control 13: 606-608, 1992.
Remove hair only if it will interfere with the operation; hair Class I data Anderson et al, 2008; Bratzler & Hunt, 2006;
removal by clipping immediately prior to the operation or Kjonniksen et al, 2002; Mangram et al,
with depilatories; no preoperative or perioperative shaving 1999; Springer, 2007
of surgical site
Use an antiseptic surgical scrub or alcohol-based hand Class II data Anderson et al, 2008; Mangram et al, 1999
antiseptic for preoperative cleansing of the operative team
members’ hands and forearms
Prepare the skin around the operative site with an Class II data Anderson et al, 2008; Digison, 2007;
appropriate antiseptic agent, including preparations based Mangram et al, 1999
on alcohol, chlorhexidine, or iodine/iodophors
Administer prophylactic antibiotics for most clean- Strong class I data Anonymous, 1999; Bratzler & Hunt, 2006;
contaminated and contaminated procedures, and selected Classen et al, 1992; Mangram et al, 1999;
clean procedures; use antibiotics appropriate for the Springer, 2007
potential pathogens
Administer prophylactic antibiotics within 1 hr before incision Strong class II data Anonymous, 1999; Bratzler & Hunt, 2006;
(2 hr for vancomycin and fluoroquinolones Classen et al, 1992; Mangram et al, 1999,
Springer, 2007
Use higher dosages of prophylactic antibiotics for morbidly Limited class II data Forse et al, 1989; Mangram et al, 1999
obese patients
Use vancomycin as a prophylactic agent only when there is a Class I data Anderson et al, 2008; Anonymous, 1999;
significant risk of MRSA infection Bolon et al, 2004; Finkelstein et al, 2002;
Mangram et al, 1999
Provide adequate ventilation, minimize operating room traffic, Class II and class III Anderson et al, 2008; Mangram et al, 1999
and clean instruments and surfaces with approved data
disinfectants
Avoid “flash” sterilization Class II data Anderson et al, 2008; Mangram et al, 1999
Carefully handle tissue, eradicate dead space, and adhere to Class III data Anderson et al, 2008; Mangram et al, 1999
standard principles of asepsis
Leave contaminated or dirty infected wounds open, with the Limited class I, class II Brasel et al, 1997; Cohn et al, 2001;
possible exception of wounds following operations for data Mangram et al, 1999
perforated appendicitis
Redose prophylactic antibiotics with short half-lives Limited class I, class II Mangram et al, 1999; Scher, 1997;
intraoperatively if operation is prolonged (for cefazolin if data Swoboda et al, 1996
operation > 3 hr) or if there is extensive blood loss
Maintain intraoperative normothermia Class I data, some Anderson et al, 2008; Barone et al, 1999;
contradictory class Bratzler & Hunt, 2006; Kurz et al, 1996;
II data Mangram et al, 1999; Sessler & Akca,
2002; Springer, 2007; Walz et al, 2006
MRSA, Methicillin-resistant Staphylococcus aureus.
Modified from Kirby JP, Mazuski JE: Prevention of SSI. Surg Clin North Am 89(2):365-389, 2009, viii.
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery 205
Discontinue prophylactic antibiotics within 24 hours after the Class I data Anonymous, 1999; Barie, 2000; Bratzler & Hunt,
procedure (48 hr for cardiac surgery and liver transplant 2006; DiPiro et al, 1986; Mangram et al, 1999,
procedures); preferably, discontinue prophylactic McDonald et al, 1998; Springer, 2007
antibiotics after skin closure
Maintain serum glucose levels < 200 mg/dL on postoperative Class II data Anderson et al, 2008; Bratzler & Hunt, 2006; Carr
days 1 and 2 et al, 2005; Furnary et al, 1999; Lazar et al, 2004;
Springer, 2007; Zerr et al, 1997
Monitor wound for the development of surgical-site infection Class III data Anderson et al, 2008; Mangram et al, 1999
Modified from Kirby JP, Mazuski JE: Prevention of SSI. Surg Clin North Am 89(2):365-389, 2009, viii.
Aim/Objective/End
Author, Year Title Study Type Patients Point Population Results and Conclusions
Yanaga et al, Intraperitoneal Retrospective 149 To examine Elective hepatectomy The rate of intraperitoneal septic complications after
1986 septic perioperative risk hepatectomy was 12.8%. Chi-square tests showed that
complications factors for significant risk factors for intraperitoneal sepsis after
after intraperitoneal hepatectomy were right or extended right lobectomy, age
hepatectomy septic > 65, operative duration > 5 hr, blood loss > 3 L, and
complications postoperative bleeding requiring laparotomy. The authors
after hepatectomy concluded that limiting operative time and blood loss
were important to prevent postoperative intraperitoneal
sepsis after hepatectomy.
Garwood et al, Infectious Retrospective 207 To assess the Hepatectomy The overall rate of infection after hepatectomy was 3.3%;
2004 complications characteristics of however, mortality among this subset was 33% (3 of 9
after hepatic surgical infections patients). All deaths from infection after hepatectomy had
resection after hepatic MRSA isolated from cultures. Operative duration was
resection to significantly longer in patients suffering infection (7.9 vs.
identify factors 5.6 hours, P = .02) compared with those without.
accounting for Although operative duration was the only statistically
increased significant risk factor for postoperative infection, the
postoperative authors concluded that advanced age, comorbid
mortality conditions, and extent of hepatic resection contribute to
infectious risk after hepatectomy.
Schindl et al, The value of Prospective 104 To examine the Elective hepatectomy The rate of postoperative infection was 31.7%. Twenty-two
2005 residual liver relationship patients had a residual liver volume <26.6%; 11
volume as a between residual developed severe hepatic dysfunction postoperatively,
PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
predictor of liver volume and and 11 did not. Eight of 11 (72.7%) patients with
hepatic postoperative postoperative severe hepatic dysfunction developed
dysfunction after complications infection, whereas only 2 of 11 (18.2%) without severe
major liver after hepatectomy hepatic dysfunction developed infection (P = .030). The
resection authors concluded that the risk of postoperative infection
is related more strongly to the incidence of postoperative
liver dysfunction rather than residual liver volume.
Togo et al, 2007 Perioperative Retrospective 535 To assess risk Hepatectomy with or The overall rate of posthepatectomy infection declined over
infection control factors for SSI without biliary or four periods of time, from 44.7% to 24.1% to 15.0% to
and its after hepatectomy intestinal 9.2%. Independent risk factors for SSI after hepatectomy
effectiveness in over four different reconstruction included use of silk suture (ARR, 4.56) and bile leak
hepatectomy time periods (ARR, 22.99). The authors advocated careful operative
patients procedure, performance of cholangiography, checking for
bile leak using indigo carmine, and the use of synthetic
absorbable sutures.
Pessaux et al, Randomized clinical Prospective 200 To assess the value Elective hepatectomy Pneumonia occurred more frequently in the patients
2007 trial evaluating of routine receiving nasogastric tube decompression (13.0% vs.
the need for nasogastric tube 5.0%, P = .047). There were no differences in mortality,
routine decompression length of stay, or return of bowel function. The authors
nasogastric after elective concluded that routine nasogastric decompression after
decompression hepatic resection hepatectomy had no advantages and that it increased
after elective the risk of pulmonary complications.
hepatic resection
Togo et al, 2008 Usefulness of Prospective rat 313 To assess the Hepatic resection In the animal model, the number of bacteria in silk used
absorbable model, usefulness of without biliary during hepatectomy was 1000 times that of Vicryl. In the
sutures in retrospective synthetic reconstruction patient analysis, the respective incidences of SSI and
preventing SSI in human absorbable infection on the cut surface of the liver in the Vicryl group
hepatectomy analysis sutures (Vicryl) in (3.2%, 1.6%) were significantly lower than in the silk
preventing SSI group (11.2%, 8.8%; P = .0045). The adjusted risk ratio
after hepatectomy (ARR) for SSI in the silk group was 3.4. Operative length
(ARR, 7.31) and bile fistula (ARR, 17.5) were also
independent predictors of SSI. The authors concluded
that the use of synthetic absorbable sutures, instead of
silk sutures, can prevent the development of SSI in
patients undergoing hepatectomy.
Okabayashi et al, Risk factors and Retrospective 152 To identify risk Hepatectomy The overall rate of postoperative infection was 14.5%.
2009b predictors for SSI factors and the Independent risk factors for SSI were BMI > 23.6 (OR,
after hepatic predictors for the 3.7), EBL > 810 mL (OR, 4.4), postoperative bile leak
resection prevention of SSI (OR, 5.2), and postoperative sliding scale insulin use (OR,
after hepatectomy 1.2) as opposed to artificial pancreas. The authors
concluded that postoperative hyperglycemia, bile leak,
obesity, and high intraoperative blood loss correlated with
postoperative infectious risk, and that postoperative
artificial pancreas use is a safe and beneficial device for
maintaining glycemic control.
Kobayashi et al, Risk factors of SSI Retrospective 405 To compare the Hepatectomy without The overall incidence of SSI was 5.8%. Independent risk
2009 after clinicopathologic biliary reconstruction factors for SSI were intraoperative bowel injury (OR,
hepatectomy for factors between 20.08), blood loss > 2000 mL (OR, 4.4), and age > 65 yr
liver cancers patients who (OR, 2.4). The authors concluded that administering
developed SSI prophylactic antibiotics to patients with risk factors for
and those who infection after hepatectomy might reduce infectious
did not after morbidity.
hepatectomy for
liver cancer
Uchiyama et al, Risk factors for Prospective 308 To clarify the Hepatectomy The overall rate of SSI was 11.0%. SSI was significantly
2011 postoperative collection, incidence of SSIs more common after resection for hepatolithiasis compared
infectious retrospective after hepatectomy to resection for HCC or metastasis (23.8% vs. 11.3% vs.
complications analysis 2.7% respectively, P < .001). The authors concluded that
after hepatectomy postoperative SSIs correlate with infected bile.
Moreno Predictors of SSI Prospective 2332 To identify predictors Segmental or The overall rate of postoperative infection ranged from 9.7%
Elola-Olaso after liver resection: of SSI after liver hemihepatectomy, for segmentectomy to 18.3% for trisectionectomy.
et al, 2012 a multicentre resection trisectionectomy Independent predictors for SSI included serum Na > 145
analysis using (OR, 6.05), hypoalbuminemia per mg/dL from mean (OR,
National Surgical 0.67), serum bilirubin > 1.0 (OR, 1.7), need for dialysis
Quality (OR, 4.46 for deep space infection), longer operative time
Improvement (OR, 1.003/min over mean) and smoking status within
Program data 1 yr of procedure (OR, 1.66 for deep space SSI).
Arikawa et al, Risk factors for SSI Retrospective 171 To elucidate risk Hepatectomy for HCC The overall rate of SSI was 21%. Independent risk factors
2011 after factors for SSI for the development of SSI after hepatectomy were bile
hepatectomy for after hepatectomy leakage and excessive blood loss. The authors
hepatocellular for cancer concluded that preventing bile leaks was paramount to
carcinoma limiting infectious morbidity after hepatectomy.
Harimoto et al, Prospective Prospective, 125 To assess the effect Hepatic resection The overall rate of SSI was 13.6%. Independent risk factors
2011 randomized randomized of suture material without biliary for SSI were blood loss > 1000 mL (OR, 7.6). Although
controlled trial on SSI after reconstruction there was no statistically significant difference in SSI rate
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery
investigating the hepatectomy for silk versus Vicryl use (15.8% vs. 11.3%), recovery
type of sutures from infection was faster in the Vicryl group (28 vs. 54
used during days), P < .05.
hepatectomy
207
Continued
TABLE 12.5 Risk Factors for Infectious Complications After Hepatectomy—cont’d
208
Aim/Objective/End
Author, Year Title Study Type Patients Point Population Results and Conclusions
Pessaux et al, Identification and Prospective 555 To determine the Elective hepatectomy The overall rate of postoperative infectious complications
2013 validation of risk collection, risk factors for was 24.3%. Independent risk factors for postoperative
factors for retrospective postoperative infectious complications were nasogastric tube (OR, 1.8),
postoperative analysis infectious blood transfusion (OR, 1.9), and diabetes (OR, 2.4). The
infectious complications only independent risk factor for a surgical postoperative
complications following partial infection was portal vein resection (OR, 5.5). Risk factors
following hepatectomy for a medical postoperative infectious complication were
hepatectomy preop biliary drainage (OR, 1.9), blood transfusion (OR,
2.1), diabetes mellitus (OR, 2.9), and atrial fibrillation (OR,
3.6). The authors concluded that addressing the above
risk factors could reduce the incidence of postoperative
infectious complications after hepatectomy.
Nakahira et al, Proposal for a Prospective 1926 To evaluate Hepatopancreatobiliary The overall rate of infectious complications after
2013 subclassification collection, differences procedures, hepatopancreatobiliary procedures was 23.2%.
of hepatobiliary- retrospective among excluding Independent risk factors for SSI after hepatectomy were
pancreatic analysis hepatobiliary cholecystectomy drain placement (OR, 2.8) and operative duration > 5 hr
operations for procedures to (OR, 2.9). The authors concluded that hepatectomy and
SSI surveillance determine the nonhepatectomy hepatopancreatobiliary procedures differ
following optimal with respect to the incidence of SSI and should be
assessment of subdivision for assessed separately for the purposes of SSI surveillance.
results of SSI surveillance
prospective
multicenter data
Sadamori et al, Risk factors for Retrospective 359 To investigate the Hepatectomy for HCC The overall rate of SSI after hepatectomy was 14.5%,
PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
2013 organ/space SSI causative without including 6.7% incisional SSI and 8.6% organ/space SSI.
after bacteria, reconstruction Independent risk factors for SSI after hepatectomy were
hepatectomy for management, operative time > 280 minutes (OR, 2.32), repeat
HCC in 359 outcome, and hepatectomy (OR, 3.43), blood transfusion (OR, 7.56 for
recent cases characteristics of incisional SSI), and bile leakage (OR, 3.01 for organ/
SSIs after space SSI).
hepatectomy
Nanashima et al, Associated factors Retrospective 526 To clarify the factors Hepatectomy The overall incidence of SSI after hepatectomy ranged from
2014, with SSIs after associated with 5% to 8% depending on the time period. Independent
hepatectomy: posthepatectomy risk factors for superficial SSI included not using a
predictions and SSI vessel-sealing device (OR, 3.1). Independent risk factors
countermeasures for deep SSI were male gender (OR, 2.0), hepatic failure
by a retrospective (OR, 3.3), and bile leakage (OR, 4.8).
cohort study
Kurmann et al, Hepatic steatosis is Retrospective 231 To investigate the Liver or colorectal The overall rate of SSI was 29.3%. The SSI rate in steatotic
2014 associated with impact of hepatic resection patients was 47.5% compared with nonsteatotics 26.6%
SSI after hepatic steatosis on SSI (P < .05). Hepatic steatosis was an independent risk
and colorectal in patients that factor for SSI in patients undergoing hepatectomy (OR,
surgery underwent open 10.33) or colectomy (OR, 6.67).
abdominal
surgery
Yang et al, 2014 Risk factors of SSI Retrospective 7388 To assess risk Hepatectomy The overall rate of SSI was 9.4%. On multivariate analysis,
after hepatic factors for SSI the only independent risk factors for both incisional and
resection after hepatectomy organ/space infections were hepatolithiasis (OR, 1.58
and 1.66, respectively), cirrhosis (OR, 1.61 and 1.70,
respectively), and blood transfusion (OR, 1.32 and 1.71,
respectively).
BMI, Body mass index; EBL, estimated blood loss; HCC, hepatocellular carcinoma; OR, odds ratio; SSI, surgical-site infection.
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery 209
such as liver biopsy and measurement of portal venous pres- developed tool allows the surgeon to estimate the probability
sures may be necessary where there is uncertainty concerning of unfavorable outcomes, including postoperative infectious
the health of the liver. complications.
The extent of parenchymal resection is addressed in this
section on preoperative risk mitigation because the amount of Operative Risk Mitigation
liver to be resected is generally addressed before the patient is There are several operative risk factors that are associated with
brought to the operating room (see Chapters 100 and 108). A postoperative infectious complications. Factors that have come
full assessment will allow the surgeon to carefully tailor the to light in the recent literature include bile leakage, length of
appropriate procedure to a particular patient. Should the risk surgery, increased blood loss, and intraoperative bowel injury
of postoperative hepatic dysfunction and its related complica- (Arikawa et al, 2011; Kobayashi et al, 2009; Moreno Elola-
tion of postoperative infection be deemed too high for formal Olaso et al, 2012; Nakahira et al, 2013; Nanashima et al, 2014;
resection, then thoughtful consideration of other treatment Okabayashi et al, 2009b; Togo et al, 2007). Therefore, in an
modalities may be needed. For example, parenchymal-sparing attempt to mitigate these risk factors, it is important to expedi-
techniques, such as segmental hepatectomy, ablation, or even tiously progress through the operation by using meticulous
arterial-based modalities, may be required. Preoperative portal technique to avoid excess blood loss and iatrogenic injury to
vein embolization can be considered in certain patients in surrounding structures. It is also essential to pay particular
whom the anticipated residual liver is questionable. When the attention to the identification and treatment of intraoperative
risk of postoperative complications is prohibitive, then not bile leaks once the liver is transected. For example, some sur-
operating or ablating may be the prudent course of action. geons routinely coat the cut surface of the liver with hydrogen
The use of systemic chemotherapy should also be taken peroxide. Small bile leaks then become more obvious at the site
into account in the overall treatment plan for patients undergo- of green bubbling.
ing hepatic resection, especially for an indication of colorectal An intraoperative air leak test was recently found to be very
liver metastasis. Neoadjuvant chemotherapy, in particular, can effective in the detection of bile leaks, thus decreasing the rate
theoretically increase the risk of infection due to its negative of postoperative biliary complications (Zimmitti et al, 2013).
effects on the liver, including steatosis, steatohepatitis, and This maneuver involves the placement of a transcystic catheter
sinusoidal obstruction syndrome, making it less than ideal from that is used to inject air into the biliary tree after the upper
the standpoint of postoperative infection. Its use continues to abdomen is submerged in saline and the distal common bile
be debated; however, a recent retrospective study conducted by duct is occluded. Bile leaks are identified at the site of streaming
Scilletta and colleagues (2014) suggested that neoadjuvant air bubbles and are directly repaired. The authors compared
chemotherapy was not a significant risk factor for SSIs in the rates of postoperative biliary complications between 103
patients undergoing liver resection for colorectal hepatic metas- patients who underwent air leak testing and 120 matched
tases (see Chapters 71 and 100). patients who underwent hepatic resection before air leak testing
Nordlinger and colleagues (2008) conducted a randomized was used. None of the hepatic resections in either group were
controlled trial comparing liver resection for resectable colorec- accompanied by biliary reconstruction. The authors noted a
tal liver metastases in patients with and without perioperative significantly lower rate of postoperative bile leaks in the air
chemotherapy. Perioperative chemotherapy was defined as six leak–tested group (1.9% vs. 10.8%, P = .008). This adjunctive
cycles of FOLFOX4 (5-fluororuracil plus leucovorin and maneuver seems easy to use and appears effective in the preven-
oxaliplatin) before and after surgery. There were 182 patients tion of bile leaks. This may have a positive impact on postopera-
within each arm of the study. Infectious complications that were tive infectious complications after hepatic resection but requires
analyzed included wound infection, intraabdominal infection, further validation.
and urinary infection. There was a trend toward higher rates of Regarding parenchymal transection techniques, no one
these complications in the perioperative chemotherapy group, method or combination of methods has been shown to be
but it was not statistically significant. Therefore it would seem superior. Therefore it is recommended that the surgeon use the
that for resectable colorectal cancer liver metastasis, chemo- technique that is most familiar, while limiting the amount of
therapy before hepatectomy is safe from a postoperative infec- necrotic liver parenchyma left behind (Yanaga et al, 1986). We
tious standpoint. also believe that it is important to suction any pooled blood and
Other preoperative contributors to postoperative infectious bile at the end of the operation (see Chapter 103).
complications after hepatic resection include advanced age, The use of absorbable suture material versus silk during
presence of diabetes mellitus, obesity, presence of an open hepatectomy has also been studied with regard to infectious
wound, hypernatremia, hypoalbuminemia, elevated serum bili- complication. The data are conflicting. In a retrospective analy-
rubin, dialysis, comorbid conditions, repeat hepatectomy, and sis, silk suture was found to be significantly associated with SSI
hepatic steatosis (Garwood et al, 2004; Kurmann et al, 2014; (Togo et al, 2007). This was confirmed in a study conducted
Moreno Elola-Olaso et al, 2012; Okabayashi et al, 2009b; on rats (Togo et al, 2008). However, a prospective randomized
Pessaux et al, 2013; Sadamori et al, 2013; Togo et al, 2007). controlled trial found no difference between silk and Vicryl
Note that many of these preexisting conditions may not be suture with regard to infection (Harimoto et al, 2011).
modifiable before the time of operation. Therefore it cannot be
overemphasized that the nature of the planned liver resection Perioperative Antibiotics
be considered in light of the general condition of the patient. The Clinical Practice Guidelines for Antimicrobial Prophylaxis
The ACS’s Risk Calculator (http://www.riskcalculator.facs.org) published in the American Journal of Health-System Pharmacy
can also provide some valuable insight into the expected post- (Bratzler et al, 2013) represent the most current recommenda-
operative recovery of an individual patient and may help with tions on preoperative antimicrobial prophylaxis. They do not
preoperative decision making. As discussed earlier, this recently include specific recommendations for hepatic resection with or
210 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
without biliary-enteric reconstruction, or cases in which the of prophylactic drainage in GI surgery in a systematic review
patient has undergone preoperative biliary drainage. The guide- and meta-analysis, concluding that many GI operations can be
lines, however, do provide recommendations on biliary tract safely performed without the use of drains. Regarding liver
procedures, including cholecystectomy, exploration of the surgery specifically, this paper suggests that surgical drains do
common bile duct, and choledochoenterostomy. The guidelines not necessarily prevent biloma formation and do not always
state that the most common organisms associated with infection prevent the need for percutaneous drainage. A grade A recom-
after these particular procedures include Escherichia coli, Kleb- mendation was given against prophylactic drainage in elective
siella species, and enterococci. The recommended antibiotic for hepatic resection. This is supported by several randomized
open biliary tract surgery is cefazolin; alternative agents are studies (Belghiti et al, 1993, Fong et al, 1996, Liu et al, 2004)
ampicillin-sulbactam, cefotetan, cefoxitin, and ceftriaxone. It is and a systematic review (Gurusamy et al, 2007). A more recent
important to note, however, that none of the cephalosporins multicenter international prospective study also concluded that
cover enterococci (see Chapters 12, 29, and 30). intraoperatively placed surgical drains do not prevent the need
A reasonable approach to the prevention of SSI in the setting for additional percutaneous drainage (Brooke-Smith et al,
of hepatic resection would be to administer antimicrobial pro- 2015).
phylaxis for all elective hepatic resections regardless of antici-
pated biliary-enteric reconstruction. As mentioned earlier, the Postoperative Risk Mitigation
recommended antimicrobial agent for biliary tract procedures Nasogastric Decompression
from the Clinical Practice Guidelines for Antimicrobial Prophy- Pessaux and colleagues (2007) conducted a randomized clinical
laxis is cefazolin. This agent can theoretically be used for hepatic trial examining the utility of postoperative nasogastric decom-
resection as well. However, we typically broaden our preopera- pression after elective hepatectomy. The authors randomized
tive coverage with a second-generation cephalosporin or a 200 patients to nasogastric tube use versus no nasogastric tube.
carbapenem. We currently favor ertapenem because it is a single The use of a nasogastric tube was significantly associated with
agent with broad coverage, dosed daily. Whatever agent is used, an increased rate of pneumonia and atelectasis but did not
it should be given within 60 minutes of skin incision and reduce overall surgical complications, medical morbidity,
redosed appropriately intraoperatively to maintain adequate in-hospital mortality, duration of ileus, or length of hospital
tissue levels. stay. The authors concluded that routine nasogastric decom-
The Clinical Practice Guidelines for Antimicrobial Prophy- pression offers no benefit. We do not routinely use nasogastric
laxis state that, in general, the “shortest effective duration of tubes in our hepatectomy patients.
antimicrobial administration for preventing SSI is not known,”
but that “postoperative antimicrobial administration is not Early Enteral Nutrition and Synbiotics
necessary for most procedures.” This notion is further sup- The concept of early enteral nutrition has been studied in
ported by a randomized controlled trial recently conducted in patients undergoing liver resection. Richter and colleagues
Japan that explored the merits of postoperative antibiotic pro- (2006) conducted a systematic review of early enteral nutrition
phylaxis after liver resection (Hirokawa et al, 2013). A total of following open liver resection, concluding that it is safe and that
241 hepatic resection patients were studied. Half of the patients it decreases the incidence of postoperative complications in
received postoperative antibiotics, whereas the other half did comparison to parenteral nutrition. The authors noted a statis-
not. There was no difference between the two patient groups tically significant lower rate of wound infections and catheter-
with regard to signs of infection, incidence of the systemic related infections with early enteral feeding versus parenteral
inflammatory response syndrome, infectious complications, nutrition. However, pneumonias and intraabdominal abscesses
SSI, or remote-site infections. The authors concluded that were not significantly decreased. It should be noted that enteral
postoperative antibiotic prophylaxis cannot prevent postopera- nutrition in this review was, in general, started on the second
tive infections after liver resection. We do not routinely continue postoperative day via an operative jejunal tube. We do not
antimicrobial prophylaxis postoperatively. advocate placement of jejunal feeding catheters in the otherwise
healthy liver resection patient. However, for the malnourished
Drains patient, early enteral nutrition perhaps via a planned jejunal
Two types of drains have been studied in the literature. tube is recommended over parenteral nutrition.
Nakayama and colleagues (2014) evaluated the utility of sub- Enteral nutrition supports gut-barrier function, mitigating
cutaneous drains in the prevention of wound infection. After the risk of bacteremia originating from the enteric system
fascial closure, a 10 Fr drain connected to negative pressure (Mizuno et al, 2010). However, a perturbation in the microbial
was placed in the subcutaneous tissue. The authors were not balance within the intestinal lumen can also pave the way for
able to significantly lower the wound infection rate. infections after liver surgery. This is particularly evident in cir-
Intraabdominal drains have been analyzed more systemati- rhotic patients (Yeh et al, 2003). Synbiotic therapy, which is a
cally. The rationale for leaving an intraabdominal drain is to combination of probiotic and prebiotic therapy, has been
detect and prevent biloma formation in the event of bile leakage studied as a method of potentially reducing infectious morbid-
after hepatic resection. Bile leakage and subsequent biloma ity after liver surgery. Probiotics are defined as live bacteria that
formation is an important contributor to infectious complica- are capable of improving the microbial balance within the
tions after hepatic resection, as stated earlier. However, the intestinal lumen. Prebiotics are chemicals that enhance the
overall trend reflected in the literature does not support the use growth of beneficial bacteria. Several studies have documented
of drains in elective hepatic surgery. Foregoing prophylactic encouraging results in the ability of synbiotic therapy to help
drainage after elective hepatic surgery is consistent with the prevent postoperative infectious complications after liver
general notion that drainage may be unnecessary in most GI surgery, especially in patients with biliary cancer (Kanazawa
operations. Petrowsky and colleagues (2004) studied the value et al, 2005; Sugawara et al, 2006; Usami et al, 2011).
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery 211
Enhanced recovery after surgery (ERAS) pathways have (Farges et al, 2013). The most recent National Comprehensive
shown promise in improving postoperative outcomes in patients Cancer Network (NCCN) guidelines recommend biliary drain-
undergoing liver surgery (Hughes et al, 2014). Important age via endoscopic retrograde cholangiography or percutaneous
components of ERAS pathways include continuing nutrition as transhepatic cholangiography and portal vein embolization in
long as 2 hours before hepatic resection, avoidance of a naso- patients with a very small FLR. Routine drainage is not
gastric tube, and early postoperative diet resumption. Although recommended.
there have been no studies specifically examining the effects of
ERAS pathways on infectious complications, avoidance of Pancreatic Resection
perioperative starvation is theoretically beneficial from an infec- The location and nature of disease within the pancreas dictates
tious standpoint and may one day be proven. ERAS pathways the specific type of pancreatic resection used. With modern
should therefore be considered for those patients undergoing imaging modalities, resection type can often be determined
routine hepatectomy. preoperatively. The most commonly performed resections
include pancreaticoduodenectomy and distal pancreatectomy
Blood Glucose Control (typically with splenectomy when performed for cancer); hence
Since the landmark paper by van Den Berghe and colleagues the studies of infectious complications after pancreatectomy
(2001) demonstrating improved outcomes with intensive focus on these two procedures. Enucleation and central pan-
insulin therapy, there has been much focus on tight blood createctomy are less common procedures.
glucose control in the surgical patient. Dysglycemia has been The range of SSI following pancreaticoduodenectomy or
studied in patients undergoing hepatectomy specifically. Huo distal pancreatectomy includes the previously defined superfi-
and colleagues (2003) demonstrated increased hepatic decom- cial incisional SSI, deep incisional SSI, and organ/space SSI
pensation in diabetic patients undergoing hepatic resection for (see Chapters 27 and 66). For pancreaticoduodenectomy,
hepatocellular carcinoma. Little and colleagues (2002) showed organ/space infection can be further categorized by the contrib-
an association with increased mortality in diabetic patients uting anastomosis: intraabdominal abscesses, or infected fluid
undergoing hepatectomy for colorectal cancer metastasis. collections can be related to an infected bile, pancreatic, or
Regarding postoperative infectious complications in particular, enteric leak, or a combination of these. Organ/space infection
Ambiru and colleagues (2008) demonstrated an increase in SSI after distal pancreatectomy is typically related to pancreatic
in HPB surgery patients with poor postoperative blood glucose leak. As with any major abdominal operation, these patients are
control. Therefore tight glycemic control is paramount after also at risk for the development of abscesses not related to
hepatectomy. Methods of glycemic control include sliding anastomotic leakage or secondary to an infected hematoma.
scales and continuous insulin infusions; however, other less Uncontained intraabdominal sepsis requiring reexploration is
conventional approaches have been used. A closed-loop artifi- also a possibility. Furthermore, these patients can develop
cial pancreas system has been shown to reduce SSI (Okabayashi remote-site infections, including bloodstream infections, chol-
et al, 2009a) as well as liver dysfunction (Okabayashi et al, angitis, respiratory tract infections, urinary tract infections, and
2011) in patients undergoing hepatic resection. Promising Clostridium difficile infections.
results have also been obtained with the hyperinsulinemic- General risk factors for SSI discussed earlier apply to patients
normoglycemic clamp technique. This method was shown to undergoing pancreatic resection; however, there are risk factors
reduce complications, including infections after hepatectomy in specific to pancreatic resection that warrant discussion.
a study by Fisette and colleagues (2012). These are presented according to each stage of patient care:
preoperative, intraoperative, and postoperative. In many
Preoperative Biliary Drainage in the Hilar instances, it may not be possible to significantly modify risk;
Cholangiocarcinoma Patient (See Chapters 27 and 51) nonetheless, it is important to understand potential risk factors
Preoperative biliary drainage before hepatic resection for extra- so that the patient can be monitored with the appropriate
hepatic hilar cholangiocarcinoma is a crucial consideration degree of vigilance in the postoperative period.
when anticipating the surgical approach and postoperative
outcomes. Postoperative outcomes after liver resection tend to Preoperative Risk Mitigation
be worse in patients with obstructive jaundice (Belghiti et al, Body Mass Index and Nutritional Status
2000). Preoperative biliary drainage was therefore initially com- Elevated BMI is a risk factor for infectious complications fol-
monplace before the performance of elective liver resection for lowing pancreatic resection (Table 12.6). House and colleagues
obstructed patients with hilar cholangiocarcinoma. However, (2008) studied postoperative complications in 356 patients who
the procedure is associated with preoperative cholangitis, and underwent pancreaticoduodenectomy for pancreatic adenocar-
relatively recent literature has confirmed that it is also associ- cinoma with the goal of identifying preoperative patient and
ated with increased postoperative complications, infectious radiographic factors associated with postoperative morbidity.
complications in particular (Ferrero et al, 2009; Hochwald Complications developed in 38% of this patient population,
et al, 1999). This has called into question whether or not with the most common pancreatic fistula/abscess, wound infec-
routine preoperative biliary drainage should be performed in tion, and delayed gastric emptying. Wound infection rates were
hilar cholangiocarcinoma patients undergoing hepatic resec- significantly higher in those patients with a BMI greater than
tion. In fact, a recent review by Liu and colleagues (2011) or equal to 30 (P = .03). The authors also determined that the
concluded that preoperative drainage should not be routinely degree of visceral fat as seen on preoperative axial imaging
performed. However, there are data to suggest that there is a correlated with higher rates of overall complications and pan-
role for preoperative biliary decompression in certain scenarios, creatic fistula.
including very small functional liver remnant (FLR) patients Su and colleagues (2010) analyzed 101 pancreaticoduode-
(Kennedy et al, 2009) and perhaps for right-sided resections nectomy patients with regard to postoperative infectious
212
TABLE 12.6 Risk Factors for Infectious Complications After Pancreatectomy: Preoperative Risk Factors
Author, Year Title Study Type Patients Aim/Objective/End Point Population Results and Conclusions
House et al, Preoperative predictors for Prospective 356 Postoperative Pancreaticoduodenectomy The overall complication rate was 38%, most
2008 complications after collection, complications commonly pancreatic fistula or abscess, wound
pancreaticoduodenectomy: retrospective infection, and delayed gastric emptying. Multivariate
impact of BMI and body fat review analysis revealed that absence of pancreatic
distribution atrophy and extent of central obesity (as measured
by visceral fat) were associated with postoperative
complications. Patients with retrorenal visceral fat
>2 cm developed significantly more complications
(51% vs. 31%) and pancreatic fistulas (24% vs
10%). Patients with BMI > 30 kg/m2 had
significantly more wound infections (21% vs. 12%).
Su et al, Factors influencing infectious Prospective 101 Postoperative Pancreaticoduodenectomy Nineteen preoperative variables were correlated with
2010 complications after collection, infectious postoperative infectious morbidity. Infectious
pancreatoduodenectomy retrospective complications complications developed in 56% of patients.
review Serious infection (bacteremia, intraabdominal
infection, pneumonia) occurred significantly more
often in patients with BMI > 25 (67% vs. 24%). BMI
significantly increased operative time and was the
only independent risk factor for postoperative
infection.
Greenblatt Preoperative factors predict Prospective 4945 30 day complication Pancreaticoduodenectomy The overall complication rate was 27.1%. Sepsis
et al, 2011 perioperative morbidity and collection, and mortality rates (15.3%), SSI (13.1%), and respiratory complications
PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
complications. Nineteen perioperative variables were studied in as independent risk factors for SSI. The authors then conducted
an effort to determine which predicted infectious morbidity. a multivariate regression analysis on just preoperative and
The authors noted infectious complications in 55% of the intraoperative risk factors (excluding the postoperative develop-
patients. They concluded that high BMI (defined as BMI > 25) ment of pancreatic fistula). A NRI of less than 97.5 remained
significantly increased operative time and was the only indepen- an independent predictor of SSI.
dent risk factor for serious postoperative infectious complica- As noted above, modification of the aforementioned preop-
tions, including bacteremia, intraabdominal infection, and erative risk factors may be difficult or even impossible prior to
pneumonia. pancreatectomy. This is particularly true if the indication for
Larger multiinstitutional data have yielded similar conclu- resection is cancer or suspicion of cancer, which is common. In
sions about the association between BMI and morbidity follow- these instances, proceeding to the operating room expeditiously
ing pancreatic resection. Greenblatt and colleagues (2011) used may be the prudent course of action, especially in the clearly
the ACS-NSQIP database in an attempt to formulate a predic- resectable and otherwise healthy operative candidate. However,
tion tool for patients undergoing pancreaticoduodenectomy. more than one-third of patients about to undergo pancreatico-
The authors examined preoperative factors that might predict duodenectomy can be considered borderline candidates from a
perioperative morbidity and mortality. Although this study was medical standpoint (Tzeng et al, 2014). These patients are at
not designed to predict who would incur an infectious compli- significant risk for postoperative morbidity (including infectious
cation specifically, the authors found that the most frequent complications) as well as mortality. Therefore, as suggested by
complications after pancreaticoduodenectomy included sepsis Tzeng and colleagues, surgeons should strongly consider
(15.3%), SSI (13.1%), and respiratory complications (9.5%). improving the condition of the patient to mitigate infectious/
The overall complication rate in 1342 patients was 27.1%. overall morbidity and mortality in these “borderline resectable
Elevated BMI was a significant predictor of morbidity (after type C” patients before surgery. Those patients receiving
adjusting for confounding variables), and morbidity increased neoadjuvant therapy should take advantage of this time and use
incrementally with BMI. Other predictors included older age, it as a “window of opportunity” to modify BMI, improve
male gender, dependent functional status, chronic obstructive nutritional/functional status, control hypertension, and/or quit
pulmonary disease, steroid use, bleeding disorder, leukocytosis, smoking. For patients seen with surgically resectable tumors
elevated serum creatinine, and hypoalbuminemia. but significant reversible functional deficits, it may be worth-
Kelly and colleagues (2011) attempted to identify preopera- while to administer neoadjuvant therapy while the patient
tive and operative risk factors for the development of complica- is medically optimized. Regardless of whether neoadjuvant
tions after distal pancreatectomy. The authors also used the therapy consists of chemoradiation or chemotherapy alone,
multiinstitutional prospective ACS-NSQIP database. Their either type of preoperative therapy is considered safe with
efforts concerned the development of a risk score for patients regard to postoperative complications (Araujo et al, 2013;
undergoing distal pancreatectomy. The study population Cheng et al, 2006; Cho et al, 2014; Heinrich et al, 2008).
included 2322 patients. The overall 30 day complication and
mortality rates were 28.1% and 1.2%, respectively. Similar to Preoperative Biliary Drainage
the analysis conducted by Greenblatt and colleagues (2011), Preoperative biliary drainage in the setting of an obstructing
this study was not designed to specifically address infectious pancreatic head mass continues to be debated. Earlier studies
complications. However, the most common complications were suggested that perioperative mortality is higher when pancre-
sepsis, SSI, and pneumonia. Multivariate analysis determined aticoduodenectomy is performed on the hyperbilirubinemic
that high BMI was a preoperative predictor of postoperative patient (Bottger et al, 1999; Braasch et al, 1977; Lerut et al,
morbidity. The other preoperative variables associated with 1984) (see Chapters 29, 30, and 66). More recent work has
postoperative complications included male gender, smoking, also shown preoperative jaundice to be a poor prognostic factor
steroid use, neurologic disease, preoperative systemic inflam- with regard to overall survival for patients undergoing resection
matory response syndrome /sepsis, hypoalbuminemia, elevated of the head of the pancreas for adenocarcinoma (Strasberg
creatinine, and abnormal platelet count. et al, 2014). However, the literature continues to suggest that
Poor preoperative nutritional status is another important attempts at normalizing the bilirubin preoperatively may have
risk factor for SSI and other postoperative morbidity in patients detrimental effects that manifest in the postoperative period.
undergoing pancreatic resection (see Table 12.6) (see Chapter Healthy patients with an intact sphincter of Oddi and a
26). La Torre and colleagues (2013) noticed a relationship normal biliary system have sterile bile for all of the reasons
between malnutrition and morbidity after pancreatic surgery in discussed previously. However, obstructive jaundice in the
their retrospective evaluation of data collected from 143 patients setting of a mass in the head of the pancreas results in bile stasis.
undergoing pancreatic resection for cancer. Malnutrition was This in turn promotes colonization of the biliary system, espe-
defined by using several different validated screening tools. It cially after the bile ducts are interrogated and drained via stents
was gleaned from multivariate analysis that malnutrition, as (Limongelli et al, 2007). The presence of bacteria in the biliary
defined by the malnutrition universal screening tool and the system is known as bacterobilia. When normal host defense
nutritional risk index (NRI), was an independent risk factor mechanisms present in the liver and biliary tree are overwhelmed
for overall morbidity, which included SSI. Shinkawa and col- by a critical level of bacterobilia and the biliary tree is not
leagues (2013) confirmed these findings in an examination of adequately drained, then pathogenic enteric organisms may
64 patients with pancreaticoduodecectomy with regard to reach the systemic circulation through the liver, causing sepsis
potential perioperative risk factors for SSI. SSI, as defined by (i.e., cholangitis).
the CDC, developed in 33% of these patients. Using multivari- It is rare for a patient with pancreatic cancer to be seen with
ate logistic regression analysis on perioperative factors, the cholangitis without having undergone attempts at biliary
authors identified pancreatic fistula and a NRI of 97.5 or less decompression. However, should this happen, the required
214 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Kondo et al, Selection of prophylactic Retrospective 116 SSI Pancreaticoduodenectomy Patients were divided into two groups based
2013 antibiotics according to the on when their surgery was performed.
microorganisms isolated Patients in the “early” group received
from surgical site infections standard preoperative antibiotics, whereas
(SSIs) in a previous series of patients in the “later” group received
surgeries reduces SSI prophylactic antibiotics selected on the
incidence after basis of the SSIs that occurred in the
pancreaticoduodenectomy “early” group. Independent risk factors for
SSI included preoperative cholangitis (OR,
2.8) and being in the “early” group (OR,
2.9).
Kitahata Preoperative cholangitis during Retrospective 127 Postoperative complications Pancreaticoduodenectomy The effect of external vs. internal biliary
et al, 2014 biliary drainage increases drainage on postoperative complications
the incidence of for patients undergoing
postoperative severe pancreaticoduodenectomy was assessed.
complications after The overall complication rate was 33%.
pancreaticoduodenectomy Preoperative cholangitis was significantly
more common in internally vs. externally
drained patients (22.4% vs. 1.7%).
Preoperative cholangitis was the only
independent risk factor for severe
complication after
pancreaticoduodenectomy (OR, 4.61).
Povoski et al, Preoperative biliary drainage: Retrospective 161 To determine the impact of Pancreaticoduodenectomy The overall rate of postoperative infectious
1999a impact on intraoperative bile preoperative biliary complications was 29%, most commonly
cultures and infectious drainage on intraoperative wound infection (14%) and intraabdominal
morbidity and mortality after bile cultures and abscess (12%). Preoperative biliary
pancreaticoduodenectomy postoperative infectious drainage was independently and
morbidity significantly associated with positive
intraoperative bile cultures (P < .001),
postoperative infectious complications (P
= .022), wound infections (P = .045), and
death (P = .021). There was also an
association with intraabdominal abscess
(P = .061). Authors concluded that
preoperative biliary drainage should be
avoided in operative candidates.
Povoski et al, Association of preoperative Retrospective 240 To determine whether Pancreaticoduodenectomy The overall rate of postoperative infectious
1999b biliary drainage with preoperative biliary complications was 34%, most commonly
postoperative outcome instrumentation and/or wound infection (16%) and intraabdominal
following drainage are associated abscess (14%). Preoperative biliary
pancreaticoduodenectomy with increased morbidity drainage but not biliary instrumentation
and mortality rates after alone was significantly associated with
pancreaticoduodenectomy overall complications (P < .025), infectious
complications (P < .014), intraabdominal
abscess (P < .022), and death (P < .037).
Again, the authors concluded that
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery
Continued
216
TABLE 12.7 Risk Factors for Infectious Complications After Pancreatectomy: Preoperative Biliary Drainage—cont’d
Author, Year Title Study Type Patients Aim/Objective/End Point Population Results and Conclusions
Jagannath Effect of preoperative biliary Prospective 144 To examine the effects of Pancreaticoduodenectomy The overall rate of postoperative infectious
et al, 2005 stenting on immediate collection, preoperative biliary stenting complications was 26.4%, including
outcome after retrospective on early outcome after wound infection (21.5%) and sepsis
pancreaticoduodenectomy analysis pancreaticoduodenectomy (13.9%). Positive intraoperative bile
cultures were significantly associated with
postoperative morbidity (0.001) and
mortality (P = .019). Significantly
associated morbidity included bleeding,
pancreatic leak, bile leak, wound infection,
sepsis, and infectious complications.
Preoperative biliary stenting was not
significantly associated with positive
intraoperative bile cultures unless stenting
was complicated by pancreatitis,
cholangitis, bleeding, or distal stent
migration.
PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
Cortes et al, Effect of bile contamination on Retrospective 79 To compare outcomes after Pancreaticoduodenectomy The overall rate of postoperative infectious
2006 immediate outcomes after pancreaticoduodenectomy complications was 49%. Sixty-five percent
pancreaticoduodenectomy in patients with sterile and of patients had positive-bile cultures, of
for tumor those with infected bile which 80% had endoscopic biliary
drainage. In the culture-negative group,
14% had preoperative drainage. Overall
morbidity was higher in the culture-positive
group (77% vs. 59%, P = .05), especially
with respect to infectious complications
(65% vs. 37%, P = .003). Among those
with infectious complications, there was
49% concordance with bile cultures.
Organisms were resistant to cefazolin in
97%.
Howard et al, Influence of bactibilia after Retrospective 138 To correlate bactibilia found Obstructive jaundice The overall rate of postoperative infectious
2006 preoperative biliary stenting after preoperative biliary complications was 22.4%. 62% of
on postoperative infectious stenting with that of the patients had preoperative biliary stenting,
complications bacteriology of whereas 38% did not. Stented patients
postoperative infectious had a higher rate of wound infection (P =
complications in patients .03) and bacteremia (P = .04). The authors
with obstructive jaundice concluded that preoperative biliary
stenting increases the incidence of
bactibilia, bacteremia, and wound infection
rates but does not increase morbidity,
mortality, or hospital length of stay.
Limongelli Correlation between Prospective 220 To examine the relationship Pancreaticoduodenectomy, The overall rate of postoperative infectious
et al, 2007 preoperative biliary drainage, collection, between preoperative total pancreatectomy, complications was 45%, including
bile duct contamination, and retrospective biliary drainage, and biliary bypass wound infection (29%), intraabdominal
postoperative outcomes for analysis intraoperative bile culture, collection (16%), and sepsis (13%).
pancreatic surgery and postoperative 51.4% had a positive intraoperative
morbidity and mortality in bile culture. Infectious complications
patients undergoing (OR, 1.8; P = .03) and wound infections
pancreatic surgery (OR, 2.8; P = .002) were significantly
associated with a positive intraoperative
bile culture. The authors concluded that
preoperative biliary drainage promotes
positive intraoperative bile cultures, which
may increase the risk of infectious
complications.
Lermite et al, Effect of preoperative Prospective 124 To report the influence of Pancreaticoduodenectomy The overall rate of postoperative infectious
2008 endoscopic biliary drainage collection, preoperative endoscopic complications was 28.6%; 89.3% of
on infectious morbidity after retrospective biliary drainage on patients who underwent preoperative
pancreatoduodenectomy: a analysis postoperative infectious biliary drainage had positive bile cultures
case-control study morbidity in patients as opposed to 19.4% in the undrained
undergoing group (P < .001). Infectious complications
pancreaticoduodenectomy occurred in 50% of drained patients, but
only in 21.4 % of undrained patients (P =
.05). The authors concluded that routine
preoperative drainage should be avoided
in surgical candidates with potential
exceptions in cases of cholangitis or
patients undergoing neoadjuvant treatment
or extensive preoperative assessment.
Sivaraj et al, Is bactibilia a predictor of poor Prospective 76 To examine the relationship Pancreaticoduodenectomy The overall rate of postoperative infectious
2010 outcome of collection, between bile infection and complications was 35.5%. Bile cultures
pancreaticoduodenectomy? retrospective infectious complications were positive in 46% and negative in 54%.
analysis following Culture-positive patients had a higher
pancreaticoduodenectomy incidence of postoperative infectious
complications and wound infection (P =
.015), intraabdominal abscess (P = .002),
bacteremia (P = .0043), renal insufficiency
(P = .037), and longer average hospital
stay (16 vs. 10 days; P = .0002). The
authors advocated preoperative biliary
drainage only in strictly selected cases.
Continued
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery
217
218
TABLE 12.7 Risk Factors for Infectious Complications After Pancreatectomy: Preoperative Biliary Drainage—cont’d
Author, Year Title Study Type Patients Aim/Objective/End Point Population Results and Conclusions
van der Preoperative biliary drainage Multicenter 202 To compare preoperative Pancreaticoduodenectomy The overall rate of postoperative infectious
Gaag for cancer of the head of randomized biliary drainage with complications was 23%. Serious
et al, 2010 the pancreas trial surgery alone for patients complications related to either biliary
with cancer of the drainage or surgery occurred in 74% of
pancreatic head those who underwent drainage as
opposed to 39% of those who did not.
Serious complications included
pancreatitis, cholangitis, GI perforation,
hemorrhage, stent occlusion or need for
exchange, pancreatic leak, delayed gastric
emptying, bile leak, anastomotic leak,
intraabdominal abscess, wound infection,
portal vein thrombosis, pneumonia,
myocardial infarction, or need for repeat
laparotomy. Drainage did not increase
mortality or hospital length of stay. The
PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
operation longer than 480 minutes (OR, 1.78). Pancreatic cant postoperative fistula, leak, or abscess in patients undergo-
fistula was clearly the strongest risk factor for organ/space ing pancreatic resection.
infection. Regarding distal pancreatectomy specifically, Hamilton and
The prevention of pancreatic fistula after pancreatectomy colleagues (2012) conducted a randomized controlled trial
remains a central question within the general and HPB surgical examining the efficacy of mesh-reinforced stapled closure of the
communities. Schmidt and colleagues (2009) studied preopera- distal pancreas. The authors randomly assigned 54 patients to
tive and perioperative risk factors for the development of a mesh reinforcement and 46 patients to nonmesh reinforcement,
pancreatic fistula in pancreaticoduodenectomy patients. First, in which the primary outcome was clinically significant pancre-
they confirmed the notion that patients in whom a pancreatic atic leak. International Study Group of Pancreatic Fistula
fistula develops have a higher rate of postoperative wound infec- (ISGPF) grade B and C leaks occurred more frequently in the
tion and intraabdominal abscess. Second, they identified several patients without mesh reinforcement (20% vs. 1.9%, P .0007).
operative risk factors for the development of pancreatic fistula. Other operative risk factors contributing to postoperative
Their multivariate analysis showed that an invaginated pancre- infectious morbidity after pancreatic resection include longer
atic anastomosis and closed suction intraperitoneal drainage operative times (Ball et al, 2010; Procter et al, 2010; Sudo et al,
were predictive of a pancreatic fistula, whereas chronic pancre- 2014; Sugiura et al, 2012; Wang et al, 2007) and need for peri-
atitis and preoperative biliary stenting were protective of a operative blood transfusion (Ball et al, 2010) (see Table 12.9).
pancreatic fistula. Despite these findings, a recent review Procter and colleagues (2010) performed a retrospective analysis
(Schoellhammer et al, 2014) suggested that no one pancreatic of 299,359 general surgical procedures (including pancreatec-
anastomosis is superior and that more studies are needed to tomy), identified through the ACS-NSQIP database, looking for
identify the best anastomotic technique. Also, the authors risk factors associated with infectious complications. Their
concluded that there is no evidence to support routine use of multivariate analysis suggested that increased operative duration
stents or topical sealing agents in the prevention of pancreatic is an independent risk factor for infectious complications and
fistula. hospital length of stay.This was confirmed by Ball and colleagues
A recent randomized trial studied pasireotide as a possible (2010), who conducted a retrospective analysis on only pancre-
adjunct to prevent postoperative pancreatic fistula (Allen et al, aticoduodenectomy patients identified via the ACS-NSQIP
2014). Pasireotide is a somatostatin analogue with a longer database. Their study involved 4817 patients and determined
half-life than octreotide. The authors randomly assigned 300 that longer operative times were associated with both morbidity
patients undergoing either pancreaticoduodenectomy or distal and mortality. Also, there was a linear relationship between
pancreatectomy to either perioperative pasireotide or placebo. preoperative RBC transfusion and 30 day morbidity. This led the
The primary end point was the occurrence of pancreatic authors to suggest blood transfusion and operative time as
fistula, leak, or abscess of grade 3 or higher. This end point was quality indicators for pancreaticoduodenectomy.
significantly lower in those patients treated with pasireotide Another commonly discussed topic concerns the use
(9% vs. 21%, P = .006). The authors concluded that this of intraperitoneal drains. Despite much literature within the
perioperative medication decreases the rate of clinically signifi- recent past suggesting that intraperitoneal drainage may be
220
TABLE 12.9 Risk Factors for Infectious Complications After Pancreatectomy: Perioperative Risk Factors
Author, Year Title Study Type Patients Aim/Objective/End Point Population Results and Conclusions
Behrman Intraabdominal sepsis following Retrospective 196 To assess risk factors, Elective pancreatectomy Of the study population, 16.3%
et al, pancreatic resection: microbiology, and experienced intraabdominal sepsis.
2008 incidence, risk factors, management of Statistically significant risk factors for
diagnosis, microbiology, intraabdominal sepsis after intraabdominal sepsis were overt
management, and outcome pancreatectomy pancreatic fistula (18.8% vs. 5%) and
soft pancreatic remnant (74.2% vs.
42.3%). Length of stay was significantly
prolonged (28.5 vs. 15.2 days) as well
as mortality (15.6% vs. 1.8%). The
authors concluded that intraabdominal
sepsis after pancreatectomy was
associated with a soft pancreatic
remnant and overt pancreatic fistula, and
that intraabdominal sepsis increased
length of stay and mortality. They also
noted that this complication often occurs
early in the postoperative course and
PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
biliary drainage.
CI, Confidence interval; OR, odds ratio; RBC, red blood cell; SSI, surgical-site infection.
221
222 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
unnecessary and even harmful (Adham et al, 2013; Behrman preference but must be done meticulously. With regard to distal
et al, 2015; Conlon et al, 2001; Correa-Gallego et al, 2013; pancreatectomy, stapled closure of the pancreas with bioab-
Fisher et al, 2011; Mehta et al, 2013; Paulus et al, 2012; van sorbable mesh buttress appears promising in the prevention of
der Wilt et al, 2013), a recent randomized prospective multi- pancreatic fistula. Perioperative administration of pasireotide
center trial concluded that “elimination of intraperitoneal has demonstrated efficacy in reducing pancreatic fistula after
drainage in all cases of pancreaticoduodenectomy increases the pancreaticoduodenectomy and distal pancreatectomy. The use
frequency and severity of complications” (Van Buren et al, of intraperitoneal drains and the timing of their removal remain
2014). This most recent study randomized 137 patients under- controversial.
going pancreaticoduodenectomy. Half of the patients had an
intraperitoneal drain left in place, whereas the other half did Postoperative Risk Mitigation
not. These patients were followed prospectively for a range of Postoperative blood glucose control is important after surgical
complications. The study was stopped early due to the fact that procedures and has an impact on patient outcomes, as discussed
there was a substantial difference in mortality between the two earlier. Two hundred and sixty-five HPB surgery patients were
groups. The drained patients had a mortality of 3%, whereas studied by Ambiru and colleagues (2008) and were prospec-
the undrained group experienced a 12% mortality rate. Beyond tively evaluated for the development of SSI. Multivariate analy-
this, pancreaticoduodenectomy without intraperitoneal drain- sis showed that poor postoperative blood glucose was an
age was significantly associated with an increase in the number independent risk factor for SSI. The rate of SSI was 20% in
of complications per patient, an increase in the number of those patients with blood glucose levels below 200 versus 52%
patients who had at least one complication rated at grade 2 or in those without insulin infusion therapy (P < .01). Therefore
higher, and a higher average complications severity. From an blood glucose control in the postoperative setting is of particular
infectious standpoint, pancreaticoduodenectomy without intra- concern in the postpancreatectomy patient, especially because
peritoneal drainage was associated with a higher rate of intraab- some patients who were not previously diabetic may eventually
dominal abscess (25% vs. 10%, P = .027). This study therefore require insulin therapy.
provides strong evidence supporting the placement of intraperi- Synbiotic therapy has shown some promising results in
toneal drains at the time of pancreaticoduodenectomy. Taken mitigating infectious complications in hepatic resection patients
in the context of other contemporary literature on this subject, (see section “Hepatic Resection”). Similar results have been
the best approach to peritoneal drainage remains unclear and seen after resection of the head of the pancreas. Rayes and
should be individualized to the specific patient. Also, placing a colleagues (2007) conducted a randomized, double-blind trial
drain intraoperatively does not always obviate the need for a to evaluate the potential benefit of synbiotic therapy in patients
percutaneous drainage procedure in the early postoperative undergoing pancreaticoduodenectomy with preservation of the
period (Conlon et al, 2001). If placed at the time of pancreati- pylorus. The study included 80 patients total. All patients were
coduodenectomy, the timing of drain removal is also controver- started on enteral nutrition immediately postoperatively via a
sial. Recent prospective studies, including a randomized trial, nasojejunal tube placed at the time of the operation. The
have suggested that early drain removal based on drain amylase experimental group received enteral nutrition plus synbiotics,
levels can lower the rate of postoperative complications, includ- whereas the control group received enteral nutrition plus
ing infectious ones (Bassi et al, 2010; Kawai et al, 2006). placebo. Postoperative infectious complications occurred in
To summarize, risk mitigation at the operative level for a 12.5% of the patients receiving synbiotic versus 40% in the
pancreaticoduodenectomy or distal pancreatectomy consists of control group (P = .005). Although this evidence appears
the efficient performance of the operation using careful opera- compelling, we do not routinely use nasojejunal tubes. We also
tive technique in an effort to avoid unnecessary blood loss. do not advocate for the routine use of surgically placed feeding
There are no universally agreed upon techniques to reduce jejunostomy tubes, because we feel that their associated mor-
pancreatic fistula during the performance of pancreaticoduode- bidity outweighs their benefit (Padussis et al, 2014).
nectomy. The pancreaticoenteric anastomosis during pan
creaticoduodenectomy is still performed according to surgeon References are available at expertconsult.com.
Chapter 12 Infections in hepatic, biliary, and pancreatic surgery 222.e1
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222.e2 PART 1 LIVER, BILIARY, AND PANCREATIC ANATOMY AND PHYSIOLOGY
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CHAPTER 13
Clinical investigation of
hepatopancreatobiliary disease
Ali W. Majeed and Ahmed Al-Mukhtar
Patients with hepatopancreatobiliary (HPB) disease are seen in hypertension and may require urgent investigation with endos-
a variety of ways, depending on the underlying condition and copy (see Chapter 81). Shortness of breath and ankle swelling
rapidity of onset. Acute conditions are often inflammatory, and may indicate hypoalbuminemia, which can occur in many acute
pain is a predominant symptom. Jaundice is a common feature and chronic HPB disorders. A family history may point to
in many benign and malignant HPB diseases. A thorough and familial HPB disorders, and a drug history is important, espe-
complete history and clinical examination, followed by basic cially when the liver function is deranged. Social circumstances
blood tests, is a crucial starting point in the patient’s journey and employment are important to establish, especially with
from presentation to diagnosis, management, and discharge. occupational associations with HPB disorders (e.g., chronic
With the ease and availability of sophisticated high-resolution alcoholic liver and/or pancreatic disease in pub landlords).
scanning, there might develop a tendency for the physician to Accurate recording of alcohol intake must be made, because
“scan first, clinic later,” and this must be avoided. A thorough ongoing heavy alcohol use impacts treatment for chronic liver
clinical assessment will guide the appropriateness and use of or pancreatic diseases. Occasionally, patients attend the clinic
further tests and must include a careful balancing of potential smelling of alcohol in their breath, yet deny ongoing alcohol
risk versus benefit of any investigation or intervention in any use, and this should be noted. A request for a blood alcohol
particular individual, depending on their fitness, comorbidity, level could be made, provided the patient consents to it. A past
and personal or family wishes. This chapter describes the medical history should be obtained to include any major ill-
common symptoms and signs of HPB disease, the value of basic nesses and any abdominal surgery. A record of comorbidities
investigations, and how this initial assessment guides further and exercise tolerance should be made, as this will guide the
management. Clinical presentations and investigation of spe- surgeon in assessing fitness for future intervention if required
cific HPB diseases are also detailed. (see later).
224
Chapter 13 Clinical investigation of hepatopancreatobiliary disease 225
Inflammatory
Hepatitis
Abscesses, amebic and pyogenic
Schistosomiasis
Cirrhosis, early
Sarcoid
Biliary obstruction, especially extrahepatic
Metabolic
Amyloid
Steatohepatitis
Glycogen storage disease
Hematologic
Leukemias
Lymphomas
Myeloproliferative disorders
Sickle cell disease
Porphyrias
Tumors
Primary, benign and malignant
Secondary
Cardiovascular
Cardiac failure
Hepatic vein obstruction
Hematologic
Leukemias
Hemolytic anemias
Hemoglobinopathies
Portal hypertension, especially extrahepatic
Neoplastic
Lymphomas
Myeloproliferative disorders
Secondary deposits
Inflammatory
Rheumatoid FIGURE 13.11 Ascites with an everted umbilicus and venous disten-
Systemic lupus sion in a patient with cirrhosis.
Amyloidosis
Extrahepatic portal hypertension is usually due to portal
vein thrombosis, and as such it is important to identify any
secondary to portosystemic anastomosis, giving rise to caput history of neonatal infection around the umbilicus, major
medusa (see Figs. 13.7 and 13.8). The more common clinical intraabdominal sepsis or pancreatitis, pancreatic cancer, or a
site of portosystemic anastomosis is at the gastroesophageal blood disorder that might lead to hypercoagulability. These
junction, leading to esophageal varices; any evidence of upper patients almost invariably have splenomegaly, often associated
gastrointestinal blood loss, whether hematemesis or melena, with pancytopenia. In such cases, the liver is normal, but ascites
should be investigated with urgent endoscopy. Rarely, hemor- may be present. A palpable spleen in the upper left abdomen
rhoidal or lower rectal varices may develop in these patients associated with portal hypertension may be found in the event
(Fig. 13.13) as a result of portosystemic anastomosis. of splenic occlusion caused by tumor or chronic pancreatitis.
228 PART 2 DIAGNOSTIC TECHNIQUES
should be counseled that cholecystectomy may not relieve any pancreatitis and tumors of the pancreas can manifest in this
or all of their symptoms (Kirk et al, 2011; Zinsmeister et al, manner. Patients with chronic pancreatitis occasionally are seen
2011). Gallstone disease increases with increasing age, with jaundice, especially during an acute-on-chronic attack,
and older patients have complex disease with poorer outcome and the jaundice may be accompanied by symptoms of endo-
(Kuy et al, 2011). crine and exocrine deficiency (diabetes, steatorrhea, malab-
sorption) (see Chapters 57 and 58).
Gallstones in the Bariatric Population Malignant disease affecting the hepatic ducts at the biliary
Epidemiology studies have historically shown a higher preva- confluence in the hilus of the liver often presents with jaundice,
lence of gallstones in patients who are obese, with an eightfold but in such instances, the gallbladder is not palpable (see
increased risk of gallstones in those with a body mass index of Chapter 51B). Itching can be an initial feature of biliary
40 kg/m2 (Banim et al, 2011) or more; rapid weight loss obstruction, but in prolonged cholestasis, itching may occur in
increases the likelihood of gallbladder stones (Grover & Kothari, association with partial biliary obstruction and significantly in
2014; Moon et al, 2014) (see Chapter 32). It is interesting that primary biliary cirrhosis. Alkaline phosphatase often is mark-
the formation of gallstones occurs in the early period after these edly increased in partial biliary obstruction, even though the
procedures and is associated with impaired gallbladder motility bilirubin may be only marginally elevated. A markedly increased
(Al-Jiffry et al, 2003). With the common performance of bar- or increasing alkaline phosphatase level may be the only sign of
iatric surgical procedures, especially those that restrict endo- an early malignant or benign biliary stricture.
scopic access to the biliary tract (e.g., gastric transection and The distinction between obstructive (surgical) jaundice and
bypass), it is relevant to consider whether prophylactic removal hepatocellular (medical) jaundice is seldom the problem it was
of the gallbladder is justifiable. The incidence of gallbladder in the past. Biochemical tests of liver function (Table 13.2)
stones in these patients varies from 5% to 30%, with a high usually indicate whether the jaundice is obstructive, but this is
proportion being symptomatic and requiring cholecystectomy not always the case. Identification of the cause and level of
(Nagem et al, 2012; Tsirline et al, 2014). A meta-analysis of biliary obstruction is essential. Ultrasound is the preferred
13 studies concluded that prophylactic cholecystectomy is not initial imaging test for diagnosis of biliary obstruction and to
justified (Warschkow et al, 2013). Laparoscopic gastric bypass determine the etiology and level of obstruction. Generally, if
procedures are now routine, and HPB units are seeing an ultrasound shows gallbladder stones, magnetic resonance chol-
increasing number of patients with symptomatic or complicated angiopancreatography (MRCP) is required to confirm the pres-
biliary lithiasis. Laparoscopically assisted transgastric endo- ence of bile duct stones (see Chapter 19). If no gallstones can
scopic retrograde cholangiopancreatography (ERCP) is feasible be seen, computed tomography (CT) scanning is more useful
in this group (Grover & Kothari, 2014). for evaluation of biliary obstruction (see Chapter 18).
Bilirubin
Total 0.1-1.0 mg/dL Raised in jaundice/biliary obstruction/cholestasis
Conjugated 0.1-0.4 mg/dL Raised in biliary obstruction or cholestasis
Unconjugated 0.2-0.7 mg/dL Raised in hemolysis or Gilbert’s disease
Alkaline phosphatase 30-120 IU/L Biliary obstruction (partial or complete)
Aspartate transaminase or serum 6-40 IU/L Prognosticates liver disease. Raised in alcoholic liver disease (ratio of
glutamic oxaloacetic transferase 2 : 1 with ALT)
(AST or SGOT)
Alanine transaminase or 7-40 IU/L Raised in hepatocyte damage (viral, alcohol, hemochromatosis).
serum glutamic pyruvic transaminase Usually lower than AST in alcoholic liver disease. Very high levels in
(ALT or SGPT) fulminant liver disease (acetaminophen, viral)
Gamma glutamyl transpeptidase (GGT) 0-42 IU/L Raised in alcoholic liver disease
Serum albumin 3.5-5.3 g/dL Low in chronic liver insufficiency, pancreatic disease with poor nutrition
Prothrombin time 10-12 sec Raised in prolonged biliary obstruction. Marker of chronic liver
insufficiency
Chapter 13 Clinical investigation of hepatopancreatobiliary disease 233
should be performed to exclude the presence of bile duct tion should be less than 40% by using a continuous intravenous
stones. Endoscopic ultrasonography (EUS) is very accurate in cholecystokinin (CCK) octapeptide infusion during a 30-minute
this setting, albeit more invasive than MRCP (Holm & Gerke, period, and there should be a positive therapeutic response
2010) but is a good option in claustrophobic patients. with absence of the recurrent pain for longer than 12 months
after cholecystectomy. Investigation of functional biliary tract
Bile Duct Stones disorders should include upper gastrointestinal endoscopy,
The human bile duct is sensitive to acute distension, and transcutaneous and endoscopic ultrasonography (to rule out
obstruction of the lower end of the bile duct by a gallstone may microlithiasis), and possibly bile sampling for microlithiasis and
cause epigastric pain that may radiate to the chest and back. cholesterol crystals. Unfortunately, no consensus exists regard-
Cholesterol bile duct stones are lighter than bile, and any dis- ing the infusion rate of CCK that in turn can directly influence
tension of the bile duct may cause these stones to float proxi- gallbladder emptying. Delgado-Aros and colleagues (2003) and
mally, releasing the obstruction. The symptoms of bile duct DiBaise and colleagues (2003) reported meta-analyses of
stones are typically intermittent jaundice associated with upper studies examining the symptomatic benefit from cholecystec-
abdominal pain. Ultrasound alone is not sufficiently sensitive tomy based on abnormal CCK-stimulated gallbladder empty-
or specific for the diagnosis of bile duct stones (Boys et al, ing. They found no good evidence to support the use of
2014), and MRCP is recommended if the liver tests are abnor- CCK-stimulated gallbladder ejection fraction to select patients
mal because abnormal LFTs are the most sensitive predictor for cholecystectomy. Similar findings were reported by Rastogi
of bile duct stones (Videhult et al, 2011) (see Chapters 36 and colleagues (2005) and Ozden and colleagues (2003). Criti-
and 37). cal evaluation of CCK-provoked gallbladder pain concludes
that this test was not a predictor of symptomatic relief after
Cholangitis cholecystectomy (Edwards, 2014; Smythe et al, 1998). It is
Acute cholangitis is an infection within a partially or completely interesting to note that in a prospective randomized study
obstructed biliary system (see Chapters 8 and 43). Charcot examining the development of symptoms in patients with
triad is the classic picture of acute cholangitis and comprises uncomplicated gallbladder stones, a CCK-stimulated ejection
jaundice, abdominal pain, rigors, and pyrexia. Hypotension and fraction greater than 60% was independently associated with
confusion are often a feature of acute suppurative cholangitis the development of symptoms.
in which the bile duct is filled with purulent bile under pressure The etiology and pathogenesis of calculous and acalculous
(Reynold pentad). The Tokyo Guidelines for the diagnosis and gallbladder pain are poorly understood despite some insights
management of acute cholangitis were originally published in by mathematical modeling (Ahmed et al, 2000; Bird et al,
2007 and have recently been updated (Takada, 2013). These 2006; Li et al, 2011, 2013; Ooi et al, 2004; Wegstapel et al,
are summarized in Box 13.5. 1999). The clinical outcomes from cholecystectomy for acalcu-
lous biliary pain are similar to those for calculous biliary pain
Acalculous (“Functional”) Biliary Pain with approximately two thirds of patients experiencing symptom
Acalculous biliary pain is considered to be the result of a “func- relief (Ahmed, 2011; Wybourn, 2013). We would therefore cur-
tional” motility disorder of the gallbladder and/or sphincter of rently recommend that patients experiencing recurrent and
Oddi (SO) (Behar et al, 2006). Gallbladder motor dysfunction severe symptoms as defined by the Rome III criteria should be
giving rise to abdominal pain has been defined by the Rome III offered cholecystectomy but should be carefully counseled
Committee on Functional Biliary and Pancreatic Disorders. regarding the uncertainty of its outcome, and this counseling
These criteria are listed in Box 13.7. Biliary and pancreatic pain should be clearly documented.
should be defined by site, severity, modality of onset, and dura-
tion, and by the absence of typical symptoms of gastrointestinal Sphincter of Oddi Dysfunction
reflux disorder, functional dyspepsia, and irritable bowel syn- SO dysfunction may be present in patients with an intact biliary
drome. There should also be the absence of gallstones, biliary tree, but it usually comes to light as a potential diagnosis when
sludge, or microlithiasis. An abnormal gallbladder ejection frac- symptoms continue after a cholecystectomy. It could be argued
that the diagnosis of SO disorder should not be made in patients
with a gallbladder in situ. The potential risks of cholecystec-
tomy are outweighed by the potential risk of endoscopic biliary
intervention, and even SO manometry and the symptoms
BOX 13.7 Rome III Criteria for Functional Gallbladder Disorder between the two conditions can be indistinguishable. SO dys-
Diagnostic criteria. Must include all of the following:
function has been subclassified into a biliary or pancreatic type
1. Criteria for functional gallbladder and sphincter of Oddi disorder (Box 13.8). Biliary type SO dysfunction in postcholecystectomy
2. Gallbladder is present patients has been arbitrarily subclassified into types I, II, and
3. Normal liver enzymes, conjugated bilirubin, and amylase/lipase III. Biliary type I SO dysfunction is defined as pain, elevated
LFTs documented on two or more occasions, delayed contrast
Rome III Criteria for Functional Biliary Sphincter of Oddi drainage, and a dilated CBD with a corrected diameter of
Disorder 12 mm or more at ERCP. Biliary type II SO dysfunction is char-
Diagnostic criteria must include both of the following: acterized as pain only with one or two of the criteria in type I.
1. Criteria for functional gallbladder and sphincter of Oddi disorder Biliary type III SO dysfunction is defined as recurrent biliary-type
2. Normal amylase/lipase
pain with none of the criteria from type I. Toouli (2009) con-
Supportive criterion
Elevated serum transaminases, alkaline phosphatase, or conjugated
cluded that accurate sphincter manometric data is crucial to
bilirubin temporarily related to at least two pain episodes establish a diagnosis of SO dysfunction. Invasive investigation
of sphincter dysfunction and/or sphincterotomy is associated
234 PART 2 DIAGNOSTIC TECHNIQUES
with a risk of pancreatitis in as many as 30% of patients. Inser- pancreatic enzymes are elevated soon after an attack of pain
tion of prophylactic pancreatic stents is advocated as a means and whether the pancreatic duct is dilated greater than 5 mm.
of reducing this risk, and some evidence exists to support this In patients seen with pancreatitis, it is important to exclude
practice. Injection of botulinum toxin into the sphincter also common causes of acute pancreatitis (see Acute Pancreatitis
has been advocated as a “therapeutic test” before a sphincter- later). Noninvasive investigations include secretin-stimulated
otomy is performed. In a literature review, Sgouros and Pereira ultrasonography of the pancreatic duct and secretin-induced
(2006) concluded that biliary sphincterotomy reliably treats MRCP. Invasive investigations include pancreatic SO manom-
symptoms in 85%, 69%, and 37% of patients with types I, II, etry, botulinum toxin, or stent drainage. Total endoscopic pan-
and III SO dysfunction, respectively, and pancreatic sphincter- creatic SO sphincterotomy is the currently recommended
otomy may benefit as many as 75% of patients. They state that treatment (Behar, 2006).
sphincter manometry is the gold standard in the investigation.
Sphincter manometry may itself cause pancreatitis, and PANCREAS
noninvasive investigation with MRCP, ultrasonography, and
hepatoiminodiacetic acid choledochoscintigraphy should be Acute Pancreatitis
conducted first. The Milwaukee criteria are a useful summary Acute pancreatitis is usually accompanied with severe upper
of expected outcomes after sphincterotomy for biliary SO dys- abdominal pain that develops rapidly, becomes constant, and
function (Table 13.3). Pancreatic type SO dysfunction is also persists for several hours (see Chapters 55 and 56). The pain
subclassified into types I, II, and III according to whether typically starts in the epigastrium but may soon spread through-
out the abdomen and radiate into the back. Sometimes the
patient may find relief by sitting forward, but usually he or she
lies still and curled up in bed. The pain can be so sudden in
BOX 13.8 Rome III Criteria for Functional Gallbladder and
onset that, at times, it can simulate a perforated peptic ulcer,
Sphincter of Oddi Disorders
and indeed, acute pancreatitis can mimic almost every cause of
Clinical Features acute abdominal pain and may even produce chest pain that
Episodes of right upper quadrant pain or epigastric pain that must simulates myocardial infarction, pneumonia, or pleurisy. Fre-
have ALL the following features: quent vomiting and sequestered fluid in the small bowel may
Episodes lasting 30 minutes or longer lead to rapid and severe dehydration. Even keeping the stomach
Recurrent symptoms occurring at different intervals (not daily)
empty with a nasogastric tube may not prevent the patient from
The pain builds up to a steady level
The pain is moderate to severe enough to interrupt the patient’s daily
retching, and marked nausea is almost a constant feature. Hic-
activities or lead to an emergency department visit coughs can also occur due to diaphragmatic irritation second-
The pain is not relieved by bowel movements ary to extension of the inflammatory process tracking up via the
The pain is not relieved by postural change retroperitoneum.
The pain is not relieved by antacids Patients with acute pancreatitis may exhibit signs of pro-
Exclusion of other structural disease that would explain the found shock with tachycardia, tachypnea, hypotension, and
symptoms confusion. At the other extreme, patients may appear well, with
little in the way of physical signs. The patient may be afebrile
Supportive Criteria on admission, but progression of the inflammatory process
The pain may present with one or more of the following:
leads to fever, facial flushing, and mild jaundice. Abdominal
Associated nausea and vomiting
Radiates to the back and/or right infra-subscapular region
examination usually reveals marked tenderness in the epigas-
Awakens from sleep in the middle of the night trium with guarding, but marked rigidity as seen in a perforated
ulcer is often lacking. The presence of a paralytic ileus may
TABLE 13.3 Milwaukee Criteria Based on the Frequency of Abnormal SO Manometry and Pain Relief by Sphincterotomy
Probably of Pain Relief by
Frequency of Sphincterotomy if Manometry
Biliary SOD Type Abnormal Manometry Abnormal Normal Manometry before Sphincter Ablation
FIGURE 13.16 Cullen sign (periumbilical bruising) in a patient with IV Laceration Proximal transection or parenchymal
acute pancreatitis. injury involving ampulla
V Laceration Massive disruption of pancreatic head
*Advance one stage for multiple injuries up to grade III.
Chronic Pancreatitis
There are few pathognomonic or diagnostic signs for chronic
pancreatitis, and diagnosis usually depends on the history and
special investigations (see Chapters 57 and 58). The patient
may appear malnourished, with signs of weight loss, they may
be icteric as a result of compression of the CBD by the fibrotic
process in the head of the pancreas, and erythema ab igne may
be present on the back (Fig. 13.18) or abdomen. Uncommonly,
a palpable mass, pseudocyst, or splenomegaly may be evident,
and occasionally pancreatic ascites, if there has been rupture of
a pseudocyst or of the duct system. FIGURE 13.18 This patient has long-standing chronic pancreatitis that
affects the entire length of the pancreas with severe flank and back pain
Chronic pancreatitis is a difficult condition both to diagnose
on the left side. Prolonged application of local heat has resulted in
and to treat. It is crucial to exclude other associated conditions, marked rash of erythema ab igne.
such as pancreatic cancer. Once the diagnosis is established, it
is important to (1) identify any predisposing cause, (2) stage
the severity of the disease, and (3) document any morphologic discomfort, but others may simply complain of intermittent
and functional changes against which any progression can be attacks. In some, severe bouts may be brought on by ingesting
assessed. One of the most common predisposing factors is alcohol, although often no clear association is made between
alcohol abuse, although chronic pancreatitis is also associated attacks and oral intake. In many the pain is so debilitating that
with biliary disease, congenital abnormalities such as an annular it interferes with the patient’s domestic, social, and occupa-
pancreas (Dowsett et al, 1989), ductal abnormalities, and tional activities and can have a devastating impact on the
rarely, hyperparathyroidism. An autosomal dominant heredi- quality of life. Indeed, in many it results in a change in person-
tary form of the condition may also be a factor, so a family ality with a manipulative tendency often associated with an
history is crucial (Teich, 2008). Polymorphisms at PRSS1- addiction to opiates. These patients can be particularly difficult
PRSS2 and CLDN2-MORC4 gene loci were found to be associ- to assess, especially if they are already addicted to alcohol.
ated with alcoholic and nonalcoholic chronic pancreatitis Other presenting symptoms include marked steatorrhea
(Derikx et al, 2015; Rai et al, 2014). Rarely is any specific drug resulting from diminished lipase production and inadequate
or dietary factor implicated. fat absorption (Di Magno, 1982). The stool frequency may be
Pain is the most common presenting symptom of chronic increased to as often as six times a day, and the stools them-
pancreatitis and is often the most difficult to control. The pain selves become pale and bulky with an offensive odor, and they
is usually situated in the epigastrium and subcostal regions and float, making them difficult to flush away. However, this is not
commonly radiates through to the back. Pain can be severe and a constant feature of chronic pancreatitis; some patients may
penetrating in nature, and often the patient will lean forward even suffer from constipation as a result of the increased use of
or curl up to relieve the discomfort. In severe cases, the patient opiate analgesia.
may even kneel on all fours to gain relief. Occasionally, the pain The incidence of diabetes mellitus is a variable and often
may radiate to the left shoulder tip. Variation in the pattern of late feature. As chronic pancreatitis progresses, there may be
pain in these patients is enormous, and some are never free of loss of endocrine function, initially requiring dietary control
Chapter 13 Clinical investigation of hepatopancreatobiliary disease 237
and subsequently oral hypoglycemic agents or even insulin. and allows the patient to proceed to endoscopy and endoscopic
Other more general features of chronic pancreatitis may include sphincterotomy when appropriate (see Chapter 29). In patients
weight loss, nausea and vomiting, jaundice, and even gastroin- with acute pancreatitis, the duodenum and small bowel often
testinal bleeding as a result of splenic vein thrombosis, although are filled with gas, and detection of CBD stones is less
this is rare. reliable.
Nutritional depletion is a common feature in patients with Serum amylase is of no value in predicting the severity of an
chronic pancreatitis and is reflected in cachexia and low serum attack, and scoring systems have been developed, such as the
albumin levels. This should be managed in conjunction with Ranson and Glasgow scores. Scoring systems are accurate in
specialized HPB (hepato-pancreato-biliary) nutritionists and predicting outcome only after 48 hours. Inflammatory markers
may include a period of fine-bore nasogastric feeding before such as CRP are also are valuable, but similarly to the Ranson
any intervention is contemplated. and Glasgow scores, such markers may not assess severity accu-
rately until 48 hours after onset. The Acute Physiology, Age,
Pancreatic Cancer and Chronic Health Evaluation score is a more accurate predic-
Regrettably, physical signs of pancreatic cancer are often absent tor of severity at admission, but its complexity limits its routine
or infrequent, until the lesion is unresectable (see Chapters 61 clinical use.
and 62). The patient may be symptomatic with weight loss, but In patients who remain unwell 1 week after onset, or in
unless the lesion is situated in the head of the pancreas such those who deteriorate after initial improvement, pancreatic
that it obstructs the CBD early, causing obstructive jaundice, ischemia and necrosis should be suspected, and a contrast-
few other signs may be evident. With distal bile duct obstruc- enhanced CT scan should be performed. Patients judged to
tion, the gallbladder may become distended (Courvoisier gall- have a severe attack of pancreatitis at onset are at high risk of
bladder). An abdominal mass and ascites are late signs and developing a systemic inflammatory response syndrome and
usually herald inoperability. Systemic signs such as flitting require very careful and repeated observation with attention to
thrombophlebitis migrans may be apparent, but this is uncom- fluid balance, nutrition, and sepsis. Prophylactic antibiotic
mon and nonspecific. All too often cachexia is the only physical therapy in this group of patients is useful and may prevent the
finding. development of infected pancreatic necrosis. Patients with
Later clinical features of pancreatic cancer are pain, weight clinically and biochemically severe pancreatitis should be
loss, and jaundice. The pain is often severe and gnawing and managed in conjunction with critical care physicians in a suit-
radiates to the back. It is often worse at night, when the patient able environment. Patients may go on to experience pancreatic
is lying flat, which usually indicates tumor extension to the pseudocysts that may cause pain or other effects as a result of
retroperitoneum, often signifying unresectability. Weight loss pressure on neighboring organs, especially the stomach.
may be marked, and in many cases of tumors in the body of Nausea, vomiting, or early satiety should alert the physician,
the pancreas, weight loss may be the only symptom, until pain as these pseudocysts are easily detectable on CT scanning.
indicates invasion of the peripancreatic tissue. The more rapid Continuing evidence of systemic sepsis usually indicates the
the weight loss, the less likely the lesion is to be resectable presence of infected pancreatic necrosis, which can be con-
(Bakkevold et al, 1992). Jaundice can be associated with severe firmed by fine needle aspiration.
pruritus, but this classic presentation only occurs when the In patients with chronic pancreatitis, serologic blood tests
lesion is in the head of the pancreas; when jaundice occurs with such as amylase, lipase, and elastase are not helpful, but CRP
tumors of the body or tail of the pancreas, it usually signifies may indicate active inflammation. Fecal elastase may indicate
hilar liver or nodal metastases. exocrine deficiency, whereas routine hematologic and biochem-
Approximately 5% of patients with pancreatic cancer will ical tests, including glycosylated hemoglobin, are important to
have diabetes mellitus within the 2 years before diagnosis provide a baseline for endocrine assessment.
(Pannala et al, 2009). Other signs such as ascites, an epigastric It may be difficult to differentiate between pancreatic carci-
mass, or enlarged supraclavicular nodes (Virchow sign) are noma and some cases of chronic pancreatitis as there are no
indications of inoperability. Because of the lack of specific signs clear-cut markers for this, although lymphoplasmacytic scleros-
and symptoms, very commonly a diagnostic dilemma arises as ing pancreatitis is usually accompanied by an elevated serum
to whether a lesion is chronic pancreatitis or pancreatic cancer. immunoglobulin G (see Chapter 57). The tumor marker CA
Frequently, diagnostic imaging cannot provide the answer, and 19-9 has a sensitivity of 80% and a specificity of 75% for pan-
even at operation, it may not be apparent which condition the creatic cancer (Kim et al, 1999), but as the level tends to
surgeon is facing; this occurred in as many as 15% of cases in correspond with tumor volume, potentially curative tumors
some series (Mao et al, 1995). may be associated with normal levels (Eloubeidi et al, 2004;
Schlieman et al, 2003), which limits its use as a screening tool.
INVESTIGATION OF PATIENTS WITH Very high levels of CA 19-9 are associated with a higher inci-
PANCREATIC DISEASE dence of metastatic disease (Maithel et al, 2008), and laparos-
copy is advocated to determine the presence of subradiologic
In patients with acute pancreatitis, diagnosis usually is made metastatic disease in patients with a CA 19-9 level greater than
based on the history and the serum amylase and lipase levels. 150 kU/L (nonjaundiced patients) and greater than 300 kU/L
An elevated serum amylase can fall quite rapidly, and it may in jaundiced patients (Halloran et al, 2008).
be normal if measured 2 to 3 days after the onset of the attack. A contrast-enhanced CT scan provides information as to the
Urinary amylase may be elevated in these patients; however, a extent and nature of any mass and in particular helps differenti-
contrast-enhanced CT scan often confirms the diagnosis but is ate solid from cystic lesions, vascular involvement or encase-
limited for identifying gallstones. An ultrasound scan is usually ment, and lymph node metastases (see Chapter 18). No
the first investigation of choice, because it detects gallstones significant advantage of gadolinium-enhanced magnetic
238 PART 2 DIAGNOSTIC TECHNIQUES
resonance imaging over multidetector CT has been seen in the in such morbidity that the patient never returns home—a poor
staging of pancreatic cancer (Park et al, 2009), but multidetec- postoperative outcome. The same applies to major hepatic
tor CT has a better diagnostic yield (Satoi et al, 2009). MRCP resections. Calculation of risk for cancer resections must include
can be useful in the differential diagnosis of pancreatic cystic all the potential oncologic outcomes: recurrent malignancy after
masses and duct delineation, and EUS may contribute substan- resection, anticipated survival without resection, survival with
tially to the assessment of ampullary tumors (Kahaleh et al, alternative treatment modalities. As well as clinical judgment,
2004), for image-guided aspiration of pancreatic cysts, and to there are a number of scoring systems that have been devised
obtain biopsies of intrapancreatic tumors (see Chapter 19). over time to assist in quantifying the risk associated with surgery:
ASA grading, Lee’s Revised Cardiac Risk Index (RCRI), and
ASSESSMENT OF FITNESS FOR MAJOR Physiologic and Operative Severity Score for the enUmeration
HEPATOPANCREATOBILIARY SURGERY of Mortality and Morbidity (POSSUM), to name a few. More
recently, objective fitness assessments have been undertaken to
Major hepatic and pancreatic resections (the majority of which assist in the prediction of the poorer outcome: 6-minute walk
will be undertaken for cancer) inflict a large physiologic and test (6MWT), intermittent shuttle walk (ISW), and cardiopul-
metabolic insult on patients with a significant risk of both peri- monary exercise testing (CPET). Of these, CPET has shown
operative mortality and morbidity. It is therefore useful to quan- the most potential to be a reliable predictor of mortality and
tify such risk so that the patient and their families can make major morbidity in patients undergoing major hepatic and pan-
informed choices (see Chapters 24 and 25). For example, creatic resections (Snowden, 2013).
surgery in an elderly patient with a borderline resectable pan-
creatic cancer requiring vascular resection and reconstruction References are available at expertconsult.com
may not lead to death within 30 days of surgery but may result
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CHAPTER 14
Emerging techniques in diagnostic imaging
Richard Kinh Gian Do
The field of radiology has undergone tremendous growth in the With single energy (or traditional) CT, the x-rays are gener-
new millennium, with continuous advances in diagnostic ated from accelerating electrons in a x-ray tube subject to a
imaging that include innovations in medical devices, such as peak voltage, kVp, that determines a predictable energy spec-
the creation of dual energy–source multidetector computed trum of the emitted x-rays. By adding a second x-ray beam with
tomography (CT); innovations in imaging agents, such as new a different kVp, one can not only create CT images based on
hepatocyte-specific gadolinium-binding contrast agents for electron density but also calculate the concentration of distinct
magnetic resonance imaging (MRI); standardization of quanti- elements present in the body. Dual-energy CT (DECT) thus
tative functional imaging, such as for MR diffusion-weighted takes advantage of the “signature” x-ray interaction profile of
imaging, and innovations in image analysis, such as texture distinct elements, such as calcium (Ca20) and iodine (I53).
analysis, as a radiomics approach to tumor heterogeneity. In The potential applications of DECT are numerous but are
this chapter, we will review a few emerging techniques in diag- primarily separated into two functions. The first is in changing
nostic imaging with relevance to hepatopancreaticobiliary the image contrast between iodine and other elements, for
tumors. example, by increasing the conspicuity of tumors that enhance
using iodinated contrast. At lower x-ray energy, the attenuation
DUAL-ENERGY COMPUTED TOMOGRAPHY of iodinated contrast is magnified compared with soft tissue,
which can alter the conspicuity of subtle enhancing lesions.
Medical imaging with CT has benefited from the development Potential applications include improving hepatocellular carci-
of multidetector technology, leading to faster scanning of the noma (HCC) detection (Altenbernd et al, 2011), liver metas-
abdomen with higher-resolution images, resulting in submilli- tasis detection (Robinson et al, 2010), and pancreatic cancer
meter isotropic image voxels that allow multiplanar reformat- detection (Macari et al, 2010) (Fig. 14.1). A second application
ting and three-dimensional volume rendering (see Chapter 18). of DECT relies on the quantification of specific elements, such
New dose modulation techniques have also reduced the radia- as calcium or iodine. Quantifying iodine can improve our ability
tion dose exposure for patients. However, one of the more to measure treatment response, for example, in therapies in
exciting techniques to have emerged in CT imaging relevant to which tumor vascularization (and enhancement) is affected and
hepatopancreaticobiliary tumors is dual-energy CT (DECT) changes in tumor attenuation are informative (Uhrig et al,
(Coursey et al, 2010; Heye et al, 2012). To understand this 2013). Fat quantification, in patients at risk for hepatic steato-
technique, it is worth discussing a few physical principles sis, for example, is also another potential application of this
underlying CT imaging. technique (Hur et al, 2014). Although DECT is gaining in
CT is based on the application of x-rays, first recognized by popularity as the applications multiply, a number of obstacles
Wilhelm C. Roentgen in 1895. X-rays represent electromag- remain, including standardization and differences in hardware
netic waves (photons) of very high energy and very short wave- and software between vendors (Morgan, 2014). Nevertheless,
lengths that can pass through most objects, allowing us to “see” the potential quantification of certain elements by DECT,
through the body. The degree of x-ray attenuation (or interac- including iodine uptake, is attractive to radiologists who are
tion) by different elements in our body is related to the number increasingly exploring quantitative tools in medical imaging.
of electrons present in each element. The higher the atomic
number of an element, the greater the number of electrons FUNCTIONAL IMAGING WITH MAGNETIC
present that can potentially interact with x-rays. In simplistic RESONANCE IMAGING
terms, x-rays will be more frequently scattered or absorbed by
the photoelectric effect when they travel through bones, which The similarities between MRI and CT are evident: cross-
are high in calcium (Ca20), than when traveling through other sectional high-resolution imaging of abdominal organs, using
soft tissues made of hydrogen (H1), carbon (C6), nitrogen (N7), intravenous contrast to highlight differences in enhancement.
and oxygen (O8), which are lower in atomic number. The Analogous to advances in CT, progress in MRI technology has
density of atoms is another factor contributing to x-ray attenu- benefited from hardware upgrades generating more rapid and
ation; lungs are radiolucent (dark) on radiographs and CT higher-resolution images. However, the added value for MRI
because of the lower density of atoms (and electrons) present versus CT arises from the ability to image patients frequently
in air. On the other hand, the utility of iodinated intravenous without the risk of ionizing radiation and from new soft tissue
contrast used in CT is partly based on the high attenuation of contrast mechanisms (see Chapter 19).
iodine (I53), which can more frequently scatter and absorb MRI is based on the principles of nuclear magnetic reso-
x-rays, thereby providing information on the vasculature and nance (NMR), which harnesses the inherent magnetic proper-
the enhancement of organs. ties of protons (H1) and their electromagnetic interactions. For
239
240 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 14.1 Computed tomography (CT) images of a patient with infiltrative hepatocellular carcinoma obtained by dual-source dual-energy CT.
Arterial phase (A and B) and portal venous phase images (C and D) on liver windows demonstrate an ill-defined right posterior hepatic mass with
arterial enhancement, better appreciated on the arterial phase of lower (60) KEV images (A) than traditional higher (77) KEV images (B). At a lower
KEV (A and C), image noise is increased compared with higher KEV images (C and D).
example, tissue contrast can be generated from differences in tiple cancers (Hylton, 2006). Tumor response to chemotherapy
chemical environment that affect tissue relaxivity (e.g., T1- vs. has traditionally been assessed by measurements of tumor size,
T2-weighted imaging), differences in microscopic and macro- such as through guidelines from the Response Assessment Cri-
scopic motion (e.g., diffusion-weighted imaging [DWI] and teria in Solid Tumors rules. With cytotoxic therapies, reduction
vascular flow-sensitive imaging), electromagnetic environment in size of tumors is expected with a good response to therapy.
(e.g., susceptibility imaging), and many others. The soft tissue However, as new targeted therapies may inhibit vascularization
contrast mechanisms generated by MRI are numerous and or act as cytostatic agents, traditional response criteria based
growing, with new sequences exploiting different biologic states on tumor shrinkage may underestimate therapeutic effective-
(e.g., oxygenation of hemoglobin) being developed continu- ness. With DCE-MRI, quantification of tumor vascularity is
ously. Two applications of MRI that emphasize function (and measured to better predict tumor response to antiangiogenic or
not just form) that have received increasing attention are targeted therapy. DCE-MRI is based on the repeated imaging
dynamic contrast-enhanced MRI (DCE-MRI) and diffusion- of an organ or body part during several minutes, during which
weighted MR imaging (DWI or DW-MRI). the initial uptake and subsequent distribution of intrave-
DCE-MRI is a technique that noninvasively characterizes nously administered contrast are recorded (Fig. 14.2). Although
the vasculature of organs and tumors and has the potential to dynamic contrast-enhanced CT is also technically feasible, the
provide predictive or prognostic response biomarkers in mul- increased ionizing radiation associated with obtaining multiple
Chapter 14 Emerging techniques in diagnostic imaging 241
FIGURE 14.2 Consecutive oblique coronal magnetic resonance (MR) images were obtained of the abdomen every 5 seconds, before (first panel,
top left) and immediately after intravenous contrast administration. Contrast can be seen arriving in the abdominal aorta (middle panel, top row),
before enhancing the periphery of the right hepatic lobe peripheral cholangiocarcinoma, on subsequent frames. The entire tumor was imaged during
this dynamic contrast-enhanced MRI sequence, with only a single representative slice through the middle of the tumor shown at various time points.
CT images has limited its development. With MRI, the arrival blood plasma or vascular space (VS) and extracellular extravas-
and distribution of gadolinium (Gd) contrast throughout the cular space (EES); kep, the rate constant between EES and VS;
vasculature and interstitial space is continuously imaged, and and ve, the fractional vascular volume. For example, parame-
through pharmacokinetic modeling, the changes in signal inten- ters can be measured at baseline and compared on follow-up
sity of an organ (or tumor) of interest are converted into perfu- posttreatment scans. Because perfusion parameters are derived
sion parameters (Do et al, 2009). from DCE-MRI, this technique was initially applied for evalu-
Quantitative perfusion parameters obtained from DCE-MRI ation of antiangiogenic therapy, but its use has expanded to
reflect the rate of exchange of Gd from vessels to the interstitial other targeted chemotherapy agents. Although there has been
space and include Ktrans, a volume transfer constant between an increasing number of studies evaluating the utility of
242 PART 2 DIAGNOSTIC TECHNIQUES
DCE-MRI in hepatobiliary tumors (Konstantinidis et al, 2014; imaging techniques may be standardized across different
Taouli et al, 2013), the imaging protocols for DCE-MRI have medical centers, the variability in imaging interpretation
differed among medical centers, limiting comparison of studies between different radiologists can remain substantial. Thus an
and dissemination of this functional imaging technique. Efforts emerging body of research has focused on the diagnostic per-
are ongoing to reduce the variability and improve standardiza- formance of radiologists. One of the criticisms of published
tion of imaging parameters by the Quantitative Imaging Bio- retrospective radiology studies that report on the accuracy of
marker Alliance, formed by the Radiological Society of North imaging modalities for different clinical questions has been the
America. use of consensus interpretation among expert readers (Bankier
An extension of DCE-MRI that is unique to liver imaging et al, 2010). Individual interpretation, rather than consensus
is the use of hepatobiliary contrast agents to simultaneously interpretation, is the norm in routine clinical practice. The
assess vascular supply (through both the hepatic artery and referring clinician is thus dependent on the training and
portal vein) as well as hepatic function (Sourbron et al, 2012). expertise of the diagnostic radiologist who is assigned to inter-
Although the majority of MR contrast agents containing Gd pret their patient’s imaging study at a particular point in time.
are excreted through the kidneys, gadoxetate (Gd-EOB-DTPA) A method to reduce the potential variability among diagnos-
undergoes both renal and biliary excretion approximately tic radiologists is the establishment of diagnostic imaging crite-
evenly. Thus it is often referred to as a dual-function contrast ria. For example, numerous criteria for the diagnosis of HCC
agent, allowing the evaluation of both tumor and liver paren- have been published by various societies (Cruite et al, 2013)
chymal enhancement in the same study (Sirlin et al, 2014). The (see Chapter 91). The role of imaging diagnosis for HCC is
role of gadoxetate has expanded and is further discussed in unique in its potential impact in patient care, guiding the choice
Chapter 19. of treatment and even affecting the allocation of liver trans-
DWI is an alternative and complementary functional plants. The American College of Radiology (ACR) first released
imaging technique to DCE-MRI that can help predict and a set of guidelines for the diagnosis of HCC termed the Liver
monitor tumor response to therapy (Hamstra et al, 2007; Imaging Reporting and Data System (LI-RADS) in 2013 (Mitch-
Padhani et al, 2009; Thoeny & Ross, 2010). With DWI, one ell et al, 2014). The ACR will regularly update LI-RADS
can measure the apparent diffusion coefficients (ADCs), guidelines to help standardize the reporting and data collection
which provide an estimate of the magnitude of water diffusion of CT and MR imaging of HCC (http://www.acr.org/quality-
in biologic tissues. When ADC is measured in tumors, it pro- safety/resources/LIRADS). Soon after its initial release, it
vides an indirect measure of tumor cellularity at baseline became clear that there were slight discrepancies among
and necrosis following treatment. There is an inverse relation- LI-RADS, the criteria published by the American Association
ship between ADC and tumor cellularity, which is explained for the Study of Liver Disease (AASLD) (Bruix et al, 2011)
by the presence of cell membranes in proliferating tumors, and the Organ Procurement and Transplantation Network
which act as barriers to water motion. Thus rapidly growing (OPTN) (Wald et al, 2013), which were later addressed in the
tumors with higher concentrations of lipid barriers will be 2014 revision. Nevertheless, for all sets of three criteria above,
lower in ADC. Most treatments will lead to disruptions of cell the imaging diagnosis of HCC relies primarily on the assess-
membrane integrity with resulting greater water diffusion and ment of tumor arterial phase hypervascularity and the detection
subsequent increases in ADC. In HCC (Chapiro et al, 2014) of “washout appearance” on portal venous phase or delayed
and colorectal liver metastases (Cui et al, 2008; Koh et al, imaging.
2007), ADC can be used to assess response to chemoemboli- The concept of washout on CT and MR imaging is straight-
zation and chemotherapy, respectively. A study using DWI forward, described as decreased enhancement in a lesion when
to monitor HCC response to sorafenib is also promising compared with the liver parenchyma after initial enhancement
(Schraml et al, 2009). As an indirect measure of tumor cel- on the arterial phase. With LI-RADS, the suggestion is to rec-
lularity and necrosis, DWI is ideally suited as a biomarker to ognize this finding only when it is unequivocally present. The
assess therapy response. Further discussion on DWI can be possibility that different radiologists may interpret “washout
found in Chapter 19. appearance” with some variability was well known (Liu et al,
2013). In fact, a large interobserver variability study since the
DIAGNOSTIC CRITERIA first release of LI-RADS demonstrated that there was only
moderate agreement between radiologists for the detection of
Although functional imaging techniques such as DCE-MRI “washout appearance” (Davenport et al, 2014). The agree-
and DWI are quantitative methods to measure tumor proper- ment for the definitive diagnosis of HCC based on imaging
ties, the majority of diagnostic radiology still relies on the sub- criteria for LI-RADS, AASLD, and OPTN guidelines was also
jective interpretations of images. For example, CT and MRI moderate to substantial at best. Thus despite efforts at stan-
have a critical role in the initial assessment of hepatobiliary dardization with the development of diagnostic guidelines,
lesions, such as in the characterization of a solitary liver mass variability in the performance of diagnostic radiologists can
that is incidentally discovered. A hypervascular solitary tumor remain substantial in specific clinical scenarios and a source of
may represent a benign neoplasm (e.g., focal nodular hyper- uncertainty for clinical management. Further efforts to reduce
plasia), a tumor with malignant potential (e.g., hepatocellular this variability may come in the form of accreditation pro-
adenoma), or a primary malignancy, such as HCC. The tem- grams, similar to that required for breast imagers through the
poral pattern of tumor enhancement, the heterogenous ACR Mammography Accreditation Program and the federal
appearance of the tumor, the conspicuity of the tumor with Mammography Quality Standards Act. These studies are
respect to the adjacent liver parenchyma on different MRI important acknowledgements of the variability inherent in
sequences are a few of the imaging features used by interpret- diagnostic imaging that extend beyond the imaging techniques
ing radiologists as diagnostic clues. Although CT and MR themselves.
Chapter 14 Emerging techniques in diagnostic imaging 243
A B
FIGURE 14.3 Example of textural differences in liver parenchyma on computed tomography images from two patients (A and B). Sample with
magnified rectangular regions of interest demonstrate greater heterogeneity in the second patient (B) than the first patient (A), which can be quanti-
fied by texture parameters.
technologies to produce more rapid and higher-resolution scan- This acknowledgement is leading to the emergence of standard-
ning. Novel imaging devices, contrast agents, and functional ization in radiologic reports and image acquisition parameters,
techniques continue to emerge and provide improvements in as well as greater interest in the use of computer-based analyses
biologic insight for medical decision making. However, the and the development of radiomics.
variability inherent to imaging technique and diagnostic radi-
ologists themselves can affect the diagnostic performance of an
imaging study, and is increasingly the subject of investigation. References are available at expertconsult.com
Chapter 14 Emerging techniques in diagnostic imaging 244.e1
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2683, 2014.
Aerts HJ, et al: Decoding tumour phenotype by noninvasive imaging Lambin P, et al: Radiomics: extracting more information from medical
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Altenbernd J, et al: Dual-energy-CT of hypervascular liver lesions in 2012.
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Bahl G, et al: Noninvasive classification of hepatic fibrosis based on Macari M, et al: Dual-source dual-energy MDCT of pancreatic adeno-
texture parameters from double contrast-enhanced magnetic reso- carcinoma: initial observations with data generated at 80 kVp and at
nance images, J Magn Reson Imaging 36(5):1154–1161, 2012. simulated weighted-average 120 kVp, AJR Am J Roentgenol
Bankier AA, et al: Consensus interpretation in imaging research: is 194(1):W27–W32, 2010.
there a better way? Radiology 257(1):14–17, 2010. Mitchell DG, et al: LI-RADS (Liver Imaging Reporting and Data
Bruix J, Sherman M, D. American Association for the Study of Liver: System): summary, discussion, and consensus of the LI-RADS
Management of hepatocellular carcinoma: an update, Hepatology Management Working Group and future directions, Hepatology
53(3):1020–1022, 2011. 61(3):1056–1065, 2014.
Chapiro J, et al: Radiologic-pathologic analysis of contrast-enhanced Morgan DE: Dual-energy CT of the abdomen, Abdom Imaging
and diffusion-weighted MR imaging in patients with HCC after 39(1):108–134, 2014.
TACE: diagnostic accuracy of 3D quantitative image analysis, Radi- Padhani AR, et al: Diffusion-weighted magnetic resonance imaging as
ology 273(3):746–758, 2014. a cancer biomarker: consensus and recommendations, Neoplasia
Coursey CA, et al: Dual-energy multidetector CT: how does it work, 11(2):102–125, 2009.
what can it tell us, and when can we use it in abdominopelvic Rao SX, et al: Whole-liver CT texture analysis in colorectal cancer:
imaging? Radiographics 30(4):1037–1055, 2010. does the presence of liver metastases affect the texture of the remain-
Cruite I, et al: Imaging-based diagnostic systems for hepatocellular ing liver? United European Gastroenterol J 2(6):530–538, 2014.
carcinoma, AJR Am J Roentgenol 201(1):41–55, 2013. Robinson E, et al: Dual source dual energy MDCT: comparison
Cui Y, et al: Apparent diffusion coefficient: potential imaging bio- of 80 kVp and weighted average 120 kVp data for conspicuity of
marker for prediction and early detection of response to chemo- hypo-vascular liver metastases, Invest Radiol 45(7):413–418, 2010.
therapy in hepatic metastases, Radiology 248(3):894–900, 2008. Schraml C, et al: Diffusion-weighted MRI of advanced hepatocellular
Davenport MS, et al: Repeatability of diagnostic features and scoring carcinoma during sorafenib treatment: initial results, AJR Am J
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current status and future directions, Magn Reson Imaging Clin N Am Simpson AL, et al: Texture feature analysis for prediction of postoperative
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ecology, Radiology 269(1):8–15, 2013. Sirlin CB, et al: Consensus report from the 6th International forum for
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2007. Sourbron S, et al: Combined quantification of liver perfusion and func-
Heye T, et al: Dual-energy CT applications in the abdomen, AJR Am tion with dynamic gadoxetic acid-enhanced MR imaging, Radiology
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CHAPTER 15
Ultrasound of the liver, biliary tract, and pancreas
Jill S. Gluskin
ULTRASOUND BASICS visibility in patients with a higher body mass index (Choudhry
et al, 2000).
Ultrasound is a favored imaging modality because of its tre- Acoustic artifacts have been described, many of which are
mendous versatility, low cost, real-time capability, and portabil- clinically useful. Acoustic enhancement is an artifact that occurs
ity. Ultrasound is considered safe at clinical, diagnostic levels, when there is increased through-transmission of sound waves
with no confirmed harmful biologic effects on the operator or in fluid-containing structures, making tissue behind the fluid
patient. Use of Doppler ultrasound also allows assessment of appear artificially bright. This occurs because ultrasound units
blood flow dynamics. Despite these advantages, certain limita- adjust for a certain attenuation of sound with depth of travel
tions influence the applicability of ultrasound. Ultrasound such that there is erroneous amplification of echoes deep to
waves are unable to penetrate bone or air, which can obscure fluid-containing structures. Acoustic enhancement is useful to
lesions and limit the field of view. The quality of ultrasound characterize structures as cystic (Fig. 15.2). Acoustic shadow-
imaging and its interpretation are also operator dependent; ing occurs when a structure attenuates sound more rapidly than
ultrasound imaging and diagnosis is greatly influenced by skill surrounding tissues and casts a dark acoustic shadow beyond
and experience. the object. This occurs with strong reflectors, such as calcifica-
tions, or strong attenuators, such as dense tumors. Acoustic
Principles of Ultrasound Interpretation shadowing is a feature of gallstones and, in conjunction with
In diagnostic ultrasound applications, brief pulses of acoustic mobility, aids in distinction between gallstones and gallbladder
energy are emitted by the transducer, transmitted into the body, polyps (Fig. 15.3).
reflected from acoustic interfaces, and received by the trans- Some artifacts suggest the presence of structures that are
ducer. The average velocity of sound in soft tissues is 1540 m/s, not present. Reverberation artifact occurs when the ultra-
with reduced velocities in fat and increased velocities in bone. sound beam is repeatedly reflected back and forth between
The ultrasound unit uses precise timing to interpret and process two parallel highly reflective surfaces, such as walls of a fluid-
information included in the returning echoes, including fre- filled structure, producing artifactual echoes due to propaga-
quency, amplitude, and phase information. Ultrasound units tion assumption by the ultrasound processor. Reverberations
assume a uniform propagation velocity of sound to compute may produce the false appearance of echoes within fluid or
the depth of the interface reflecting the pulse and then to gener- make a cystic structure appear solid. Comet tail artifact is a
ate an imaging display. This pulse-echo principle allows infer- type of reverberation that occurs when two reflective inter-
ence of the position, nature, and motion of the interface from faces are closely spaced, such as within a punctate crystal,
which the received echo originated. The intensity of the producing posterior echoes that are parallel, evenly spaced
reflected echo is interpreted as varying shades of gray. echogenic bands with a triangular tapered shape. Comet tail
Different ultrasound transducers are optimized for specific artifact allows identification of surgical clips and is a feature of
frequencies. Lower-frequency transducers have poorer resolu- gallbladder adenomyomatosis (Fig. 15.4). Twinkle artifact is a
tion with greater depth of penetration, and thus are used color Doppler artifact that helps to detect and verify crystals
to image deeper structures such as abdominopelvic tissues. and calcifications, particularly if a calculus does not demon-
Higher-frequency transducers have better spatial resolution, strate acoustic shadowing. Twinkle artifact occurs posterior to
but higher-frequency sound attenuates rapidly and has poorer strong reflectors and appears as turbulent color Doppler flow
tissue penetration. Thus it is best used for superficial soft with a mix of red and blue pixels; however, spectral Doppler
tissues. The depth of the target structure is a major determinant tracing demonstrates noise. Additional artifacts have been
of the transducer frequency. described and are outside the scope of this chapter; the reader
is referred to specialized texts (Campbell et al, 2004; Feldman
Gray Scale Ultrasound Terminology and Artifacts et al, 2009; Rubens et al, 2006).
Echogenicity of tissue refers to the reflection or transmission of
ultrasound waves relative to surrounding tissues. Based on gray Doppler Ultrasound
scale imaging, a structure on the image display can be charac- Doppler ultrasound is used to identify and evaluate blood flow
terized as anechoic (uniformly black), hypoechoic (dark gray), in vessels based on the backscatter of blood cells. Echoes
or hyperechoic (light gray) (Fig. 15.1). returning from moving targets change in frequency compared
Tissue harmonic imaging is a gray scale ultrasound setting with the transmitted pulse. This change in frequency is propor-
that is useful in transabdominal ultrasound for depicting cystic tional to the velocity of the reflector relative to the transducer
lesions and lesions containing echogenic material such as air, and is defined by the Doppler effect. Doppler imaging allows
calcification, or fat. Harmonic imaging also improves lesion assessment of vessel patency, direction of blood flow, flow
245
246 PART 2 DIAGNOSTIC TECHNIQUES
hv
FIGURE 15.2. Benign hepatic cyst with a thin, smooth wall. Note the
posterior acoustic enhancement (arrows) that is a characteristic feature
of a cystic lesion.
0 19.6 .046
5
19.6
cm/s
.046 GB
PV
10
IVC
A B
15
.13
MHV
.13
PW:3MHz θ = 58°
.40
m/s
C.60
FIGURE 15.5. Doppler ultrasound of the liver. A, Color Doppler mode shows mean flow velocity and direction of flow toward or away from the
transducer, as indicated in the bar display at left of the image. The portal vein (PV) indicates hepatopetal flow. The inferior vena cava (IVC) shows
flow away from the transducer. The hepatic artery (arrowhead) has mixed signals due to high-velocity flow and aliasing. B, Power Doppler shows
amplitude of flow but not direction. It is useful for small vessels and low flow, as shown in this image of vessels in the gallbladder (GB) wall (arrow-
heads). C, Spectral Doppler shows flow pattern over time; when angle corrected, it can measure true velocity. A sample cursor is placed within the
vessel, as shown in this transverse image of the middle hepatic vein (MHV). Flow variations are due to changes in right atrial pressure.
gray scale and pulsed-wave Doppler analysis. Limitations color Doppler image. Arterial waveforms are characterized as
of color Doppler imaging include dependence on angle of high resistance by limited flow during diastole or low resistance
insonation, inability to display the entire Doppler spectrum in by continuous flow during diastole. At sites of stenosis, flow is
the image, and artifacts caused by aliasing and noise. not laminar; instead, flow becomes turbulent, and the spectral
Power (or amplitude) Doppler is a complementary tech- Doppler waveform reflects the red blood cells moving at varying
nique that displays total amplitude of the echo signal but not velocities. Instead of a narrow and well-defined tracing, spectral
flow direction. Power Doppler signal is more sensitive for flow broadening is seen at sites of stenosis with filling-in of the area
detection than color Doppler and is less dependent on the under the spectral waveform.
angle of insonation. It is not subject to aliasing and is less sen- The resistive index (RI) is a useful metric obtained with
sitive to noise. Power Doppler is most useful in showing spectral Doppler that reflects the strength of the inflow pressure
areas of low flow, depicting slow flow in an area of subtotal and the resistance of the downstream microvascular bed. This
occlusion, and demonstrating intralesional vascular patterns. calculation is performed on arterial spectral Doppler waveforms
Modern scanners have programmed settings that automatically and measures the difference between the peak systolic and end-
optimize the velocity scale and pulse repetition frequency to diastolic velocities. A lower-than-expected resistive index may
increase sensitivity for low flow, whether in color or power result from (1) decreased systolic velocity, indicating impaired
Doppler modes. inflow, or (2) increased diastolic flow due to disorganized or
In spectral Doppler, a sample volume cursor is placed within increased overall vascularity downstream. An elevated resistive
the target vessel and displays a waveform of the entire range of index near 1 implies nearly absent diastolic flow and high-
velocities during time, rather than the mean velocity as in a resistance downstream.
248 PART 2 DIAGNOSTIC TECHNIQUES
GB
4A 4B
2 3
PV
IVC
LH
A B
LONG RT
5
8
6
RHV
RK
7
C
FIGURE 15.6. Normal liver longitudinal ultrasound images. A, Left hepatic lobe. Segments are numbered. LH, Left hepatic vein. B, Left lobe
segment IV. Hepatic segments are numbered. GB, Gallbladder; IVC, inferior vena cava; PV, portal vein. C, Right lobe. Hepatic segments are num-
bered. RHV, Right hepatic vein; RK, right kidney.
TRANS TRANS
4
4 2 3
L
L
M
8 1
R
M
R
IVC
A B
TRANS
TRANS
4B
L
1 5 RA
R
IVC
A RP IVC
RK 6
C D
FIGURE 15.7. Transverse images of the liver. A, Transverse sonogram at the level of the hepatic veins. Hepatic segments are numbered. IVC,
inferior vena cava; L, left hepatic vein; M, middle hepatic vein; R, right hepatic vein. B, Transverse section of the left lobe at the level of the portal
vein bifurcation. L, Left portal vein; M, uppermost main portal vein; R, right portal vein;. C, Transverse image of the left portal vein (LPV) and right
portal vein (RPV) at the bifurcation. Segments IVB and I are indicated. A, Aorta; IVC,inferior vena cava; L, left hepatic vein; R, right hepatic vein; RK,
right kidney;. D, Transverse image of the inferior right lobe segments V and VI. IVC, inferior vena cava; K, Right kidney; RA, anterior right portal vein;
RP, posterior right portal vein.
anterior and posterior sectoral branches to be mistaken as the masses are benign (see Chapters 46, 75, and 90B). Hypoecho-
left and right portal veins. genicity is a feature of many malignancies. Hyperechoic masses
include both benign etiologies, such as hemangioma or focal
Hepatic Masses fat, as well as malignant hepatic neoplasms, such as hepatocel-
Liver Mass Detection and Characterization lular carcinoma (HCC) and metastases.
Echogenicity is the dominant factor determining lesion conspi- Coregistration of ultrasound, CT, and MRI images can
cuity on ultrasound. Markedly hypoechoic or hyperechoic facilitate lesion localization and intervention. Electromagnetic
lesions may be readily detected and characterized by ultra- sensors placed near the scanning area and sensors attached
sound, even when small (Eberhardt et al, 2003). Larger masses to the ultrasound probe allow tracking of transducer position
that have echogenicity similar to adjacent liver may be more and orientation. Anatomic landmarks are identified on initial
difficult to appreciate. Lesion size and body habitus are signifi- scanning, and with navigation software the landmarks are
cant factors that influence lesion detection (Eberhardt et al, coregistered with CT or MR images that have been down-
2003). On gray scale ultrasound, liver masses are differentiated loaded into the ultrasound unit (Ewertsen et al, 2008). While
by internal architecture and are described as cystic, hypoechoic, the ultrasound scan is performed in real time, CT or MR
or hyperechoic relative to the liver. The majority of cystic images are reconstructed into a similar orientation plane
250 PART 2 DIAGNOSTIC TECHNIQUES
ULTRASOUND MRI
FIGURE 15.8. Coregistration technology shows a transverse ultrasound image of the liver and a magnetic resonance image that have been coreg-
istered to display identical orientation and plane of section. (Courtesy GE Healthcare, Little Chalfont, United Kingdom.)
(Fig. 15.8). Images may be displayed side by side or in a tained enhancement and washout may occur in any phase.
blended, overlapped format. In a study of contrast-enhanced Healthy liver parenchyma enhances brightly during the PV
ultrasound fused in real time with CT, Jung and colleagues phase. Lesions enhance differently than background paren-
(2009) found that more lesions were identified with image chyma and thus will show increased conspicuity within the
fusion than with CT alone. Similar instrumentation allows enhanced parenchyma. Sustained enhancement, meaning that
global positioning system navigation for needle tracking and the lesion remains isoechoic or hyperechoic to the liver, is a
volume acquisition. favorable sign and associated with benignity. In the PV phase,
benign hemangiomas and focal nodular hyperplasia (FNH)
Role of Contrast-Enhanced Ultrasound in Evaluation of Focal have sustained enhancement equal to or greater than the liver
Liver Lesions (see Chapter 90). Washout during the PV phase, meaning the
Contrast-enhanced ultrasound (CEUS) has evolved as a lesion becomes hypoechoic compared with adjacent liver, is an
problem-solving tool for the characterization of focal liver unfavorable sign and correlated with malignant histology such
lesions due to its noninvasive real-time imaging capability. as HCC and metastases (Brannigan et al, 2004; Quaia et al,
Ultrasound contrast agents are intravenously injected micro- 2004; von Herbay et al, 2010; Wilson et al, 2009). These pat-
bubbles that are highly echogenic and oscillate in an ultrasound terns of enhancement can be used to differentiate benign from
field to enhance ultrasound signal in gray scale, color, and malignant focal hepatic lesions and will be described in the
spectral Doppler. Bubbles are capable of transpulmonary lesion subsections (Brannigan et al, 2004; Ding et al, 2005;
passage for left-side blood pool enhancement. Ultrasound con- Wilson & Burns, 2006).
trast agents are purely intravascular and do not diffuse into the CEUS improves both characterization of focal liver masses
interstitium. Multiple injections can be performed to assess and liver lesion detection, with improved ability to see a greater
different features of a lesion (i.e., kinetic curves) or assess dif- number and smaller lesions than on nonenhanced ultrasound.
ferent lesions. Ultrasound is sensitive to extremely low concen- Contrast agents also improve diagnostic accuracy and diagnos-
trations of contrast due to amplification of echoes from tic confidence (Albrecht et al, 2003; Albrecht et al, 2004;
resonating microbubbles in the blood pool. To obtain images Blomley et al, 1999; Bryant et al, 2004; Harvey et al, 2000;
of best quality, ultrasound scanning techniques should optimize Quaia et al, 2004; Strobel et al, 2009). Diagnostic performance
imaging settings, which can vary depending on the contrast of CEUS has been compared with that of CT and MRI, with
agent. Low mechanical index (LMI) settings are usually utilized similar accuracy in recognition of malignancy when performed
to minimize bubble destruction. with expert operators (Trillaud et al, 2009). There is high con-
Microbubbles stay in the circulation, allowing continuous cordance for lesion appearance in arterial phase imaging,
assessment as the contrast agent traverses the imaging field. and less so in the portal phase; this is usually attributed to
Vascular phases are divided into the arterial (10 to 40 ultrasound contrast agents remaining intravascular, compared
seconds), portal venous (PV) (40 to 120 seconds), and late with CT and MR contrast agents that may diffuse into the
parenchymal (>120 seconds) phases (Wilson & Burns, 2006). interstitium (Wilson & Burns, 2006). Ultrasound contrast
Observations are made of the liver and focal liver lesions, agents are not nephrotoxic, and impaired renal function is not
including wash-in, peak enhancement, and washout. Sus- a contraindication (Jang & Yu, 2009).
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 251
A B
FIGURE 15.10. Hemangiomas. A, Longitudinal sonogram of the right lobe shows a brightly echogenic hemangioma (arrow) with a circumscribed
border. B, Atypical hemangioma (arrow) with areas of internal heterogeneity, a result of fibrosis or myxomatous degeneration, and a thin echogenic
rim (arrowhead).
to the lesion (Buetow et al, 1996; Hussain et al, 2004). A key Malignant Liver Neoplasms
to ultrasound diagnosis of FNH is the characteristic Doppler
Hepatocellular Carcinoma
appearance of a central feeding artery with tortuous spoke-
wheel vascularity (Fig. 15.12). A central scar may be evident, Ultrasound is used to screen for hepatocellular carcinoma
yet is usually better depicted on CT, MRI, or CEUS. Classic (HCC) in high-risk patients (see Chapter 91) (Bruix & Sherman,
contrast enhancement of FNH in the arterial phase includes a 2011; European Association for the Study of Liver, 2012).
central stellate-enhancing artery. The lesion becomes homo- When used as a surveillance test, ultrasound has a sensitivity
geneous during late arterial phase and on PV phase there is ranging from 58% to 89% (Bolondi, 2003). A meta-analysis of
sustained enhancement, often with a hypoechoic central scar surveillance ultrasound for detecting early-stage HCC demon-
(Brannigan et al, 2004; Dietrich et al, 2005; Kamaya et al, strated an average sensitivity of 63%, with higher sensitivity for
2009; Quaia et al, 2004; Ungermann et al, 2007; Wilson ultrasound performed every 6 months than with annual surveil-
& Burns, 2006; Wilson & Burns, 2010). Persistent portal lance (Singal et al, 2009). Although ultrasound can detect 1- to
phase enhancement helps differentiate FNH from malignant 2-cm nodules in patients with chronic liver disease, there is a
liver lesions (Kim et al, 2009; von Herbay et al, 2010) high false-positive diagnosis, mostly due to high-grade dysplas-
(Fig. 15.13). tic nodules (Serste et al, 2012). A study comparing ultrasound
screened versus unscreened patients with cirrhosis showed
Hepatic Adenoma improved median survival (17 vs. 12 months) and improved
Hepatic adenomas (see Chapter 90A) have variable echo- survival rates at 1, 3, and 5 years for HCC arising in the
genicity but are often hyperechoic due to high lipid content. screened Child-Pugh class B patients but not in the class C
Internal hemorrhage within adenomas may produce cystic patients (Trevisani et al, 2007).
areas, and calcification may also be present (Grazioli et al, HCC may be solitary, multiple, or diffuse, and may also
2001). Intratumoral veins are often identified on Doppler extend into the bile ducts and cause biliary obstruction or
imaging (Bartolozzi et al, 1997; Golli et al, 1994). On CEUS hemobilia (Kojiro et al, 1982). Small HCC tumors (< 5 cm)
arterial phase, adenomas characteristically show diffuse or cen- are often hypoechoic but may be hyperechoic from fatty meta-
tripetal hypervascular enhancement from dysmorphic arteries. morphosis (Caturelli et al, 2001; Choi et al, 1993). Larger
PV phase appearance is variable, either showing equal enhance- HCC are often heterogeneous because of liquefaction necrosis
ment or soft washout relative to the liver (Bartolotta et al, 2007; and fibrosis (Tanaka et al, 1983). Sonographic depiction of
Kim et al, 2006; Kim et al, 2008; Ricci et al, 2008; Wilson & HCC may be limited in the setting of severe cirrhosis (Bennett
Burns, 2010). et al, 2002).
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 253
RT RT
A B
RT
C
FIGURE 15.11. Giant atypical hemangioma. A, Baseline gray scale image demonstrates a mainly isoechoic left lobe mass (arrows) found in a
patient with abdominal pain. B, Contrast-enhanced ultrasound in early arterial phase (19 seconds) demonstrates that the mass has globular peripheral
enhancement but no central enhancement. C, In the portal venous phase (56 seconds), the mass demonstrates more marked peripheral globular
enhancement consistent with hemangioma. (Courtesy Paul S. Sidhu, King’s College Hospital, London.)
254 PART 2 DIAGNOSTIC TECHNIQUES
A B
FIGURE 15.12. Focal nodular hyperplasia (FNH). A, Gray scale image of a hypoechoic FNH. FNH lesions are often subtle. The echogenic hepatic
parenchyma consistent with steatosis increases conspicuity of the FNH in this patient. B, Color Doppler image demonstrating a tortous vessel with
spoke-wheel pattern that demonstrated arterial waveform on spectral Doppler.
HCC has a propensity for venous involvement with throm- et al, 1999; Smith et al, 2008). Regional lymphadenopathy is
bosis of the portal or hepatic veins (Fig. 15.14). Both acute common.
bland thrombus and tumor thrombus can expand the portal
vein, so vein expansion is not a distinguishing feature. Spectral Liver Metastases
Doppler interrogation of bland thrombus will only show noise. Sonographic appearance of metastases may vary according to
Spectral Doppler of tumor thrombus may reveal hepatofugal the primary malignancy (see Chapters 92, 93, and 94). The
arterial flow, a pathognomonic finding (Giorgio et al, 2004; most common appearance of metastases is hypoechoic lesions
Lencioni et al, 1995; Shah et al, 2007; Tanaka et al, 1993). or lesions with peripheral hypoechoic halos (Fig. 15.16). The
CEUS offers diagnostic advantage in the detection of malignant hypoechoic halo corresponds to fibrosis, compressed sinusoids,
portal vein and hepatic vein thrombosis compared with and tumor neovascularity surrounding the metastatic deposit
conventional gray scale, color Doppler, and spectral Doppler (Kruskal et al, 2000; Wernecke et al, 1992). Hypoechoic
ultrasound (Rossi et al, 2006). metastases are commonly due to metastatic breast, lung, pan-
CEUS improves HCC characterization and is highly con- creatic, gastric, and esophageal carcinoma. In addition to
cordant with CT findings, but contrast-enhanced ultrasound is metastases, lymphoma and HCC should be considered in the
best at identifying lesions greater than 2 cm (Giorgio et al, differential diagnosis of hypoechoic lesions or lesions with
2004; Inoue et al, 2009; Jang et al, 2009; Quaia et al, 2007). hypoechoic halos. Lymphoma is hypoechoic because of its
On arterial phase, HCC typically shows dysmorphic arteries uniform cellularity and may appear as diffusely infiltrative or as
and is hypervascular, sometimes isovascular. HCC classically multiple well-defined hypoechoic lesions; this latter pattern is
demonstrates a washout appearance on PV phase, yet some- more common in non-Hodgkin lymphoma or acquired immu-
times demonstrates delayed washout or no washout. Observa- nodeficiency syndrome (AIDS)-related lymphoma (Townsend
tion during the portal phase should be extended as long as et al, 1989).
300 s, because as many as 22% of HCCs have delayed washout Echogenic metastases tend to arise from HCC or gastroin-
(Jang et al, 2007) (Fig. 15.15). testinal tract malignancies. Vascular metastases are also typi-
Fibrolamellar HCC, a variant of HCC with better prognosis, cally hyperechoic, such as those from renal cell carcinoma, islet
characteristically presents as a large solitary mass in an adoles- cell tumors, carcinoids, and choriocarcinoma (Marchal et al,
cent or young adult without underlying liver disease. On 1985; Rubaltelli et al, 1980; Tanaka et al, 1990). Calcified
ultrasound, a fibrolamellar HCC is well defined, lobulated, and metastases may be found with mucinous adenocarcinoma of
with variable echogenicity. Calcifications may be present the colon as well as other primaries. When metastases are dif-
(Chung et al, 2009). A central scar may be visible on gray scale fusely infiltrative, such as in breast or lung carcinoma, it can
ultrasound in one third to two thirds of patients, but scars are be difficult to detect individual lesions. Diffuse hepatic metas-
better seen with contrast-enhanced ultrasound (McLarney tases are especially prone to pseudocirrhosis; treated or
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 255
A B
C D
FIGURE 15.13. Focal nodular hyperplasia (FNH) on contrast-enhanced ultrasound. A, An isoechoic mass (arrows) is seen in the left hepatic lobe
on gray scale imaging. B, Twelve seconds after contrast injection, the FNH (arrows) shows enhancement in a central scar and a characteristic spoke-
wheel vascular pattern. C, The FNH (arrows) enhances brightly at 18 seconds. D, Five minutes after contrast injection, the FNH (arrows) is still
enhanced and is echogenic relative to the liver. (Courtesy GE Healthcare, Little Chalfont, United Kingdom.)
untreated metastases can elicit a fibrotic response mimicking that have diminished in size or changed in echogenicity as a
cirrhosis (Fennessy et al, 2004; Young et al, 1994). result of chemotherapy.
Cystic hepatic metastases are seen in ovarian and pancreatic
cystadenocarcinomas, as well as mucinous colon carcinomas. Sonography of Diffuse Liver Disease
Ovarian cystic metastases are characteristically located periph- Fatty Liver Disease
erally due to tumor implants on the hepatic surface. Metastases Fatty liver is commonly encountered incidentally on sonograms
undergoing central necrosis, such as sarcomas, also may appear of the liver and in patients referred for imaging evaluation of
cystic, yet thick complex walls and internal contents are usually abnormal liver function tests (see Chapters 71 and 100). Fat
evident and distinguish the metastasis from a simple cyst. deposition within hepatocytes results in increased echogenicity
CEUS improves detection of individual metastases com- of the liver, decreased acoustic penetration, and loss of the
pared with gray scale ultrasound and in some cases may reveal echogenic borders of portal vessels (Fig. 15.18A and B). Sono-
more lesions than are evident on CT (Fig. 15.17) (Albrecht graphic diagnosis of fatty liver is challenging because echo-
et al, 2003). Liver metastases are frequently detected sono- genicity is not a quantitative measure. Appearance will vary
graphically, yet CT is the preferred modality to determine depending on whether fat deposition is focal or generalized and
extent of disease, number of hepatic lesions, and extrahepatic on the presence of associated liver disease. Although unproven,
disease. Response to therapy is also better evaluated by CT and some investigators advocate comparing the relative echogenicity
MRI because treatment-related fatty liver may obscure lesions between the liver and right kidney with that between the spleen
256 PART 2 DIAGNOSTIC TECHNIQUES
TR LIVER
Long PV
RT
A B
Long PV .20
.20
PV
C D
FIGURE 15.14. Hepatocellular carcinoma (HCC) with portal vein thrombosis. A, Transverse image shows a hypoechoic HCC in the right hepatic
lobe (arrows). B, Transverse image of the main portal vein reveals only a trickle of blood flow (arrow). The lumen is nearly filled with echogenic
thrombus. C, Longitudinal image of the main portal vein shows the extent of thrombus (arrow). D, Color Doppler image of the main portal vein
confirms arterial flow (arrow) within the hypoechoic thrombus; this is pathognomonic for tumor thrombus. PV, Portal vein.
and left kidney. Because the normal spleen is more echogenic also be lobar, rounded and masslike, or perivascular in distribu-
than liver, if the difference in echogenicity between the liver and tion. In the latter two cases, MRI is useful to confirm that the
right kidney is greater than the difference between the spleen focal abnormality truly represents fat deposition and not a mass
and left kidney, then the liver is abnormally echogenic (Tchel- lesion. Focal fat deposition should not have mass effect, and
epi et al., 2002). therefore intrahepatic vessels should traverse these areas of
In fatty liver disease, the liver contour remains smooth. increased echogenicity without displacement. However, this
Hepatomegaly may be present. Steatosis degrades the quality finding is not entirely specific, because occasionally some mass
of sonographic evaluation of the hepatic parenchyma because lesions may likewise fail to displace vessels.
of decreased acoustic penetration and focal lesions may escape Certain regions may be spared within a diffusely fatty liver
detection. In addition, lesions that typically appear echogenic (Fig. 15.18C). These are typically areas of nonportal venous
against a background of normal liver, such as hemangiomas, inflow, such as around the gallbladder (cystic veins) and in the
may appear hypoechoic in the fatty liver. region of the porta hepatis. Focal fatty sparing appears as a
Fat deposition in the liver may be diffuse and uniform, hypoechoic region with geographic margins and segmental dis-
patchy, or focal. Areas of focal fat deposition are commonly tribution, usually located in segment IV anterior to the portal
wedge shaped and echogenic and occur in characteristic loca- bifurcation or adjacent to the gallbladder, and leaves vessels
tions, such as along the ventral surface of segment IV and undisturbed. These distinctive features allow a more confident
adjacent to the falciform ligament. Focal fat deposition may diagnosis.
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 257
ivc
A B
C D
FIGURE 15.15. Hepatocellular carcinoma. A, Transverse gray scale image reveals a large hepatocellular carcinoma (HCC); the mass (m) splays
the hepatic veins. ivc, Inferior vena cava. B, Contrast-enhanced ultrasound, early arterial portal venous phase, shows dysmorphic vessels in the
hypervascular hepatocellular carcinoma (HCC) (arrows). C, Peak arterial portal phase image shows brightly enhancing HCC. D, The HCC (arrows)
has very slow and weak washout, not shown until more than 4 minutes from the end of the saline flush. (Courtesy Stephanie R. Wilson.)
Viral Hepatitis appearance known as the “starry night” liver for the striking
Most imaging modalities, including sonography, are neither prominence of the periportal echoes against the abnormally
sensitive nor specific for the diagnosis of acute hepatitis. Defini- dark background liver (Mortele & Ros, 2001; Tchelepi et al,
tive diagnosis of hepatitis (see Chapter 70) is usually based on 2002). Hepatitis may also produce secondary changes in the
clinical and laboratory findings, with imaging useful for exclud- gallbladder, with irregular lamellated thickening of the gallblad-
ing other diagnoses (Mortele & Ros, 2001). The most common der wall, especially in hepatitis A (Tchelepi et al, 2002).
sonographic abnormality in hepatitis is hepatomegaly. Peripor-
tal edema may be appreciated sonographically, but it is better Cirrhosis
seen on CT or MRI. Occasionally, sonography may demon- Sonography is neither sensitive nor specific for the diagnosis of
strate very low hepatic parenchymal echogenicity, producing an cirrhosis, yet certain findings may suggest its presence. Surface
258 PART 2 DIAGNOSTIC TECHNIQUES
A B
C
FIGURE 15.17. Hepatic metastases evaluated with contrast-enhanced ultrasound. A, Gray scale image reveals a hypoechoic mass (arrow) repre-
senting a metastasis. B, In the arterial portal phase after contrast injection, the liver metastases (arrows) have peripheral rim enhancement, and an
additional lesion is now evident. C, The metastases (arrows) show complete washout of contrast in less than a minute; image taken at 54 seconds.
(Courtesy Stephanie R. Wilson.)
Hepatic arterial waveform is a low-resistance waveform with hypoechoic, isoechoic, or hyperechoic. The portal vein diam-
a brisk systolic upstroke and continuous antegrade diastolic eter may be normal or expanded. Doppler imaging may show
flow, with expected RI of 0.55 to 0.7. absent color flow or areas in the vessel that do not fill with color
completely. Tumor thrombus may be distinguished from bland
Portal Vein Thrombosis and Cavernous Transformation thrombus by the presence of arterial waveforms within the
Portal vein thrombosis may be caused by hypercoagulable thrombus, a finding that is specific, but not very sensitive (Rossi
states, inflammatory diseases, sepsis, myeloproliferative disor- et al, 2006) (see Fig. 15.14). CEUS improves both detection
ders, neoplasms, and most commonly portal hypertension and characterization of thrombi in the portal system (Rossi
(Rossi et al, 2006) (Fig. 15.19). Gray scale findings include et al, 2006). Very slow flow in the PV system may result in a
solid material within the portal vein lumen that may be anechoic, false-positive sonographic diagnosis of portal vein thrombus.
260 PART 2 DIAGNOSTIC TECHNIQUES
gb
A B
pv
ivc
C D
FIGURE 15.18. Diffuse liver disease. A, Hepatic steatosis, longitudinal right lobe. Hepatic parenchyma of fatty liver is very echogenic relative to the
right kidney. B, Severe hepatic steatosis produces marked attenuation of sound, such that the posterior liver is poorly visualized. gb, Gallbladder.
C, Focal sparing in an otherwise fatty liver. Transverse image shows a hypoechoic region (arrow) in segment IV anterior to the porta. ivc, Inferior vena
cava; pv, portal vein. D, Cirrhosis. The liver is small with coarsened echogenicity and a nodular surface (arrows). a, Aorta.
CT or MRI may be used for confirmation of portal vein throm- segments I and IV and atrophy of the left lateral segment and/
bus, especially in the evaluation of patients prior to liver or periphery of the liver (Tublin et al, 2008; Vilgrain, 2001;
transplantation. Vilgrain et al, 2006).
In the setting of long-standing portal vein thrombosis, a
collateral hepatopetal venous circulation develops in the hepatic Budd-Chiari Syndrome and Venoocclusive Disease
hilum through recanalization of the thrombus and enlargement Budd-Chiari is a group of disorders characterized by hepatic
of collateral veins (de Groen et al, 1999). This phenomenon is venous outflow obstruction, with obstruction at the level of the
known as cavernous transformation of the portal vein, and it IVC, hepatic veins, or hepatic venules (see Chapter 87).
manifests on sonography as numerous serpiginous vessels in the Hepatic venoocclusive disease is rare and involves diffuse nar-
periportal region and nonvisualization of the main portal trunk rowing at the venule level. Etiologies of Budd-Chiari are varied,
(Fig. 15.20A). Overall flow in these collateral vessels is toward including hematologic abnormalities causing venous thrombus,
the liver (hepatopetal). In patients with cirrhosis, spectral venous obstruction by intrahepatic tumor, venous webs, or
Doppler should be used to confirm the venous character of the injury to hepatic venules from irradiation and chemotherapy
varicosities because enlarged and tortuous hepatic arteries may (Cura et al, 2009).
have a similar appearance on color Doppler. In chronic portal Venous obstruction and ascites are key features of Budd-
vein thrombosis and cavernous transformation, the morphology Chiari syndrome in the acute phase. The liver becomes enlarged
of the liver may become distorted, with enlargement of and heterogeneous in echogenicity. Imaging of the hepatic vein
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 261
A B
FIGURE 15.19. Left portal vein thrombus due to portal hypertension in this patient with cirrhosis. A, Nonocclusive echogenic material in the left
portal vein on gray scale ultrasound image. B, Correlative finding on contrast-enhanced computed tomography.
confluence may show narrowed hepatic veins, tumor encase- liver, such arterial collateral vessels are initially absent, requir-
ment, intraluminal thrombus, or absence of normal hepatic ing at least 2 weeks to develop. Therefore, in the early post-
venous structures. On color Doppler, hepatic vein flow altera- transplant period, bile ducts are supplied solely by the hepatic
tions and venous collaterals are readily evident. Spectral artery.
Doppler analysis may show flattened waveforms from more The frequency of early hepatic arterial thrombosis is higher
central obstruction or areas of high-velocity flow due to stenosis in children than adults and has been decreasing with improve-
(Grant et al, 1989; Ralls et al, 1992) (Fig. 15.20B-D). In the ments in perioperative care. A review of 71 clinical studies of
more chronic phase, intrahepatic and extrahepatic venous col- early hepatic arterial thrombosis published between 1990 and
laterals develop, and regenerating nodules are also present 2007 found an overall incidence of 4.4%, with a rate of 8.3%
(Brancatelli et al, 2002; Brancatelli et al, 2007). The caudate in children and 2.9% in adults (Bekker et al, 2009). Causes of
lobe is typically spared because of its unique hepatic venous hepatic arterial thrombosis include technical anatomic causes
drainage into the IVC; intrahepatic venous collaterals will form (kinking, stenotic anastomosis) and nonanatomic causes, such
to drain through the caudate lobe, resulting in caudate hyper- as immunologic factors, clotting abnormalities, and infections,
trophy (Bargallo et al, 2003). Approximately 25% of patients particularly cytomegalovirus (Pastacaldi et al, 2001). The
with Budd-Chiari syndrome also have portal vein thrombosis median time to detection of hepatic arterial thrombosis is
(Mahmoud et al, 1997). approximately 7 days (Bekker et al, 2009). Most cases of
hepatic artery thrombosis are identified through routine sono-
Liver Transplant Evaluation graphic surveillance, when patients are either asymptomatic or
Ultrasound is the modality of choice for evaluation of liver have elevation of liver function tests. Bile duct ischemia as a
transplants. Early detection of transplant complications is result of hepatic artery thrombosis results in recurrent cholan-
essential for preservation of graft function; therefore sono- gitis, intrahepatic abscess, bile duct stenosis, or bile leak. Ful-
graphic expertise must be readily available in any transplant minant hepatic necrosis is uncommon (Garcia-Criado et al,
setting. The frequency of sonographic surveillance varies by 2002).
institution, although initial assessment of vascular patency is On sonographic evaluation, the normal hepatic artery wave-
generally performed within 1 day following transplant (see form shows a brisk systolic upstroke and continuous diastolic
Chapters 113 and 120). flow with a resistive index between 0.5 and 0.8. The normal
The overall incidence of vascular complications following systolic acceleration time, measured from end diastole to the
liver transplantation is approximately 9% (Caiado et al, 2007; first systolic peak, is usually less than 0.08 s. Hepatic artery
Quiroga et al, 2001), and Doppler ultrasound is the mainstay thrombosis is diagnosed on ultrasound when flow is absent in
of evaluation. Hepatic arterial thrombosis is a serious complica- the proper hepatic artery and intrahepatic arteries on color and
tion because it impairs the viability of the bile ducts within the spectral Doppler.
transplanted liver. In the native liver, arterial collaterals, primar- Stenosis of the hepatic artery occurs in an estimated 5% to
ily from the phrenic arteries, can sustain bile ducts following 11% of transplant recipients and usually develops at the anas-
hepatic artery ligation (Bekker et al, 2009). In the transplanted tomotic site within 3 months of transplantation (Caiado et al,
262 PART 2 DIAGNOSTIC TECHNIQUES
gb
A B
TRANS
ivc
PW:3MHz θ = 55°
.60
m/s
C D .60
FIGURE 15.20. Vascular disorders of the liver. A, Cavernous transformation of the portal vein. The portal supply has a serpiginous appearance
because of numerous collateral vessels. gb, Gallbladder. B, Outflow obstruction in a patient with venoocclusive disease. On transverse view, the
intrahepatic inferior vena cava (arrow) is markedly narrowed, and portions of the right hepatic vein (arrowhead) are obliterated. C, The middle hepatic
vein (arrows) is narrowed. ivc, Inferior vena cava. D, The middle hepatic vein shows flattened Doppler flow consistent with partial venous
obstruction.
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 263
2007). If the anastomotic site can be directly visualized, color than 0.5 and a prolonged acceleration time in excess of 0.08 s
Doppler may show focal aliasing and spectral Doppler will (Caiado et al, 2007; Tamsel et al, 2007). Occasionally, a tardus-
demonstrate elevated velocities. More commonly, the hepatic parvus waveform may be present in the intrahepatic arteries in
artery can only be visualized in the porta hepatis downstream the setting of chronic hepatic artery thrombosis. This implies
of the anastomosis. With anastomotic stenosis, there will be a that a collateral arterial supply has developed, and its damp-
tardus-parvus waveform in the downstream proper hepatic and ened flow resembles the waveform seen in hepatic artery ste-
intrahepatic arteries (Fig. 15.21). This waveform is character- nosis (Caiado et al, 2007). Therefore both the main hepatic
ized by a blunted, delayed peak systolic velocity with RI less artery in the porta hepatis and the intrahepatic right and left
.20
LIVER
.20 artifact
V1 = 0.233m/s
V2 = 0.138m/s
Rl = 0.41 V = –0.27m/s
S/D = 1.69 ±Mean = –0.13m/s
m/s
A.30 B
.51
IVC HV ANAST
.51
PW:2.5MHz
.50
m/s
1.0
C
FIGURE 15.21. Vascular complications after liver transplantation. A, Left hepatic artery (LHA) tardus-parvus waveform indicates hepatic artery
stenosis or thrombosis. The waveform has blunted arterial upstroke and high diastolic flow with resistive index less than 0.5. B, Duplex spectral
Doppler image of the right hepatic vein (RHV) in a patient after orthotopic liver transplant with piggyback anastomosis (ANAST) shows monophasic
flattened flow, indicating anastomotic stricture. C, Duplex Doppler with the sample placed over the area of flow aliasing shows high-velocity turbulent
flow (arrows) at the stenotic venous anastomosis, localizing the area of focal narrowing. IVC, Inferior vena cava.
264 PART 2 DIAGNOSTIC TECHNIQUES
hepatic arteries must be interrogated on all Doppler studies of The common bile duct is best seen from the right intercos-
transplanted livers. In the early postoperative period, the tal approach with the patient in the left lateral decubitus posi-
hepatic artery RI may be elevated, a finding sometimes associ- tion, which allows use of the liver or gallbladder as an
ated with an older donor age or prolonged cold ischemia time acoustic window. However, the left lateral decubitus position
(Caiado et al, 2007; Shaw et al, 2003). brings bowel gas to the right side and may obscure the distal
On the venous side, portal and hepatic vein transplant duct. Alternatively, upright or right lateral decubitus positions
complications are relatively rare (see Fig. 15.21). Portal vein fill the stomach with fluid, improving visualization of the
stenosis and thrombosis each have an incidence of approxi- distal common bile duct. The right and left hepatic ducts lie
mately 1% to 2% (Caiado et al, 2007; Tamsel et al, 2007). anterior to the portal vein confluence and are best visualized
Portal vein thrombosis may result from technical problems at on transverse subcostal ultrasound images. Second-order
surgery, prior portal vein thrombosis, increased downstream branches may also be seen adjacent to the segmental portal
resistance (e.g., hepatic venous outflow impairment), sluggish vein branches.
portal vein inflow, or hypercoagulable states. Diagnosis of Several techniques help enhance visualization of the biliary
portal vein thrombosis is made when flow is absent in the ducts. Tissue harmonic imaging improves contrast and reduces
various Doppler modes or an echogenic thrombus is visual- reverberation and side lobe artifacts when evaluating biliary
ized on gray scale ultrasound. Suspected thrombosis may ducts (Ortega et al, 2001). Use of compression and optimal
be confirmed with another imaging modality, such as CT technical parameters of frequency, gain, filter, and scale will
or MRI. produce the most favorable ultrasound images.
A B
C
FIGURE 15.22. Gallbladder. A, Normal longitudinal gallbladder image with visualization of the gallbladder neck. B, Thickened gallbladder wall
(arrows) resulting from inflammation. Sludge (arrowheads) layers posteriorly. C, Gallbladder polyps (arrows). Note the lack of acoustic shadowing.
90% to 94% for the diagnosis (Harvey & Miller, 1999; Ralls greater than 15,000 cells/mL (Fagan et al, 2003). Ultrasound
et al, 1985). Ultrasound findings of acute calculous cholecysti- features of gangrenous cholecystitis include floating intralumi-
tis include gallstones, gallbladder wall thickening greater than nal membranes from sloughed mucosa, shadowing foci from
3 mm, pericholecystic fluid, and a positive sonographic Murphy air in the gallbladder wall, disrupted gallbladder wall, and peri-
sign. Gallstones, wall thickening, and Murphy sign together cholecystic abscess formation (Jeffrey et al, 1983).
have a positive predictive value of 92% to 95% (Ralls et al, Gallbladder wall thickening is nonspecific and may be seen
1985; Smith et al, 2009; Teefey et al, 1991) (Fig. 15.24). in a wide range of gallbladder disease and extracholecystic
In emphysematous cholecystitis, echogenic air bubbles in pathologic conditions. Diffuse gallbladder wall thickening in
the gallbladder wall produce reverberation artifact. In this patients without primary gallbladder wall disease occurs in a
entity, there is possibility of gallbladder necrosis, gangrene, and variety of systemic processes, such as hypoalbuminemia, con-
perforation. Gangrenous cholecystitis occurs more often in gestive heart failure, hepatitis, and pancreatitis (van Breda
patients with diabetes mellitus or a white blood cell count Vriesman et al, 2007).
266 PART 2 DIAGNOSTIC TECHNIQUES
liver
3 4
2
1
RK
A B
W
E
m
C D
FIGURE 15.23. Gallstones and gallbladder carcinoma. A, Longitudinal view of the gallbladder shows layering stones (numbered) with acoustic
shadow. A small amount of sludge (arrow) is also seen in the dependent portion of the gallbladder. B, Views of the fundus show focal mural thicken-
ing (arrows) suspicious for tumor. RK, Right kidney. C, Flow is seen within the mass (m) on color Doppler imaging. D, Gallstones fill the gallbladder
lumen, producing a Wall-Echo-Shadow (WES) sign from the anterior gallbladder wall, the echogenic anterior surface of gallstones, and posterior
acoustic shadowing by the gallstones.
Hyperplastic Cholecystoses and Gallbladder Polyps thickening is most common in the fundus; when it occurs in
Hyperplastic cholecystoses (see Chapter 49), such as choles- the gallbladder body, there is annular constriction producing
terolosis and adenomyomatosis, can cause focal or polypoid an hourglass-shaped gallbladder. Masslike areas of adenomyo-
gallbladder wall thickening. Cholesterolosis results from abnor- matosis are called adenomyomas.
mal cholesterol deposits in the gallbladder wall creating wall The majority of incidentally detected polypoid gallbladder
irregularities or polypoid intraluminal masses. Cholesterolosis lesions are nonneoplastic and represent cholesterol polyps or
usually presents as multiple small (1 to 10 mm) nonshadowing inflammatory polyps (Corwin et al, 2011). Rarely, these may
polyps arising from the nondependent wall with echogenic be neoplastic, such as adenomas, and malignant transformation
speckles and lobular contour (see Fig. 15.22C). Cholesterol to adenocarcinoma is a concern. Adenomas tend to be solitary
polyps are benign with no malignant potential (Ito et al, 2009; and uniformly hyperechoic yet become more heterogeneous as
Levy et al, 2002; Terzi et al, 2000). Adenomyomatosis is a they increase in size and may either be pedunculated or sessile.
benign hyperplastic cholecystosis with no malignant potential Thickening of the gallbladder wall adjacent to an adenoma may
that results from hyperplasia of both the mucosa and muscula- suggest malignancy.
ris propria of the gallbladder wall. Intramural diverticula are In patients with polypoid gallbladder lesions, risk factors for
called Rokitansky-Aschoff sinuses, which trap bile that accumu- malignancy include age of patient (> 60 years of age), coexis-
lates cholesterol crystals appearing as cystic spaces in a thick- tence of gallstones, and size of the polypoid lesion (>10 mm in
ened gallbladder wall with a characteristic comet tail artifact diameter) (Terzi et al, 2000). The prevalence of malignancy in
(Levy et al, 2002) (see Fig. 15.4). The gallbladder wall thicken- polyps greater than 10 mm ranges from 37% to 88% (Ishikawa
ing in adenomyomatosis may be focal or diffuse. Focal wall et al, 1989; Koga et al, 1988). Surgical consultation for
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 267
A B
FIGURE 15.24. Acute cholecystitis. A, Longitudinal sonogram shows a distended gallbladder with thickened irregular wall (arrows) and layering
sludge (arrowheads). B, Computed tomographic scan shows gallbladder wall thickening (arrows).
A B
FIGURE 15.25. Gallbladder carcinoma. A, Gray scale longitudinal image of the gallbladder shows a solid irregular mass in the fundus. B, Transverse
color Doppler image of this lesion demonstrates internal vascularity, suspicious for tumor. Pathology demonstrated gallbladder adenocarcinoma.
asymptomatic polyps greater than 10 mm and for symptomatic into the adjacent liver (Wibbenmeyer et al, 1995) (Fig. 15.25).
gallbladder polyps irrespective of size has been proposed (Wiles When the mass occupies the gallbladder lumen, it can result in
et al, 2014). Often, asymptomatic gallbladder polyps smaller a displaced or “trapped” stone that is fixed in position due to
than 10 mm are followed sonographically, and those smaller intraluminal tumor. Secondary signs of gallbladder cancer
than 6 mm may not be followed or followed at extended inter- include discontinuity of the echogenic mucosal lining, absence
vals (Pedersen et al, 2012). of echogenic specks seen in cholesterol crystals, and high-
velocity arterial flow greater than 60 cm/s. Selective mucosal
Gallbladder Carcinoma calcification of the gallbladder wall is significantly associated
Carcinoma of the gallbladder (see Chapter 49) may appear as with gallbladder cancer, whereas diffuse intramural calcifica-
a sessile or polypoid mass, a thickened gallbladder wall, or tion is not (Stephen & Berger, 2001). Gallbladder carcinoma
infiltrative mass that fills the gallbladder lumen and extends often contiguously extends into hepatic segments IVB and V,
268 PART 2 DIAGNOSTIC TECHNIQUES
or into the hepatic hilum, possibly directly involving the main be no change or only a slight increase in diameter after chole-
bile duct to cause secondary biliary obstruction. Adjacent ade- cystectomy (Abbitt, 2002; Feng & Song, 1995; Mueller et al,
nopathy may also be present. Ultrasound performs well for 1981 ). The effect of age is controversial, yet even in the elderly
detection of the gallbladder primary and local tumor spread, the common duct diameter usually does not exceed 7 mm
but CT is necessary to more accurately determine resectability, (Bachar et al, 2003; Horrow et al, 2001; Perret et al, 2000).
distant disease spread, and peritoneal metastases (Bach et al, Variable threshold values in literature are due to differences in
1998). sample size, patient population, and control of confounding
In the era of laparoscopic surgery for gallstone disease, it is variables.
important to assess the gallbladder carefully on preoperative Intrahepatic biliary dilatation is less well defined. Intrahe-
ultrasound to exclude occult gallbladder cancer and to plan an patic ducts should measure greater than 2 mm or greater than
appropriate surgical approach. Approximately 47% of gallblad- 40% of the adjacent portal vein to be considered dilated. The
der carcinomas are detected incidentally at laparoscopic chole- “double-track” sign is caused by dilated bile ducts parallel to
cystectomy (Duffy et al, 2008). For these patients, reexploration the portal vein branches (Fig. 15.26). Intrahepatic bile duct
with definitive resection and reexcision of laparoscopic port dilatation is best appreciated in transverse images of the left
sites is recommended (D’Angelica et al, 2009; Duffy et al, hepatic lobe. The pattern of bile duct dilatation should be
2008; Winston et al, 1999). assessed to determine whether it is symmetric in both lobes or
localized to one portion of the liver. To determine the level of
Biliary Ducts obstruction, the left and right main ducts are followed trans-
Choledochal Cysts versely to their junction, and transverse views of the common
Choledochal cysts (see Chapter 46) are classified according to hepatic and common bile ducts are obtained. With this approach
the location of the dilated ductal segment: type I is fusiform it is possible to differentiate intrahepatic from extrahepatic
extrahepatic duct dilatation, type II is diverticulum of the extra- obstruction, and usually the etiology of the obstruction can be
hepatic duct, type III is a choledochocele from a dilated termi- determined (Fig. 15.27).
nal portion of the common bile duct, type IV is multifocal Bile duct dilatation is most often caused by an obstructive
dilatation, and type V is cystic dilatation of the intrahepatic bile process. Bile duct calculi appear as intraluminal filling defects
ducts that is synonymous with Caroli disease (Todani et al, (see Fig. 15.26B), which may be intrahepatic or extrahepatic.
1977). For Caroli disease, the cysts may be large, and the con- Calculi may form or reflux into the intrahepatic ducts, and
nection with the bile duct is not always evident sonographically. small calculi can be mistaken for air (see Chapters 36 and 37).
On imaging, it is important to demonstrate the connection with Because there is little bile surrounding the ductal calculi, and
the bile ducts to differentiate this condition from polycystic because the stones may be small, acoustic shadowing may not
disease. Arterial signals from the fibrovascular bundle at the always be elicited. Transabdominal ultrasound remains opera-
margin of the saccules may also aid in diagnosis (Miller et al, tor dependent, but, when performed by experienced examiners,
1995). has high diagnostic accuracy for choledocholithiasis (Rickes
et al, 2006). Debris or thick bile within the ducts may cause
Biliary Obstruction internal echoes within ducts and fluid levels, but debris does
Measurement of the extrahepatic duct is usually performed not shadow and will shift with positional variation. Hemobilia
near the crossing of the hepatic artery, with measurement of may layer or appear echogenic and masslike if the clot is orga-
the lumen from inner wall to inner wall. The common bile duct nized (see Chapter 125). Intraductal tumor from colorectal
lumen normally measures 6 mm in diameter or less. There may metastases or HCC may also appear as an intraductal mass.
gb
cbd
A B
FIGURE 15.26. Biliary obstruction from choledocholithiasis. A, Transverse sonogram of the liver reveals the “double-track” sign (circled areas),
consistent with intrahepatic biliary dilatation. B, Longitudinal view of the common bile duct (cbd) shows an echogenic stone (arrow) that produces
acoustic shadowing (arrowheads). gb, Gallbladder; v, portal vein.
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 269
m
m
v
v
v
ivc
A B
C
FIGURE 15.27. Biliary obstruction and vascular encasement from adenopathy at the porta hepatis. A, Mass (m) obstructs a mildly
dilated common bile duct (arrows) and involves the main portal vein (v). B, Nodal masses (m) encase the portal vein (v) that is markedly narrowed
(arrows). ivc, Inferior vena cava. C, Color Doppler image shows narrowed hepatic artery (a; arrow) with dilatation proximal to the encased segment.
v, Portal vein.
Tumor often expands the duct and does not produce acoustic In patients with biliary obstruction who are being considered
shadowing (Ghittoni et al, 2010; Jhaveri et al, 2009). Obstruc- for surgical resection or palliative biliary drainage, the distribu-
tion as a result of biliary ascariasis is associated with tubular tion of biliary ductal dilatation should be carefully evaluated to
structures within the bile duct, and movement of the worms is determine management. Any isolated biliary ductal segments
pathognomonic (Lim, 1990). Pancreatic carcinoma, gallblad- that do not communicate with the main ducts should be noted,
der carcinoma, and cholangiocarcinoma can all cause biliary because isolated segments may alter surgical approach, and
dilatation. biliary drainage may require placement of multiple catheters.
The pattern of biliary obstruction and the appearance of the (Jarnagin et al, 2001).
duct wall are also useful for diagnosis. Recurrent pyogenic
cholangitis is evidenced by dilated ducts with intraductal calculi Cholangiocarcinoma
and segmental dilatation, frequently in the left lobe (see Chapter Cholangiocarcinoma is a ductal tumor of the intrahepatic or
39). Lobar atrophy may also be present. Primary sclerosing extrahepatic bile ducts (see Chapter 47). Tumors of the periph-
cholangitis causes a beaded appearance of the ducts with wall eral intrahepatic ducts tend to present at a larger size, whereas
thickening, strictures, and discontinuous areas of dilatation; tumors of the extrahepatic duct tend to be smaller and often
intraluminal echoes in the dilated ducts represents debris such manifest as obstructive jaundice. Cholangiocarcinomas may be
as pus, sludge, or sloughed epithelium (see Chapter 41). Mural hyperechoic or hypoechoic.
thickening of the ducts also is seen with AIDS-associated chol- The intrahepatic peripheral form of cholangiocarcinoma
angitis. For tumors adjacent to the umbilical portion of the left presents as a focal hepatic mass, which may be solitary or with
portal vein, subtle bile duct dilatation or wall thickening may satellite lesions. Intrahepatic cholangiocarcinoma has associ-
be a clue to biliary ductal involvement. ated peripheral biliary ductal dilatation in 25% of cases, may
270 PART 2 DIAGNOSTIC TECHNIQUES
have capsular retraction, lack a hypoechoic halo, and lack Because of its midline and posterior location, the pancreas
venous thrombosis; these features help differentiate peripheral is often partially obscured by overlying gas in the stomach when
cholangiocarcinoma from HCC (Chung et al, 2009; Soyer the patient is in the supine position. Optimally, patients should
et al, 1995) (see Chapter 50). be fasting for several hours before the scan to reduce bowel gas.
Hilar cholangiocarcinomas occur at the biliary confluence Applying pressure with the transducer will displace bowel gas.
and classically produce segmental upstream dilatation with It is best to begin abdominal ultrasound with pancreatic images,
abrupt cutoff and nonunion of the right and left dilated ducts because the deep inspiratory scans used to image the liver lead
at the porta hepatis. The majority of hilar cholangiocarcino- to aerophagia and diminish the likelihood of pancreatic visual-
mas are isoechoic, and some larger tumors may have ization. Positional maneuvers, such as sitting the patient
hypoechoic rim, especially if liver is involved (Bloom et al, upright, may gather fluid into the gastric antrum and displace
1999). The extent of tumor involving bile ducts is demon- air into the fundus, affording better visualization. Patients may
strated sonographically by the location of tumor and the dis- be asked to drink 500 mL of water and examined 10 to 15
tribution of bile duct obstruction (Hann et al, 1997). Hilar minutes afterward, to use the fluid-filled stomach as an acoustic
tumors are often associated with hepatic lobe atrophy (see window.
Chapter 51). The following should be assessed in pancreatic ultrasound
On ultrasound, extrahepatic cholangiocarcinoma may appear examination: parenchymal abnormalities, the distal common
as infiltrative spread along the duct walls, nodular mural thicken- bile duct in the region of the pancreatic head, the pancreatic
ing, or papillary (Hann et al, 1997). The papillary form, which duct for dilatation or other abnormalities, and the peripancre-
is a polypoid expansile intraductal mass, has a better prognosis atic region for adenopathy or fluid. The pancreas is rarely seen
and surgical outcome (Jarnagin et al, 2005). With experienced sonographically in its entirety, and therefore when primary
operators, ultrasound can correctly identify 96% of extrahepatic pancreatic pathology is suspected, CT or MRI are preferred
cholangiocarcinomas and can demonstrate tumor infiltration modalities.
along the duct wall (Lim, 2003; Robledo et al, 1996).
Tumor involvement of the biliary ducts is best evaluated by Pancreatitis
ultrasound before placement of biliary drainage catheters, Acute pancreatitis is a common cause of abdominal pain and
because pneumobilia or stent artifact may obscure tumor is usually diagnosed with clinical and laboratory findings (see
margins, and the pattern of biliary obstruction may not be Chapter 55). Sonographic findings of pancreatitis are usually
evident after decompression. The portal vein is frequently subtle and include heterogeneous parenchymal echogenicity or
directly involved and may be encased or occluded. Both portal focal alterations in echogenicity; focal masslike abnormalities
vein status and ductal spread help determine surgical approach with contour convexity; indistinct anterior border; and peripan-
(de Groen et al, 1999; Jarnagin et al, 2001) (Fig. 15.28). creatic fluid (Finstad et al, 2005). Acute pancreatitis may be
Ultrasound contrast agents aid diagnosis and staging of focal or diffuse, and differentiation from a focal mass may not
cholangiocarcinoma (Lim et al, 2006; Xu et al, 2010). Khalili be possible. Additional findings evaluated in the setting of pan-
and colleagues (2003) reported that correct prediction of creatitis are biliary findings such as stones or ductal dilatation,
resectability improved from 69% on noncontrast ultrasound to ascites, and pleural effusions. The main purpose of sonography
96% after contrast. Staging workup generally involves other in evaluation of suspected pancreatitis is to detect biliary and
imaging modalities. gallbladder abnormalities. Although CT is the preferred tech-
nique for gauging the severity and extent of acute pancreatitis,
ULTRASOUND OF THE PANCREAS sonography is useful to determine whether the disease was trig-
gered by gallstones, because the sensitivity of CT for detection
Anatomy and Technique of gallstones has been reported to be as low as 25% (Chan et al,
The pancreas is oriented transversely in the epigastric anterior 2006).
pararenal space and lies deep to the stomach and left lobe of Complications of acute pancreatitis may be seen with sonog-
liver (see Chapter 2). The splenic vein marks the dorsal/ raphy, such as peripancreatic fluid collections and vascular
posterior border of the pancreatic body and tail (Fig. 15.29). complications (e.g., splenic or portal vein thrombosis, splenic
The pancreatic neck is marked by the confluence of splenic and artery pseudoaneurysm). Pancreatic parenchymal and extra-
superior mesenteric veins. Pancreatic head and uncinate process pancreatic fluid collections develop and evolve during time, and
may wrap around the portosplenic confluence such that pan- may be sterile, infected, or hemorrhagic. The classic pseudocyst
creatic tissue lies both anterior and posterior to the vein (Sirli is a circumscribed, smooth-walled spheric anechoic mass with
& Sporea, 2010). Celiac trunk marks the cranial border of the posterior acoustic enhancement (Fig. 15.30), sometimes mul-
gland. The pancreatic tail has a slight cranial trajectory and may tilocular, and during time may develop mural calcification.
extend to the splenic hilum. Color Doppler should always be used to evaluate any epigastric
Normal pancreatic echogenicity is fine, homogeneous, and cystic mass, including those seen in the setting of pancreatitis,
isoechoic or hyperechoic to liver. The pancreatic duct may be to distinguish fluid collections from other complications of
visible, particularly in thin patients, as an anechoic tubular pancreatitis such as pseudoaneurysms. Color Doppler will also
structure oriented along the long axis of the pancreas, usually enable detection of splenic vein thrombosis, which occurs in
measuring no larger than 2 mm in diameter, which tapers or 1% to 3% of patients following acute pancreatitis (Balthazar,
becomes invisible in the tail. On transverse images, the common 2002). The presence of pancreatic necrosis, abscess, or hemor-
bile duct can usually be visualized in cross-section in the pos- rhage cannot be determined reliably with ultrasound; CT or
terior aspect of the head of the pancreas (see Fig. 15.29). The MRI provides more accurate evaluation. CEUS may be used
gastroduodenal artery can often be seen in cross-section along to evaluate acute pancreatitis to identify complications such as
the right anterior aspect of the pancreatic head. pancreatic necrosis, which appears as heterogeneous areas of
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 271
pv
ivc
A B
rpv
C
FIGURE 15.28. Klatskin tumor. A, Longitudinal view of the common hepatic duct shows a tapered segment (arrow) consistent with tumor stricture.
ivc, Inferior vena cava; pv, portal vein. B, Transverse image at the biliary confluence reveals an echogenic mass (arrow) at the bifurcation and dilated
bile ducts in both lobes. C, The left portal vein is narrowed and encased (arrows), as shown on color Doppler transverse image. rpv, Right portal
vein.
nonenhancement (Ardelean et al, 2014). A benefit of contrast- may occur in chronic pancreatitis and can be difficult to dif-
enhanced ultrasound is that it can be performed at the patient’s ferentiate from adenocarcinoma. The finding of calcifications
bedside. within a hypoechoic focal mass is helpful for differentiating the
Chronic inflammation of the pancreas eventually causes two entities and suggests chronic pancreatitis, rather than car-
scarring and destruction of pancreatic parenchyma, producing cinoma, as the etiology (see Chapter 57).
a small atrophic gland with poorly defined margins and patchy Autoimmune pancreatitis classically appears as focal or
mixed echogenicity. The main pancreatic duct may become diffuse gland enlargement with indistinct anterior margin and
dilated and irregular (Bolondi et al, 1989). Calcifications may nondilated pancreatic duct (Araki et al, 2006; Sahani et al,
be intraductal or intraparenchymal and may show twinkle arti- 2004) (Fig. 15.31). This type of pancreatitis is typically res
fact on color Doppler. Focal hypoechoic inflammatory masses ponsive to steroids, and recent studies of contrast-enhanced
272 PART 2 DIAGNOSTIC TECHNIQUES
v v
a
A
ivc
A
ivc
A B
FIGURE 15.29. Normal pancreas. A, Transverse image of the normal pancreas and adjacent vascular anatomy. Pancreatic body (arrows) is shown.
a, Superior mesenteric artery; A, aorta; ivc, inferior vena cava; v, splenic vein. B, Common bile duct (cursors; arrow) in the head of the pancreas.
A, Aorta; ivc, inferior vena cava; v, splenic vein.
ivc
*
a
A B
FIGURE 15.30. Pancreatic pseudocyst. A, Transverse sonogram of the pancreas reveals a cyst (asterisk) in the tail and extension into the body
(arrows). a, Aorta; ivc, inferior vena cava. B, Computed tomography scan confirms extensive pseudocyst (arrows).
Pancreatic Neoplasms
Solid Neoplasms of the Pancreas
Although best staged by CT, adenocarcinoma of the pancreatic
head may be detected on sonography, because ultrasound can
be the initial imaging study for evaluation of jaundice, right
v
upper quadrant pain, or epigastric pain. Pancreatic adenocar-
cinoma classically appears as an ill-defined hypoechoic mass
associated with abrupt dilation of the upstream pancreatic duct
and atrophy of the more distal pancreas (Fig. 15.32) (see ivc
Chapters 61 and 62). The “double-duct sign,” which is dilation a
of the pancreatic duct and common bile duct, is a suspicious
imaging finding for pancreatic head adenocarcinoma. Tumors
in the body or tail of the pancreas are inconsistently visualized
on sonography because of variables such as patient body
habitus and overlying bowel gas. Color Doppler sonography FIGURE 15.31. Autoimmune pancreatitis. Transverse image of the
typically does not show increased vascularity within pancreatic pancreas shows diffuse pancreatic enlargement, well-defined margins,
and lobulated appearance (arrows). a, Aorta; ivc, inferior vena cava; v,
splenic vein.
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 273
A B
C D
FIGURE 15.32. Examples of pancreatic adenocarcinoma. Hypoechoic solid pancreatic head mass causing upstream main pancreatic ductal dilatation
(A), common bile duct dilatation (B), and intrahepatic biliary dilatation (C). D, A different patient with a hypoechoic mass in the pancreatic tail.
adenocarcinoma. Nevertheless, Doppler evaluation can be tumors. In patients with multiple endocrine neoplasia type I,
useful to visualize the peripancreatic vasculature, such as the real-time intraoperative scanning can also help identify addi-
celiac axis and superior mesenteric vessels, which are often tional subcentimeter neuroendocrine tumors that may escape
encased in locally advanced disease. Pancreatic applications of CT detection (Shin et al, 2009).
ultrasound elastography are undergoing investigation, with the There are several mimics of pancreatic masses on ultraso-
endoscopic ultrasound approach more widely studied than the nography. Either focal fatty sparing or fatty replacement of the
transabdominal approach. Initial studies propose use of elas- pancreas can appear masslike, as well as focal pancreatitis, such
tography to distinguish malignant lesions, which are densely as groove pancreatitis. Additional pitfalls include congenital
fibrotic and firm, from benign lesions such as focal inflamma- contour abnormalities, complicated pseudocysts, and lipomas
tion, which tend to be less fibrous. Another proposed use for that may mimic pancreatic masses.
endoscopic ultrasound elastography is to aid in selection of a
target for fine needle aspiration. Cystic Neoplasms of the Pancreas
In contrast to adenocarcinomas, neuroendocrine tumors of Cystic pancreatic neoplasms (see Chapter 60) fall into two
the pancreas are commonly hypervascular masses, isoechoic major categories: serous and mucinous cystic neoplasms. Dif-
or hypoechoic, well defined, and smoothly marginated (see ferentiation may be made on imaging studies based on the
Chapter 65). Functional tumors typically present early and at internal architecture and size of the cysts.
a smaller size than nonfunctioning tumors. Larger tumors may Serous cystadenomas are generally benign neoplasms with
demonstrate internal necrosis and calcifications. Intraoperative well-circumscribed lobulated borders. Internal appearance
ultrasound may be used to localize pancreatic neuroendocrine depends on size of individual cystic components that range
274 PART 2 DIAGNOSTIC TECHNIQUES
mass
A B
FIGURE 15.33. Serous cystadenoma of the pancreas. Transverse intraoperative ultrasound images of the pancreas. A, Mass in the pancreatic
tail has a small cyst (arrow). B, On magnified higher frequency images, the mass has honeycomb architecture.
A B
C D
FIGURE 15.34. Main duct intraductal papillary mucinous neoplasm (IPMN). Gray scale (A) and color Doppler (B) images demonstrate main pan-
creatic duct dilatation and tortuosity. Correlative coronal magnetic resonance images (C and D) showing dilated pancreatic duct throughout its course
without obstructing mass.
Chapter 15 Ultrasound of the liver, biliary tract, and pancreas 275
from 1 to 20 mm in size. Numerous tiny cystic spaces may not the potential to develop carcinomas, and any solid compo-
be resolved individually and create multiple interfaces, such nent or mural nodularity is concerning for malignancy (see
that the cystic component is often echogenic or solid appearing; Chapter 60).
internal architecture is often described as having a honeycomb Endoscopic ultrasound is useful in evaluation of cystic pan-
or spongy appearance (Fig. 15.33). Serous tumors composed creatic neoplasms due to better demonstration of internal cyst
of relatively larger cysts will appear as partially solid masses with architecture and potential for fluid aspiration (see Chapter 16).
peripheral cystic areas on sonography. A central stellate scar is
a characteristic feature of many serous cystadenomas and may CONCLUSION
be visible as an echogenic or calcified focus with shadowing
(Hutchins & Draganov, 2009; Yeh et al, 2001). Ultrasound is a useful and safe imaging modality to evaluate
Mucinous cystic neoplasms usually appear as unilocular or and follow up abnormalities of the liver, gallbladder, biliary
multilocular cystic lesions, with thick septations and thick tree, and pancreas. In particular, the gallbladder and biliary tree
walls, and are usually located in the pancreatic body and tail. have inherently excellent contrast resolution due to their cystic
Mucinous cystic neoplasms have malignant potential, and a nature relative to adjacent solid organs. Doppler ultrasound is
solid mural nodule is suspicious for malignancy. Intraductal an important and valuable component of the hepatic vascular
papillary mucinous neoplasms (IPMNs) are cystic neoplasms evaluation. Abdominal sonography is often used as an initial
that arise from the epithelium of the pancreatic ductal examination to determine the site of abnormality and can
system, characterized by intraductal papillary growth and often provide a diagnosis or a short differential diagnosis.
abundant mucin production, leading to ductal dilatation. The addition of cross-sectional CT or MR imaging to abdomi-
Side-branch–type IPMNs commonly appear as small unilocu- nal ultrasonography aids in diagnosis when sonography is
lar cysts or multilocular cystic masses within the pancreatic inconclusive.
parenchyma. Main-duct–type IPMNs may solely appear as
main pancreatic duct dilatation (Fig. 15.34). IPMNs have References are available at expertconsult.com.
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CHAPTER 16
Endoscopic ultrasound of the biliary tract
and pancreas
Suhail Bakr Salem, Mark Andrew Schattner, and Hans Gerdes
276
Chapter 16 Endoscopic ultrasound of the biliary tract and pancreas 277
A B
FIGURE 16.4. Endoscopic (A) and endoscopic ultrasound (B) imaging of an ampullary tumor (arrow).
FIGURE 16.7. Multiseptated mucinous cystic lesion in the head of the FIGURE 16.8. Typical microcystic appearance of a serous cystade-
pancreas (arrow). noma in the head of the pancreas (arrow).
Chapter 16 Endoscopic ultrasound of the biliary tract and pancreas 279
Pancreatic Tumors
Diagnosis*
Tumor >3 cm 86%-95% 94%-99% 86%-94%
Tumor <3 cm 85%-95% 87%-100% 93%-100%
Tumor staging — — 72%-98%
Nodal staging — — 44%-66%
Ampullary Tumors — —
Diagnosis — — 93%-100%
Resectability — — 61%-88%
Bile Duct Tumors — —
Diagnosis* — — 43%-86%
FIGURE 16.9. Large debris-filled pseudocyst adjacent to the tail of the TN staging — — 60%-80%
pancreas.
*Includes the use of fine-needle aspiration to obtain cytology. EUS, Endoscopic ultrasound;
TN, tumor node.
TABLE 16.2 Imaging Characteristics and Fluid Analysis of Pancreatic Cystic Lesions
Communication with
EUS Morphology Pancreatic Duct Fluid Amylase Fluid CEA Fluid Cytology
Retention cysts Unilocular, thin walled No Variable Low Normal duct or centroacinar cells
Pseudocyst Unilocular, thick-walled with Yes Very high Low Inflammatory cells, no epithelial
debris cells
Serous Microcystic with central No Low Low Small cuboidal cells, positive
cystadenoma calcification glycogen stain
Mucinous Macrocystic with thick Occasionally Low High Atypical ductal cells, positive
cystadenoma septations mucin stain
IPMN Dilated, tortuous pancreatic Yes High High Atypical ductal cells, positive
duct and/or side branches mucin stain
CEA, Carcinoembryonic antigen; EUS, endoscopic ultrasound; IPMN, intraductal papillary mucinous neoplasm.
communicate with the pancreatic duct. FNA will yield thick optimal cutoff is not universally agreed upon, a cyst-fluid CEA
fluid with inflammatory cells, but no epithelial cells and tumor concentration of more than 192 ng/mL predicts a mucinous
marker levels (carcinoembryonic antigen [CEA]) in the cyst lesion with a sensitivity of 73%, specificity of 84%, and an
fluid are low or undetectable; by contrast, fluid amylase is accuracy of 79% (Brugge et al, 2004; Cizginer et al, 2011).
usually markedly elevated. Although helpful for diagnosing mucinous lesions, cyst-fluid
Regarding cystic neoplasms, it is important to distinguish CEA levels do not correlate with the presence of malignancy.
mucinous and papillary tumors from serous lesions (see Another limitation of cyst-fluid CEA analysis is that it requires
Chapter 60). Serous tumors have no malignant potential and aspiration of at least 1 mL of fluid, which can be difficult if the
do not require resection unless symptoms occur or they cavity is small or the fluid is very viscous, making it difficult to
encroach on vascular structures. Typically, serous cystadeno- pull through a fine needle. More recently, cyst-fluid DNA anal-
mas are composed of a honeycomb of microcysts with no com- ysis has shown promise in differentiating mucinous from non-
munication with the pancreatic duct (see Fig. 16.8). They can mucinous cysts. This analysis can be done on as little as 200 µL
be large and exhibit central stellate calcification on imaging of fluid. The presence of a KRAS mutation, high DNA content,
studies. Papillary lesions and solid pseudopapillary tumors, and loss of polymorphic alleles are indicators of mucinous cysts.
carry the risk of malignant transformation and should be In a large validation study, early KRAS mutation followed by
referred for resection. Mucinous lesions—mucinous cystic allelic loss was 96% specific and 37% sensitive for a malignant
neoplasm (MCN) and intraductal papillary mucinous neo- cyst (Khalid et al, 2009). Interleukin-1β (IL-1β) has recently
plasm (IPMN)—also harbor malignant potential. Mucinous been identified as a potential biomarker for high-grade dyspla-
cysts are generally composed of one or more large cystic spaces sia or malignancy (Maker et al, 2011). Cyst fluid aspirated
with thickened walls or septa (see Fig. 16.7). Features that ahead of surgical resection was found to contain higher con-
may indicate malignant potential of MCNs include size greater centrations of IL-1β in specimens with evidence of high-grade
than 4 cm, mural nodules, mass-forming lesions, and periph- dysplasia or carcinoma. Nonetheless, a reliable and sufficiently
eral egg-shell calicifcations (Reddy et al, 2004). In the case of sensitive biomarker for malignancy is still lacking.
IPMNs, distinguishing main-duct from side-branch types is
important clinically because the former are associated with
Complications of Endoscopic Ultrasound
malignancy in as many as 62% of patients (Tanaka et al, Fine-Needle Aspiration
2012). Although cross-sectional imaging may help in this EUS-FNA of the pancreas is a safe procedure. The reported
regard by demonstrating a dilated pancreatic duct characteris- rate of pancreatitis is 0% to 2% (Eloubeidi et al, 2004b; Gress
tic of main-duct IPMN, communication with the main pan- et al, 2002a; O’Toole et al, 2001; Williams et al, 1999). In a
creatic duct can also be demonstrated on EUS. multicenter analysis of almost 5000 EUS-FNAs of solid pan-
Although these anatomic characteristics are helpful, EUS creatic masses, the incidence of pancreatitis was 0.3%, and the
cyst morphology alone is insufficient to characterize the lesion majority of cases were clinically mild (Eloubeidi et al, 2004b).
(Ahmad et al, 2003; Brugge et al, 2004; Tanaka et al, 2012). EUS-guided aspiration of pancreatic cysts is similarly safe, with
Aspiration of cyst fluid via EUS-FNA can further aid in the a pancreatitis rate of less than 1% and an overall complication
diagnosis. Cyst fluid can be analyzed for tumor markers, rate of about 2% (Lee et al, 2005). Bacteremia is uncommon
amylase, and molecular markers, and it provides material for following EUS-FNA of solid lesions, with a rate similar to that
cytopathologic assessment. Cyst fluid tends to be paucicellular; for diagnostic upper endoscopy; thus prophylactic antibiotic
thus the sensitivity and negative predictive value of cytology is administration is unwarranted (Janssen et al, 2004; Levy et al,
low (Centeno et al, 1997; Sedlack et al, 2002). The presence 2003). However, early data evaluating EUS-guided cyst aspira-
of thick, viscous fluid and a positive mucin stain is suggestive tion showed increased infectious complications, leading to the
of a mucinous lesion. The concentration of several tumor recommendation of routine antibiotic prophylaxis for all
markers in pancreatic cyst fluid has been examined, and CEA patients undergoing this procedure (Adler et al, 2005). Major
has been found to be the most useful. Higher concentrations extraluminal hemorrhage is a rare complication and occurs at
of CEA most accurately predict mucinous lesions, although the a rate of less than 1% (Affi et al, 2001).
Chapter 16 Endoscopic ultrasound of the biliary tract and pancreas 281
reported sensitivity, specificity, PPV, and NPV of EUS for extrahepatic cholangiocarcinoma (Mohamadnejad et al, 2011).
vascular invasion were 50%, 58%, 28%, and 82%, respectively, Tumor detection was superior with EUS compared with tripha-
but the results were better when only the portal, superior mes- sic CT scan and MRI. EUS-FNA added significant diagnostic
enteric, and splenic veins were considered. A meta-analysis of yield, particularly with distal bile duct tumors, with an overall
29 studies, including 1308 patients, evaluating the assessment sensitivity of 73%. In addition, EUS determined resectability
of vascular invasion by EUS, showed a pooled sensitivity of with a sensitivity and specificity of 53% and 97%, respectively.
73% and pooled specificity of 90.2% (Puli et al, 2007). Another Intraductal US can also provide staging information with
recent report compared EUS and MRI staging of resectability respect to depth of invasion, the maximal longitudinal extent
based on arterial invasion or encasement. The sensitivity, speci- of the lesion, and the presence of invasion into other organs
ficity, NPV, PPV, and accuracy of MRI were 78%, 96%, 92%, and major blood vessels, particularly portal vein invasion, with
88%, and 91%, respectively, compared with 33%, 100%, 81%, a reported accuracy of 60% to 80% (Inui & Miyoshi, 2005;
100%, and 82% for EUS, but these differences were not sta- Tamada et al, 1995, 1998). Standard echoendoscopes are less
tistically significant (p = 0.13) (Borbath et al, 2005). accurate for tumor staging but can detect regional lymphade-
nopathy and allow tissue acquisition via FNA.
Preoperative Reassessment after Neoadjuvant
Chemoradiotherapy ENDOSCOPIC ULTRASOUND-GUIDED THERAPY
Studies on the treatment of pancreatic cancer have recently
focused on neoadjuvant treatment with chemotherapy and Celiac Plexus Neurolysis
radiation therapy, followed by attempted radical resection (see In patients with pain as a result of pancreatic cancer, EUS-
Chapter 68). Several studies have investigated the ability of guided celiac plexus neurolysis has been shown to be a safe and
EUS to reassess patients who have completed neoadjuvant effective alternative to surgical or percutaneous approaches (see
therapy, with most suggesting that EUS is no better than CT Chapter 62). The celiac axis is easily identified using a linear-
for determining resectability. In one report, EUS correctly array echoendoscope positioned in the stomach (Fig. 16.12),
assessed residual tumor stage in 40% and node status in 90%, and it provides a quick method of palliating cancer-related
but it incorrectly suggested venous invasion in 43% (Bettini pain in patients undergoing staging and diagnosis of pancreas
et al, 2005). These results suggest that inflammatory changes cancer. Two recent meta-analyses demonstrated improved sus-
in the tumor bed, pancreas, and lymph nodes alter the anatomy tained pain relief in 72% to 80% of patients at a follow-up
and blur the distinction between normal tissue planes and range of 1 to 6 months (Kaufman et al, 2010; Puli et al,
between tumor and normal tissue. 2009). In addition, decreased analgesic requirements and
fewer opioid-induced side effects can be expected after EUS-
DIAGNOSIS AND STAGING OF guided neurolysis. Recent studies have suggested that bilateral
CHOLANGIOCARCINOMA ethanol injection to the right and left of the celiac axis is
more effective than unilateral or central injection (Puli et al,
Primary bile duct cancers (see Chapters 51 and 59) usually 2009; Sahai et al, 2009), and no reports of neurologic compli-
present with painless jaundice. Although transcutaneous US cations or pancreatitis have been reported with this technique
and CT scanning reliably show biliary dilatation, they are less (O’Toole & Schmulewitz, 2009; Puli et al 2009). A random-
accurate for delineating tumors, especially if tumors are smaller ized, double-blinded, controlled trial was performed of early
than 2 cm. ERCP is the dominant invasive modality used to EUS-guided neurolysis to prevent pain progression in patients
evaluate extrahepatic bile duct strictures. Diagnostic specimens
can be obtained by rubbing a cytology brush against the stric-
ture, but the sensitivity is low, with a yield of only 40% to 50%
(Ponchon et al, 1995; Victor et al, 2012; Wakatsuki et al,
2005). EUS has now emerged as a useful diagnostic and staging
technique in this regard through the use of linear and radial
echoendoscopes, as well as high-frequency radial miniprobes C
(passed into the bile duct over a guidewire through the working
channel of an ERCP scope), to perform intraductal US.
For detecting benign causes of biliary obstruction, such as SMA
AO
CBD stones, EUS, with a sensitivity of 89% to 94% and specific-
ity of 94% to 100%, is more accurate than transcutaneous US,
CT, magnetic resonance cholangiopancreatography (MRCP),
ERCP, or intraoperative cholangiography (Garrow et al, 2007;
Tse et al, 2008) (see Chapters 15, 18, 19, and 23). If a biliary
stricture is visualized, malignancy is suggested by the presence
of an irregular, thickened (>3 mm) bile duct wall (see Fig. 16.5).
Hypoechoic infiltration invading through the biliary wall layers
or an adjacent pancreatic mass can also be seen. The accuracy
of EUS-FNA in the diagnosis of bile duct strictures has a
reported sensitivity ranging from 43% to 86% (DeWitt et al,
2006; Eloubeidi et al, 2004a; Rosch et al, 2004) (see Table FIGURE 16.12. Endoscopic ultrasound appearance of the longitudinal
16.1). More recently, results of a large single-center experience course of the aorta (AO) with celiac (C) and superior mesenteric artery
suggest that EUS can be very useful in the assessment of (SMA) origins.
Chapter 16 Endoscopic ultrasound of the biliary tract and pancreas 283
with inoperable pancreatic cancer (Wyse et al, 2011). Patients et al, 2009; Gress et al, 2002b). This precludes the need for
who received EUS-guided neurolysis had significantly less pain intraoperative US and may allow the surgeon to perform a more
at 3 months as well as a tendency toward less narcotic use. limited pancreatic resection. A role for EUS-guided intratu-
moral placement of gold fiducials in localizing pancreatic
Drainage of Pseudocysts and Peripancreatic Collections tumors for targeted radiation therapy has also been demon-
The role for EUS as a minimally invasive and effective tech- strated (Pishvaian et al, 2006; Sanders et al, 2010; Yan & Van
nique for guiding drainage of peripancreatic fluid collections Dam, 2008). This modality of radiotherapy minimizes toxicity
after acute pancreatitis (Lopes et al, 2007; Varadarajulu et al, to the surrounding tissue by allowing delivery of highly confor-
2007) (see Chapters 27, 30, and 56) or after pancreatic resec- mal radiation treatments.
tion has been established. A fine needle is used to puncture the
fluid collection, and a guidewire is used for transluminal stent- NOVEL THERAPEUTICS
ing. Using real-time imaging and Doppler flow, intervening
organs and vascular structures can be avoided. Thus there are EUS-guided ethanol ablation of cysts has been previously
fewer complications, such as bleeding and perforation, com- reported (DeWitt et al, 2009; Gan et al, 2005). Patients with
pared with the percutaneous approach. Pseudocysts often asymptomatic, unilocular pancreatic cysts were treated by injec-
contain a large amount of necrotic debris that typically requires tion and lavage of the cyst with ethanol through an FNA needle,
endoscopic debridement and is not effectively drained by stent with complete cyst resolution documented in 30% to 35% of
placement alone. This technique has also been applied to the patients. More recently, ethanol has been combined with pacli-
drainage of peripancreatic fluid collections after distal pancre- taxel (Oh et al, 2011), with complete resolution achieved in
atectomy (Tilara et al, 2014; Varadarajulu et al, 2009) (see 62% to 78% of patients. Radiofrequency ablation of pancreatic
Chapter 66). EUS-guided drainage of pancreatic fluid collec- cysts has also been described recently in a small series of patients
tions compares favorably with percutaneous drainage tech- (Pai et al, 2013). Despite these advances, concerns remain
niques, with similarly high success rates (Kwon et al, 2013) about residual epithelium, which could remain after ablation.
(see Chapter 27). EUS-guided drainage eliminates the need In addition, evidence that ablation reduces the risk of malig-
for an external drainage apparatus as well as the risk of cysto- nancy, the need for resection, or continued surveillance is
cutaneous fistula compared with percutaneous drainage tech- lacking.
niques. Recent improvements in stent design have made In patients with advanced abdominal malignancies, simul-
drainage of pancreatic fluid collections more simple and effec- taneous duodenal and biliary obstruction can occur. Tradition-
tive (Shah et al, 2015). Ultimately, a collaborative multidisci- ally, these patients have required percutaneous or surgical
plinary approach taking into consideration the size and location biliary drainage because transpapillary decompression via
of the fluid collection will determine the best approach for ERCP is often not possible. EUS-guided transduodenal or
drainage. transgastric biliary drainage is a novel approach that allows
internal drainage (Will et al, 2007; Yamao et al, 2008; Park
Tumor Localization et al, 2009). Similar to pseudocyst drainage, the dilated CBD
Preoperative localization of small pancreatic tumors by fine or left hepatic duct is localized with EUS and punctured with
needle tattooing can be performed safely using EUS (Farrell an FNA needle. A cholangiogram is performed (Fig. 16.13A),
A B
FIGURE 16.13. A, Cholangiogram obtained by endoscopic ultrasound (EUS)-guided puncture of the common bile duct by fine-needle aspiration
in preparation for EUS-guided biliary drainage. B, EUS image after deployment of self-expanding metal stent.
284 PART 2 DIAGNOSTIC TECHNIQUES
followed by guidewire insertion, dilation of the tract, and biliary tree. It provides detailed images of the pancreas and bile
deployment of a self-expandable metal stent across the choledo- ducts and complements the findings of noninvasive radio-
choduodenostomy or hepaticogastrostomy tract (Fig. 16.13B). graphic imaging. For patients seen initially with suspected pan-
A recent study directly compared ERCP with EUS-guided creatic or bile duct cancer, multidetector CT scanning assists
biliary drainage (Dhir et al, 2015). Short-term outcomes have in identifying those with obvious masses, metastatic disease,
been shown to be comparable to ERCP, with a similar rate of and vascular involvement. The usefulness of EUS in this setting
adverse events and lower risk of pancreatitis. EUS-guided is limited, except to provide tissue diagnosis through the use of
biliary drainage was also recently compared with percutaneous EUS-guided fine-needle aspiration. For patients with small
drainage in patients who failed ERCP (Khashab et al, 2015) tumors, ampullary lesions, or equivocal findings detected by
(see Chapter 29). EUS-guided biliary drainage was equally CT or MRI, the high sensitivity of EUS helps provide a diag-
effective, with fewer adverse events, reduced need for reinter- nosis, with a high accuracy for tumor staging and determining
ventions, and reduced cost. resectability. Because EUS has poor sensitivity for identifying
EUS-guided intratumoral therapy of solid masses is being distant metastatic disease, CT scanning and laparoscopy will
actively investigated. Several therapeutic agents have been eval- remain important tools in the evaluation of patients with pan-
uated, including activated lymphocyte cultures, viral vectors, creatic and bile duct cancer who are being considered for
oncolytic viruses, and radioactive seeds (Chang et al, 2000; surgery. EUS-FNA is a safe and valuable tool in the evaluation
Hecht et al, 2003; Hecht et al, 2012; Jin et al, 2008; Senzer of patients with a suspected solid or cystic mass of the pancreas
et al, 2004). Early studies have established safety and demon- or extrahepatic bile ducts. It has a higher diagnostic sensitivity
strated partial response or disease stabilization in most patients. and specificity than noninvasive imaging and allows tissue sam-
The feasibility and safety of performing radiofrequency ablation pling as part of the same procedure. As molecular testing
and cryotherapy of the pancreas by using a EUS platform has improves, the utility of EUS-FNA as a diagnostic modality is
been established in animal models (Carrara et al, 2008; Gold- likely to grow. Similarly, EUS-FNA has evolved from a diag-
berg et al, 1999). nostic to a therapeutic procedure in the management of biliary
and pancreatic disease.
SUMMARY
References are available at expertconsult.com.
EUS is an essential tool in the preoperative evaluation of
patients with abnormalities that involve the pancreas and the
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CHAPTER 17
Role of nuclear medicine in diagnosis and
management of hepatopancreatobiliary disease
Simone Krebs and Mark Dunphy
Nuclear medicine specialists prescribe radioactive pharmaceu- other guidelines, especially when these make judgments on the
ticals, radiopharmaceuticals, for diagnostic imaging and internal diagnostic accuracy or clinical impact of nuclear medicine;
radiotherapy of a variety of diseases. This chapter discusses sometimes guidelines cite outdated nuclear medicine research
clinical applications of diagnostic nuclear medicine imaging for from decades past. Such guidelines might be designed in recog-
the care of patients with hepatic, pancreatic, and biliary (hepa- nition that nuclear medicine clinical practice varies worldwide,
topancreatobiliary, HPB) diseases. Radioembolization of liver as reflected in the often widely varying diagnostic sensitivities
tumors with radiolabeled microspheres is discussed separately and specificities reported by different medical centers perform-
(see Chapter 96B). Other standard forms of nuclear medicine ing a particular NMI procedure. Although the same term is used
therapy, involving radiopharmaceuticals administered in thera- (e.g., fluorodeoxyglucose [FDG] PET/computed tomography
peutic amounts of radioactivity, are not specific to HPB diseases, [CT]), when extremely different diagnostic performance out-
but a few are mentioned when relevant (e.g., somatostatin comes are reported between centers, the differences in diagnostic
receptor–targeted radionuclide therapy), with citations for performance are likely attributable in significant part to differ-
further information. ences in hardware (e.g., scanners) or methodology (e.g.,
In general, the role of diagnostic nuclear medicine imaging administered tracer doses, software-based data-processing
(NMI), or scintigraphy, including positron emission tomography algorithms, adjunctive medications) that may or may not be
(PET), is to provide HPB clinicians with a noninvasive method considered “state of the art.” This chapter discusses the essential
to aid in detecting and localizing certain types of HPB disease criteria defining state-of-the-art for the major HPB-related
and evaluating HPB organ function, as well as evaluating the diagnostic and therapeutic nuclear medicine procedures, as well
effects of treatment. In general, NMI can be considered a clini- as the diagnostic accuracy and clinical relevance of state-of-the-
cal assay of cellular biology in the tissues of patients; the in vivo art nuclear medicine in the care of the patient with HPB disease.
tissue accumulation, or uptake, of most radiopharmaceuticals State-of-the-art clinical nuclear medicine is based on a rela-
depends on the biomolecular composition of living cells, in tively expensive infrastructure. A notable example is PET
body tissues, as well as tissue perfusion. imaging with the standard radiopharmaceutical fluorine 18
The diagnostic accuracy of scintigraphy varies according to (F-18, 18F) FDG used for imaging HPB tumors (among other
the specific scintigraphic study (including the specific radio- applications). To perform FDG PET, a highly expensive cyclo-
pharmaceutical used and how it is assayed) and the specific tron facility, costing multiple millions of US dollars (2015) for
disease or condition being studied. The HPB specialist must construction, besides annual costs for staff, supplies, and
integrate diagnostic data from any scintigraphic study of a maintenance, is required for production of the radioactive
particular patient with signs, symptoms, and data from other isotope 18F, used in synthesis of FDG. After FDG is adminis-
relevant assays for optimal diagnostic accuracy and therapeutic tered to a patient, the patient is then, in state-of-the-art practice,
decision making. NMI has a major positive impact on patient scanned for disease using a PET camera combined with an
care, improving therapeutic strategy. x-ray computed tomography (CT) camera, a hybrid PET-CT
This chapter discusses the published clinical evidence camera system that is also highly expensive to purchase and
regarding the impact of nuclear medicine in HPB diseases and maintain (again, millions of US dollars). Even in the wealthiest
focuses on state-of-the-art nuclear medicine and, as such, nations with comparable well-developed nuclear medicine
concentrates predominantly on published medical literature infrastructures, the availability of certain state-of-the-art nuclear
from the past 10 years. In our experience, most clinical nuclear medicine diagnostic and therapeutic procedures often varies
medicine research publications before 10 years ago often significantly for the “average” citizen, depending on socioeco-
employ methodology and technology that is no longer reflective nomic factors (an important discussion but beyond the scope
of current state-of-the-art clinical practice in nuclear medicine. of this chapter). Other diagnostic and therapeutic nuclear
The state-of-the-art in nuclear medicine, in its diagnostic and medicine procedures important to management of HPB dis-
therapeutic procedures, has improved rapidly in the past 10 eases, however, are relatively low cost and are available to
years and continues to evolve and innovate, including major patients in most nations. If unsure of the availability of any
improvements in commercially available nuclear imaging particular nuclear medicine procedure discussed here, the
camera systems (particularly the advent of hybrid “fusion reader can contact his or her local radiology department or
imaging” camera systems), image data processing, new types of search the Internet to find the nearest medical center offering
instrumentation, and clinical introduction of new radiopharma- the procedure of interest.
ceuticals, both for diagnostic imaging and nuclear therapy. After a concise introduction to the pharmacology and tech-
Therefore, we strongly advise the reader to note the dates of nology of diagnostic imaging and therapy in radiopharmaceu-
nuclear medicine references cited in HPB bibliographies and ticals and the general role of nuclear medicine in HPB diseases,
285
286 PART 2 DIAGNOSTIC TECHNIQUES
we discuss current state-of-the-art nuclear medicine procedures elemental radioisotope atom typically is incorporated within a
for specific HPB clinical indications. For diagnostic imaging molecule by chemical bonding. The molecule is said to be
procedures, discussion focuses on how well a particular clinical radiolabeled.
NMI study performs for a specific HPB indication, in terms of As with any pharmaceutical, each type of radiopharmaceuti-
its diagnostic accuracy (sensitivity, specificity) and potential cal has in vivo pharmacokinetic (PK) properties specific to and
pitfalls, including necessary patient preparation, when appli- determined by its molecular structure and associated physico-
cable. For the few nuclear medicine therapeutic procedures chemical properties. PK properties include the radiopharma-
applicable specifically to HPB diseases, this chapter focuses on ceutical’s distribution in tissues throughout the body
summarizing medical literature regarding clinical therapeutic (biodistribution), metabolism, and bodily elimination (by hepa-
efficacy. Each section discusses specific standard nuclear medi- tobiliary and urinary excretion for all relevant radiopharmaceu-
cine radiopharmaceuticals and procedures that have clinical ticals). The in vivo PK properties are also determined, to some
applications for particular HPB diseases, as used in state-of- degree, by the physicochemical properties of excipients (vehi-
the-art clinical practice. The chapter also includes a concise cles) in the radiopharmaceutical formulation (e.g., formulation
look at select new, currently investigational radiopharmaceuti- of an orally administered radiopharmaceutical compound may
cals relevant to HPB disease. affect its bioavailability and biodistribution), as well as by the
Radiopharmaceuticals can be placed into three major catego- route of administration (e.g., peripheral intravenous injection,
ries of applications in HPB disease: detection and evaluation of hepatic arterial catheter infusion).
cancerous HPB tumors, treatment of HPB cancers, and evalu- The mass-amount of radioactive molecules (per se) in any
ation of HPB organ function (and indirectly for detection of prescribed radiopharmaceutical formulation is only a trace
disease entities causing HPB organ dysfunction). The complete amount, typically in the picogram (pg) range. This tiny mass-
pharmacopoeia used in current clinical practice, approved dose of radioactive molecule is incapable of exerting detectable
by the US Food and Drug Administration (FDA), includes pharmacologic effects on body tissues in vivo, but the typical
numerous different radiopharmaceuticals, each with diagnostic picogram amounts of radioactive molecules emit radioactivity
and/or therapeutic applications in one or more of the major sufficient for diagnostic imaging and therapeutic applications.
medical specialties, most not specifically relevant to HPB dis- With exceptions, the nonradioactive constituents of radiophar-
eases. It is beyond the scope of this chapter to discuss all general maceutical compounds typically used only for clinical diagnostic
nuclear medicine tests that an HPB specialist or their patients imaging are present in somewhat higher mass-amounts but are
may encounter clinically. Only those radiopharmaceuticals of still scant, typically less than 100 micrograms (µg), and allergic
major importance to the diagnosis and treatment of HPB dis- reactions, other side effects, or pharmacodynamic effects are
eases are discussed here. Similarly, we include no comprehensive rarely reported. Nuclear medicine specialists may prescribe the
review of the novel tracers described in medical literature; radiopharmaceutical compound to be administered in conjunc-
rather, we focus on select radiopharmaceutical “front-runners” tion with a relatively high and biologically effective mass-amount
that HPB specialists may see at their own medical center in the (e.g., milligrams or grams) of a nonradioactive, or unlabeled,
next 10 years. version of the same compound or a related compound, with
therapeutic intent (relevant compounds are discussed later).
RADIOPHARMACEUTICALS The term “radiotracer,” “tracer dose,” or “radiotracer dose”
commonly refers to the use of a radiolabeled molecule in tiny
Nuclear medicine specialists prescribe radiopharmaceuticals for (trace) amounts to study molecular biology. The trace amount
diagnostic imaging and internal radiotherapy of a variety of of radioactivity and the trace mass of the administered radio-
diseases, with this chapter exclusively focused on HPB applica- tracer are unable to affect (and therefore unable to interfere
tions. A radiopharmaceutical is a radioactive compound con- with measurements of) the biomolecular system or target being
taining a radionuclide, also (loosely) referred to as a “radioisotope” assayed. Following this common convention, in this chapter we
(radioactive isotope). A radioisotope is an energetically unstable use radiotracer to refer to radiopharmaceutical administered
atom that will achieve a stable or more stable, lower-energy state specifically as a trace, biologically ineffective amount of radio-
(transitioning from a parent to a daughter state) by releasing activity useful solely for diagnostic imaging. We use therapeutic
(radiating) energy (radiation), in some form (e.g., emitting a radiopharmaceutical to refer to administration of a relatively high
gamma ray, positron particle, or beta particle, as discussed amount of radioactivity with the intent of inducing therapeutic
later). The release of energy by the (parent) radioisotope atom radiobiologic effects in vivo, as discussed later. The radioactivity
may be called a physical decay, disintegration, or transition. The emitted by a therapeutic radiopharmaceutical may be useful for
energy decay makes the elemental atom either become a differ- diagnostic imaging as well as radiotherapy. The clinical diag-
ent isotope of the same element (e.g., the radioisotope techne- nostic imaging of therapeutic radiopharmaceuticals’ biodistri-
tium 99m decays to the stable isotope technetium 99) or become bution in vivo in patients (e.g., to detect or quantify tumor
a different element, by transmutation (e.g., the radioisotope 18F targeting by the radiopharmaceutical) is known as theranostics.
decays to become a stable form of the element oxygen, Most radiopharmaceuticals in current clinical practice rel-
i.e., oxygen 18). Other forms of nuclear decay are possible evant to HPB diseases are administered intravenously. One
(e.g., transitions from a higher-energy unstable radioisotope to notable exception is hepatic arterial infusion of radiotracer.
a lower-energy, but still unstable, daughter radioisotope). A
radiopharmaceutical is administered in a trace amount (with no DIAGNOSTIC IMAGING IN NUCLEAR MEDICINE
detectable radiobiologic effects) or therapeutic amount, for use
as a diagnostic imaging agent or therapeutic agent. A radiophar- The diagnostic images of the patient analyzed by the nuclear
maceutical also contains other active and inactive ingredients in medicine specialist are the result of technology, pharmacology,
the compound formulation. In the radiopharmaceutical, the and biology. This section focuses on what the clinical imaging
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 287
specialist and referring clinician need to know to interpret decay with its characteristic radioactive emissions. The emitted
nuclear scan images properly and to avoid misinterpretations energy detected by a modern nuclear scanner (e.g., PET
that might negatively impact patient care, as well as diagnostic scanner, gamma camera) is always in the form of photons. The
pitfalls by properly preparing patients. detection of photons by the camera system generates signals
In general, diagnostic nuclear imaging is a noninvasive pro- processed and analyzed by computer software to determine the
cedure that uses scanning hardware to examine the distribution direction/location from which the photons originated (whether
of a radiopharmaceutical within the internal environment of the in a two-dimensional plane or a three-dimensional space). The
body. As discussed, imaging the in vivo distribution of a signal data analysis is processed to create imagery that visualizes
radiopharmaceutical can be considered an in vivo assay of the in vivo biodistribution of the radiopharmaceutical in the
radiopharmaceutical pharmacokinetics, not just in blood (as for patient studied.
conventional plasma pharmacokinetics) but also in tissues/ Does the biodistribution of the radioisotope atoms visual-
organs throughout the body. In diagnostic imaging, it is not the ized by the nuclear scan represent the biodistribution of the
radiopharmaceutical itself that is of interest (although measuring administered radiopharmaceutical (molecules)? If the radio-
tumor concentrations of a radiolabeled therapeutic can be of pharmaceutical undergoes no in vivo chemical transformation
major interest, for research in tumor dose-response correla- to another form (e.g., catabolite or metabolite) before imaging
tions). Rather, the in vivo radiopharmaceutical distribution is of the patient, the answer is yes. Otherwise, the radioisotope
most often used as a diagnostic imaging biomarker; that is, the biodistribution imagery may represent a composite of biodis-
tissue concentration of tracer detected by the scanner is used as tributions, including those of the (unmodified) administered
noninvasive biologic marker, a radiologic surrogate for obtaining radiopharmaceutical and the radioactive products of in vivo
tissue (e.g., by biopsy) to assay an in vivo biophysiologic process chemical reactions (i.e., reaction products that still incorporate
or tissue biomolecular target of interest. In general, as with any the radioisotopic atom). Usually, in vivo metabolism of the
pharmaceutical in the modern age of “molecular medicine,” a radiopharmaceutical causes in vivo production of metabolites,
particular radiopharmaceutical compound is typically designed one or more of which include the radioisotope; these are radio-
with the intent of specifically targeting one or more in vivo metabolites. Such metabolism may be the diagnostic imaging
biophysiologic processes and tissue biomolecular targets specific target of the nuclear scan (e.g., PET imaging with F-18 FDG
to a disease or physiologic condition of interest. to detect tumor concentrations of the FDG metabolite). Some
No radiopharmaceutical compound yet designed has been radiometabolites may be radiolabeled molecules, or in vivo
found to bind exclusively to one particular biologic molecule. metabolism may yield radioisotope in free, unattached elemen-
Some compounds, however, such as radiolabeled antibodies, tal form. These radiometabolites often have different in vivo PK
radiolabeled “small molecules,” and other types of agents, do properties from the intact parent radiopharmaceutical. Thus,
bind with very high selectivity and affinity to relatively few the radiotracer biodistribution visualized by nuclear imagery
biologic molecules and not at all to other types of molecules will represent a combination of biodistributions: that of the
and are called “targeted agents.” Still, the biophysiologic pro- intact radiopharmaceutical and that of one or more radiome-
cesses and biologic molecules targeted by such agents for tabolites. In vivo metabolism occurs but typically does not
diagnostic imaging (or “targeted therapy”) of a particular interfere with diagnostic interpretation. On the contrary,
condition of interest can almost invariably be found in other metabolism may yield a radiometabolite “trapped” in a tissue
physiologic or pathologic conditions, again precluding 100% of interest, such as enzymatic trapping of the PET imaging
specificity. For example, the biologic molecule prostate-specific FDG in tumor cells; the cytoplasmic enzyme hexokinase yields
membrane antigen (PSMA, now more properly referred to as the radiometabolite fluorodeoxyglucose-6-phosphate, which is
glutamate carboxypeptidase II), once thought to be uniquely trapped intracellularly.
expressed by prostate tissues and thus a good biomarker for Because the radioisotope is the same for the parent radio-
prostate cancer (e.g., for imaging by PSMA-targeted radiola- pharmaceutical and each of its radiometabolites, image data
beled antibody), was later found to be expressed by certain analysis alone cannot separate the composite biodistributions
other tissues in the body and in the neovasculature of most in nuclear imagery. In clinical practice, however, this is rarely
tumors. However, PSMA is highly expressed in only a few types relevant, because radiopharmaceuticals that have achieved
of nonprostatic tissues and therefore still possesses high selec- widespread clinical use did so by having favorable in vivo
tivity for prostatic tissues. Therefore, “perfect” specificity should pharmacokinetics, typically including in vivo metabolism that
not be expected for diagnostic imaging agents, even radiola- yields a biodistribution that predominantly represents that of
beled antibodies, considering the underlying imperfect pharma- one parent compound or relevant radiometabolite, with one
cologic and biologic specificity, as well as potentially misleading predominant biologic “meaning.” This chapter discusses the
imaging artifacts. meaning of each radiopharmaceutical scintigraphic biomarker
Nevertheless, scintigraphy can be highly accurate, noninva- scan relevant in HPB diseases. Once administered to a patient,
sive in vivo virtual histochemistry, as long as scintigraphic evi- the radioisotope used for diagnostic imaging emits radiation
dence suggesting a particular type of disease is consistent with that can be detected by a nuclear scanner.
the clinical picture (i.e., pretest likelihood of that disease being Diagnostic imaging with radiopharmaceuticals, in standard
present, based on signs and symptoms from clinical and labora- clinical practice, may be referred to in various ways, including
tory examinations). If not, further confirmation of scintigraphic (1) general terms such as nuclear imaging or scintigraphy, (2)
findings may be warranted to ensure accurate therapeutic deci- reference to one of two general types of scintigraphic camera
sion making. technology (PET, SPECT/SPET), and (3) procedure involved
The imaging signal detected by nuclear scanners is produced (e.g., theranostic imaging).
by the radiopharmaceutical administered to the patient. The The term scintigraphy (Latin scintilla, “spark”) in medicine
radioisotope in the radiopharmaceutical undergoes its physical refers to the light produced by crystalline detectors in clinical
288 PART 2 DIAGNOSTIC TECHNIQUES
scintigraphic cameras when those crystals are struck by gamma energy produced by positron-electron annihilation is always the
rays emitted from radiopharmaceuticals (e.g., as emitted from same, 1022 kiloelectron volts (keV), regardless of the positron-
within a patient scanned after receiving a radiopharmaceutical emitting isotope involved (e.g., F-18, carbon 11, gallium 68).
injection). These scintillations produced in the crystalline The 1022-keV annihilation energy splits instantly into two
detectors are recognized and processed by the camera system photons: gamma rays of 511 keV each. This pair of gamma rays
to yield nuclear imagery. travels in opposite directions. The modern PET system is basi-
Of the basic types of scans found in a radiology department cally composed of a ring of crystalline detectors surrounding a
(e.g., plain radiography, CT, MRI, US), diagnostic nuclear gantry bed. Exiting the body at the speed of light, a pair of these
imaging scans are typically of the longest duration, in terms of annihilation photons may strike two of the detectors on the
both the time the patient must physically spend with the scanner PET ring, each strike-incident occurring practically at the same
and the time required for the entire study (start to finish), often moment. This coincidence of two strikes, of about 511 keV each,
with necessary delays before scanning or between scanning (i.e., is recognized by the PET circuitry as a true signal, whereas
if the patient is scanned more than once after a single radio- signals without a coincidence pattern or with incorrect energies
pharmaceutical administration) to allow the radiopharmaceuti- are dismissed as noise. A true signal informs the system that an
cal time to undergo desired in vivo physiologic processes. The annihilation occurred along the spatial line between the two
total duration of a diagnostic nuclear imaging study thus detectors. By analyzing millions of such signals gathered during
depends on a variety of technical, biologic, as well as typical PET imaging, along all the ring of different “lines of response”
clinical logistical variables. Most frequently, a radiopharmaceu- (imaginary lines between pairings of detectors,) sophisticated
tical is administered intravenously, by bolus injection. After the computer algorithms can deduce the distribution and concen-
injection, a standard time-delay may be necessary before the tration of radioactivity within the patient (i.e., biodistribution
patient undergoes scanning, to allow the radiopharmaceutical of isotope). Importantly, PET scanners cannot distinguish
to spread throughout the body and achieve a biodistribution between different positron-emitting isotopes (e.g., 18F, 11C,
68
considered optimal for imaging. To acquire data for a single Ga). The energy signal generated by different positron-
image, the time that a patient spends “in front of the camera” emitting isotopes and detected by PET scanners is always the
must be of sufficient duration for the scanner to collect a sta- same: coincident 511 keV gamma rays. Thus, if one patient
tistically robust number of radioactive signals, or counts, to received two different radiopharmaceuticals simultaneously
ensure that the derived imagery will be satisfactory for visual (e.g., one radiolabeled with 18F and the other with 68Ga), and
analysis. Low-count images are visually “noisy.” How long it the patient was then scanned, the PET scanner could not sepa-
takes for the camera to collect enough photons for a sufficient- rate the radioactive signal emitted by the 18F compound from
quality diagnostic image depends primarily on intrinsic proper- the radioactive signal emitted by the 68Ga compound. There-
ties of the radioisotope involved, how much radiopharmaceutical fore, patients do not receive two different PET radiopharma-
is administered, how well the radiopharmaceutical concentrates ceuticals simultaneously, because the result is one PET scan of
in tissues of interest (e.g., tumors) compared with surrounding mixed “meaning.” In this scenario, one cannot know how much
tissues in vivo, how well the camera system detects photons, of a radioactive signal in one tissue site represents one PET
and how the photon data are constructed into imagery. Depend- tracer versus the other.
ing on the type of nuclear imaging study, before imaging even The design of the standard (non-PET) gamma camera is
starts, there may be a standardized delay after the radiophar- tailored to detect isotopes that decay by emitting (unpaired)
maceutical administration to allow the radiopharmaceutical gamma rays of relatively lower energy, typically energy lower than
time to achieve an in vivo biodistribution considered optimal the 511 keV energy (photopeaks) of PET imaging. This is often
(i.e., 1 hour after FDG injection before PET scan acquisition). referred to as single-photon imaging, to distinguish such imaging
Lastly, the imaging specialist decides whether to have the from PET imaging that involves detecting a pair of two photons
patient undergo scanning at additional time points or using simultaneously. In contrast, single-photon imaging refers to
special techniques, if thought necessary to increase the diagnos- camera detection of (unpaired) photons from nonpositron-
tic accuracy of the study. The referring clinician’s staff can help emitting radioisotopes. Some non-PET radioisotopes have
prepare patients mentally by advising them of the prolonged radioactive decay characterized by emitting photons of more
duration typical of diagnostic nuclear imaging. than one energy level; for example, the common single-photon
Nuclear scanners may be categorized into two general types: imaging isotope indium 111 simultaneously emits two types of
PET scanners and standard gamma cameras. Their designs are photons relevant for imaging—photons differing in energy—with
tailored to image two fundamentally different types of radio- two energy levels (photopeaks) of 173 and 247 keV.
pharmaceuticals (radioisotopes): those that emit positrons (for After the scanner system processes the photon data to
PET cameras) and those that emit gamma rays (for standard determine the spatial origin of the signals in vivo, a nuclear
gamma cameras). medicine technologist at a computer workstation uses software
In PET imaging, the radiation detected by the crystals of to reconstruct the data for visual display and analysis by the
PET cameras comes from gamma rays that are produced by physician imaging specialist. How the in vivo radiopharmaceu-
positron-electron annihilations that occur, after a decaying radio- tical biodistribution is displayed depends on how the imaging
isotope emits a positron. The positron emitted by the PET data was acquired. This biodistribution imagery can have a flat,
radiopharmaceutical encounters its antimatter: any electron in two-dimensional (2D), or planar, appearance; or a (virtual)
its immediate environment. The two particles “annihilate” three-dimensional (3D) appearance (e.g., allowing display of
during the encounter, converting all particulate mass (m) to sections of data in conventional transaxial, coronal, and sagittal
pure energy (E). This annihilation reaction is an everyday views, similar to CT). The imagery may represent biodistribu-
example of Einstein’s theory of relativity, E = mc2. Because the tion at one or a few time points, or imagery may display time-
mass of positrons and electrons are universally constant, the dependent changes in biodistribution in cinematic fashion.
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 289
Planar images of radiotracer biodistribution in the anterior- receives an 18F FDG injection for FDG PET, based on the
posterior plane will result in an image in which in vivo tracer known half-life of 18F (~1.9 hours) and the amount of tracer we
accumulations in two or more organs or other tissues may administer to a patient (maximal tracer dose of 12 mCi). Thus,
overlap (in the 2D plane) and thus potentially obscure detec- one must wait until the PET isotope has disappeared (decayed)
tion or evaluation of the radiotracer uptake of interest (e.g., sufficiently before attempting to image another radiopharma-
tumor detection). Tomographic (SPECT and PET) nuclear ceutical. A common rule of thumb is waiting 10 half-lives, a
imaging can help avoid this potential issue by permitting tracer half-life referring to the physical half-life of the isotope.*
biodistribution to be evaluated in three dimensions. However, In general, however, single-photon radiopharmaceutical
the limited spatial resolution of scintigraphic imaging may make imaging studies can be performed immediately before PET
it difficult to localize a particular tracer accumulation in a small scans, without needing to wait for the single-photon radiophar-
tissue structure (e.g., tracer uptake in a small tumor may be maceutical to disappear; this is because the photons of non-PET
hidden if the tumor is located within or immediately adjacent radioisotopes typically are relatively low energy and thus cannot
to a normal organ that also accumulates tracer). Additionally, interfere with detection of the relatively high-energy 511 keV
for single-photon imaging agents, SPECT often requires a photons of PET radiopharmaceuticals. A few non-PET radio-
significantly longer duration scan than a 2D planar scan using isotopes do emit high-energy photons at or above the 511 keV
standard SPECT camera systems, and often 2D imaging may range, but even the presence of these high-energy photons from
be sufficient for the clinical data desired. The necessity for a prior non-PET radiopharmaceutical injection do not neces-
SPECT imaging is guided by the reason for a particular exami- sarily preclude immediately performing a PET study. Because
nation, available clinical research, and the particular patient the high-energy photons of the non-PET radioisotope are not
context. For PET, by definition, tomography (3D imaging) is produced as pairs, these photons will strike PET detectors in
always used, involving ring-type dedicated PET camera systems random directions. The PET scanner, however, will ignore
with sophisticated signal analysis algorithms (discussed later). photons that are not detected in the coincidence pattern typical
For a brief time, planar (2D) imaging and even 3D imaging of annihilation photon pairs. As such, the PET scanner often
with single-photon emission with PET radiopharmaceuticals can detect the desired PET radiopharmaceutical signal without
(e.g., FDG) were explored by using gamma cameras, which are significant interference from any residual non-PET radiophar-
still standard for nuclear imaging with gamma-emitting (non- maceutical in the patient’s system. The opposite, however, is
PET) radiopharmaceuticals. However, gamma camera imaging not the case: residual PET radiopharmaceutical will interfere
of PET radiopharmaceuticals is clearly inferior diagnostically with detection of another PET or a non-PET radiopharmaceu-
and not state-of-the-art practice. tical until a certain number of half-lives elapse. The referring
clinician ordering two or more diagnostic imaging nuclear
“Can I Order Two Nuclear Medicine Scans medicine scans for a single patient in a short period must be
on the Same Day?” aware of this potential problem of “conflicting” radioisotopes
The distinction between positron-emitting (PET) and solely and should consult with an imaging specialist or others expe-
gamma photon–emitting (non-PET) isotopes is relevant for rienced on how best to schedule and prioritize the different
referring specialists primarily because of this question, fre- scans, if uncertain.
quently posed to nuclear medicine specialists or their schedul-
ing staff. Unlike positron-emitting radioisotopes, the gamma
Advantages of Positron Emission Versus
ray–emitting isotopes of radiopharmaceuticals used for single- Single-Photon Imaging
photon imaging come in a variety of energy levels. Gamma The advantage of PET imaging versus single-photon gamma
cameras can distinguish and potentially use these energy levels imaging is that the PET coincidence-detection method permits
to separate the biodistributions of one radioisotope from more precise determination of where the radiation originated.
another, if a patient were to receive two radiopharmaceuticals Thus, the scan imagery reconstructed from PET data has a
with different radioisotopes simultaneously; that is, by having much better spatial resolution (typically 4-5 mm, vs. <1 mm on
the camera only accept detected photons of the energy level CT) than that reconstructed from single-photon gamma data
characteristic of the particular radioisotope of interest, then (typically 12-15 mm). According to the Nyquist principle, this
doing the same for the other radioisotopes. However, the energy superior resolution results in PET-acquired data providing
emissions of different single-photon imaging radioisotopes can superior quantification of radioactivity concentrations in imaging
overlap, particularly if one of the radioisotopes emits relatively data analyses compared with single-photon imaging. As one
high-energy emissions, because some emitted rays will lose potential advantage versus PET imaging, single-photon imaging
energy and fall into the energy (keV) range of the other radio- can simultaneously detect and distinguish two or more different
isotope. The 511 keV coincidence gamma rays of PET radio- gamma-emitting radiopharmaceuticals in a single patient in
pharmaceuticals are relatively high energy and will interfere
with imaging of single-photon radiopharmaceuticals, whether
to a significant degree depends on other technical factors. Thus,
after a PET scan, some period of delay is necessary, to allow *Physical half-life is an intrinsic property of the radioisotope: the rate at which it
undergoes its nuclear decay. For example, for an amount of radioisotope in a
the PET radiopharmaceutical to undergo physical decay and bottle, after one physical half-life, there will be half as much radioisotope (half as
biologic clearance from the patient, before performing another much radioactivity) remaining in the bottle. Biologic half-life is a PK parameter:
the rate at which the patient’s body clears a (radio)pharmaceutical (e.g., by
imaging study with a single-photon radiopharmaceutical or urination/defecation). Thus, after a patient receives a dose of radiopharmaceuti-
another PET radiopharmaceutical. cal, the rate at which it disappears from the body is determined by a combination
For example, for the common radiopharmaceutical, 18F of the physical half-life and the biologic half-life, called the effective half-life. After
10 physical half-lives of 18F (~19 hours), more 18F FDG will have disappeared
FDG, our institution allows a subsequent different nuclear from a patient’s body than predicted by physical half-life alone, because 18F FDG
imaging study typically 20 hours or more after the patient is also eliminated by urinary excretion.
290 PART 2 DIAGNOSTIC TECHNIQUES
vivo, whereas PET imaging cannot distinguish between differ- can vary considerably; it can be of standard diagnostic quality
ent PET isotopes. Gamma rays emitted by non-PET isotopes (i.e., exactly the same technical-quality CT scan as obtained
for single-photon imaging can have a variety of signature energy from a separate, stand-alone, state-of-the-art CT scanner), or it
levels, which can distinguished and separated by signal process- can be of inferior diagnostic quality, sometimes to a great degree.
ing. Single-photon imaging has the added practical advantage The CT scan might be acquired with a lower current (mA),
of being more disseminated and available to clinicians and yielding relatively noisier images, with less detail and greater
patients worldwide. susceptibility to certain artifacts (e.g., beam hardening). Chest
In general, PET imaging is less available because of the imaging may be acquired at pulmonary end expiration rather
higher costs of imaging hardware and the need for access to an than the standard maximal pulmonary inspiration. The CT scan
institutional or commercial source of PET isotopes, which must might be acquired with the patient’s upper extremities posi-
be local due to the short half-life of isotopes such as 18F (~2 tioned along the torso if the patient cannot tolerate having the
hours). However, the PET infrastructure is rapidly growing arms raised (the standard chest CT position) for the 15 to 25
worldwide. Currently, an estimated 80% of the US population minutes of a standard torso FDG PET/CT. In this position, the
is within the service area of a PET imaging facility. arms are “in the way” of the CT current and can reduce the
Policies of regulatory agencies also can pose obstacles to quality of the torso CT images obtained. Also, the CT scan
patient access to nuclear medicine procedures, both general and might not use the oral or intravenous iodinated contrast material
specific. For example, cancer patients in certain parts of Europe routinely used in standard CT protocol. Acquiring this relatively
overall have access to a wider range of PET tumor-imaging inferior-quality CT scan is in fact common clinical practice,
agents than US cancer patients. The U.S. pharmacopoeia of often acquired intentionally, even possibly using a hybrid CT
these agents is essentially one agent, the FDA-approved and scanner fully capable of acquiring standard diagnostic-quality
widely available FDG. Many other PET tumor-imaging agents CT scans. It is usually done, for example, if the patient already
are used clinically in the United States, but essentially only at had a recent diagnostic-quality CT scan. In that case, a com-
select few medical centers, under the auspices of FDA-approved panion lower-dose, noncontrast companion CT may be suffi-
Investigational New Drug (IND) applications that detail the cient to the basic needs of the PET or SPECT scan. In synergic
specific conditions under which the PET agents will be used fusion imaging particularly, a “nondiagnostic” companion CT
and for a prespecified number of patients. Moreover, synthesis usually (but not always) provides sufficient anatomic detail to
of these IND-sponsored PET radiopharmaceuticals must meet identify what tissues are involved in radiotracer uptake within
stringent FDA regulatory standards that only certain commer- an organ and provides attenuation correction, a modification of
cial entities and few medical centers have the capacity to meet. the scintigraphic data based on tissue densities and depth
In certain European countries, regulatory standards regarding measured by CT that improves scintigraphic image quality,
radiopharmaceutical synthesis for human use recognize the especially for quantification (e.g., for PET quantitative mea-
inherently low-risk nature of administering microgram amounts surements known as the standardized uptake value [SUV]).
of radiopharmaceutical compounds and are relatively less Decay photons emitted from within deeper or denser body
stringent than US standards. tissues will lose more energy from tissue interactions than
photons from superficial or less dense tissues. The attenuation
Fusion Imaging correction attempts to account for that artifact to provide more
Scintigraphic imaging of PET and single-photon emission accurate measurement of tissue tracer concentrations.
radiopharmaceuticals is often combined with computed tomog- In essence, the nondiagnostic companion CT scan is a
raphy (CT) imaging, for fusion imaging: PET/CT and SPECT/ blurry image; some images might have a slight blur, and the
CT, respectively. In fusion imaging, the 3D imagery of PET or reader still can identify subcentimeter tissue structures (e.g.,
SPECT is combined with CT data so that tracer biodistribution/ small pulmonary nodules), whereas others might be fairly
localization is visualized within the internal anatomy. Clinical worthless (e.g., whole subregions of the body may be affected
studies have overall demonstrated that fusion imaging can have by beam-hardening or other CT artifact). The physician who
a synergistic effect on the accuracy of scintigraphy and CT image orders a fusion PET/CT or SPECT/CT must know whether
analyses for various clinical applications. A notable general the companion CT is of diagnostic quality or must be specifi-
example is improved accuracy for detection of radiotracer-avid cally ordered to be a diagnostic-quality CT scan, or whether a
tumors; often, on fusion imagery, scintigraphy (PET or SPECT) diagnostic-quality CT scan must be obtained separately. Simi-
highlights findings poorly detected or easily overlooked on CT, larly, the imaging specialist providing a PET/CT or SPECT/
or vice versa. The CT information also serves as data for an CT report can assist the referring physician by stating whether
important technical function, called attenuation correction, which the companion CT is considered equivalent to a standard
improves the quantitative accuracy of measurements derived diagnostic-quality CT scan. The imaging specialist often will
from PET or SPECT analyses. Fusion imaging has done much describe companion CT findings, even in a poor-quality
to rescue diagnostic nuclear medicine from its former moniker nondiagnostic companion CT, if relevant CT findings are
(deserved or not) of “unclear medicine.” detectable; however, the referring physician should not con-
In state-of-the-art practice, a SPECT or PET scanner is clude that the presence of CT findings described in a fusion
physically joined to a CT scanner so that the CT scan is PET/CT or SPECT/CT report means that CT used was of
acquired immediately before the scintigraphic imaging, without diagnostic quality. In our experience, the quality of the com-
the patient changing position, laying on the scanner bed as it panion CT varies considerably between medical centers and
passes within the conjoined central tunnel of the hybrid scanner. between fusion scanner models. The referring clinician is
One important caveat remains regarding the CT scans advised to assess the quality of the companion CT when evalu-
involved in fusion PET/CT and SPECT/CT imaging: the ating the results of a fusion imaging study, particularly if the
companion CT scan. The quality of the companion CT image study was performed at an outside facility.
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 291
Beyond the companion CT scan, first-generation clinical imaging (e.g., tumor detection) or incidental findings (e.g.,
PET/magnetic resonance imaging (MRI) and SPECT/MRI pneumonia in a patient referred for tumor detection). Various
camera systems are already available at a few major medical pathologies may have a similar scintigraphic appearance with a
centers and will begin disseminating to other medical centers particular radiopharmaceutical. For example, a patient with
during the next 10 years. At this point, clinical experience is cancer referred for tumor detection by nuclear scintigraphy may
relatively scant, with published clinical research predominantly have a nodular, noncancerous lesion that avidly accumulates a
focused on technical validations and optimizations of the radiopharmaceutical, appearing as an abnormal focus of radio-
companion MRI. activity in the patient’s body, mimicking a cancerous tumor.
The diagnostic specificity of nuclear scintigraphy varies
“Are All PET and SPECT Scanners Created Equal?” according to the radiopharmaceutical used, the disease entity
How does one know if one’s medical center has a state-of-the-art or biologic process being assayed, and the pretest likelihood of
PET or SPECT scanner? Currently, fusion PET/CT and false-positive results. For example, specificity of FDG PET is
SPECT/CT scanners are the state of the art. The medical lit- lower for patients who live in areas where tuberculosis (TB) is
erature indicates that the diagnostic accuracy of fusion imaging endemic; TB lesions absorb FDG and can mimic tumor sites
for tumors that is derived from a physically integrated, hybrid on FDG PET. The specificity of conventional hepatobiliary
PET/CT is superior to the diagnostic accuracy of combined scintigraphy for detection of gallbladder cystic duct obstruction
reading of PET and CT data obtained from separate scanners, (in the context of suspected cholecystitis) is lower for patients
even if fused by software. Each year now, new models of com- who do not fast properly for the procedure. Obstruction is
mercial PET/CT scanners enter the marketplace. excluded on scintigraphy if the radiopharmaceutical, after
There is some support for the belief that these innovations hepatobiliary excretion, is detected filling the gallbladder
improve patient care. For example, clinical research shows that lumen (having entered via cystic duct). However, normal
modern iterative methods are superior to older, filtered back- digestive processes associated with recent feeding trigger physi-
projection methods for reconstruction of PET images, in terms ologic contraction of the gallbladder, creating a pressure gradi-
of the ability of imaging specialists to detect tumor sites. Oth- ent through the cystic duct that prevents excreted-radiotracer
erwise, the benefits are theoretic but tenable, robustly supported from filling the gallbladder. The absence of gallbladder
by data models and phantom studies. filling caused by physiologic processes mimics a pathologic
cystic duct obstruction (e.g., caused by cystocholelithiasis) on
PHARMACOLOGY AND BIOLOGY IN scintigraphy.
RADIOPHARMACEUTICAL IMAGING Radiation Dose in Nuclear Medicine
Radiopharmaceuticals constitute a large pharmacopoeia of When administered solely for diagnostic imaging, conventional
different radioactive agents used for imaging, radiotherapy, or radiopharmaceuticals expose the receiving patient to a low
both (theranostic agents). An administered dose of a typical radiation dose, typically one or more orders of magnitude below
diagnostic nuclear imaging agent typically contains a trace the level of radiation exposure conventionally accepted as being
(microgram) amount of molecular compound with no expected associated with an increased risk of harmful radiation effects,
biologic effect and minimal risk of toxicity; this is labeled with based on decades of dosimetric research. Certain radiopharma-
isotope that emits radiation suitable for imaging. FDA-approved ceuticals are administered at relatively high doses of radioactiv-
radiopharmaceuticals, administered in standard diagnostic ity with therapeutic intent; the administered radioactivity is
imaging doses, expose patients to levels of internal irradiation sufficiently high (and concentrates in body tissues at levels
considered low by radiologic safety standards. sufficient) to induce acute radiobiologic effects on diseased
As with other pharmaceuticals, each radiopharmaceutical tissues and other organs within a patient, with potential thera-
is distinguished by its pharmacologic profile (e.g., route peutic benefit as well as adverse side effects.
of administration/bioavailability, metabolism, biodistribution, The radiation dose absorbed by the patient from the radio-
pharmacokinetics), including potential interactions with other pharmaceutical is determined by the specific type of radioactive
drugs or substances. Sometimes, a particular diagnostic nuclear isotope involved, the administered activity (amount) of radio-
imaging study may require special patient preparation, hours pharmaceutical (quantified in becquerels, typically megabec-
or days before the radiopharmaceutical is administered; for querels [MBq], or curies, typically millicuries [mCi]), and the
example, patients may need to abstain from certain over-the- pharmacokinetics and distribution of radiopharmaceutical
counter or prescription drugs that may affect the in vivo throughout the body (biodistribution), which is again deter-
behavior of a certain radiopharmaceutical. Patient preparation, mined by the physicochemical characteristics of the radiophar-
when necessary, is specific to the particular radiopharmaceuti- maceutical molecule (or element).
cal employed in the nuclear imaging study. The oncologist
unfamiliar with a particular study should contact an imaging DIAGNOSTIC NUCLEAR IMAGING IN
specialist for information on patient preparation. HEPATOPANCREATOBILIARY ONCOLOGY
The expertise of the nuclear imaging specialist lies in his or
her in depth knowledge of the diversity of the nuclear medicine Radiopharmaceuticals localize to tumors according their physi-
pharmacopoeia (e.g., in vivo bioavailability, metabolism, biodis- cochemical molecular properties and route of administration
tribution) of each radiopharmaceutical and the variety of condi- (e.g., intravenous, oral). These factors also dictate the distribu-
tions under which these may be altered from the norm (e.g., tion of the radioactive compounds throughout the rest of the
pathologic conditions, normal variations in patient physiology, body (biodistribution) and their clearance from the body
interactions with endogenous or exogenous substances). Patho- (almost always involving urinary and hepatobiliary excretion).
logic conditions may include the indication for diagnostic Only a few radiopharmaceuticals with oncologic applications
292 PART 2 DIAGNOSTIC TECHNIQUES
are relevant to and frequently used in patients with HPB cancer staging, therapy evaluation) as well as clinical applications
care, where state-of-the-art nuclear medicine practice is avail- unique to nuclear imaging (e.g., tumor pharmacokinetics and
able, with significant variation in the availability of specific biologic phenotype, disease prognosis, biomolecular pharmaco-
radiopharmaceuticals between countries, predominantly for dynamics, drug biodistribution). These unique clinical applica-
economic and regulatory reasons. tions are specific to particular radiopharmaceuticals and cancer
The complete pharmacopoeia of radiopharmaceuticals types; in HPB cancers, these unique applications remain inves-
includes those that have no oncologic clinical application but tigational, although in certain non-HPB cancers, particular
that are important in the general medical care of patients with examples have become routine clinical practice, such as use of
HPB cancer (e.g., preoperative myocardial perfusion imaging, FDG PET to characterize residual soft tissue masses in lym-
“nuclear stress test”). This section focuses on oncology-specific phoma or germ cell tumors as viable tumor or nonviable treated
applications of diagnostic and therapeutic nuclear medicine for disease.
clinical management of HPB cancers. Ongoing cancer imaging research is exploring nuclear
Diagnostic radiology in general has vital clinical applications imaging for clinical applications of tracking the distribution and
in the care of patients with HPB cancer, notably tumor detec- pharmacokinetics of radiolabeled cancer drugs inside living
tion; disease staging; treatment planning; and evaluation of patients (in vivo) by scintigraphy (particularly by PET imaging),
tumor response to various forms of anticancer treatment. For allowing clinicians to follow cancer drugs in vivo to evaluate
radiologic imaging intended for these primary clinical applica- drug uptake and retention or clearance by tumors and organs.
tions, major HPB oncology guidelines recommend use of Providing unprecedented pharmacokinetic data about the
standard CT (see Chapter 18), MRI (Chapter 19), and/or ability of cancer drugs to target tumors, such novel scintigraphic
ultrasound (US; Chapter 15) for radiologic evaluation of HPB assays may expand the oncologic applications of nuclear
cancer patients (National Comprehensive Cancer Network imaging to guiding patient selection, dosing strategy, and
[NCCN], 2015). These guidelines do not provide a standard role response assessment (Dunphy & Lewis, 2009). This chapter
for diagnostic nuclear medicine imaging (e.g., PET), except for concentrates on the role and efficacy of state-of-the-art diag-
a few minor specific applications. CT, US, and MRI, as well as nostic nuclear imaging techniques and technology, with pre-
plain radiography, are superior to nuclear medicine imaging views of new nuclear imaging agents in development.
modalities for definition of anatomy. Nuclear medicine imaging
is the preeminent clinical imaging modality for evaluation in Fluorodeoxyglucose Positron Emission Tomography
vivo physiology and molecular biology in general. We sometimes In the past 15 years, FDG PET has rapidly emerged as a revo-
state that PET/CT is superior to CT, which is not the same as lutionary imaging modality in clinical oncology, demonstrating
stating PET is superior to CT (noting again, however, that the diagnostic efficacy in tumor staging and tumor-response evalu-
CT of PET/CT often is of lower quality than standard CT), ation for histologies across the spectrum of cancer. FDG,
In general, HPB cancer guidelines recognize the potential 2-deoxy-2-(18F)fluoro-D-glucose, is an analogue of glucose;
value of FDG PET/CT imaging as a diagnostic adjuvant, if fluorine-18 occupies the molecular 2′ position in which a
first-line radiologic imaging (CT, MRI, US) yields indetermi- hydroxyl group is found in glucose (Fig. 17.1). The substitution
nate results. Importantly, the guidelines do not endorse a affects the metabolism of FDG compared with glucose. In vivo,
standard role for FDG PET as a first-line imaging modality, intravenous (IV) FDG extravasates into tissues, followed by its
often because clinical research regarding the added value of uptake into tissue cells by glucose transporter proteins. Blood
FDG PET in these major applications in HPB oncology is FDG concentrations decrease to relatively low levels 45 to 90
simply insufficient, not because clinical trials have already minutes after injection; at this point, further FDG uptake in
shown that FDG PET has no such value. Moreover, PET/CT most tissues is relatively minor, and after that time, FDG
technology and methodology have undergone considerable concentrations in most tissues and tumors remain relatively
evolution, improving diagnostic accuracy significantly in recent stable. Acquiring a single FDG PET scan, beginning 45 to 90
years, and these remain in flux. Recent clinical research, as minutes after injection, has become the standard clinical
discussed here, may prompt future revisions of HPB oncology approach. Usually, as for HPB cancer imaging, the scan spans
guidelines. from “eyes to thighs,” including the entire head or extremities
only if there is a patient-specific clinical reason.
Nuclear Oncology After FDG enters the cell, intracellular hexokinase converts
Broadly, oncologic applications of nuclear imaging include FDG to FDG-6-phosphate, making it too polar to traverse the
those common to CT, MRI, and US (tumor detection, disease cell membrane. In most cells, this traps the tracer, in the form
OH OH
O O
HO HO
HO HO
18F
OH
OH OH
FIGURE 17.1. Molecular structures of glucose (left) and fluorine-18 fluorodeoxyglucose (right).
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 293
of FDG-6-phosphate, intracellularly. After phosphorylation of the same as the glucose metabolism of normal cell counter-
FDG, the product FDG-6-phosphate is not metabolized further parts). The Warburg hypothesis, however, is outdated: the shift
to other forms, to any relevant degree, and will not become a of glucose metabolism from the mitochondrial TCA cycle to
substrate for the enzymes that use glucose-6-phosphate (G6P) cytosolic glycolysis is not an inefficient use of glucose; rather,
as a substrate. One notable exception is G6P in the hepatocytes it is a “repurposing” of glucose. In multiple cell lines, abnormal
of normal liver tissues. FDG-6-phosphate is converted back to cytosolic glycolysis has become understood as advantageous to
FDG to a detectable degree, and the nonpolar FDG can then cancer cell proliferation. Cytosolic glycolysis yields fewer ATP
potentially diffuse back across the plasma membrane, leaving molecules, but it yields glucose-derived metabolites during the
the hepatocyte and, possibly, the entire liver. Clinical FDG multiple intermediate steps of glycolysis that the cell can use in
PET demonstrates this, as liver concentrations of FDG begin other anabolic pathways as components for synthesizing mac-
to decline approximately 1 hour after injection. In other healthy romolecules necessary for building cellular biomass before cell
tissues, dephosphorylation and cellular efflux of FDG is rela- division and tumor growth. To meet the bioenergetic needs of
tively minor. In most tumor types that have been studied at two these cells, instead of predominantly relying on glucose, these
or more delayed time points after injection, FDG appears cells depend on other nutrient molecules, notably glutamine,
effectively trapped. In tissues affected by infectious or inflam- to fuel the TCA cycle (Wise & Thompson, 2010).
matory disease, on the other hand, tissue concentrations of The Warburg effect explains the avidity of tumors for FDG,
tracer reportedly often decline significantly with time, similar the glucose analogue, when visualized by PET, but only in part.
to liver, beginning approximately 1 hour after injection. This PET visualizes the FDG-avidity of tumors at the macroscopic
suggests that detecting FDG efflux in suspicious FDG-avid tissue level (again, with spatial resolution of ~4 mm). The
tissues by PET imaging at two or more delayed time points may “FDG-avid tumor” visualized by PET and described in PET/
be a radiologic biomarker for distinguishing FDG-avid inflam- CT reports represents a complex composite of FDG avidities
matory tissues (e.g., infected tissues, posttreatment inflamma- of tumor cells and nonneoplastic cell constituents within the
tory tissue infiltrates) that can mimic FDG-avid tumor (i.e., tumor internal microenvironment, under the influence of
false-positive PET results) from true FDG-avid tumor. The complex biomolecular and other processes. Detected FDG
clinical reports testing this hypothesis are somewhat inconsis- avidity in a particular tumor often does primarily represent
tent, however, and clinical research remains ongoing; at present, tumor cell FDG-avidity (i.e., the sum of FDG-uptake from all
FDG PET imaging at a single time point is the norm. tumor cells within the tumor), more than the FDG-avidity of
The basic rationale for using FDG PET for tumor detection other cells in the same tumor. However, the FDG avidity of
is the observation that neoplastic cells often (but not always) other constituents of the tumor microenvironment sometimes
accumulate FDG more than the nonneoplastic cells of origin, contributes a clinically significant degree, particularly in the
and that the difference in FDG concentration between the posttreatment setting, potentially causing diagnostic confusion,
tumor and surrounding normal tissues in an organ is detectable as discussed. Within the neoplastic cell, FDG avidity can be
by PET. This avidity of tumors for FDG manifests on PET induced by oncogenic mutations changes directly or indirectly
imagery as a “hot spot,” or a focus, of FDG accumulation that affecting glucose metabolism. For example, oncogenic muta-
is of abnormally high concentration relative to other, healthy tions that drive cell proliferation, typical of aggressive tumors,
tissues. often are associated with the shift of glucose metabolism to
Why do many tumors concentrate FDG so avidly, and why cytosolic glycolysis and increased glucose consumption; tumor
are other tumors not so avid? The physician-scientist and Nobel cell FDG avidity can also be increased by epigenetic metabolic
laureate Otto Warburg long ago observed in multiple tumor cell changes induced by conditions in the tumor microenvironment
lines that he studied an abnormally high rate of glycolysis in (e.g., tumor hypoxia). In certain cases, overall tumor FDG-
cancer cells compared with their normal cellular counterparts, avidity can be caused, in relatively large part or even primarily,
even in the presence of normal levels of oxygen. In normal cells by tumor cellular constituents other than the neoplastic cells,
with adequate environmental oxygen, glucose metabolism is such as infiltrating inflammatory cells, especially when the
typically directed into the mitochondrial tricarboxylic acid tumor cells do not have intrinsically high FDG avidity and
(TCA) cycle; glucose–TCA cycle metabolism yields the when inflammatory cells are present in relatively high tissue
maximal amount of energy substrate (adenosine triphosphate, concentrations. For example, inflammatory cells can accumu-
ATP) from each glucose molecule metabolized for meeting the late around the necrotic cores of tumors before treatment and
bioenergetic needs of the cell. The TCA cycle depends on can infiltrate heavily throughout tumors after treatment. Stan-
oxygen to function; in normal cells, if environmental oxygen is dard FDG PET guidelines often advise that posttreatment PET
low, glucose metabolism instead occurs in the cytosol by an be deferred for 6 to 8 weeks after chemotherapy and 2 to 3
oxygen-independent glycolytic process that yields much less months after radiotherapy. It was empirically observed in clini-
ATP per glucose molecule. In cancer cells, however, Warburg cal PET trials that successfully treated tumors often demon-
observed that glucose metabolism occurred predominantly by strate apparently suspicious residual FDG avidity in the first
glycolysis in the cytosol, regardless of whether or not the tumor few weeks after treatment because of inflammatory cells infil-
cells were well oxygenated. This preference of tumor cells is the trating the treated tumors, presumably to clear the necrotic/
Warburg effect. According to the Warburg hypothesis, cancer cell apoptotic debris associated with successful treatment.
metabolism of glucose was inefficient because it yielded fewer Whenever using PET to characterize or localize tumors,
ATP molecules per glucose cell; and this inefficiency was caused the oncologist (and imaging specialist) should be aware
by a defect in the mitochondrial metabolism of cancer cells. of key factors that affect the apparent FDG avidity of a
The Warburg effect remains a valid observation, although not tumor and the diagnostic sensitivity of FDG PET: tumor size;
a universal phenomenon among all cancer cell lines and types cancer treatment(s); and background organ FDG avidity. As
(i.e., glucose metabolism of some cancer cell lines is essentially the Nyquist principle indicates, the apparent FDG avidity of
294 PART 2 DIAGNOSTIC TECHNIQUES
subcentimeter tumors will be underestimated, because such during therapy have frequently predicted favorable clinical
small lesions fall below the spatial resolution of PET technol- outcomes, whereas stable or increasing FDG avidity portend
ogy. It is still possible for PET to detect a subcentimeter tumor, worse outcomes across a variety of cancers. Evaluation of
if the tumor is so FDG avid that the FDG accumulation in tumor FDG avidity, after cytotoxic therapy without a pretreat-
tumor is detectably higher than that in background tissues of ment PET study for comparison can be performed but can
the organ involved. Frequently, however, subcentimeter tumors yield potentially confusing findings; for example, reactive
lack apparent FDG avidity and may be reported as “too small lymph nodes and partially treated metastatic adenopathy can
to characterize by FDG PET.” have similar appearances on PET (heterogeneous nonspecific
Cancer treatments, depending on action and efficacy, also FDG avidity). Tumors may have marked residual FDG avidity
affect apparent tumor FDG avidity (Liu et al, 2006). Tumor after treatment, which may provoke concerns about tumor
FDG avidity represents the sum of the FDG avidity of constitu- resistance. However, if a pretreatment FDG PET had been
ent tumor cells. Various studies indicate FDG PET is unable obtained, the residual FDG avidity might have been observed
to detect microscopic residual disease; for example, a partially as a marked decrease from baseline tumor FDG avidity, sug-
treated tumor containing FDG-avid cells may be of macro- gesting a favorable tumor response. In other words, the change
scopic size on CT or MRI, but contains a depleted cell popula- in tumor FDG avidity before versus after treatment can be
tion with a sum FDG avidity that appears minimal to nil on more predictive of tumor response than merely the posttreat-
PET imagery. For staging, FDG PET is expected to be less ment FDG avidity alone. As mentioned, certain tumor histolo-
accurate after therapy than before therapy (Liu et al, 2006). gies seem frequently to lack FDG-avidity, despite the presence
FDG PET can also be false positive, detecting FDG uptake at of viable, macroscopic neoplastic disease. A lack of tumor
a former tumor site in the absence of residual disease. With FDG avidity on a posttreatment PET scan can be potentially
systemic therapy, residual FDG uptake may indicate inflamma- misleading as an indicator of tumor response, unless a pretreat-
tory cells (extremely FDG avid, when active) infiltrating tissues ment PET scan has demonstrated the tumor being treatment
to remove the debris of treated disease. Radiotherapy and was originally FDG avid.
surgery, for tumor treatment or resection, both evoke local
tissue inflammation that can be greatly FDG avid, mimicking Colorectal Cancer Metastasis to Liver
local residual or recurrent neoplastic disease on PET imagery. The most recent guidelines from NCCN (2015), European
FDG PET is usually deferred for several weeks after surgery or Society of Medical Oncology (ESMO) (van Cutsem et al,
radiotherapy, when evaluation for local disease is desired. 2014), and European Registration of Cancer Care (EURECCA)
Certain organs and organ systems have marked FDG avidity agree on the potential roles and limitations of FDG PET/CT
consistently or variably that may exceed that of primary tumors in clinical management of colorectal cancer (CRC) (van de
and metastases, obscuring tumor detection. The brain is con- Velde et al, 2014). This discussion focuses on the CRC patient
sistently FDG avid because it normally depends glucose with potentially resectable liver metastases.
metabolism; FDG PET has limited sensitivity for detection of In cancer patients with liver metastases, but no extrahepatic
brain metastases. Myocardium, skeletal musculature, adipose metastases, complete resection of liver metastases improves
tissues, adrenal glands, and alimentary tract tissues have vari- long-term survival better than other treatments currently avail-
able FDG avidity that may or may not interfere with PET able (see Chapter 92). Before surgery, it is essential to confirm
analysis. Bone marrow can have high levels of FDG avidity, that liver metastases are likely resectable (based on CT and/or
usually associated with a hematopoietic response to ongoing or MRI imaging) and that no extrahepatic metastatic disease is
recent systemic cancer therapy or marrow stimulants (e.g., present. In the search for CRC metastases, metastatic disease
GCSF). When evaluation of osseous structures is vital, experts is detected most often in the liver, followed by the lungs;
advise deferring FDG PET for several weeks after the last dose metastases in central nervous system, bones, adrenal glands,
of systemic therapy or marrow stimulant, to allow marrow and spleen occur in less than 10% of CRC patients (Kemeny
effects and associated FDG avidity to subside. FDG is excreted et al, 2014).
through the urinary tract; the radioactive signal from excreted- For CRC staging, FDG PET/CT is currently considered a
FDG in the collecting systems typically obscures PET evalua- diagnostic adjunct to dedicated structural CT and MRI, which
tion of the kidneys and urinary bladder. The liver, lungs, and remain primary and indispensable imaging modalities for their
other tissues have lesser degrees of background FDG avidity superior spatial resolution, providing the most precise structural
that usually do not obscure tumor detection significantly. detail about a patient’s anatomy that can currently be obtained
The diagnostic specificity of FDG PET is limited by the noninvasively, information essential for surgical planning and
existence of other pathologies that demonstrate marked FDG fro evaluating tumor structural response (shrinkage or growth)
avidity, which may mimic neoplastic disease on scintigraphy. to therapy. Despite its inferior spatial resolution, however, FDG
Such etiologies broadly include various types of infectious or PET/CT is often found to be the most sensitive modality for
other inflammatory diseases and hyperplastic or dysplastic detection of colorectal metastases, which radiologically is the
conditions. Certain normal variants in FDG biodistribution or primary determinant of resectable versus nonresectable disease.
a focal accumulation of excreted FDG in the urinary tract may FDG PET/CT had the highest sensitivity for detection of
also mimic an FDG-avid neoplasm. colorectal liver metastases (mean weighted sensitivity of 90%-
Besides tumor detection, for disease (re)staging, FDG PET 92%), with equivalent overall specificity, compared with US,
may be used to evaluate tumor response to cancer therapy. CT, and MRI in a meta-analysis (Kinkel et al, 2002) cited by
Frequently, FDG PET is performed twice, before and after current EURECCA guidelines (van de Velde et al, 2014). It
therapy, for comparison, using changes in tumor FDG avidity should be noted that a meta-analysis from 2002 would include
as an index of changes in tumor cell population size (i.e., CT and MRI techniques that are no longer considered state of
tumor response). Marked decreases in tumor FDG avidity the art. Regardless, FDG PET/CT currently is not considered
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 295
surgical candidates (e.g., due to extent of tumor, underlying concordant with 2015 NCCN guidelines, suggesting a limited,
liver disease, or comorbid conditions). For the patient with an as-needed role for nuclear imaging in liver cancer staging.
unresectable primary or secondary liver malignancy, nuclear One potential rationale for advising no routine role for FDG
medicine offers both diagnostic and therapeutic options. PET in HCC is that HCC tumors can be undetectable (false
Radionuclide therapy with yttrium 90 (90Y)–labeled resin negative) on FDG PET. An untreated, fully viable HCC tumor
or glass microspheres, delivered by hepatic intraarterial cath- mass, easily detectable by CT or MRI, may concentrate FDG
eter infusion as a radioembolization treatment for liver tumors, no more avidly than surrounding normal, nontumorous liver,
has FDA-approved indications for patients with liver-only or and thus the HCC can appear indistinct or invisible on PET.
liver-predominant tumor burden (see Chapter 96B). Soma- In other HCC patients, tumors can demonstrate detectable,
tostatin receptor (SSTR)–targeted radionuclide therapy is a visually distinct FDG-avidity on PET; even in such cases,
treatment for malignant carcinoid tumors, including primary however, the visual intensity of the HCC tumor uptake is only
or secondary liver tumors (and not restricted to liver-only/ mildly or moderately greater than the uptake in the surrounding
predominant disease) (see Chapter 93). Considered investiga- normal liver. Research suggests potential biologic explanations
tional in the United States but more widely available for the typically low FDG avidity of HCC, notably HCC
in Europe, SSTR-targeted radionuclide therapy is discussed overexpression of the enzyme glucose-6-phosphatase (thus
later. inhibiting metabolic trapping of FDG as FDG-6-phosphate,
FDG PET/CT has been suggested as a promising radiologic which is otherwise a poor substrate for glucose-6-phosphatase)
assay for detecting a favorable liver tumor response to 90Y (Torizuka et al, 1995). In particular, well-differentiated HCC
microsphere radioembolization (Kennedy et al, 2012), as well can demonstrate this non–FDG-avid PET phenotype, whereas
as for evaluating hepatic tumor response to other forms of higher-grade HCC tumors more frequently have detectable
treatment. However, current hepatobiliary oncology guidelines FDG avidity (Lee et al, 2004; Torizuka et al, 1995). Therefore,
cite insufficient published clinical evidence to support routine although a lack of FDG avidity may be frustrating from a
use of FDG PET/CT in hepatobiliary tumor-response evalua- diagnostic viewpoint, it also appears to be associated with a less
tion, whether for unresectable or resectable tumors. Standard aggressive tumor and a more favorable patient prognosis
CE CT and MRI are considered indispensable for tumor (Shiomi et al, 2001).
assessment, and FDG PET/CT is still deemed to be of unproven Another potential rationale for advising no routine role for
added value. We expect future guidelines will deem use of FDG FDG PET in HCC is that HCC is usually a liver-limited
PET/CT for evaluation of hepatic tumor “metabolic response” disease. The main clinical impact of FDG PET/CT in other
as appropriate for tumors that demonstrate FDG avidity. types of cancers (e.g., non–small cell lung cancer) is often in
Additionally, FDG PET/CT imaging is currently use within the detecting regional and distant metastases.
interventional radiology (IR) suite (with the scanner located Beyond FDG, separate PET clinical trials with investiga-
physically within the IR suite) of a few major medical centers tional radiopharmaceuticals carbon 11 (11C) acetate (Hwang
as an investigational procedure to assess the effectiveness of et al, 2009) and 11C choline (Yamamoto et al, 2008) provided
percutaneous tumor ablation therapy immediately after abla- preliminary data suggesting that these novel tracers are better
tion, permitting immediate repeat tumor ablation as needed than FDG PET for detection of well-differentiated HCC. At
(Ryan et al, 2013). This technique should gain acceptance as the same time, FDG PET appeared better than both novel
clinical outcome data accumulate. tracers for detection of poorly differentiated HCC, suggesting
Nuclear scintigraphy with a SSTR-targeted imaging agent, FDG PET and either tracer may be complementary options for
notably indium 111 (111In)–radiolabeled octreotide (111In pen- HCC scintigraphy. However, 11C has a physical half-life of only
tetreotide), has potential clinical application in evaluation of 20 minutes, precluding commercial supply of 11C imaging
liver tumors, usually for detection of carcinoid tumors, which agents. To perform patient studies with 11C PET tracers, a
may be undetected by FDG PET. As with FDG PET, 111In medical center must have a multimillion-dollar cyclotron facil-
octreotide scintigraphy is not recommended by consensus ity and radiochemistry expertise to synthesize 11C tracer on site.
guidelines for evaluation of hepatic tumor response, although
it is typically used to predict carcinoid tumor response to Tumor-Response Evaluation
(nonradioactive) therapy with octreotide analogues (discussed As stated, no current major guidelines advocate routine use of
later). nuclear imaging, including PET, for HCC tumor imaging,
including evaluating tumor response to therapy. FDG PET/CT
has become a tumor-response radiologic biomarker with a major
Management of Patients With
clinical impact on the management of a growing number of
Hepatocellular Carcinoma other cancers, now standard for breast cancer, lymphoma,
Initial Presentation (See Chapter 91) esophageal cancer, gastric cancer, and other malignancies. In
Hepatocellular carcinoma (HCC) is detected and characterized these types of cancer, overall robust clinical literature demon-
by US, CT, and MRI in standard practice. NCCN guidelines strates that a therapy-induced decrease in tumor FDG avidity,
(2015) do not provide a role for FDG PET/CT in HCC, as a biomarker of a decrease in tumor metabolism and tumor
without discussion of rationale. NCCN guidelines advise con- cell mass, correlates with histopathologic response and is often
ventional bone scintigraphy with technetium 99m (99mTc)– prognostically powerful, often when conventional changes in
radiolabeled bisphonates, such a methylenediphosphate (MDP), tumor volume (e.g., anatomic criteria such as RECIST) mea-
for staging of HCC patients with suspicious skeletal symptoms. sured by CT or MRI failed to predict either pathologic response
The 2012 European Association for the Study of the Liver or prognosis (Wahl et al, 2009).
(EASL) and the European Organization for Research and Prerequisites for using FDG PET/CT to assess tumor
Treatment of Cancer (EORTC) joint guidelines are generally response to treatment are that the tumor demonstrates FDG
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 297
avidity before treatment, as a biomarker of tumor metabolic PET/CT has reported sensitivity no greater than 90% (usually
activity, and that the FDG avidity is sufficiently high so that much lower) for HCC in the pretreatment setting.
PET can detect a therapy-induced decrease in tumor FDG
avidity, as a biomarker of a prognostically favorable decrease in Cholangiocarcinoma (See Chapters 50 and 51)
tumor metabolism and tumor cell mass. For example, well- Cholangiocarcinoma is the second most common primary
designed PET response criteria called the PERCIST guidelines hepatic tumor. Cholangiocarcinoma is usually an FDG-avid,
(Wahl et al, 2009) define sufficient pretreatment FDG avidity PET-positive disease. A 2014 meta-analysis of 10 studies found
as being tumor FDG avidity (quantified by the standardized that FDG PET/CT, on a per-patient basis, had an overall
uptake value [SUV]) that is greater than 1.5 times higher than sensitivity of 82% and specificity of 75% for detection of
the PET-measured average FDG avidity (SUV) of the individual cholangiocarcinoma, and diagnostic sensitivity was higher for
patient’s liver plus 2 standard deviations (SD) of that average intrahepatic tumors than for perihilar and other extrahepatic
liver avidity (the SD figures automatically calculated by PET tumors (Annunziata et al, 2014). FDG-avid inflammation
analysis software). along the biliary tree (i.e., cholangitis) can mimic or obscure
Whereas other cancer types (e.g., breast, lymphoma) are detection of FDG-avid biliary tumor (see Chapter 43).
frequently FDG avid and PET scan positive, HCC tumors FDG PET/CT appears sensitive for detection of intrahepatic
frequently demonstrate minimal to nil FDG avidity, undetect- and extrahepatic metastases. Although current NCCN guide-
able or barely detectable above the background liver FDG lines state that the role of FDG PET/CT in management of
avidity. For HCC, obtaining FDG PET/CT before any particu- biliary cancers has overall “not yet been established,” these
lar form of treatment would be necessary to establish that the same guidelines also state “emerging evidence from retrospec-
HCC tumor is sufficiently FDG avid for PET-response evalu- tive studies indicates that it may be useful for the detection of
ation, although the cost-effectiveness of such an approach regional lymph node metastases and distant metastatic disease
might be questionable, with a single FDG PET/CT scan rela- in [biliary] cancer patients with otherwise potentially resectable
tively expensive (several thousand 2015 US dollars). Because disease” (NCCN, 2015).
HCC tumors are frequently PET scan negative, many baseline
PET scans with no potential value for evaluating subsequent Focal Liver Lesions
tumor response would be obtained. A cost-effective approach The differential diagnosis of a focal liver lesion, or collection of
may be to find a combination of clinical, histologic, and labora- liver lesions, generally includes tissue entities such as focal
tory blood test biomarkers that reliably predict that a particular nodular hyperplasia (FNH), hepatic adenoma, HCC, fibrola-
patient’s HCC tumor will be sufficiently FDG avid before PET/ mellar carcinoma, regenerative nodules, hemangioma, and
CT. This approach has been demonstrated in FDG PET in metastases (see Chapter 90A). Characterization and usually
prostate cancer, in which blood test biomarkers (specifically, initial detection of liver lesion(s) usually begin with structural
serum PSA-doubling time) predict tumor FDG avidity and imaging modalities: CT, US, and MRI (Agency for Healthcare
PET scan positivity, allowing a more patient-specific, cost- Research and Quality [AHRQ], 2014). Structural imaging
effective application of FDG PET in cancer management characteristics in proper clinical context may be sufficient for
(Schoder et al, 2005). diagnosis (e.g., as with simple hepatic cysts or liver hemangio-
Despite the frequent PET negativity of HCC, a few groups mas). For more solid liver lesions, blood tests may refine the
have demonstrated the ability of PET to evaluate the efficacy diagnosis (e.g., serum α-fetoprotein for suspected HCC), or
of certain types of treatments against FDG-avid HCC tumors, tissue-biopsy may be indicated, if structural imaging character-
such as transcatheter arterial (transarterial) chemoembolization istics are suspicious for cancerous lesions. The role of scintig-
(TACE) (Torizuka et al, 1994). raphy in characterizing liver lesions is typically limited and
confined to second-line imaging (AHRQ, 2014), but it can be
Recurrence helpful in selected cases when the differential diagnosis has
Hepatocellular carcinoma usually arises within a background been narrowed by initial evaluation of the liver lesion by CT/
of liver cirrhosis (of viral or other etiology), and metastatic US/MRI, clinical history, and blood test findings.
disease tends to be entirely or predominantly intrahepatic (see American College of Radiology (ACR) Appropriateness
Chapters 76 and 89). Similarly, recurrence typically manifests Criteria for characterization of newly discovered lesions (AHRQ,
as tumor regrowth at a prior site of treatment (e.g., ablation) 2014) suggest a limited role for nuclear scintigraphy, with CT
or as tumor appearing at a new site in the liver. Hayakawa and or MRI always the preferred initial imaging modality (see Chap-
colleagues evaluated FDG PET/CT for detecting recurrent ters 18 and 19). For a patient with a known extrahepatic malig-
HCC postoperatively in patients with either suspected recur- nancy, if CT or MRI characterizes a liver lesion as indeterminate,
rence on CT or MRI (group 1) or suspected recurrence because FDG PET/CT is considered potentially helpful for further
of abnormal serum tumor markers, but with no disease evident characterization, especially if the patient had a prior FDG PET/
on CT or MRI (group 2). FDG PET/CT had a 53 and 41% CT demonstrating the extrahepatic cancer was FDG avid (pre-
sensitivity and 100% specificity for recurrent tumor in both dicting that the liver lesion, if a metastasis, also would be FDG
groups 1 and 2, respectively. The data from group 1 support avid). Alternatively, radiolabeled SSRT-targeted scintigraphy is
the idea that FDG PET/CT cannot replace CT or MRI as the considered potentially useful if the extrahepatic cancer was a
first-line imaging modality for detection of recurrence; the data known neuroendocrine tumor (NET), particularly if the NET
from group 2 invite the hypothesis that FDG PET/CT may be was viable (e.g., pretreatment) but demonstrated a non–FDG-
of value as second-line imaging if CT or MRI fails to detect avid/PET-negative scan phenotype. FDG PET–negative NETs
recurrence (Hayakawa et al, 2014). Wang and colleagues (2013) tend to be better differentiated and associated with a more
reported a remarkably high sensitivity of FDG PET/CT for concentrated accumulation of SSTR-targeted tracer (see
HCC detection of 97%, with a specificity of 83% (n = 32). FDG Chapter 93).
298 PART 2 DIAGNOSTIC TECHNIQUES
Diagnostic nuclear medicine imaging for cancerous liver than 1.5 cm, which is smaller than the spatial resolution of
tumors most importantly includes the common PET imaging SPECT camera systems; this increases partial volume–averaging
agent 18F FDG, and for hepatic metastases of NETs, SSTR effects that diminish the detectability of tracer uptake by
scintigraphy with the SPECT agent 111In pentetreotide or colloid-avid FNH lesions, amid surrounding hepatic uptake.
68
Ga-radiolabeled octreotide analogues (e.g., DOTA). However, Some FNH lesions, including some greater than 1.5 cm, appear
benign tumors and nonneoplastic lesions can be FDG avid, to accumulate colloid tracer poorly, less than in surrounding
mimicking FDG-avid tumors. Similarly, note that a variety of normal liver, appearing as a focal paucity of tracer uptake,
non-NET cancers can also be avid for SSTR-targeted tracers sometimes referred to as a “cold spot.” Other FNH lesions
(e.g., HCC, prostate cancer, certain types of lung cancer) and accumulate SC equivalent to surrounding normal-liver colloid
possibly certain relevant benign liver tumors as well (see later). uptake, appearing indistinguishable from surrounding liver
Thus, the ACR guidelines advise FDG PET/CT as potentially (i.e., invisible) on 99mTc SC SPECT. The indistinguishable
useful for patients with known extrahepatic primary cancers and uptake of such invisible lesions is sometimes called “warm,”
SSTR-targeted scintigraphy (e.g., OctreoScan) for patients meant to imply that it is neither a hot spot nor a cold spot.
with a known history of NET, both to increase pretest likeli- “Warm” is a vague term likely to be misinterpreted (e.g., as
hood that any FDG avidity or SSTR-targeted tracer avidity meaning uptake that is not “hot” but still faintly detectable as
detected in liver lesions can be ascribed as more likely attribut- above liver-background lesion uptake). We prefer the scinti-
able to tracer-avid hepatic metastases. The improve the posttest graphic term isointense to describe lesion uptake that is equiva-
likelihood of FDG-avid liver lesions representing true-positive lent to and indistinguishable from surrounding normal-liver
liver metastases in patients with a colorectal primary, correla- uptake.
tion with serum CEA levels is useful. The specificity of 99mTc SC SPECT for FNH, using a visible
Certain benign, focal liver lesions (neoplastic and nonneo- hot spot as the diagnostic criterion, is very high; to our knowl-
plastic) are well recognized to concentrate 18F FDG, mimicking edge, no other non-FNH liver lesions (e.g., hepatic adenoma)
the appearance of an FDG-avid cancerous liver tumor (see concentrate SC sufficiently to produce a hot spot on 99mTc
Chapter 90A). Other types of tumors, not of neuroendocrine SPECT. Various non-FNH lesions also can accumulate SC
cell origin, can avidly concentrate the octreotide radiotracer, equivalent to normal-liver colloid uptake. Again, the indistin-
including HCC (variably) (Dimitroulopoulos et al, 2007). The guishable uptake of such “invisible” lesions refers to uptake by
octreotide-analogue radiotracers target SSTRs, particularly 2, lesions that was isointense with surrounding normal-liver
3, and 5. It must be remembered that although SSTRs are uptake.
expressed at high tissue concentrations in NETs, the SSTRs As an alternative to 99mTc SC for scintigraphic detection of
are not mutant, cancer-specific “oncoproteins” or even neuro- FNH, others have tested cholescintigraphy, the use of biliary
endocrine tissue specific. Whether SSTR expression is also high tracers such as 99mTc-radiolabeled disofenin or mebrofenin (see
for the common differential of a focal liver lesion (e.g., FNH) Hepatobiliary Scintigraphy, later). Hepatocytes in the FNH
is unclear. Few reports detail abnormal concentrations of lesion produce bile, as usual, and thus will uptake and secrete
radiolabeled octreotide analogues in benign liver lesions; one these biliary tracers. However, biliary canaliculi within the
described an absence of radiolabeled octreotide binding to FNH lesion are often characterized by disordered drainage
hepatic adenoma, but it would be a non sequitur to infer that connections with the remainder of the intrahepatic biliary tree.
false-positive results do not occur only because no literature As such, the classic (chole)scintigraphic appearance of FNH is
states that they do occur (Reubi et al, 1999). Other data, if abnormal focal accumulation and prolonged focal retention of
available, could hypothetically overturn the conclusions of the a biliary radiotracer. Small studies suggest cholescintigraphy
scant small studies discovered. Therefore, the clinician who has promising diagnostic sensitivity (e.g., 92%) (Boulahdour
wants to order an octreotide tracer scintigraphy scan to char- et al, 1993). Well-differentiated HCC can demonstrate a similar
acterize a hepatic lesion as an NET should consider pretest cholescintigraphic phenotype, as an abnormal focal, prolonged
likelihood and possible use of scintigraphy to guide tissue retention of biliary tracer. Some propose FNH and well-
biopsy confirmation. differentiated HCC differ in cholescintigraphic phenotype,
If structural imaging studies have narrowed the differential suggesting that HCC will usually clear biliary tracer more
diagnosis down to a suspicion of FNH (see Chapter 90A) but quickly than will FNH (e.g., when assessed at 5-10 minutes
diagnostic uncertainty remains, scintigraphy with technetium after injection). Whether cholescintigraphy can reliably differ-
99m–radiolabeled sulfur colloid (99mTc SC) may be useful. entiate FNH from HCC is subject to question, given limited
SPECT imaging with 99mTc SC visualizes FNH as a focus of clinical data. The FDG PET appearance of FNH is variable but
abnormally high SC concentration, attributable to a high typically “mild” or indistinct scintigraphically. FNH can appear
concentration of phagocytic Kupffer cells accumulating 99mTc mildly hypermetabolic (or FDG avid), mildly hypometabolic,
SC within a scintigraphically detectable FNH lesion, with rela- or isointense with surrounding hepatic FDG uptake. In our
tively less colloid accumulation in surrounding normal liver experience, FNH lesions are rarely, if ever, intensely FDG avid
parenchyma. Thus, the FNH lesion manifests as a hot spot on (Kurtaran et al, 2000).
99m
Tc SC SPECT. The sensitivity of 99mTc SC 3D SPECT is Scintigraphic characteristics of a hepatic hemangioma (see
superior to 2D planar scintigraphy (thus SPECT is standard). Chapter 90A), another notable entity on the differential diag-
However, the sensitivity of 99mTc SC SPECT for FNH, using nosis of a hepatic lesion, includes its absence of sulfur colloid
a visible “hot spot” as the diagnostic criterion, is poor, probably uptake, appearing as a cold spot on 99mTc-labeled SC scintig-
approximately 50% to 60%, suggesting that not all FNH lesions raphy, and tracer activity on FDG PET that is equivalent or
have relatively high concentrations of phagocytic Kupffer cells less than cardiac blood pool activity and also generally less than
compared with surrounding liver (Chung et al, 2010). The surrounding liver FDG uptake. Hemangioma also demonstrates
sensitivity is even poorer if the hepatic lesion in question is less a scintigraphic hot-spot appearance on radiolabeled red blood
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 299
cell (RBC) studies. These scintigraphic phenotypes are usually contract, can help identify and separate coexistent pancreatic
distinctly evident for lesions greater than 1.0 to 1.5 cm; smaller disease processes.
lesions tend to blend into surrounding hepatic tracer uptake, While the term intense as a descriptor of hypermetabolic
due to partial volume averaging associated with the limited activity is subjective, the use of a quantitative parameter such
spatial resolutions of PET and particularly SPECT. The liver as the conventional SUV does not appear to improve diagnostic
hot-spot appearance, on 99mTc-labeled RBC scintigraphy, is accuracy and may actually lower it. Moreover, any particular
considered almost pathognomonic for a hemangioma (specific- SUV threshold defined by one medical center’s experience, as
ity ~100%), although case reports do describe other pathologic best separating cancer from noncancer, will not necessarily be
entities (e.g., liver angiosarcoma) also demonstrating a liver applicable to another medical center, considering the technical
hot-spot appearance. Hemangiomas larger than 1.4 cm can differences and lack of mandatory calibrations among the
be detected by 99mTc-labeled RBC scintigraphy with high numerous models of PET/CT scanners. Also, some noncancer-
sensitivity. ous pancreatic lesions (e.g., infectious) will appear more FDG
avid than some cancerous pancreatic lesions (e.g., predomi-
nantly cystic). Assessment of a pancreatic lesion requires con-
DIAGNOSIS AND FOLLOW-UP sideration of the CT appearance of the lesion, for which a CE
OF PANCREATIC DISEASES CT is preferred, for optimal anatomic characterization. If the
lesion is predominantly cystic, one expects that even a cancer-
Pancreatic Cancer (See Chapters 59 and 62) ous tumor may be FDG PET negative, although even solid
Detection noncancerous pancreatic lesions can be as FDG avid as cancer-
For identification of pancreatic cancer, a 2012 meta-analysis of ous solid pancreatic lesions (e.g., benign solid pseudopapillary
16 studies with 804 patients found FDG PET/CT offered a tumor) (Kim et al, 2014). In fact, if a solid tumor has activity
diagnostic sensitivity of 87% and specificity of 83% (Wu et al, close to blood pool activity (i.e., minimal FDG-avidity), it is
2012). The likelihood ratio for a suspicious lesion on PET/CT more likely to be a pancreatic adenocarcinoma or NET than a
was 5.84 (95% CI, 4.59, 7.42) and, if PET was negative, the solid pseudopapillary tumor, which are usually FDG avid
ratio was 0.24 (95% CI, 0.17, 0.33). A 2014 meta-analysis (Guan et al, 2013).
(including much of same data as 2012 analysis) obtained similar Optimal PET/CT analysis therefore appears to be predomi-
results: FDG PET/CT for evaluation of suspected pancreatic nantly a qualitative assessment of CT appearance (cystic or
cancer was calculated to offer pooled sensitivity of 90% and solid), extent on PET (focal vs. diffuse pancreatic FDG-avid
specificity of 76% (Rijkers et al, 2014). disease), and relative intensity on PET (greater FDG avidity
Clinical reports consistently indicate that FDG PET/CT generally increasing suspicion for cancer). However, the diag-
that includes a standard-quality, CE CT scan offers superior nostic accuracy of FDG PET/CT for characterizing a pancreatic
diagnostic accuracy compared with PET/CT performed with a mass as cancer (or not) is limited.
noncontrast, low-mA-dose, “nondiagnostic” CT protocol, with
diagnostic sensitivity of 91% (95% CI, 86%-96%) versus 88% Staging (See Chapter 62)
(95% CI, 78%-100%), and specificity of 88% (95% CI, 73%- Clinical data on the potential added value of FDG PET/CT in
100%) versus 81% (95% CI, 69%-94%), respectively, although staging of pancreatic cancer, beyond that offered by standard
these were not statistically significant differences (P > .05) (Wu radiologic imaging (CT, MRI, US), is considered by standard
et al, 2012). This type of nondiagnostic CT protocol, as men- guidelines to be insufficient to recommend FDG PET/CT as a
tioned, is a standard approach for fusion PET/CT imaging, standard component of pancreatic cancer staging. However,
where the study is primarily performed for the sake of obtaining 2015 NCCN guidelines state “[FDG] PET/CT may be con-
PET data, and a standard CT will be obtained or has already sidered after formal pancreatic CT protocol in high-risk patients
been obtained separately. to detect extra-pancreatic metastases;” high-risk status includes
A variety of noncancerous pancreatic diseases can cause patients with borderline resectable disease, “markedly” elevated
hypermetabolic pancreatic disease, visualized by PET variably serum CA19-9, large primary tumors, or large regional lymph
as focal hypermetabolic lesions or relatively diffusely hyper- nodes (on CT) (NCCN, 2015). The main impact of FDG
metabolic pancreatic disease (Santhosh et al, 2015). Literature PET/CT on pancreatic cancer is to upstage patients by accurate
reports of false-positive FDG PET include noncancerous enti- detection of distant metastases not detected by previous con-
ties such as focal acute and chronic pancreatitis, mass-forming ventional CT or MRI. FDG PET/CT offers an overall diagnos-
pancreatitis, autoimmune pancreatitis, and infectious pancre- tic specificity for metastases typically reported as 90% or higher
atic disease (see Chapters 55 and 57). (Wang et al, 2014) and changed resectability status in more
A focus of qualitatively “intense” hypermetabolic activity in than 20% to 30% of patients in two studies (Bang et al, 2006;
the pancreas, however, has often been reported to have a rela- Chang et al, 2014).
tively high diagnostic accuracy for pancreatic cancerous lesion, One potential limitation of PET/CT for pancreatic cancer
with a sensitivity and specificity of 90% and 93%, respectively, staging is the companion CT, often a low-dose, noncontrast,
in one study (Santhosh et al, 2013). Following the “focal” “nondiagnostic” image. The nondiagnostic companion CT is
criterion strictly can reduce diagnostic sensitivity, if applied often used because it is suitable for providing anatomic localiza-
indiscriminately; for example, a diffuse or extensive hyper tion and attenuation correction of PET data, while exposing
metabolic pancreatitis (e.g., from pancreatic duct obstruction) the patient to less radiation dose (mA) than conventional CT.
can occur with a focal hypermetabolic pancreatic cancerous However, the relatively low mA dose and lack of IV contrast
tumor, with the hypermetabolic disease appearing inseparable make the companion CT truly nondiagnostic for pancreatic
and nonfocal overall on FDG PET. Close examination of the cancer tumor (T) staging (i.e., T designation of standard TNM
companion CT or a recent CT, standard quality with IV classification) (AJCC, 2010). Nonenhanced companion CT
300 PART 2 DIAGNOSTIC TECHNIQUES
often fails to detect vascular invasion (Strobel et al, 2008), and PET/CT for detecting pancreatic cancer response indicates that
PET alone is typically inferior to CT for assessment of size it is superior in general to conventional CT or MRI for predict-
because of its inferior spatial resolution. ing favorable histopathologic response and for predicting
The potential advantage of PET/CT for staging is in detect- patient prognosis (i.e., stratifying patient outcomes). Multiple
ing nodes and metastases (N and M). Available studies to date clinical trials have shown that changes in pancreatic tumor
report a wide range of sensitivity values for FDG PET/CT for hypermetabolic activity, measured by comparing a pretreat-
detection of pancreatic cancer nodal metastases, ranging ment PET scan with a posttreatment or on-treatment PET
from 0% to 57% in a 2014 literature review by Wang and scan, correlated with (predicted) histologic response, radiologic
colleagues. The variation is probably indicative of the small size (CT or MRI) response, or patient response (e.g., overall survival
of the studies cited (n = 14 or less, per study), but suggests or progression-free survival) (Wang et al, 2014). Notably, in
that PET/CT nodal (N) sensitivity is much too low to guide patients with locally advanced unresectable pancreatic carci-
surgical decision making on the necessity and extent of noma (n = 32), Topkan and colleagues (2011) showed that
lymphadenectomy. those with more than average decreases in tumor hypermeta-
For metastasis (M) staging, FDG PET/CT appears to have bolic activity (i.e., SUV parameter) after chemoradiotherapy
relatively high specificity for detection of distant metastases, with 50.4 Gy (1.8 Gy per fraction), 5-fluorouracil (5-FU), and
with specificity values as high as 91% to 100% (Wang et al, gemcitabine enjoyed a superior median overall survival (17.0
2014). For liver metastases, a common site for pancreatic vs. 9.8 months; P = .001), progression-free survival (8.4 vs 3.8
metastases, the reported sensitivity of FDG PET/CT varies months; P = .005), and locoregional progression-free survival
widely between medical centers, from 22% to 88%. Liver (12.3 vs. 6.9 months; P = .02). The predictive value of a favor-
metastases can be subcentimeter, and PET has lesser sensitivity able “metabolic response” on FDG PET/CT remained statisti-
for subcentimeter tumors because of partial volume averaging cally significant for each of these three outcomes on multivariate
(discussed earlier). Also, the normal liver accumulates FDG analysis. Others have reported statistically significant correla-
physiologically. While normal hepatic FDG uptake is usually tions between favorable FDG PET/CT tumor metabolic
considered relatively low in its signal intensity by PET readers response to chemoradiotherapy and favorable survival outcome
(e.g., compared with the intense physiologic accumulations of in unresectable, locally advanced pancreatic cancer as well
FDG in the normal brain or sometimes the myocardium), the (Bang et al, 2006; Chang et al, 2014; Schellenberg et al, 2010).
hepatic uptake is sufficiently high that it can reduce visibility of One study showed similar predictive power of FDG PET/CT
liver metastases, in terms of tumor/background contrast on for treating unresectable disease with chemotherapy (without
PET imagery, particularly for pancreatic tumors that also radiation) (Maisey et al, 2000).
demonstrate relatively low-level FDG avidity. Despite the vari- For resectable pancreatic cancer, FDG PET/CT accurately
ability in reported percentages, clinical studies predominantly predicts histologic response to neoadjuvant chemotherapy with
report that FDG PET/CT seems to perform better than con- gemcitabine and cisplatin, although neither PET response nor
ventional CT for detection of liver metastases, although most histologic response correlated with survival outcomes (Heinrich
were small studies, with fewer than 20 patients, limiting statisti- et al, 2008) (see Chapters 62 and 68). This particular neoad-
cal confidence (Wang et al, 2014). MRI appears to offer juvant treatment was clearly able to eradicate a majority of
superior diagnostic sensitivity for liver metastases compared tumor burden in some patients, but one can hypothesize that
with FDG PET/CT, on a per-lesion basis, particularly for the effect was insignificant compared to the impact of the
detection of subcentimeter liver metastases. subsequent surgery. The neoadjuvant therapy might have had
The sensitivity of FDG PET/CT for detection of distant an impact on residual microscopic tumor burden; both neoad-
metastases in the bones is clearly superior to standard CT. Bone juvant responders and nonresponders had microscopic disease
metastases may be associated with only subtle osteolytic changes after surgery, but the responders had less microscopic disease.
on CT or may be entirely invisible; CT-occult metastases pre- Differences in microscopic amounts of residual disease likely
dominantly involve those infiltrating the bone marrow. MRI is produce survival benefits not easily detected by such a small
at least as diagnostically accurate as FDG PET/CT for detec- study (n = 24). The study results strongly support use of FDG
tion of osseous metastases. Body MRI is not a standard workup PET/CT as an investigational clinical response biomarker in
for pancreatic cancer, whereas FDG PET/CT typically offers a pancreatic cancer. This study demonstrates that FDG PET/CT
torso field of view. At other sites, such as lungs and peritoneum, can noninvasively detect pancreatic cancer histologic response
the diagnostic accuracy of FDG PET/CT appears similar to at the end of neoadjuvant therapy. Future pancreatic cancer
that of standard CT; a dedicated CE CT scan improves PET/ studies should explore whether tumor FDG PET/CT response
CT detection of peritoneal metastases significantly compared early during neoadjuvant therapy predicts subsequent histologic
to PET with a nondiagnostic companion CT. response at the end of neoadjuvant therapy, as demonstrated in
For radiation therapy planning with an image-guided other cancer types. FDG PET/CT appears to be an excellent
intensity-modulated approach, FDG PET/CT assists in optimal noninvasive biomarker for identifying ineffective pancreatic
contouring of the radiation field, better defining pancreatic cancer neoadjuvant therapy and might be used to identify poor
gross tumor volume and pathologic adenopathy, in conjunction tumor response early during treatment, avoiding needless
with dedicated structural imaging (CT or MRI), than possible neoadjuvant toxicity and enabling alternative neoadjuvant regi-
with structural imaging alone (NCCN, 2015). mens to be pursued.
Pancreatic cancer recurrence can be detected by elevation
Pancreatic Tumor Response and Recurrence of serum levels of the tumor marker with high diagnostic sen-
NCCN guidelines do not currently advise a role for FDG sitivity; but serum assays do not distinguish the anatomic
PET/CT in evaluating tumor response to chemotherapy or location of the disease recurrence (e.g., in a tumor resection
radiotherapy. However, a review of the potential role of FDG bed or as new metastases). A few small studies indicate that
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 301
positively charged amino acids is mandatory in PRRT (Bodei BOX 17.1 Clinical Indications for Hepatobiliary Scintigraphy
et al, 2003).
Recent approaches to improve antitumoral efficacy include 1. Functional biliary pain syndromes in adults
combining treatment approaches, such as PRRT with radiosen- 2. Functional biliary pain syndromes in pediatric patients
3. Acute cholecystitis
sitizing chemotherapeutic agents (e.g., camptothecin, gem-
4. Right upper quadrant pain variants
citabine, 5-FU or its prodrug capecitabine) (Barber et al, 2012; 5. Biliary system patency
van Essen et al, 2008) or other targeted therapies, such as 6. Bile leak
everolimus or sunitinib. Application of other radionuclides, 7. Neonatal hyperbilirubinaemia (biliary atresia versus neonatal
such as α-emitters or radionuclide combinations, and intraarte- hepatitis “syndrome”)
rial administration (hepatic artery) are under evaluation. 8. Assessment of biliary enteric bypass (e.g., Kasai procedure)
Applications of PRRT in the neoadjuvant setting to achieve 9. Assessment of liver transplant
tumor size reduction and thus allow curative surgery are in 10. Afferent loop syndrome
preparation. This was successfully performed in two patients 11. Assessment of biliary dilation (e.g., choledochal cyst)
with pancreatic NETs (Kaemmerer et al, 2009; Stoeltzing et al, 12. Calculation of gallbladder ejection fraction
13. Functional assessment of the liver before partial hepatectomy
2010).
14. Demonstration of anomalous liver lobulation
Another approach in targeting somatostatin relies on the 15. Enterogastric (duodenogastric) reflux assessment
implementation of a binding-receptor antagonist instead of a 16. Esophageal bile reflux after gastrectomy
receptor agonist. Whereas binding of SSTR agonists leads to 17. Sphincter of Oddi dysfunction
receptor-mediated internalization, degradation, and intracel- 18. Differentiation of focal nodular hyperplasia from other hepatic
lular trapping, the somatostatin antagonist is not internalized, neoplasms
offering the possibility to bind to more receptor sites and with
From Tulchinsky M, et al: SNM practice guideline for hepatobiliary scintigraphy 4.0. J Nucl Med
a longer retention time (Ginj et al , 2006; Hanyaloglu & von Technol 38:210-218, 2010; and American College of Radiology, Society for Pediatric Radiology:
Zastrow, 2008; Wang et al, 2012). Antagonists such as DOTA- ACR-SPR practice parameter for the performance of hepatobiliary scintigraphy. Amended 2014
BASS and DOTA-JR11 are under evaluation (Wild et al, 2011, (Resolution 39). www.acr.org.
2014).
Recent advances in the field of nuclear medicine play pivotal
roles not only for diagnosing and staging but also for identifica- cholestasis, with MR cholangiopancreatography (MRCP) and
tion of biologic characteristics of NET, thereby guiding and endoscopic ultrasound (EUS) as potential next diagnostic
validating novel treatment approaches and increasing the scope imaging assays, for unexplained cholestasis.
of personalized medicine. In current state-of-the-art practice, hepatobiliary scintigra-
phy uses an iminodiacetic acid (IDA)–derivative pharmaceuti-
HEPATOBILIARY SCINTIGRAPHY cal radiolabeled with 99mTc; most commonly, 99mTc-radiolabeled
disofenin or mebrofenin. Many clinicians still loosely refer to
Hepatobiliary scintigraphy (or cholescintigraphy) refers to hepatobiliary scintigraphy with these radiotracers as a “HIDA
diagnostic imaging of radiotracers that assess hepatic perfusion, scan,” although HIDA is actually the name of a specific 99mTc-
hepatocellular function, and hepatobiliary drainage (see radiolabeled IDA compound, lidofenin, which was the preemi-
Chapter 3). The most common clinical application of hepato- nent radiopharmaceutical in use at the time that hepatobiliary
biliary scintigraphy is for detection of cholecystitis, including scintigraphy disseminated into widespread clinical medical
acute cholecystitis, typically induced by cystic duct obstruction, practice. Lidofenin is no longer in widespread use because the
and chronic cholecystitis, typically associated with impaired subsequent agents, notably disofenin and mebrofenin, offer
gallbladder ability to contract normally. State-of-the-art hepa- more favorable in vivo pharmacokinetics (Fig. 17.4 and Table
tobiliary scintigraphy has high diagnostic sensitivity and speci- 17.1).
ficity for detection of both acute and chronic cholecystitis, The radiolabeled IDA compounds share common PK
typically 90% to 95% or higher, when optimal methodology is properties, differing predominantly in degrees or particular
used. Other notable but less common clinical indications for characteristics. All are injected intravenously and bind loosely
hepatobiliary scintigraphy are listed in Box 17.1; the diagnostic to plasma proteins, mainly albumin; exiting the bloodstream,
accuracy varies for each. the IDA tracers dissociate from plasma proteins in the space of
In general, despite the wide range of hepatobiliary diseases Disse and then undergo hepatic uptake by hepatocytes, fol-
that exist, most hepatobiliary medical society guidelines ascribe lowed by hepatic excretion into the intrahepatic biliary tree and
a role for diagnostic hepatobiliary scintigraphy in only a very subsequent clearance by biliary flow into the intestines via the
few specific clinical indications, typically as a second-line sphincter of Oddi.
imaging modality. This is because the information about hepatic These compounds also share PK properties with bilirubin.
function and biliary drainage obtained by scintigraphy can Bilirubin, the end product of heme catabolism, is taken up from
often confirm the existence of hepatobiliary dysfunction, which the blood circulation into hepatocytes by a high-affinity,
can usually be diagnosed without imaging by clinical examina- sodium-independent, organic anion transport protein shared
tion and blood tests, but typically does not clarify the underlying with IDA radiotracers. Inside hepatocytes, bilirubin is metabo-
etiology in many types of disease. For example, cholestasis can lized to a more water-soluble conjugated form; the IDA radio-
usually be positively identified by cholescintigraphy, but tracers, however, do not change form. Conjugated bilirubin and
cholestasis syndromes in adults have a variety of etiologies. the IDA radiotracers both exit hepatocytes by energy-dependent
EASL (2009) guidelines make no mention of hepatobiliary active transport (particularly transporter ABCC2; Bhargava
scintigraphy; rather, ultrasound is the primary noninvasive et al, 2009), then are excreted into the biliary tree along with
imaging procedure to distinguish intrahepatic from extrahepatic other components of bile (e.g., cholesterol, bile acids).
304 PART 2 DIAGNOSTIC TECHNIQUES
H
O
H
H O H O
O O O O
N O O
N H
O O
N
H
O
H
O N O
H H
N N O
Br
FIGURE 17.4. Iminodiacetic acid (IDA) molecular components of discussed biliary radiotracers. IDA molecules shown here without attachment to
technetium 99m (99mTc) isotope radiolabel. Left, Diisopropyl IDA, or disofenin. Middle, Bromotriethyl IDA, or mebrofenin. Right, Dimethyl IDA, or
lidofenin, better known as HIDA (hepatic IDA tracer). The compounds differ primarily in constituents along the phenyl ring. When radiolabeled, each
biliary radiotracer comprises a bis structural complex of two IDA ligands bound to one 99mTc atom (not shown).
In marked hyperbilirubinemia, the hepatic uptake of IDA minutes after injection (Fig. 17.5) (Kwatra et al, 2013).
radiotracers can be inhibited by competition in carrier-mediated However, uptake of IDA radiotracers can remain relatively
transport of IDA radiotracers, due to high circulating levels of intact in the acute phase of hepatic injury, noting again that
bilirubin, which uses the same transporters. In severe hyperbili- hepatocellular uptake of IDA radiotracers is not ATP depen-
rubinemia, a higher activity (MBq) of IDA radiotracer may be dent. In the early acute phase of hepatic injury, the cessation
injected, but not in hopes of reducing competitive inhibition by of ATP-mediated hepatocellular excretion of IDA radiotracers
“mass effect,” because the higher radiotracer dose still involves may precede any significant (i.e., scintigraphically detectable)
only nanogram (trace) amounts of IDA compound; rather, the decrease in overall hepatic uptake of IDA radiotracer. The dif-
liver will likely absorb the same percentage of the radiotracer ferential analysis and clinical scenarios where this may be
dose, regardless of the activity. It is hoped, however, that this encountered are discussed later. Essentially, however, a marked
absorbed percentage, by using a higher administered activity decrease in IDA radiotracer and bile excretion and an associ-
(MBq), will yield more photons and more signal from the liver ated lack of bile (tracer) flow through the biliary tree is a sign
and biliary tree, for better-quality scintigraphic imagery. In of a severe hepatic dysfunction, which may be caused by a
moderate to severe hyperbilirubinemia, 99mTc-radiolabeled primary hepatic dysfunction (e.g., severe hepatitis) rather than
mebrofenin is probably preferable to disofenin, because mebro- a mechanical obstruction of biliary tree drainage (and thereby
fenin has higher hepatic extraction (Tulchinsky et al, 2010). secondary hepatic dysfunction).
Hepatobiliary scintigraphy is first an assay of hepatic paren- Bile production depends on normal hepatocellular function.
chymal function (see Chapter 3). Hepatic excretion of the If hepatic parenchymal dysfunction is severe, bile production
radiolabeled IDA compounds is an energy-dependent, active and bile flow will slow down, perhaps even stop, until hepato-
transport process, dependent on intact hepatocellular function. cellular recovery. Similarly, with severe hepatic parenchymal
An absent or abnormally low hepatic uptake of IDA radiotracer dysfunction and associated scant hepatic IDA radiotracer
is indicative of hepatic parenchymal dysfunction, often a diffuse uptake, hepatic excretion of the IDA radiotracer and its drain-
hepatic pathology (e.g., hepatitis). One proposed definition of age through the biliary tree will also be scant or undetectable
“poor hepatic uptake” is hepatic tracer uptake that is visually on scintigraphy.
equivalent, in scintigraphic intensity, to that of tracer present
in the cardiac blood pool, 5 minutes after tracer-injection. Normal Hepatobiliary IDA Radiotracer Scan
Normally, hepatic tracer concentration should be greater than Again, note that “HIDA scan” often referred specifically to
99m
that of circulating tracer in the cardiac blood pool tracer by 5 Tc-lidofenin, which is no longer commonly used. This
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 305
FIGURE 17.5. This study shows severe hepatocellular dysfunction, with the kidneys exhibiting increased clearance of the tracer. Note the parallel
reduction in activity in the cardiac blood pool and the liver. The two bright foci beneath the liver are caused by activity in the pelvis of the right and
left kidneys. The straight arrow points to the left renal pelvis; the curved arrow points to the right ureter. Images were acquired at 2, 15, 25, and 60
minutes after injection.
section discusses state-of-the-art imaging with the commonly BOX 17.2 Hepatobiliary Scintigraphy: Key Points
used 99mTc-labeled IDA tracers mebrofenin and disofenin,
unless otherwise specified. Scintigraphy with both tracers A “normal” hepatobiliary scan appearance is defined by the
yields similar findings in healthy individuals after standard amount of tracer present in the blood pool, liver, biliary tree,
and bowels, at different times after injection.
preparation.
Patient preparation varies, depending on the specific clinical Normal Patient Preparation
indication, but usually includes fasting (unless the patient has Fasting (only if gallbladder present):
no gallbladder; e.g., after cholecystectomy) and avoiding or • ≥2 hours for infants
counteracting recent use of opioids (Box 17.2) (Tulchinsky • ≥2-6 hours for adults
et al, 2010). Fasting is advised in patients with a gallbladder, • But not >24 hours fasting
because one important parameter of normalcy in hepatobiliary Opioids: wait ≥4 half-lives, or counteract (e.g., naloxone).
scintigraphy is detection of the excreted-radiotracer within the
gallbladder lumen, especially if the patient has clinical signs and
symptoms suggestive of cholecystitis. If excreted radiotracer is receiving a bolus of nutrients from the stomach, releases the
not detected within the gallbladder lumen, this can be a sign of hormone cholecystokinin (CCK); CCK causes contraction of
cystic duct obstruction, as seen in acute cholecystitis in adults. the gallbladder and relaxes the sphincter of Oddi, allowing
For excreted radiotracer in the extrahepatic biliary tree to enter concentrated bile from the gallbladder stores to be pumped into
the gallbladder via the cystic duct, there must be a pressure the duodenal lumen. Thus, in the recently fed patient with rela-
gradient moving bile in that direction. When the gallbladder tively high levels of circulating CCK, the gallbladder often will
contracts, the pressure gradient is in the opposite direction, be contracting, and excreted-tracer may not enter the gallblad-
moving bile from gallbladder lumen out the cystic duct into the der lumen. The absence of excreted tracer in the gallbladder
common bile duct (CBD) lumen. This occurs physiologically lumen caused by physiologic contractions of a healthy gallblad-
during feeding, as the bile passes into the duodenum to aid der mimics the appearance of a (pathologic) cystic duct
digestion of food entering from the stomach. The duodenum, obstruction, potentially being misdiagnosed as consistent with
306 PART 2 DIAGNOSTIC TECHNIQUES
acute cholecystitis on scintigraphy (see Chapter 33). Guidelines acquisition of a series of scintigraphic images of the liver region
typically advise a fasting period of at least 2 hours, but prefer- during time, often anterior and posterior planar images, which
ably 6 hours, for adults, likely based on the normal gastric (and can then be displayed as frames in a motion picture for visual
duodenal) clearance times after a typical solid meal. For infants, and quantitative assessment of whether tracer uptake and
a fasting period of only 2 hours is typical, likely because the excretion occur in a normal amount and in the normal time
infant diet is liquid, and gastroduodenal clearance of liquid frame (Fig. 17.6). For example, hepatobiliary scintigraphy often
meals is faster than that of solid meals. In the fasting state, begins with a series of consecutive planar images of the liver
neural and hormonal impulses cause the sphincter of Oddi to region, each planar image being a frame 1 minute in duration,
be predominantly closed and the cystic duct of the gallbladder acquired for a total of 1 hour, starting at the time of radiotracer-
to remain predominantly open; this halts bile flow into the injection. Nuclear medicine societies provide guidance docu-
intestines (via sphincter of Oddi) and creates a pressure gradi- ments (available online) with detailed technical suggestions for
ent directing bile (and IDA tracer) into the gallbladder. During image acquisition protocols (Tulchinsky et al, 2010).
fasting, some phasic contractions of gallbladder and relaxation Analysis of hepatobiliary scintigraphy imagery is based on
of the sphincter of Oddi still occur, possibly to churn the bile visual detection of tracer in expected locations at expected time
and avoid precipitation of some bile constituents. Therefore, a points and often on semiquantitative visual estimation of
normal variability (i.e., range of normal values) occurs in the whether the amount of tracer present in blood pool, liver, biliary
time required to observe excreted tracer in the gallbladder and tree, and bowels is appropriate for the time point after injection.
bowels in well-prepared, healthy individuals. Quantitative analysis may be facilitated by digital region-of-
Prolonged fasting for longer than 24 hours (including during interest (ROI) analysis to generate numeric indices.
hyperalimentation) is also associated with excreted IDA tracer Both 99mTc-labeled IDA tracers clear rapidly from the
failing to enter the gallbladder lumen, creating a potentially bloodstream. Typically, less than 15% of the radiotracer dose
misleading appearance scintigraphically. This is likely attribut- remains in the blood circulation by 10 minutes after injection;
able to accumulation of biliary sludge in the gallbladder lumen, the amount of tracer in the cardiac blood pool, if in the scinti-
obstructing the cystic duct in a nonpathologic manner. Clinical graphic field of view, drops greatly during that time. Both
research demonstrates that for patients who have undergone tracers are eliminated from the body predominantly by hepa-
prolonged fasting, it is beneficial to administer a synthetic CCK tobiliary excretion, usually with minor urinary excretion and
octapeptide (sincalide) to “clean out” the gallbladder as part of with no tracer accumulation in other organs. The tracers achieve
patient preparation for hepatobiliary scintigraphy. Pretreatment maximal hepatic concentration approximately 10 minutes after
with sincalide is typically 0.02 µg/kg intravenously during 30 to injection and have hepatic uptake that is visually distinct typi-
60 minutes by slow infusion. One guideline suggests that hepa- cally by 5 minutes. Both tracers are detectable in the extrahe-
tobiliary tracer injection can occur 15 to 30 minutes after slow patic biliary tree in 100% of normal individuals by 1 hour after
sincalide infusion pretreatment (Tulchinsky et al, 2010). injection, and in approximately 90%, excreted tracer is detect-
Attempts to administer sincalide more rapidly are associated able in the CBD by 30 minutes. The intrahepatic biliary tree is
with unpleasant patient symptoms, particularly gastrointestinal often detectable earlier, sometimes 10 minutes after injection.
(e.g., crampy abdominal pain), and can induce a contractile Frequently, the intrahepatic biliary tree is more distinctly
spasm of the gallbladder neck, especially if given as a bolus, visualized in the lateral region of the left hepatic lobe than in
creating a cystic duct obstruction that the sincalide pretreat- the right lobe, probably because of the normally greater mass
ment is intended to relieve; the spasm lasts approximately 1 of the right hepatic lobe causing attenuation of the scintigraphic
hour (Mesgarzadeh et al, 1983). signal emanating from within it.
If the patient has no gallbladder, no fasting is required for The amount of excreted tracer present in the extrahepatic
hepatobiliary scintigraphy. biliary tree is an important variable, as well the timeliness of its
Opioid medications (e.g., morphine) acutely induce strong, appearance after injection. After achieving maximal liver uptake,
prolonged contraction of the sphincter of Oddi. If a patient has the liver clears tracer (via excretion) with a typical half-time of
recently received opioid medications, passage of excreted about 30 (±15) minutes (Drane & Johnson, 1990; Williams
radiotracer from the biliary tree into the duodenum can be et al, 1984). Typically, one-third of the injected dose has passed
delayed as a side effect. If biliary-to-bowel transit is delayed into or through the common bile duct by 30 to 60 minutes after
beyond 3 to 4 hours after injection from lingering opioid effects, injection. Excreted tracer clears from the CBD with a half-time
this can mimic the appearance of CBD obstruction (e.g., (from peak CBD activity) of approximately 30 (±20) minutes
caused by choledocholithiasis). To avoid this potential diagnos- (Drane & Johnson, 1990).
tic pitfall, patients should avoid opioid medications before Excreted tracer passes from the biliary tree into the duode-
hepatobiliary scintigraphy; one guideline suggests waiting for num via the sphincter of Oddi in healthy persons with normal
four times the half-life of the particular opioid drug (Tulchinsky biliary anatomy. This is evident scintigraphically to the trained
et al, 2010). Alternatively, naloxone may be administered to eye of the imaging specialist, becoming most evident if intestinal
attempt to reverse the opioid effects (Patch et al, 1991). peristalsis sweeps the tracer through the duodenum into distal
Additional forms of patient preparation for less common bowel loops during imaging. Excreted tracer is detectable in the
indications of hepatobiliary scintigraphy are discussed later. intestines in most healthy people (80%) by 1 hour after injec-
The in vivo hepatobiliary parameters typically assessed on tion. Biliary-to-bowel transit takes longer in some healthy
scintigraphy are hepatic uptake and excretion of the adminis- individuals, particularly those who receive sincalide before
tered IDA tracer and subsequent biliary drainage of the treatment (a paradoxical phenomenon) (Kim et al, 1990). How
excreted-radiotracer through the biliary tree into small bowel. to distinguish physiologic delay from pathologic CBD obstruc-
These are time-dependent biologic processes. Thus, hepatobili- tion is discussed later. Excreted tracer that enters the intestines
ary scintigraphy typically involves dynamic imaging, with the remains in the intestines, with no significant intestinal tracer
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 307
FIGURE 17.6. Normal hepatobiliary iminodiacetic acid study. Serial images of the liver, in anterior projection, acquired beginning immediately after
tracer injection; each image is 5 minutes in duration. The serial images show prompt systemic clearance of radiotracer (e.g., disappearing cardiac
blood pool, gray arrowhead) via hepatic uptake, followed by prompt hepatobiliary excretion of tracer. Excreted tracer flows promptly through the
extrahepatic biliary tree, including into the gallbladder lumen (large arrow). Excreted tracer passes from biliary tree into the duodenum, carried away
into distal bowel loops by peristalsis (black arrowhead). One atypical incidental finding is enterogastric reflux of the biliary tracer (small arrow).
reabsorption or enterohepatic recycling of radiotracer. Entero- (half-time ~40 minutes) is much slower than that of the 99mTc-
gastric reflux of tracer can occasionally be observed; its clinical radiolabeled disofenin and mebrofenin compounds (both
significance is not well defined. ~15-20 minutes). Older literature and even recent hepatobiliary
Lastly, the gallbladder should be visualized within 1 hour scintigraphy guidelines often suggest obtaining delayed imaging
after injection. Gallbladder nonvisualization after 1 hour in the at 3 to 4 hours or later after radiotracer injection. With 99mTc-
proper clinical setting can diagnose cystic duct obstruction, a lidofenin, imaging at 3 to 4 hours or longer after injection was
hallmark of acute cholecystitis, with high diagnostic accuracy. possible because of the slow hepatobiliary excretion of the
In certain patients, confirmatory measures (e.g., morphine tracer; if gallbladder filling or biliary-to-bowel transit had not
augmentation) may be pursued. yet been visualized by the expected 1 hour after injection,
Pathology in hepatobiliary scintigraphy is thus indicated by delayed imaging was possible because a significant amount of
one or more of the following: radiotracer would still be in the liver undergoing hepatobiliary
• An abnormally low amount of hepatic tracer uptake transit. However, with 99mTc-radiolabeled disofenin and mebro-
• An abnormally prolonged hepatic retention of tracer fenin, the hepatobiliary clearance is relatively rapid. The liver is
• An abnormally delayed appearance of excreted tracer in often essentially “empty” of radiotracer by 2 to 4 hours after
the biliary tree injection, precluding delayed imaging. At this time, one cannot
• An abnormally delayed appearance of excreted tracer in expect delayed filling of the gallbladder with radiotracer if it has
the intestines already essentially cleared from the liver and the remainder of
Again, the radiotracer 99mTc-lidofenin is now rarely used the biliary tree. On the other hand, delayed imaging with the
compared with current agents such as 99mTc-radiolabeled dis- newer agents remains a logical approach in certain cases. In
ofenin and mebrofenin. The hepatic clearance of 99mTc-lidofenin patients with severe hepatocellular dysfunction (whether
308 PART 2 DIAGNOSTIC TECHNIQUES
secondary to biliary tract obstruction or from a separate hepatic to the operating room for cholecystectomy without preoperative
disease), uptake and secretion of biliary tracer by dysfunctional imaging, or an urgent abdominal US evaluation may be
hepatocytes may be abnormally delayed and associated biliary obtained. If US visualizes cystocholelithiasis and signs of cho-
flow through the biliary tree likewise greatly slowed; delayed lecystitis, cholecystectomy might be pursued. If gallstones and
imaging at 4 or even 24 hours may be useful to evaluate biliary sonographic signs of cholecystitis are absent, hepatobiliary
flow in these patients (Ziessman, 2014). scintigraphy might be pursued to identify cystic duct obstruc-
tion, which is the typical etiology of acute calculous or acalcu-
Augmented Hepatobiliary Scintigraphy lous cholecystitis in adults. For chronic or recurrent abdominal
Hepatobiliary scintigraphy can employ pharmacologic inter- pain in adults, evaluation must exclude nonbiliary etiologies as
ventions, most notably with phenobarbital, morphine, and well as biliary. Hepatobiliary scintigraphy with CCK might be
sincalide. used to confirm a diagnosis of gallbladder functional disorder
Phenobarbital is used in cholescintigraphic evaluation of (Zakko et al, 2015). For children, cholecystitis is uncommon
neonatal jaundice (see Chapters 1 and 40). Patient pretreat- and is usually associated with a predisposing risk factor, such
ment with phenobarbital will stimulate bile production and as sickle cell disease or cystic fibrosis; the scintigraphic findings
biliary flow and increase the likelihood of visualizing hepatobili- can also differ from adult scintigraphic signs.
ary radiotracer excretion, if biliary atresia is absent. It reduces
the likelihood of false-positive scintigraphic appearance of Acute Cholecystitis (See Chapter 33)
biliary flow obstruction. The reported sensitivity and specificity of cholescintigraphy for
Morphine is used in in cholescintigraphic evaluation of suspected acute calculous cholecystitis ranges from 87% to
gallbladder cystic duct obstruction (see Chapters 33 and 49). 98% and 81% to 100%, respectively, in the original clinical
If accumulation of excreted biliary tracer in gallbladder lumen studies up to 2000 (Ziessman, 2003). Reviewing their experi-
is not observed in the expected time frame, morphine admin- ence with patients seen in the emergency department with
istration normally contracts the sphincter of Oddi and relaxes acute upper abdominal pain (n = 406) from 2010 to 2012,
any physiologic gallbladder contraction; this increases the likeli- Kaoutzanis and colleagues (2014) reported that patients vari-
hood that biliary radiotracer can accumulate within the gall- ably underwent abdominal US alone (n = 132), scintigraphy
bladder, if no pathologic obstruction of the gallbladder cystic alone (n = 46), or both (n = 228), according to the clinician’s
duct (e.g., associated with calculous or acalculous cholecystitis) judgment at the time. Their sensitivity for acute cholecystitis
is present. It reduces the likelihood of false-positive scintigraphic was US alone, 73%; scintigraphy alone, 92%; and both, 98%.
appearance of gallbladder cystic duct obstruction. Because Although selection bias must be suspected to impact the results,
morphine contracts the sphincter of Oddi, scintigraphically, the findings indicate that hepatobiliary scintigraphy (1) contin-
entry of biliary tracer into small intestines is typically confirmed ues to have a standard role in the evaluation of the patient with
visually before use of morphine, first to exclude CBD obstruc- acute abdominal pain, often combined with abdominal US,
tion before attempting to exclude a cystic duct obstruction. If which remains the first-line imaging modality, and (2) offers
the decision to use morphine is made based on nonvisualization high sensitivity for preoperative diagnosis of acute cholecystitis,
of the gallbladder, but the injected biliary tracer has already alone or combined with US, in the proper clinical context.
essentially cleared from the liver and biliary tree into the bowels, While the radiotracer is injected, hepatobiliary scintigraphy
it is often necessary for patients to receive a “booster” injection typically begins with collection of an uninterrupted series of
of biliary tracer before administration of morphine, to renew a brief (1 to 3 second), consecutive images of the liver for 1 to 2
flow of radiotracer through the biliary tree. minutes, called the flow phase. These images can be displayed
Sincalide is used in cholescintigraphy for evaluation of gall- in dynamic, cinematic fashion to visualize the passage of the
bladder cystic duct or CBD obstruction or gallbladder dyski- tracer through the bloodstream, including its initial passage
nesia (see Chapter 33). Patient treatment with sincalide causes through the liver. If cholecystitis is present, the surrounding
contraction of the gallbladder and relaxation of the sphincter hepatic parenchyma may also be inflamed. This tissue inflam-
of Oddi. Sincalide can be given before radiotracer to evacuate mation is often associated with relative tissue hyperemia that
the gallbladder lumen if gallbladder accumulation of a biliary can be visualized as an abnormal “blush” of activity around the
sludge is possible (e.g., from patient hyperalimentation or gallbladder during the flow phase, called the “rim sign.” The
prolonged fasting) or evident sonographically; such sludge can rim sign, indicating inflammation of liver around the gallblad-
impede gallbladder accumulation of biliary tracer, creating a der, is typically associated with severe inflammation of the
scintigraphic appearance mimicking a cystic duct obstruction gallbladder itself. The rim sign has been associated with an
(false-positive). If the gallbladder lumen accumulates biliary increased risk of complicated cholecystitis, specifically gangrene
tracer (no cystic duct obstruction), but gallbladder dyskinesia and gallbladder perforation. The rim sign is visualized in
is suspected (e.g., associated with cholecystitis), sincalide can approximately 25% to 35% of patients with acute cholecystitis
then be administered to assess the normalcy of gallbladder (Ziessman, 2014).
sincalide response in terms of its ejection fraction—what per- After the flow phase, hepatocellular uptake and excretion of
centage of radiotracer is evacuated from the gallbladder lumen the radiotracer is monitored scintigraphically, typically as an
in response to sincalide. uninterrupted series of 1 to 5 minute consecutive images of the
liver for at least 60 minutes. During this period, the imaging
Right Upper Quadrant Pain specialist evaluates hepatobiliary tracer clearance for the
The approach to an adult patient with abdominal pain is expected normal scintigraphic findings (described earlier).
detailed elsewhere in this textbook (see Chapter 33). In brief, Acute cholecystitis in adults is almost always associated with a
however, for acute clinical signs and symptoms strongly sugges- pathologic obstruction of the cystic duct, whether cholelithiasis
tive of acute cholecystitis, the patient might be taken directly impacted in the cystic duct or acalculous cholecystitis (i.e.,
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 309
inflammation and edema in the walls of the gallbladder neck, Most often, chronic cholecystitis is associated with cysto
thereby occluding the duct). Again, in most healthy patients, cholelithiasis, detected sonographically. The US presence of
gallbladder accumulation of excreted biliary radiotracer occurs gallbladder stones and classic clinical signs and symptoms are
within 30 to 60 minutes after injection. The imaging specialist the main indications for cholecystectomy. Cholescintigraphy
must be wary of the “cystic duct sign,” which mimics gallblad- might be obtained for patients with questionable chronic cho-
der tracer accumulation. The cystic duct sign is a nonelongated, lecystitis (e.g., atypical clinical signs and symptoms, absent
spotlike focus of tracer accumulation in the expected location cystocholelithiasis) or who might poorly tolerate cholecystec-
of the cystic duct, along the common hepatic and bile duct tomy (e.g., because of comorbidity). In chronic cholecystitis,
course. The cholescintigraphic cystic duct sign represents a calculous or acalculous, the cystic duct is typically patent, and
focal accumulation of biliary radiotracer within the proximal the gallbladder will be visualized as accumulating radiotracer.
cystic duct (closest to and communicating with the common The scintigraphic hallmark of cholecystitis is gallbladder dyski-
duct) that can occur in cystic duct obstruction when choleli- nesia, manifest as an abnormally low gallbladder ejection frac-
thiasis obstructing bile passage from the gallbladder is lodged tion (GBEF) of less than 38%, on sincalide-stimulated
more distally within the cystic duct. The cystic duct sign should cholescintigraphy (Tulchinsky et al, 2010; Ziessman, 2014).
be suspected when biliary tracer accumulation in the gallblad- Gallbladder dyskinesia (low GBEF) can be observed with acute
der region is not elongated, but rather is more spotlike and cholecystitis as for chronic cholecystitis, because of dysfunction
smaller than usual. In cases of diagnostic uncertainty, a sus- of inflamed gallbladder smooth musculature in both acute and
pected cystic duct sign can be evaluated further by SPECT/CT, chronic cases. The GBEF study begins after the expected tracer
to confirm an absence of excreted tracer in the gallbladder accumulation in the gallbladder lumen has been visualized.
lumen. Again, if morphine augmentation was required, sincalide GBEF
As previously discussed, in a minority of healthy patients testing can still be pursued, and normal GBEF results reliably
with no pathologic obstruction of the cystic duct, the gallblad- exclude gallbladder dyskinesia and cholecystitis, although low
der lumen does not accumulate excreted tracer within the first GBEF results are nondiagnostic. When the gallbladder is
hour because of a physiologic obstruction of inward biliary flow “filled” sufficiently with excreted tracer (typically 30-60 minutes
associated with physiologic contractions of the gallbladder. To after tracer injection), sincalide is then administered.
minimize these contractions, patients are advised to fast before Besides morphine, a variety of medications have been associ-
the study. Even with proper fasting, however, this contraction ated with low GBEF results that could lead to a false diagnosis
can occur. In these healthy patients, gallbladder relaxation and of cholecystitis; medications include (but are not limited to)
tracer accumulation will usually occur by 3 to 4 hours after atropine, calcium channel blockers, octreotide, progesterone,
injection. To increase the diagnostic specificity of gallbladder indomethacin, theophylline, benzodiazepines, and histamine-2
nonvisualization as a scintigraphic biomarker of cystic duct receptor antagonists. As such, patient medications should be
obstruction, guidelines suggest that the imaging specialist reviewed at the time of the study. A variety of conditions other
obtain either delayed imaging or, without delay, administer than cholecystitis have been associated with low(er) GBEF
morphine (Tulchinsky et al, 2010). If the gallbladder remains results as well, including obesity, celiac disease, cirrhosis, myo-
nonvisualized after morphine, cystic duct obstruction can be tonic dystrophy, and diabetes.
diagnosed with greater specificity. Thus, standard guidelines
advise routine use of morphine augmentation or, alternatively, Extrahepatic Bile Duct Obstruction
delayed imaging, if the gallbladder does not accumulate excreted As discussed, in healthy volunteers, cholescintigraphy tracers
tracer in the first hour, but only after biliary tracer transit undergo hepatobiliary drainage with detectable passage of
though the sphincter of Oddi into bowel is confirmed, to excreted tracer into the duodenum within 1 hour after injection
exclude CBD obstruction. in most cases. In approximately one-third of healthy volunteers,
Regarding false-negative results, cholescintigraphy appears passage of excreted tracer into the duodenum is not evident on
to have less diagnostic sensitivity for acalculous acute cholecys- scintigraphy until the second hour or so; this is probably attrib-
titis, perhaps 70% to 80%, compared with more than 90% for utable to transient/phasic physiologic contraction of the sphinc-
calculous acute cholecystitis (Tulchinsky et al, 2010; Ziessman, ter of Oddi. In these healthy volunteers, with relatively delayed
2014). A significant number of patients with acalculous acute passage of tracer into bowels, excreted tracer is visible in the
cholecystitis will demonstrate gallbladder tracer accumulation extrahepatic biliary tree, awaiting passage into bowel once the
(no cystic duct obstruction). Acalculous cholecystitis can be sphincter of Oddi relaxes. Additionally, patients pretreated with
diagnosed despite gallbladder tracer accumulation in the pres- sincalide before cholescintigraphy paradoxically seem to be
ence of the rim sign or abnormally low gallbladder ejection more likely to demonstrate a nonpathologic delay in biliary
fraction, to increase diagnostic sensitivity (Ziessman, 2014). In transit into bowel, at least if sincalide is infused relatively rapidly
adults, cholecystitis is typically calculous cholecystitis, whereas (Kim et al, 1990).
acalculous cholecystitis is relatively uncommon. In pediatric Pathologic obstruction of the common hepatic duct or CBD
patients, however, acute cholecystitis is frequently acalculous. can be diagnosed by cholescintigraphy. Extrahepatic bile duct
For suspected acalculous cholecystitis, both adult and pediatric, obstruction can be caused by cholelithiasis (choledocholithiasis
our standard practice is to assay gallbladder ejection fraction, or rarely Mirizzi syndrome) (see Chapters 36 and 37) or tumor
if cystic duct obstruction is absent scintigraphically, to optimize (e.g., pancreatic head mass compressing adjacent duct) (Chap-
diagnostic sensitivity. ters 51, 59, and 62). Tumor-associated biliary obstruction is
usually identifiable by structural imaging (CT, US, or MRI),
Chronic Cholecystitis (See Chapter 33) because biliary duct dilation is often already present at diagno-
Chronic cholecystitis patients typically report biliary colic–type sis. Obstructive cholelithiasis, in contrast, often presents clini-
symptoms that have been recurrent over a prolonged period. cally as an acute biliary-type pain; in the first 24 to 72 hours
310 PART 2 DIAGNOSTIC TECHNIQUES
FIGURE 17.7. Complete biliary obstruction. Images were obtained immediately after injection and at 30 minutes, 60 minutes, and 3 hours. No
severe hepatocellular dysfunction is evident; systemic tracer clearance is somewhat delayed (cardiac blood pool still detectable at 30 minutes), but
the liver demonstrates prompt, visually distinct tracer uptake. No excreted tracer is detectable in the extrahepatic biliary tree at 1 hour after tracer
injection. This constellation of scintigraphic findings is suspicious for an acute high-grade extrahepatic bile duct obstruction, in the proper clinical
setting. The continued absence of detectable excreted tracer at 3 to 4 hours after tracer-injection increases diagnostic confidence, when hepatocellular
function is impaired.
after bile duct obstruction by cholelithiasis, bile duct distension If these two findings are present, extrahepatic bile duct
may not yet be marked enough to be suspicious on structural obstruction is the likely diagnosis, with other etiologies relatively
imaging. Cholescintigraphy can confirm a clinical suspicion of rare (Ziessman, 2003). If hepatic function is poor, however,
acute extrahepatic bile duct obstruction in patients with nega- passage of excreted tracer into the extrahepatic bile ducts can
tive structural imaging. Additionally, patients with previously be delayed because hepatic bile production is slow. Hepatic
treated bile duct obstruction can have persistent bile duct dila- function may be poor because of a true bile duct obstruction
tion after treatment; if these patients return to the clinic with (in which case it was more likely chronic than acute) or because
suspicious biliary colic, structural imaging may demonstrate a of a separate nonobstructive etiology (e.g., hepatitis, cirrhosis).
chronically distended bile duct of uncertain significance. Cho- If hepatic function is poor, delayed imaging will improve test
lescintigraphy can confirm a clinical suspicion of acute recur- specificity (i.e., help avoid false diagnosis of bile duct obstruc-
rent extrahepatic bile duct obstruction in such patients. tion (Fig. 17.7) (Ziessman, 2003).
Acute extrahepatic bile duct obstruction has been described A partial obstruction of the extrahepatic bile ducts is associ-
as having cholescintigraphic appearances that favor either a ated with the following cholescintigraphic appearance:
“high-grade” or a lesser, “partial” degree of biliary obstruction • Hepatic uptake is normally prompt (unless the patient also
(Ziessman, 2014). An acute high-grade obstruction of the has hepatic dysfunction unrelated to biliary obstruction).
extrahepatic biliary tree can be diagnosed if the following find- • Excreted-tracer appears promptly within the extrahepatic
ings are present: biliary tree.
• The patient has good hepatic function, as indicated by blood • Clearance of excreted tracer from the extrahepatic biliary
tests and on cholescintigraphy by rapid hepatic tracer-uptake tree is absent or scant during the first hour after injection.
and rapid tracer clearance from the blood pool. • Further clearance of excreted tracer from the extrahepatic
• Excreted biliary tracer is not detectable or scantly present biliary tree into bowels, after sincalide administration or at
in the extrahepatic biliary tree by 1 hour after injection. delayed time points, is less than expected.
Chapter 17 Role of nuclear medicine in diagnosis and management of hepatopancreatobiliary disease 311
Normally, approximately half of biliary tracer has passed Biliary Tract Complications After Surgery
from the hepatobiliary tree into the bowels by 1 hour after Cholescintigraphy can positively impact diagnostic evaluation
tracer injection, and a progressive decline in the net amount of of patients for biliary tract complications associated with a
tracer in the extrahepatic biliary tree is usually visibly evident variety of procedures, such as laparoscopic cholecystectomy
scintigraphically in that first hour (Drane & Johnson, 1990). (see Chapters 38 and 42), partial hepatic resections (Chapters
However, an absence of bowel activity at 1 hour after tracer 27 and 103), or liver transplantation (Chapter 120). Bile duct
injection is sensitive for partial obstruction (~98%) but not injuries are complications associated with laparoscopic chole-
highly specific, because of the normal variation in drainage of cystectomy, for example, with a reported rate of occurrence
bile into bowel associated with phasic physiologic contractions ranging from 0.4% to 0.6% (McMahon et al, 2000). Bile duct
of the sphincter of Oddi (Williams et al, 1984). Delayed imaging injuries may lead either to biliary duct obstruction or bile
can be obtained to allow for detection of biliary passage into leakage. CT and US are first-line imaging modalities to evalu-
bowel, allowing for the possibility of a physiologic contraction ate for suspected complications; nonspecific findings include
of the sphincter of Oddi. Alternatively, relaxation of the sphinc- fluid collection in the gallbladder fossa or peritoneal cavity.
ter of Oddi can be induced by sincalide treatment, to avoid Cholescintigraphy allows the noninvasive evaluation of the
delay. The gallbladder, if present, must accumulate excreted biliary tree for obstruction and leakage and can be used to
tracer normally, before use of sincalide, to exclude cystic duct characterize fluid collections detected by US or CT, particularly
obstruction. If clearance of excreted tracer from the extrahe- benefiting from the use of SPECT/CT to visualize both the
patic biliary tree into bowels, after sincalide administration or fluid collection (on CT) and the abnormal tracer accumulation
at delayed time points, remains less than expected, a partial bile within the collection (on fusion SPECT/CT). Most leaks
duct obstruction can be diagnosed with a specificity of approxi- are observed at the cystic duct stump, and characteristic
mately 85% (Ziessman, 2014). For clarity, cholelithiasis is not scintigraphy findings include tracer accumulation at the
a contraindication to use of sincalide. gallbladder fossa, near the porta hepatis or in the subphrenic
space. SPECT/CT is also advantageous for patients with com-
plicated postsurgical hepatobiliary anatomy (e.g., status post-
Postcholecystectomy Syndrome and Sphincter of Oddi hepaticojejunostomy), to help clarify biliary flow patterns.
Dysfunction (See Chapter 38)
Postcholecystectomy syndrome refers to the recurrence of similar Liver Transplantation
abdominal pain as experienced before cholecystectomy, mainly Biliary imaging objectives for postoperative liver transplant
upper abdominal pain (right upper quadrant) and dyspepsia, patients include detection of biliary anastomotic strictures
with or without jaundice. It is based on a variety of possible caused by thrombosis or stenosis of the hepatic artery or by
hepatobiliary findings and occurs in 10% to 20% of patients recurrent primary sclerosing cholangitis or primary biliary cir-
who have had surgery for chronic cholecystitis (Black et al, rhosis, if applicable, per standard liver transplantation guidelines
1994). One study reported an incidence of even 40%, more (see Chapter 120). For these objectives, the standard guidelines
often occurring in women (Macaron et al, 2011). Onset of focus on endoscopic retrograde cholangiopancreatography,
symptoms can occur from 2 days to as long as 25 years after MRCP, and US. Little to no mention of scintigraphic imaging
surgery. Hepatobiliary causes include retained or recurrent is included, although much clinical research has been conducted
stones, biliary strictures, bile leakage, formation of chronic into the potential value of scintigraphy in the liver transplant
biloma or abscess, long cystic duct remnant, obstruction of the population. Hepatobiliary scintigraphy with IDA-type tracers
sphincter of Oddi, and bile salt–induced diarrhea or gastritis. has been shown to provide accurate diagnosis of biliary com-
In the majority of patients, however, other extrahepatic disor- plications in adult and pediatric patients (Gelfand et al, 1992;
ders (e.g., reflux esophagitis, gastritis, irritable bowel syndrome, Kim et al, 2002; Kurzawinski et al, 1997). However, studies
chronic pancreatitis) are responsible for the postcholecystec- reporting assessment of organ rejection (usually diagnosed by
tomy pain syndrome (Jaunoo et al, 2010). liver biopsy) are limited, particularly in reliable differentiation
Sphincter of Oddi dysfunction is a condition that has been between cholestasis and organ rejection (Brunot et al, 1994;
implicated in 1% to 14% of this patient group (Baillie, 2010; Kim et al, 2002).
Bar-Meir, 1984). The dysfunction can be caused by true ste-
nosis or secondary to spasm of the sphincter. The establishment PEDIATRIC IMAGING
of a diagnosis as well as treatment approaches is challenging.
Sphincterotomy, advocated as effective therapy, is associated Neonatal Jaundice
with bleeding and pancreatitis. Cholescintigraphy and sphincter The incidence of neonatal jaundice in the United States
of Oddi manometry have been explored as assays to confirm has been increasing, currently affecting approximately two-
diagnosis in support of therapeutic intervention. thirds of newborns (Schwartz et al, 2011). In most infants, the
Various protocols assessing qualitative image analysis based etiology of jaundice is physiologic. However, high concentra-
on cholescintigraphy have been published recommending an tions of unconjugated bilirubin may cause permanent neuro-
infusion of sincalide during 3 to 10 minutes, completed 15 logic damage, known as chronic bilirubin encephalopathy or
minutes before radiotracer injection (Sostre et al, 1992). kernicterus. Even moderately elevated levels of bilirubin may
However, another study indicated that sphincter of Oddi induce permanent neurodevelopmental impairment (NDI)
manometry is superior to scintigraphy (Cicala et al, 1991). or bilirubin-induced neurologic dysfunction (BIND). The
Subsequently, another report indicated that although the sensi- various etiologies include infections, isoimmunization, inherited
tivity of scintigraphy is less compared with superior manometry, disorders of bilirubin conjugation and transport, and biliary
the higher accuracy in predicting treatment success compares malformation. Biliary atresia, inspissated bile syndrome and
favorably (Cicala et al, 2002). choledochal malformation are associated with a relatively good
312 PART 2 DIAGNOSTIC TECHNIQUES
99m
Tc-labeled SC can become evident by scintigraphic signs of lipiodol). HAIS applications may be used, when applicable, (1)
catabolic production of free 99mTc pertechnetate; signs of 99mTc to ensure the integrity and function of the infusion system (e.g.,
pertechnetate include (delayed–time point) accumulation of a hepatic pump reservoir-catheter system) and that the biodis-
radioisotope in stomach and thyroid and urinary radioisotope tribution of the infusate meets expectations (discussed next),
excretion. and/or (2) to predict or measure hepatic radiation dosimetry,
Focusing the discussion on liver considerations, a notable before or after infusion of therapeutic radioactive microspheres
abnormality in colloid biodistribution is colloid shift, a term or ethiodized oil (lipiodol).
denoting hepatic 99mTc-labeled SC concentration that is visu- Placement of the arterial catheter used for HAIT and HAIS
ally less than splenic concentration, which is an abnormal involves different possible techniques. The catheter may be
scintigraphic biodistribution. Splenic concentration of 99mTc- surgically implanted (e.g., Watkin technique) or guided into the
labeled SC normally is less than the scintigraphic-intensity of hepatic artery using a minimally invasive approach (e.g., IR)
hepatic concentration. This abnormality can be caused by (see Chapters 99 and 102). Catheters may be placed intermit-
abnormally low hepatic uptake or abnormally high splenic tently (e.g., as part of sequential or cyclic treatments) or longer
uptake of 99mTc-labeled SC. Broad examples of etiologies term (e.g., connected to an implanted drug-delivery device or
associated with low hepatic uptake include diffuse hepatic infusion port). Catheters may connect to a subcutaneously
diseases such as advanced cirrhosis and severe hepatitis. With implanted port or an infusion pump system. Pumps enable
such associations observed, investigators have explored whether slow, continuous drug infusion, typical of hepatic arterial che-
hepatic colloid uptake might offer a semiquantitative biomarker motherapy; such systems are more often found in the United
of hepatic function. In at least one study (Esmaili et al, 2008), States. In a port-catheter system, the implanted port may
no correlation was found between scintigraphic semiquantita- accessed for connection to an external pump system. In Europe,
tive uptake measurements and Child-Pugh classification, an transiently placed catheters and port-catheter systems are more
index of liver function. The finding of diminished colloid uptake common.
in the right and left liver lobes, along with sparing of the caudate The radiotracer used for HAIS, when performed before
lobe, has been associated with Budd-Chiari syndrome (hepatic treatment, is 99mTc macroaggregated albumin (MAA). A radio-
vein thrombosis) (Oppenheim et al, 1988). Various causes of labeled particulate, 25 to 50 µm in mean diameter, the infused
99m
hypersplenism can manifest as abnormally high splenic uptake Tc MAA physically occludes the first microvascular lumen
(Rutland, 1992). it encounters. Several hundred thousand MAA particles are
The differential for “cold defects” or photopenic defects— injected, labeled with a trace amount of activity. Radiolabeled
foci of absent or relatively low colloid uptake—within the liver MAA particles remain intact in vivo for several hours. The
parenchyma is extensive(Oppenheim et al, 1988), including infusate tracer, suspended in a small volume of saline (e.g.,
hepatoma, metastases, and many other pathologic entities. 2 cc), is injected into the pump or transiently placed catheter
Because of limited resolution of the planar and SPECT scans, by a nurse or physician trained in the technique and equipment
only hepatic lesions greater than 1.5 to 2 cm can be reliably necessary for accessing the device. The tracer infusate, followed
detected as colloid-tracer cold-spot or hot-spot lesions. As by a saline flush, traverses the connected catheter into the
previously discussed, to our knowledge, the only hepatic lesion bloodstream of the hepatic artery or accessed branch. Injection
entity reported to produce a focally increased concentration of an infusate can be slow (e.g., <1 cc/min), which mimics
(hot spot) of 99mTc-labeled SC, compared to surrounding liver somewhat the slow rate typical of pump-infusions in HAI
uptake, is focal nodular hyperplasia. Whereas a 99mTc-labeled chemotherapy. Injection of an infusate can be fast (e.g. ≥1 cc/
SC liver hot spot appears to have very high specificity in diag- sec; bolus), which introduces infusate rapidly into the hepatic
nosis of FNH, possibly pathognomonic (Herman et al, 2000; artery, creating turbulence in the bloodstream that mixes
Shamsi et al, 1993), the hot-spot sign has relatively poor sen- infusate and blood more-homogeneously and more rapidly.
sitivity for detection of FNH. Hepatic arterial blood flow is laminar, particularly along
straighter lengths of the artery. Bolus infusions of tracer infusate
Hepatic Arterial Perfusion Studies are typically not advised for HAIS, because the bolus pressure
Hepatic arterial infusion therapy (HAIT) is direct infusion of a may cause retrograde flow of tracer into other celiac branches
therapeutic compound (e.g., chemotherapeutic or radioembolic and associated extrahepatic tracer accumulations (Kaplan et al,
agents) to treat cancerous liver tumors (primary or secondary) 1978).
(see Chapters 96, 99, and 102). Clinical studies demonstrate Extrahepatic tracer accumulations, when tracer is infused
that arterial infusion improves tumor uptake of certain chemo- slowly, are usually attributable to variant hepatic arterial
therapeutic agents compared with portal venous or systemic anatomy, such as branches supplying extrahepatic viscera (e.g.,
venous infusion (Callahan & Kemeny, 2010). Cancerous liver stomach, pancreas, gastrointestinal tract). When the tracer is
tumors derive/stimulate a nutrient blood supply from the arte- bolused, however, such extrahepatic tracer accumulations can
rial system (by tumor neoangiogenesis). Healthy liver receives be mere artifact of bolus technique. True aberrant arterial
blood mostly from the portal venous system. branches typically must be embolized before HAIT, to avoid
Hepatic arterial infusion scintigraphy (HAIS), also called extrahepatic organ toxicity. One of the purposes of HAIS is
hepatic arterial perfusion scintigraphy, is the imaging of the therefore to exclude extrahepatic infusion caused by variant
biodistribution of a radionuclide delivered directly into liver hepatic arterial anatomy.
through an arterial catheter, typically in the (proper) hepatic To identify (1) whether the infused MAA is properly dis-
artery, for delivery of chemotherapy, or potentially into hepatic tributed throughout the downstream liver or targeted hepatic
lobar or segmental arterial branches, when HAIS is conducted subregion and (2) that no extrahepatic infusion is present, a
associated with HAIT radioembolization (e.g., treatment with correlation with abdominal anatomy is needed. SPECT/CT
90
Y-radiolabeled resin or glass microspheres or 131I-radiolabeled provides excellent anatomic localization of infused 99mTc MAA.
314 PART 2 DIAGNOSTIC TECHNIQUES
MAA (NET)
ANTERIOR 1 2 3 4
R L
5 6 7 8
9 10 11 12
MAA NET FLOW 5SE 5 SEC/FR
FIGURE 17.9. Normal appearance of hepatic arterial infusion scintigraphy. Serial abdominal images were obtained during slow bolus injection of
technetium 99m (99mTc) macroaggregated albumin (MAA) into the common hepatic artery via an implanted hepatic pump-catheter system. Each
image is 5 seconds in duration. On the first image, before the 99mTc MAA has been infused into the liver, faint activity is detectable in the liver and
spleen regions (arrowheads); this faint activity is from 99mTc-labeled sulfur colloid tracer, used immediately before to obtain a gross anatomic outline
(see text). The 99mTc MAA is visualized transiting through the pump catheter, as it is slowly infused (arrow). Progressive accumulation of the 99mTc-MAA
infusate throughout the liver is visualized as the infusion is completed. No abnormal extrahepatic accumulation of 99mTc-MAA infusate is evident.
Unlike the liver, the splenic activity remains low and constant across the frames; thus, dynamic imaging allows confirmation that the splenic activity
is only 99mTc-labeled sulfur colloid.
Alternatively, 99mTc-labeled SC scintigraphy can immediately residual 99mTc-SC or free-pertechnetate signal will remain
precede HAIS, to provide a gross outline of hepatic (and unchanged during dynamic imaging of the 99mTc-MAA infu-
splenic) anatomic contours (see Fig. 17.8). Because 99mTc- sion (Fig. 17.9). 99mTc-MAA SPECT/CT without 99mTc SC
MAA HAIS and 99mTc-SC scintigraphy use the same 99mTc has the advantage of having SPECT imagery that solely rep-
isotope, a larger amount (activity, MBq) of 99mTc MAA is resents 99mTc-MAA biodistribution, although CT typically is
administered than 99mTc SC, so that the signal on the subse- associated with a higher radiation dose to the patient than
quent HAIS scan predominantly represents 99mTc MAA. 99m
Tc-SC scintigraphy.
However, confusion can arise regarding overlap between Abnormal HAIS findings include subtotal hepatic infusion,
99m
Tc-SC and 99mTc-MAA signals, as in evaluation of the extrahepatic organ infusion, catheter obstruction, and catheter
homogeneity of 99mTc-MAA hepatic distribution. Additionally, leakage (Fig. 17.10). Abnormal HAIS findings such as these
if any delay occurs after 99mTc SC is injected, before 99mTc- typically undergo further workup by x-ray angiography (fluo-
MAA scintigraphy is performed, 99mTc-SC catabolic breakdown roscopy) or CT hepatic arteriography, to guide subsequent
and release of free pertechnetate can yield gastric tracer-uptake, management. In a clinical study of patients with implanted
potentially mimicking extrahepatic infusion of the stomach on hepatic arterial pump-catheter systems, HAIS studies revealed
99m
Tc-MAA scintigraphy. Obtaining dynamic images of 99mTc- abnormalities in 9% of patients after pump implantation; pre-
MAA uptake as it is infused slowly during 2 minutes or more, dominantly extrahepatic infusion (63% of abnormal studies)
permits detection of increases in hepatic or extrahepatic tracer (Sofocleous et al, 2006). Abnormal subtotal intrahepatic infu-
uptake indicative of true 99mTc-MAA signal, whereas any sion (i.e., infusion distributed to only a portion of the liver,
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CHAPTER 18
Computed tomography of the liver, biliary tract,
and pancreas
Seth S. Katz
316
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 317
A B
FIGURE 18.1. A, Thick-slab maximum intensity projection (MIP) through the portal veins reveals standard bifurcation of the main portal vein into
the right (arrow) and left (arrowhead) portal veins. The anterior and posterior sectoral branches of the right portal vein are evident, as are the medial
and lateral sectoral branches of the left portal vein. B, Thick-slab MIP image through the hepatic veins reveals the three major hepatic veins
(arrowheads) and an accessory hepatic vein (arrow) draining into the inferior vena cava.
Fissure for
falciform ligament
A B
FIGURE 18.2. A, Volume-rendered three-dimensional (3D) image of the external contour of the liver created from contrast-enhanced axial computed
tomographic data. Note the fissure for the falciform ligament seen en face (arrow). B, Volume-rendered 3D image of the same patient rotated upward
reveals the undersurface of the liver. Note the surgical clips in the gallbladder fossa and the bare area of the liver (short arrow).
The increasing use of the modality, the propensity of early control systems (McCollough et al, 2006), until relatively
MDCT to generate higher radiation doses per examination, and recently, the traditional algorithm by which raw acquired data
increasing use of multiphasic studies in liver and pancreas CT are transformed into images, called filtered back projection
have made dose reduction a priority (Brenner & Hall, 2007). (FBP), had remained untouched throughout almost 40 years
Although some headway (20% to 40% dose reduction) had of CT progress. Around 2011, an improved “partially iterative”
been made early in the past decade with automatic exposure reconstruction algorithm called adaptive statistical iterative
318 PART 2 DIAGNOSTIC TECHNIQUES
An exciting methodology called texture analysis, not yet in (see Chapter 2) and to assess the proximity of lesions to the
clinical use, is being brought to bear in interpretation. Not inflow and outflow vessels. This information determines the
specific to CT, the analysis of pixel intensity variation can be extent of potential hepatic resection required to achieve clear
made using data produced by any modality. Preliminary results surgical margins (Figs. 18.7 and 18.8). If a proposed operation
suggest that certain hepatic texture features can predict survival will be extensive, postprocessing of CT images with 3D volume
in colon cancer patients (Miles et al, 2009), can identify the rendering can also identify segmental or lobar hepatic atrophy
presence of colon cancer hepatic micrometastases not yet visible (Fig. 18.9) and compensatory hypertrophy. Manual or auto-
by standard visual image review (Rao et al, 2014), and can mated segmentation with volumetric calculation can help predict
preoperatively stratify risk for postoperative hepatic failure in whether postoperative liver volume will be sufficient to safely
candidates for major hepatic surgery (Simpson et al, 2015).
Texture analyses also show promise in discriminating among
hypervascular liver lesions, potentially increasing specificity in
the noninvasive diagnosis of HCC, hepatocellular adenoma,
and focal nodular hyperplasia (FNH).
7 2
8 4a
3
4b
5
6
FIGURE 18.10. Arterial phase image reveals the right hepatic artery
(arrow) coursing anterior to the common hepatic duct, which contains
avoid hepatic failure (see Chapters 100 and 108). Steatosis and
air from a papillotomy.
cirrhosis, processes that affect the remnant liver’s ability to
regenerate, can also be recognized (although not as clearly as by
MRI).
Early arterial-phase high-resolution images (CT angiogra- angiography. Because most neoplasms involving the liver are
phy) are obtained to assess tumor involvement of arteries and hypovascular relative to adjacent normal liver parenchyma,
evaluate variant celiac axis anatomy, which occurs in more than routine abdominal imaging generally uses only the portal
half of the population (Michels, 1955). Because visualization of venous phase, in which these are most conspicuous. Hypervas-
the surgical field is often limited in patients with prior surgery, cular neoplasms such as HCC and certain types of metastasis,
obesity, hepatobiliary malignancy, and local inflammation, including neuroendocrine tumors, renal cell carcinoma, mela-
preoperative knowledge of variant celiac anatomy can assist noma, and thyroid cancer, are generally evaluated using a tri-
in surgical planning (see Chapters 2, 103, and 104), facilitate phasic protocol that includes precontrast and late arterial-phase
dissection, and help the surgeon avoid iatrogenic injury images as well as portal venous phase images. Delayed phases
(Winston et al, 2007). Identification of variant anatomy is also (see later) are now deemed important to add in evaluating for
crucial to decisions regarding hepatic arterial embolization and possible HCC (Bruix & Sherman, 2011) and in follow-up of
placement of hepatic arterial chemoinfusion pumps; gains in known HCC (Lencioni et al, 2010). Five-millimeter axial slices
image resolution during the MDCT era have allowed CT through the liver are routinely reviewed. Thinner images can be
angiography to largely supplant invasive direct catheter angiog- requested by the radiologist on any type of examination in
raphy for planning placement of intraarterial chemoinfusion problem-solving situations, provided the raw image data are still
pumps (Kapoor et al, 2003) (see Chapter 99). Vascular mapping extant on the scanner, usually for a day or two after the acquisi-
may now also be performed with CT. The relationship of arter- tion. Coronal and sagittal reformatted images (2.5 mm) are
ies to the bile ducts can be identified, which is also valuable for generally routinely generated for review in addition to axial
surgical planning (Fig. 18.10) (see Chapters 2 and 103). Late images on all examinations, and more advanced 3D postpro-
arterial-phase images (included in the “triphasic” examination, cessing is generally made available on certain studies, such as
unlike early arterial images) are obtained for detection and CT angiographic examinations.
delineation of hypervascular hepatic lesions.
Noncontrast Computed Tomography of the Liver
Technique and Protocols An unenhanced scan is generally included in the triphasic
State-of-the-art CT evaluation of the liver for hepatic resection dedicated liver evaluation. The normal unenhanced liver typi-
now may include, depending on the indication, any combina- cally has attenuation values between 54 and 60 Hounsfield
tion of image acquisition in the precontrast, IV contrast- units (HU), approximately 8 HU greater than the spleen due
enhanced early (CT angiography) and late arterial phase, portal to hepatic glycogen and iron stores. Abnormally increased
venous phase, and delayed phases. Oral hyperattenuating “posi- attenuation may be seen in hemochromatosis (Fig. 18.11),
tive” contrast medium (water-soluble iodinated agent or dilute glycogen storage diseases, Wilson disease, β-thalassemia, sickle
barium) is typically administered for routine examinations, cell disease, and after administration of certain drugs (amioda-
although some institutions now advocate regular use of oral rone, cisplatin), whereas abnormally decreased hepatic attenu-
water as a negative contrast agent (Kammerer et al, 2015; ation is most frequently attributable to steatosis (Fig. 18.12).
Makarawo, 2013), as is the standard practice with CT These processes may be obscured by the administration of
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 321
A B
FIGURE 18.14. A, Arterial phase image through the inferior right hepatic lobe reveals branches of the right hepatic artery. Faint enhancement of
a hypervascular mass is seen in segment VI, which proved to be focal nodular hyperplasia (arrow). B, Portal venous phase image through the same
level reveals enhancement of the right portal vein (long arrow) and the sectoral branches. The mass (short arrow) is nearly hypointense to the liver.
A B
FIGURE 18.15. Arterial and portal venous phase images as part of a triphasic examination in a patient with metastatic renal cell carcinoma.
A, Late arterial-phase image reveals multiple hypervascular enhancing foci of metastatic renal cell carcinoma (arrows). B, Portal venous phase image
at the same level does not reveal the numerous masses. The low-attenuation lesion represents a partially treated hypoattenuating metastasis.
PORTAL VENOUS PHASE IMAGING. Normal noncirrhotic hepatic “equilibrium” phase) may be added to the traditional triphasic
parenchyma enhances maximally at approximately 70 seconds examination—a four-phase CT. Some intrahepatic cholangio-
after injection initiation. At this time, referred to as the portal carcinomas may be inconspicuous on the traditional components
venous phase of enhancement, maximal contrast differential of the triphasic examination, and considerably delayed imaging
between typical hypovascular liver lesions and the surrounding may be added when this entity is suspected (see Chapter 50). No
parenchyma is achieved, as well as clear delineation of the specific optimal timing for this indication has been firmly estab-
portal and hepatic veins. Routine evaluation of the liver should lished, but a delay of 5 to 12 minutes is typically used.
be performed using this phase timing.
Anatomy
DELAYED IMAGING PHASES. Malignant hypervascular tumors, An extensive and detailed discussion of hepatic and biliary
particularly HCC (see Chapter 91), typically become hypoat- anatomy, some of it using CT images, can be found in Chapter
tenuating to adjacent normal hepatic parenchyma at some point 2. Axial CT images are displayed by convention as if the patient
after the late arterial phase. Although this is often seen in the were lying face up with feet toward the viewer and head away
routinely acquired portal venous phase, it may only be appreci- from the viewer into the viewing screen, so that the patient’s
ated on further delayed imaging (Iannaccone et al, 2005; right side, including the liver is to the interpreter’s left—the
Liu et al, 2012). Therefore, when HCC is suspected, a 3- to viewer is effectively looking cephalad at the caudal surface of
5-minute delayed phase (variably described as “late venous” or each slice.
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 323
M L
M L
R ivc R ivc
A B
pvl
pvr
c c
ivc
ivc ivc
C D
GB
pv c
ivc
E
FIGURE 18.16. Normal hepatic segmental and vascular anatomy on computed tomography. A, On cephalad sections, the three hepatic veins (R,
right hepatic vein; M, middle hepatic vein; L, left hepatic vein) are seen to enter the inferior vena cava (ivc). B, The lines of the hepatic veins divide
the liver into sectors. The right hepatic vein divides the right liver into anterior and posterior sectors, the middle hepatic vein separates the right from
the left liver following the line of the interlobar scissura, and the left hepatic vein separates segments II and III of the left lobe. C, Approaching the
midpoint of the liver, the left portal vein (pvl) is seen. The fissure for the ligamentum venosum (arrows) separates the caudate lobe (c) from the left
lateral segments. D, The next section shows the horizontal portion of the right portal vein (pvr). The fissure for the ligamentum teres is now seen
anteriorly (large arrows) separating segment IV from the left lateral segments. E, On the most caudad section, the gallbladder (GB) has come into
view; a line drawn along its axis to the IVC represents the inferior extent of the interlobar scissura.
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 325
ha
pv
A B
FIGURE 18.20. Contrast-enhanced computed tomography in a patient with a minimally dilated biliary system. A, The intrahepatic bile ducts are
seen as branching, low-attenuation structures adjacent to the portal veins. At the porta hepatis, the hepatic artery (arrow) is seen to pass between
the main portal vein (pv) and the common hepatic duct. B, A scan caudal to the porta hepatis shows the common hepatic duct and the cystic duct
running adjacent to each other in the hepatoduodenal ligament (arrows). The hepatic artery (ha) is in a more medial position.
CBD
*
FIGURE 18.21. Coronal reformatted image of the confluence of the
right (solid arrow) and left (open arrow) hepatic ducts reveals bilobar
intrahepatic biliary ductal dilation. Note subtle soft tissue thickening
and enhancement along the common bile duct (arrowheads), reflecting FIGURE 18.22. Coronal reformatted image created from axial com-
recurrent gallbladder carcinoma in a patient after cholecystectomy. puted tomographic data acquired after intravenous administration of
contrast medium. Bile is displayed as bright areas with marked dilation
of the intrahepatic bile ducts and the common bile duct (CBD). Note the
distended gallbladder (asterisk) and the aberrant biliary drainage of
obstruction secondary to a large cyst (Fig. 18.25); in such cases, segment VI (arrowheads) directly into the CBD.
therapeutic intervention may be indicated.
A B
C D
FIGURE 18.26. Cavernous hemangioma of the right liver showing typical enhancement starting at the periphery of the lesion (A to C) and finally
showing complete opacification (D).
A B
FIGURE 18.27. A, Volume-rendered three-dimensional image of a giant hemangioma. The image is oriented such that the patient is facing forward,
with the observer looking down from above. Note the peripheral nodular, clumplike enhancement (black arrow) and the central low-attenuation scar
(white arrow). The hemangioma is in contact with the left hepatic vein (arrowhead) and with the inferior vena cava (IVC). B, Volume-rendered coronal
image of the same patient. The giant hemangioma exerts mass effect on a long segment of the IVC (arrows), which is displaced to the left of midline.
The right kidney (arrowhead) is displaced inferomedially by the mass. Resection was performed with a good result. (Courtesy L.H. Blumgart, MD.)
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 329
A B
FIGURE 18.28. Focal nodular hyperplasia. A, Contrast-enhanced computed tomographic image acquired in the late arterial phase reveals the
arterial supply to a well-circumscribed hypervascular mass in the right hepatic lobe. B, Oblique coronal, volume-rendered three-dimensional reformat-
ted image of the same patient reveals early venous drainage from the mass via a large vein (arrow) into the inferior vena cava (arrowhead). The major
hepatic veins have not yet opacified with contrast material.
A B
FIGURE 18.29. Focal nodular hyperplasia. A, Arterial phase image shows a well-circumscribed, brightly enhancing lesion in segment IV/V. B, During
the portal phase, the lesion is isoattenuating to liver parenchyma and cannot be identified.
adenomatosis, a term coined in 1985, refers to multiple (>10) immunohistochemistry have allowed subtyping of HCA into
adenomas in a patient without known risk factors (Flejou et al, four groups: HNF1α-mutated, β-catenin–mutated, inflamma-
1985). A strong association with oral contraceptive use has long tory (most common), and unclassified (Zucman-Rossi et al,
been established (Blumgart et al, 2001), and other risk factors 2006). The inflammatory type appears most prone to hemor-
for the development of HCA include type I glycogen storage rhage, and the β-catenin–mutated type confers the most risk of
disease (Labrune et al, 1997) and use of androgen-containing developing HCC (Katabathina et al, 2011).
steroids (Soe, 1992). The CT appearance of adenomata often overlaps with FNH
Adenomas contain large plates of hepatocytes separated by and HCC. Adenomata tend to have similar attenuation to
dilated sinusoids perfused solely by peripheral arterial feeding normal liver on unenhanced scans, enhance homogeneously
vessels. Intracellular and intercellular lipids manifest as macro- after contrast administration in the arterial phase with sharply
scopic fat within the tumor (Ichikawa et al, 2000). The combi- marginated hypervascularity and occasional (30%) capsulated
nation of poor connective tissue support and central necrosis appearance, and fade on portal venous phase images (Grazioli
predisposes to hemorrhage (Levy & Ros, 2001), particularly et al, 2001). Larger adenomas are more heterogeneous in
the large lesions (Leese et al, 1988). Recent advances in appearance than smaller lesions, presumably because of the
330 PART 2 DIAGNOSTIC TECHNIQUES
predilection to hemorrhage. Peripheral enhancement reflects bubbles may be seen if anaerobic bacteria are present, and
the presence of large subcapsular feeding vessels, with a resul- the periphery and internal septa may enhance after contrast
tant centripetal pattern of enhancement. Hemorrhage and fat agent administration. Abscesses often have a thick wall, which
within lesions can be best detected on unenhanced imaging as enhances with contrast administration (Fig. 18.30). In addition,
well as calcifications, which are present in a small minority there may be hepatic enhancement peripheral to the enhancing
(10%) of lesions (Grazioli et al, 2000, 2001). Although these wall, secondary to increased capillary permeability. This is
features are nonspecific, recent studies attempting to correlate referred to as the double-target sign (Mendez et al, 1994; Murphy
recently designated subtypes with MRI imaging features (van et al, 1989).
Aalten et al, 2011) suggest that presence of homogeneous fat
within HCA is associated with the HNF1α-mutated subtype. Fungal Abscesses (See Chapter 72)
We are unaware of any similar large studies correlating MDCT Fungal hepatic abscesses generally are disseminated microab-
features with subtype (Katabathina et al, 2011). scesses that occur in immunosuppressed patients. The most
common fungal organism implicated is Candida albicans. Other
Biliary Hamartoma (See Chapters 48 and 90A) fungal infections that cause microabscesses include cryptococ-
Bile duct hamartomata, also known as the von Meyenburg cus, histoplasmosis, and mucormycosis.With contrast-enhanced
complex, are common benign tumors composed of disorganized CT, hepatic microabscesses appear as small, hypodense lesions,
bile ducts and ductules with a fibrocollagenous stroma (Horton ranging from several millimeters to 1.5 cm in size. A bull’s-eye
et al, 1999). The tumors usually range from 1 to 15 mm, do appearance may be identified, with a small, high-attenuation
not communicate with the biliary tree, and are scattered focus centrally surrounded by a low-attenuation zone. Authors
throughout the liver (Wei et al, 1997); although they are often have reported significant increase in the sensitivity and lesion
multiple (Blumgart et al, 2001), they may be solitary. They have conspicuity using arterial-phase CT, compared with portal
a nonspecific imaging appearance most often confused with venous phase CT, when evaluating liver lesions in immunocom-
cysts although they may also be mistaken on CT for metastases promised patients suspected to have hepatosplenic fungal
or microabscesses with greater clinical consequence (Eisenberg infections (Metser et al, 2005).
et al, 1986; Lev-Toaff et al, 1995; Sada & Ramakrishna, 1994).
On MRI, they are more readily recognized as cystic in Echinococcus (See Chapter 74)
appearance. In endemic areas, involvement of the liver by hydatid disease is
a common finding. Echinococcus granulosus presents with a large
Bile Duct Adenoma (See Chapters 48 and 90A) solitary mass or multiple well-defined cystic lesions, which
Bile duct adenomata are usually incidentally detected, benign, often contain internal “daughter” cysts (Fig. 18.31). Coarse
asymptomatic lesions (Welch et al, 1985). They are usually calcifications of the wall are present in 50% of patients
solitary, subcapsular, and small, ranging in size from 0.1 to (Fig. 18.32) and internal calcification in the matrix may also
1 cm. On CT, bile duct adenomata are well-defined hypoat- be seen. Dense or complete lesion calcification implies parasite
tenuating or isoattenuating lesions, enhancing little or not at all death, though partial cyst calcification does not necessarily
after contrast administration. No specific imaging findings are indicate inactivity (Pedrosa et al, 2000). Daughter cysts are
known, however, and definitive diagnosis can be made only at identified in approximately 75% (de Diego Choliz et al, 1982;
histologic analysis (Horton et al, 1999). Murphy et al, 1989). Communication between the cysts
and the biliary tree is found in approximately 25% of patients
Inflammatory Conditions
Pyogenic Abscess (See Chapter 72)
Recent surgery, biliary disease, diverticulitis, Crohn disease,
and alcoholism all predispose to pyogenic hepatic abscess,
commonly caused by Clostridium species and gram-negative
bacteria such as Escherichia coli and Bacteroides, which enter the
liver via the biliary tree or portal venous system (Mergo & Ros,
1997). Ascending cholangitis and portal phlebitis are the most
common causes of pyogenic hepatic abscesses (Murphy et al,
1989).
As a result of the widespread use of broad-spectrum antibi-
otics, the clinical presentation and CT appearance vary widely
(Halvorsen et al, 1984). Pyogenic hepatic abscesses may be
classified as either microabscesses (<2 cm) or macroabscesses,
larger confluent lesions. Microabscesses appear as small, well-
defined, hypodense lesions on contrast-enhanced CT. They
may be widely scattered or clustered with a tendency to coalesce
(Jeffrey et al, 1988). Larger pyogenic abscesses range in appear-
ance from unilocular cavities with smooth outer margins to
highly complex and septated structures with internal debris and
irregular contours. Most large pyogenic abscesses appear as a
well-defined mass of low attenuation on unenhanced CT. The FIGURE 18.30. Contrast-enhanced computed tomography of a
attenuation value of the abscess cavity depends on the age of pyogenic liver abscess shows enhancement of the walls and internal
the abscess; it becomes lower as the abscess matures. Gas septa. A sympathetic right-sided pleural effusion is seen.
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 331
A B
FIGURE 18.31. Contrast-enhanced axial computed tomography reveals a multiseptated echinococcal cyst in the right hepatic lobe. Note eccentric
calcifications along the wall of one of the cysts (arrow).
A B
FIGURE 18.33. Numerous foci of fat deposition at two different levels through the liver (left and right panels). Contrast-enhanced computed
tomography reveals numerous hypoattenuating lesions (white arrows) lesions in a patient with breast cancer. Note lack of mass effect or distortion
of the hepatic vessels. Lesions were stable over time and were shown to represent focal fatty deposition on magnetic resonance imaging.
A B
FIGURE 18.35. Cirrhosis. A, The liver has an irregular outline. B, The interlobar fissure, delineated by the gallbladder, is deviated toward the right
as a result of atrophy of the right liver with hypertrophy of the left liver and the caudate lobe.
splenorenal and gastrorenal shunts, and paraumbilical and and hepatitis B and C viruses. Approximately 70% of HCCs
abdominal wall veins (Kang et al, 2002). develop in cirrhotic livers (Blumgart et al, 2001) in which the
parenchyma is often distorted by nodular regeneration and
Budd-Chiari Syndrome (See Chapter 88) fibrosis, and in which alterations in arterial and portal venous
Budd-Chiari syndrome is caused by chronic hepatic venous blood flow are common. These changes can both simulate
congestion secondary to obstruction to hepatic venous outflow. disease and obscure malignant lesions (Baron & Peterson,
The CT appearance is characterized by hepatomegaly and 2001), making detection of HCC in the cirrhotic liver an even
ascites; the hepatic veins either contain thrombus (Fig. 18.36) greater diagnostic challenge than in noncirrhotic livers.
or are obliterated. Precontrast scans show decreased attenua- A limitation to noninvasive diagnosis of HCC has been its
tion of hepatic parenchyma because of congestion; postcontrast variable imaging appearance. On CT, HCCs are typically
scans show normal enhancement of the caudate lobe, which is hypervascular in the arterial phase, subsequently becoming
hypertrophied in chronic cases, and patchy enhancement of the hypoattenuating to surrounding liver in later phases, a pattern
remainder of the liver (Vogelzang et al, 1987). Concomitant termed “washout appearance” (Fig. 18.37). However, some
portal vein thrombosis is present in 20% of patients with Budd- tumors exhibit washout appearance only on delayed imaging or
Chiari syndrome. A similar CT appearance of the liver, with not at all, and others are not hypervascular. Another classic
patchy enhancement, is seen in patients with congestive heart feature is the presence of an enhancing tumor capsule hyperat-
failure; in contrast to patients with true Budd-Chiari syndrome, tenuating to the lesion and the surrounding parenchyma on
these patients have patent and enlarged hepatic veins (Moulton portal venous or delayed phases. HCC has a propensity to
et al, 1988). invade adjacent portal (Fig. 18.38) or hepatic veins and IVC
(Fig. 18.39) (Freeny et al, 1992) particularly in cirrhotic livers
Hepatic Infarction (Smalley et al, 1988); identification of enhancing tumor in the
Hepatic infarction is rare and implies compromise to the arte- portal vein is a highly specific sign of HCC in cirrhotic livers.
rial and portal venous supply to a segment or lobe of the liver. Larger lesions (>5 cm) tend to be heterogeneous with a mosaic
CT findings include a well-defined, wedge-shaped area of pattern of enhancement (Stevens et al, 1996) and may contain
low attenuation in a segmental or subsegmental distribution, necrosis and fatty metamorphosis. Approximately 5% of HCCs
extending to the liver surface. After contrast administration, the are associated with spontaneous rupture and hemoperitoneum
affected zone enhances minimally, often with a peripheral thin (Blumgart et al, 2001), and tumor may also invade bile ducts,
subcapsular enhancing rim. Gas formation within sterile infarcts causing obstruction. Whereas HCC in a noncirrhotic liver typi-
is a recognized finding and does not imply superimposed infec- cally presents as a large hypervascular solitary or dominant mass
tion. A late complication of hepatic infarction is formation of with small satellite nodules and central necrosis (Fig. 18.40)
bile lakes in the affected segments as a result of disruption of (Brancatelli et al, 2002; Winston et al, 1999b), in a cirrhotic
biliary radicles. liver, HCC commonly appears as multifocal small lesions.
In the context of cirrhosis, a large study at an experienced
Malignant Lesions of the Liver liver transplant center demonstrated a false-positive HCC
Hepatocellular Carcinoma (See Chapter 91) diagnosis rate of 8% on the basis of CT findings in 1329
HCC is the most common primary hepatic malignancy world- patients referred for hepatic transplantation (Brancatelli et al,
wide, with highest incidence in Asia, Southeast Asia, and sub- 2003). Benign lesions often mistaken for HCC include focal
Saharan Africa. Although less common in the West, the incidence confluent fibrosis, transient hepatic attenuation difference,
of HCC in the United States has been increasing (Arakawa flash-filling hemangiomata, peliosis, and regenerative nodules
et al, 1986). The most significant risk factors include cirrhosis with or without dysplastic change. Regenerative nodules are
334 PART 2 DIAGNOSTIC TECHNIQUES
CL
A B
C
FIGURE 18.36. A, Contrast-enhanced computed tomography (CT) in a patient with acute hepatic venous thrombosis leading to Budd-Chiari
syndrome shows nonenhancement of the thrombosed hepatic veins. There also is patchy peripheral parenchymal enhancement. B, In a patient with
chronic Budd-Chiari syndrome resulting from a congenital stricture of the intrahepatic inferior vena cava, enlargement of the caudate lobe (CL) and
marked homogeneity of parenchymal enhancement are seen. Splenomegaly also is seen. C, Contrast-enhanced CT reveals mottled parenchymal
enhancement and enlargement of the caudate lobe (arrows) in a patient with occlusion of the hepatic veins secondary to paroxysmal nocturnal
hemoglobinuria.
only detectable on CT when they contain iron (and are thus reduce variability and errors in imaging interpretation. Subse-
hyperattenuating on unenhanced scans) or when they distort quently, it has undergone two updates, the latest in 2014,
the hepatic contour. They typically do not enhance during the (American College of Radiology. LI-RADS version, 2014)
arterial phase, an important characteristic distinguishing them bringing it into alignment with the Organ Procurement and
from typical HCC, and during the portal venous phase, they Transplantation Network (OPTN) classification. The most
enhance homogeneously to the same degree as surrounding central aspect of the system is to consider a lesion “definitely
fibrotic parenchyma, rendering them invisible (Baron & Peter- HCC” if either (1) enhancing tumor is observed in the portal
son, 2001). vein, (2) it is greater than or equal to 1 and less than 2 cm in
Dysplastic nodules are precursor lesions to frank HCC with diameter, hypervascular, and has at least two of three major
cellular atypia and abnormal “nontriadal” arterial supply that features, or (3) it is greater than or equal to 2 cm in diameter
distinguish them from regenerative nodules. Although the and hypervascular, with at least one major feature. Major fea-
majority are invisible on CT, like regenerative nodules, some tures are washout appearance, enhancing tumor capsule, and
particularly higher-grade lesions do enhance in the arterial “threshold growth” defined as diameter increase of greater than
phase and may mimic HCC (Baron & Peterson, 2001). or equal to 50% in less than or equal to 6 months, greater than
The elevated pretest probability of HCC in patients with or equal to 100% increase in greater than 6 months, or any new
cirrhosis or other risk factors and the difficulties associated with lesion greater than or equal to 1 cm. Lesions only partly meeting
diagnosis by CT and MRI prompted development in 2011 of these criteria are considered “probably HCC” or “intermediate
the Liver Imaging Reporting and Data System (LI-RADS). probability.” Although an initial evaluation of the system using
Advocating use of consistent terminology, its goal was to catego- MRI (Davenport et al, 2014) suggested that LI-RADS creates
rize liver findings, specifically in high-risk patients, aiming to too many strata of HCC probability for robust interreader
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 335
A B
C
FIGURE 18.37. Precontrast, arterial-phase, and portal venous phase images in a patient with a large hepatocellular carcinoma. A, Unenhanced
imaging reveals a hypoattenuating mass. B, Arterial-phase images reveal the mass is heterogeneously hypervascular with supply from small arteries
(arrow). C, Portal venous phase image reveals the “washout appearance” with tumor now enhancing to a lesser degree than surrounding
parenchyma.
A B
FIGURE 18.38. A, Contrast-enhanced computed tomography reveals an exophytic hepatocellular carcinoma (arrow) with tumor thrombus extend-
ing up the main portal vein (arrowheads). B, Coronal maximum intensity projection image in the same patient reveals extensive collateral venous flow
(arrows) about the mass.
336 PART 2 DIAGNOSTIC TECHNIQUES
A B
FIGURE 18.39. Hepatocellular carcinoma (HCC). Contrast-enhanced computed tomography reveals HCC involving segment I of the liver (arrow).
Tumor thrombus extends into the inferior vena cava and right atrium (arrow).
hepatic involvement is seen in 50% of patients with non- Diffuse or infiltrative forms of the disease result in irregular
Hodgkin lymphoma and in 60% of patients with Hodgkin infiltration in the portal areas.
disease. Approximately 6% to 20% of patients with Hodgkin
disease have hepatic involvement at presentation (Castellino, Hepatic Metastases (See Chapters 92 to 94)
1982; Fishman et al, 1991; Sandrasegaran et al, 1994). Liver The second most common site for metastases behind only
involvement usually is associated with lymph node disease and lymph nodes, the liver provides a receptive environment for
almost invariably is associated with splenic disease. The more metastases not only because of its dual blood supply by systemic
extensive the splenic involvement, the greater the likelihood of and portal systems but also because of humoral factors that
hepatic involvement (Figs. 18.41 and 18.42). promote cell growth. The CT appearance of metastases varies,
On CT, hepatic involvement usually appears diffuse; discrete depending on the size and vascularity of the primary tumor, the
nodular lesions are seen in only 10% of cases. The sensitivity degree of necrosis, and the CT technique used (see “Liver and
of CT in the detection of hepatic disease is low, presumably Biliary Technique and Protocol” section). Lesion morphology
because liver involvement is diffuse. It is thought that extensive may be round, ovoid, or irregular, and borders may be sharp,
disease must be present before becoming apparent at imaging, poorly defined, or nodular. Attenuation is usually lower than
and CT may reveal only hepatomegaly with no focal lesion. that of surrounding hepatic parenchyma on unenhanced CT.
IV contrast enhancement during the appropriate phase
increases the sensitivity of lesion detection. Hypovascular
metastases enhance less and are hypoattenuating compared
with surrounding enhancing hepatic parenchyma during portal
venous phase scanning, whereas hypervascular metastases may
be obscured during the portal venous phase and are usually
most clearly visualized during the arterial phase (see Fig.
18.15). Metastases from mucinous carcinomas tend to contain
punctate or amorphous calcification. Cystic metastases often
contain mural nodules, fluid-fluid levels, or septations, whereas
benign cysts tend to have a less complex appearance. The
appearance of metastases may change in response to treatment.
The attenuation of lesions may decrease as they undergo
necrosis (Figs. 18.43 and 18.44); for instance, hepatic metas-
tases from gastrointestinal stromal tumors (GISTs) that respond
to imatinib become near cystic on contrast-enhanced CT (Choi
et al, 2007). Therefore, when evaluating the liver on CT in a
patient with a history of GIST, it is important to know whether
the patient has undergone treatment, and comparison with
pretreatment images becomes essential. Metastases may cause
focal biliary ductal dilation by compressing or invading an
FIGURE 18.41. Contrast-enhanced computed tomography reveals adjacent bile duct (Fig. 18.45).
multiple hepatic masses in a patient with lymphomatous involvement of
the liver and spleen. Note the low-attenuation mass in the spleen (arrow). Biliary System
Advances made earlier in the MDCT era expanded the role of
CT in evaluating the biliary tree. Acquisition of high-resolution
thin-collimation images obtained in a single breathhold and
image review in cine mode and multiple planes facilitate tracing
dilated bile ducts to the point of obstruction. Biliary obstruc-
tion is diagnosed by CT on the basis of dilated intrahepatic or
extrahepatic bile ducts (see Fig. 18.21) that appear as tubular
branching or circular structures of fluid attenuation that enlarge
as they approach the ductal confluence in the porta hepatis.
However, a direct correlation between ductal caliber and the
presence of clinically significant obstruction is not always found.
Normal-caliber bile ducts may be observed despite the presence
of intermittently obstructing calculi, subtle strictures of the
extrahepatic duct, and surgically correctable causes of jaundice.
Conversely, the biliary tree may remain permanently dilated
after surgical or spontaneous relief (e.g., stone passage) of
biliary obstruction; in such patients, the CT appearance may
falsely suggest biliary obstruction. When a discrepancy exists
between the CT findings and clinical or biochemical evidence,
clinical findings generally carry greater weight, and magnetic
resonance cholangiopancreatography (MRCP) or direct percu-
FIGURE 18.42. Large unifocal lymphomatous mass in the right taneous or endoscopic cholangiography may be performed to
hepatic lobe (arrow). Small splenic lesions are also seen. resolve the issue.
338 PART 2 DIAGNOSTIC TECHNIQUES
A B
FIGURE 18.43. Metastatic colon cancer. A, Before treatment. B, After treatment.
A B
FIGURE 18.44. Contrast-enhanced computed tomography in a patient with metastatic gastrointestinal stromal tumor. A, Before treatment, het-
erogeneous solid enhancing masses are seen in the right and left hepatic lobes (arrows). B, After treatment, lesions have lower attenuation and
appear more cystic (arrows).
A B
FIGURE 18.47. Mirrizi syndrome. A, Contrast-enhanced computed tomography reveals a large calcified gallstone associated with gallbladder wall
thickening and extensive pericholecystic inflammatory change (arrowheads). B, Extensive inflammatory change surrounds the internal biliary stent
(arrow).
Associated biliary dilation resulting from infiltrative tumor appearance: mass forming, periductal infiltrating, and intraductal
along the cystic duct to the extrahepatic bile duct, lymphade- growing, corresponding in older literature to the terms “nodular,”
nopathy compressing the bile duct, or intraductal spread of “sclerosing/infiltrating,” and either “exophytic” or “papillary,”
tumor is apparent on CT (Levy et al, 2001). Tumor growth respectively. A combination of periductal infiltrating and mass
through the gallbladder wall away from the liver results in forming types is also common. Cholangiocarcinoma has also
peritoneal carcinomatosis. been divided by the seventh edition of the American Joint
Laparoscopic cholecystectomy has become increasingly Committee on Cancer Cancer Staging Manual (Edge et al,
accepted as a treatment for symptomatic uncomplicated chole- 2010) into perihilar, distal, and intrahepatic types, which are
lithiasis (Southern Surgeon’s Club, 1991), and approximately distinct clinical and radiologic entities (Han et al, 2002). The
15% to 30% of gallbladder carcinomas are detected incidentally perihilar location is most common at 60% to 70%, distal sites
at microscopic review of cholecystectomy specimens (Clair are less common at 20% to 30%, and intrahepatic is least
et al, 1993). A serious potential complication of laparoscopic common at 5% to 15% (Matos et al, 2010; Patel, 2006).
cholecystectomy is the inadvertent dissemination of unsus-
pected gallbladder carcinoma (Winston et al, 1999a). Wib- PERIHILAR CHOLANGIOCARCINOMA (SEE CHAPTER 5). Imaging fea-
benmeyer and colleagues (1995) reported that gallbladder tures of perihilar tumors, in general, include intrahepatic seg-
carcinoma recurs more rapidly after laparoscopic cholecystec- mental biliary dilatation, ductal wall thickening, endoluminal
tomy than after open cholecystectomy. Tumor can recur in the lesions and tumor spread to adjacent liver and/or vessels. Seg-
laparoscopic port tracks, even if surgical resection of the port mental intrahepatic biliary dilation is often seen just peripheral
sites is performed at subsequent hepatic resection for attempted to an ill-defined perihilar mass with abrupt transition between
cure. Recurrent tumor may appear as a mass along the anterior dilated and nondilated ducts. Because this is a key diagnostic
abdominal wall with extension into the subjacent omental fat feature, diagnosis is impeded by biliary drainage prior to scan-
(Fig. 18.51) (Winston et al, 1999a). These observations under- ning (Valls C, et al, 2013). Other clues to the presence of a
score the need to correctly identify findings suggestive of gall- cholangiocarcinoma include crowding of bile ducts and lobar
bladder carcinoma on preoperative imaging when elective atrophy (Engelbrecht et al, 2015). CT (after the advent of
laparoscopic cholecystectomy is planned. helical scanning) is excellent at detecting and localizing these
tumors; one study reported accuracy of 91% (Feydy et al,
Cholangiocarcinoma (See Chapters 50 and 51) 1999).
Cholangiocarcinoma is a relatively rare adenocarcinoma of the In this location, the periductal infiltrating morphologic
bile duct epithelium presenting mostly after the sixth decade of subtype is most common (Valls et al, 2013), accounting for
life. Although most patients have no known risk factors, condi- more than 70% of cases (Matos et al, 2010) (Fig. 18.52). This
tions conferring increased risk include liver fluke infestation, tumor subtype often appears as focal duct wall thickening with
primary sclerosing cholangitis, choledochal cyst (including obliteration of the lumen (Han et al, 2002) but may only mani-
Caroli’s disease), hepatolithiasis, bile stasis, abnormal choled- fest as ductal enhancement or merely narrowing. Hypoenhanc-
ochopancreatic junction, hepatitis C viral infection, cirrhosis, ing soft tissue infiltration of adjacent periductal fat may also be
alcoholic liver disease, ulcerative colitis, type 2 diabetes, thyro- visible with delayed-phase hyperenhancement, although this
toxicosis, and pancreatitis (Valls et al, 2013). infiltration may sometimes be hypervascular, as is seen in the
The Liver Cancer Study Group of Japan (1997) categorized intrahepatic tumor type (Valls et al, 2013). Most strictures are
cholangiocarcinomas into three subtypes based on macroscopic malignant and are thus considered worrisome until proven
otherwise. Malignant strictures tend to be longer (≥18 to
22 mm) and have a thicker wall (≥2 mm) than benign strictures,
and they show arterial- or portal-phase bile duct hyperenhance-
ment (Choi et al, 2005).
Mass-forming perihilar tumors, like their intrahepatic coun-
terparts, appear as heterogeneous hypovascular masses with
peripheral rim enhancement in the arterial and portal phase
and central enhancement in delayed phases.
Tumors in the least common intraductal-growing subtype
(8% to 18%) predominantly have multiple lesions along various
segments of the bile ducts with papillary histologic features
differentiating them from the other types of cholangiocarcinoma
(Engelbrecht et al, 2015). The World Health Organization
endorses the term “intraductal papillary neoplasm of the bile
ducts” to encompass all variants of biliary intraductal neoplasia,
which has been recognized as a biliary counterpart of pancreatic
intraductal papillary mucinous neoplasm. These tumors are
more likely resectable and carry a more favorable prognosis
than other types (Pitt et al, 1995). On CT, asymmetric biliary
dilation is usually noted with enhancing, expansile, well-defined
FIGURE 18.51. Contrast-enhanced computed tomography in a intraductal soft tissue mass in the most dilated ducts. Unlike
patient who had previously undergone laparoscopic cholecystectomy. mass-forming or periductal-infiltrating subtypes, there is no
The enhancing mass (arrow) within the anterior abdominal wall reflects invasion of adjacent liver parenchyma (Han et al, 2002; Valls
recurrent gallbladder carcinoma within a laparoscopic port tract. et al, 2013).
342 PART 2 DIAGNOSTIC TECHNIQUES
C
FIGURE 18.52. Hilar cholangiocarcinoma. A, Axial contrast-enhanced computed tomography (CT) reveals an infiltrative hypoattenuating tumor
(arrow) surrounding an internal biliary stent (arrowhead) causing bilobar intrahepatic biliary duct dilation. B, Axial contrast-enhanced CT reveals conflu-
ent tumor (large arrows) encasing a replaced right hepatic artery (small arrow) that arises from the superior mesenteric artery and causing intrahepatic
biliary duct dilation. C, Oblique axial maximum intensity projection image reveals narrowing of the right portal vein (large arrow) by infiltrative tumor,
also causing bilobar intrahepatic biliary ductal dilation (smaller arrows).
Because long-term survival is possible only with en bloc hepatic arteries can also be identified with CT angiography. In
resection of the liver and the extrahepatic biliary ducts (Jarnagin a recent meta-analysis (Ruys et al, 2012), MDCT had sensitiv-
& Winston, 2005), preoperative high-resolution MDCT is typi- ity and specificity of 89% and 92%, respectively, for portal
cally used (see Fig. 18.52) to address the factors that determine venous involvement, and 84% and 93%, respectively, for hepatic
resectability per the staging system for hilar cholangiocarcinoma arterial involvement (as well as 86% accuracy in assessing
developed by Jarnagin and colleagues (2001): extent of ductal involvement). In another small study of 27
1. Level and extent of tumor within the biliary tree patients (Park et al, 2008), ductal staging accuracy was 87%
2. Vascular invasion for MDCT versus 85% for MRI, with somewhat observer-
3. Hepatic lobar atrophy dependent sensitivity and specificity for vascular involvement.
4. Distant metastatic disease Lobar atrophy should be readily apparent on CT. Although
On CT, individual dilated bile ducts can be traced to the long-standing obstruction of the ipsilateral bile duct may cause
point(s) of obstruction (Fig. 18.53), and the cause of biliary moderate atrophy, associated portal venous obstruction causes
obstruction can be correctly identified with good accuracy rapid and severe atrophy of the affected lobe (Fig. 18.54)
(Zandrino et al, 2002). Tumor extent along the portal veins and (Jarnagin & Winston, 2005). Atrophy should also be recognized
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 343
FIGURE 18.53. Cholangiocarcinoma. Contrast-enhanced computed tomography at two levels through the liver (left and right) reveals bilobar central
intrahepatic biliary duct dilation as a result of an obstructing enhancing mass at the hepatic hilum (arrow).
A B
FIGURE 18.55. Late arterial-phase and portal venous phase images of a patient with a peripheral cholangiocarcinoma. A, Late arterial-phase image
reveals peripheral enhancement of a heterogeneous mass in the right hepatic lobe (arrows). B, Portal venous phase image reveals heterogeneous
enhancement of the central portion of the mass.
FIGURE 18.56. Biliary cystadenoma. Contrast-enhanced computed depends on its content, which may be hemorrhagic, mucinous,
tomography reveals a large cystic mass with a very subtle internal septa- proteinaceous, or bilious (Buetow et al, 1995a). Multiple
tion (curved arrows). studies suggest BCTs are more often located in the left lobe.
Calcifications may be present within the wall of the cyst or
within septa, and septa may enhance with IV contrast (Fig.
between 42 and 55 years of age (Ishak et al, 1977). Although 18.57). Ultrasound is considered more sensitive than CT for
benign, these lesions may recur after excision and have the detection of these characteristic septa. Thickening of septa in
potential to develop into biliary cystadenocarcinomas (BCACs). particular is a predictor of BCT versus simple cysts (Choi et al,
BCACs at presentation are more evenly distributed between 2010). Nonetheless the accuracy of cross-sectional imaging in
men and women and generally occur a decade later (Soares distinguishing the different types of complex cystic lesions
et al, 2014). BCAs are most often intrahepatic (83%), but they (including hemorrhagic cysts) remains relatively low (Soares
may also occur within the extrahepatic bile ducts (13%) or et al, 2014). It had been reported in a small series that intra-
gallbladder (0.02%) (Devaney et al, 1994). cystic debris, associated bile duct dilation, and mural nodularity
On CT, biliary cystic tumors (BCT) tend to be multilocu- suggest BCAC over BCA (Seo et al, 2010). However, a recent
lated cystic lesions with internal septations; only rarely are large multiinstitutional analysis (primarily using CT) investi-
they unilocular (Fig. 18.56). The attenuation of the cyst fluid gating features, including multiloculation, mural nodularity,
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 345
and biliary ductal dilation (Arnaoutakis et al, 2015), has once The dedicated pancreas protocol uses 750 to 1000 mL of
again failed to demonstrate imaging findings reliably predictive oral water as a negative contrast agent administered before the
of BCAC, concordant with older reports (Buetow et al, 1995a). examination, to aid distinction of enhanced vessels from the
gastrointestinal tract (Lawler & Fishman, 2002; Soriano et al,
COMPUTED TOMOGRAPHY IN PANCREATIC 2004; Takeshita et al, 2002) and to facilitate identification of
IMAGING: HISTORY AND ROLE tumor invasion into adjacent bowel. Avoiding positive oral
contrast also facilitates analysis on the 3D workstation. Images
CT evaluation of the pancreas was revolutionized by the advent are typically reviewed at 2.5-mm collimation in all planes.
of helical scanning, which enabled rapid evaluation of the Routine evaluation for the follow-up of pancreatic cancer in
pancreas during different phases of contrast injection (Ferrucci, a postoperative patient or for evaluation of response to medical
1999; Ishiguchi et al, 2001; Mertz et al, 2000; Van Hoe & therapy uses 500 to 1000 mL of oral water-soluble iodinated
Baert, 1997). MDCT scanners improved pancreatic imaging contrast solution or equivalent 2% barium sulfate suspension
further by allowing extremely rapid data acquisition, retrospec- administered 45 minutes before scanning. This examination
tive change in slice thickness and location, and 3D image review type requires an injection rate of only 2.5 mL/sec, so a small
in multiple projections (Ferrucci, 1999; Horton & Fishman, 20-gauge catheter may be used. Only the routine portal venous
2000; Ishiguchi et al, 2001; Johnson et al, 2003; Mertz et al, phase is acquired. Five-millimeter axial slices are typically
2000; Rubin, 2003; Van Hoe & Baert, 1997). The role of CT reviewed, although thinner images may always be requested by
now includes initial evaluation and characterization of solid and the radiologist provided the raw image data are still extant.
cystic lesions, preoperative local staging of known and suspected
malignant disease, and follow-up of suspected benign, suspected Anatomy of the Pancreas
and known premalignant, and treated malignant lesions. CT is The normal pancreas (see Chapter 2) is well imaged on routine
also routinely used to evaluate suspected pancreatitis. As with CT of the abdomen. It is a retroperitoneal structure bounded
liver examination, the spatial resolution of the modality particu- anteriorly by the stomach and posteriorly and inferiorly by the
larly suits preoperative evaluation of vascular involvement by third portion of the duodenum, and it lies medial to the C-loop
malignant disease. of the duodenum and medial to the spleen. Crucial to the
evaluation of the pancreas and possible tumor resection is its
Technique and Protocols relationship to vessels. The body and tail of the pancreas lie
CT imaging of the pancreas relies on the differential IV contrast immediately anterior to the splenic vein, and the neck, head,
enhancement between tumor tissue and normal pancreatic and uncinate process of the pancreas are in close relationship
parenchyma. The use of IV contrast agent is mandatory for to the superior mesenteric artery (SMA) and vein and lie just
accurate diagnosis, and timing of the contrast injection and caudal to the celiac axis. The normal pancreas has a fat plane
accurate delivery of the appropriate volume requires use of a completely surrounding the SMA, whereas no fat plane lies
dedicated CT power injector. As with liver imaging, several between the superior mesenteric vein and the pancreatic head
methods are available to determine the time of maximal arterial (Fig. 18.58).
enhancement for each patient. These include fixed timing Patients may sometimes be seen with fatty replacement of a
(subject to suboptimal imaging due to variation in cardiac portion of the pancreas or involving the gland diffusely (Fig.
function and hydration state), timing bolus (Kalra et al, 2004), 18.59). In such instances, the gland is best identified by iden-
and commercially available solutions in which scanning may be tification of surrounding vascular structures and bowel. Severe
triggered automatically when a vascular structure reaches a fatty atrophy permits visualization of fine vascular detail within
predefined attenuation. the pancreas, but a potential pitfall is that a small island of
Initial scan protocols for dedicated pancreas evaluation/CT residual normal pancreatic parenchyma may be confused with
angiography recommended four phases, but more modern an intrapancreatic mass.
practice uses three acquisitions, omitting early arterial imaging
because pancreatic parenchyma and peripancreatic arterial
anatomy are both well evaluated in the late arterial phase
(Fletcher et al, 2003). The precontrast scan permits evaluation
of pancreatic calcifications and allows localization of the gland
and pertinent arteries in the z-axis for subsequent acquisition
of contrast-enhanced phases. IV contrast medium is injected
at a high flow rate of 4 to 6 mL/seconds. The late arterial or
pancreatic parenchymal phase, acquired roughly 30 to 40 seconds
after initiating contrast injection, is designed to maximize dif-
ferences in contrast enhancement between pancreatic neoplasms
and adjacent normal pancreatic tissue and is also useful in
evaluating hypervascular liver metastases seen in patients with
pancreatic endocrine neoplasms. Last, the routine portal venous
phase acquired at approximately 70 to 90 seconds from the start
of IV contrast injection provides the best evaluation of hepatic
metastases from pancreatic ductal adenocarcinoma (Bashir &
Gupta, 2012; Cantisani et al, 2003; Takeshita et al, 2002) and
in some cases offers the best contrast to identify the primary FIGURE 18.58. Normal pancreas. Note the gastroduodenal artery
pancreatic lesions themselves. along the anterior margin of the pancreas (arrow).
346 PART 2 DIAGNOSTIC TECHNIQUES
SA
LHA
RHA
CHA
SMA
PHA
GDA
the histologic diagnosis of pancreatic cancer were interpreted 2003; Lygidakis et al, 2004; Nakao et al, 2004; Yoshimi et al,
as definite or suspicious for pancreatic carcinoma upon retro- 2003). Because strong correlation has been demonstrated
spective review (Gangi et al, 2004). A mass in the head is fre- between the extent of vessel contact at imaging and histologic
quently associated with biliary or pancreatic ductal dilation, tumor vascular invasion, detailed evaluation of vascular involve-
with atrophy of gland parenchyma upstream of the obstruction ment is essential at imaging. Reformations of acquired axial
a helpful secondary indication of the tumor site in subtle images in the coronal and sagittal planes in the arterial and
nonadvanced cases. venous phases are now typically created for image review in
Detection at an advanced stage, however, is common and is dedicated pancreatic imaging. 3D workstations also permit
associated with involvement of major local arteries and veins, visualization of vascular involvement using maximum intensity
peripancreatic adenopathy, hepatic metastases, or ascites (Figs. projections or volume rendering (Prokesch et al, 2003; Tamm
18.63 and 18.64). Invasion of the superior mesenteric artery or & Charnsangavej, 2001; Tamm et al, 2001), and curved-plane
vein, common hepatic artery, or celiac axis has historically been reformatted images can offer a superb demonstration of vascu-
considered to preclude curative resection. Involvement of the lar involvement (Gong et al, 2004; Vargas et al, 2004).
main portal vein is not an absolute contraindication to surgery A recent consensus statement on standardized reporting of
because a portion of the main portal vein may be resected and ductal adenocarcinoma from the Society of Abdominal Radiol-
reanastomosed proximal to the jejunal branches (Chae et al, ogy and the American Pancreatic Association (Al Hawary et al,
A B
D
FIGURE 18.63. Pancreatic cancer with vascular encasement. A, Cancer in the body of the pancreas tracks posteriorly to encase the celiac axis,
proximal hepatic artery (black arrowhead), and splenic artery (white arrowhead). B, Curved multiplanar reconstruction showing the mass (arrow) in
the body of the pancreas. C, Coronal volume-rendered image shows a mass in the body of the pancreas occluding the splenic vein (arrowhead)
and encasing celiac axis branches (arrows). D, Sagittal volume-rendered image shows mass encasing the celiac axis (arrow).
348 PART 2 DIAGNOSTIC TECHNIQUES
C
FIGURE 18.64. Large pancreatic mass with vascular encasement and collateral vessels. A, Mass in the body and tail of the pancreas encases the
celiac artery and its branches. B, Coronal volume-rendered image shows the pancreatic mass and encasement of the celiac and superior mesenteric
arteries (arrows) by tumor. C, Coronal volume-rendered image shows extensive collateral vessels in the abdomen from encasement of the splenic
vein by pancreatic cancer.
2014) advocates consistent terminology in describing vascular neoplasms. They present most frequently in the fourth to sixth
involvement: “Encasement” of a vessel is defined as greater than decades of life without significant gender predilection. Most
180-degree circumferential contact, whereas “abutment” is PENs occur sporadically; only 1% to 2% are associated with
defined as less than or equal to 180 degrees of contact. These familial syndromes, most commonly multiple endocrine neo-
should always be reported, as well as narrowing and contour plasia type 1, von Hippel-Lindau syndrome, neurofibromatosis
deformity of a vessel in question. type 1, and tuberous sclerosis (Lewis et al, 2010). Presentation
Regarding metastatic disease, one study (Kitagawa H et al, often depends on the hormonal activity (or lack thereof) of
2008) found specific spread patterns from tumors of the head tumor products (Kulke, 2003). Hormonally active tumors may
depending upon the origin of the cancer in either the dorsal or present earlier than nonhormonally active tumors. As a whole,
ventral pancreatic embryologic anlage. Tumors confined to the these tumors generally have a much more favorable prognosis
ventral pancreas had metastases along the SMA and peripan- than PDAC.
creatic nodes, whereas tumors that arose from the dorsal pan- Multiphase CT is the first imaging choice for patients with
creas metastasized to common hepatic artery, hepatoduodenal suspected PEN, with a median sensitivity of ≈84%. Multiple
ligament, and peripancreatic nodes. Tumors involving both studies confirm the increased sensitivity of arterial-phase images
ventral and dorsal domains metastasized widely. compared with portal venous phase images (Megibow, 2012).
However, the two phases are complementary, and some lesions
Pancreatic Endocrine Neoplasm (See Chapter 65) may be seen only on venous phase images (Lewis et al, 2010).
Also called neuroendocrine cancer of the pancreas, pancreatic Although their imaging appearance may be quite variable,
endocrine neoplasms (PENs) are predominantly well- the most typically expected imaging appearance of PEN on CT
differentiated pancreatic or peripancreatic tumors with endo- is a well-circumscribed hypervascular focus best seen during
crine differentiation. They do not arise from the islets of the pancreatic phase of enhancement (Figs. 18.65 and 18.66).
Langerhans as once thought, but rather from ductal pluripotent Smaller lesions tend to be more homogeneous, whereas larger
stem cells. PENs are relatively rare, with a prevalence of ≈1 in lesions tend to enhance more heterogeneously due to areas
100,000 people, accounting for 1% to 2% of pancreatic of cystic degeneration, necrosis, fibrosis, and calcification,
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 349
A B
C
FIGURE 18.66. Pancreatic endocrine neoplasm (PEN). A, Arterial-phase scan shows hypervascular liver metastasis from PEN. B, Arterial phase
scan shows hypervascular PEN (arrow). C, Liver metastasis from PEN has a lower attenuation than hepatic parenchyma on portal venous phase.
350 PART 2 DIAGNOSTIC TECHNIQUES
Findings Committee in 2010 (Berland et al, 2010) and a con- that contain no invasive carcinoma, actuarial risk of future
sensus statement by the International Association of Pancreatol- carcinoma development is also much higher among main and
ogy updated in 2012 (Tanaka et al, 2012). The ACR white paper mixed types (Levy P, 2006).
proposes an algorithmic approach to all incidentally detected On CT, branch-duct IPMN may appear as a fluid attenua-
cystic lesions lacking solid elements in asymptomatic patients, tion (0 to 20 HU) cluster of round or tubular lesion(s) or as a
whereas the International Consensus Guidelines are aimed single lesion of greater than 5 mm (Fig. 18.67). Connection to
more specifically at handling suspected mucinous lesions in any a nondilated main duct may be seen (Pedrosa et al, 2010).
patient. Although there are differences in focus and recom- Presence of the lesion in the pancreatic head, its most common
mendations, both guidelines support, under certain circum- location, may compress the CBD with resulting dilation of the
stances, a role for imaging surveillance that had been suggested intrahepatic bile ducts (Fig. 18.68). Main-duct IPMN is char-
by previous work (Allen et al, 2003; Visser et al, 2004). Both acterized by diffuse or segmental dilation of the main duct to
guidelines indicate preference for MRI over CT in characteriz- greater than 5 mm in caliber without other identifiable causes
ing lesions, but because published reports suggest little differ- of obstruction. The mixed type is designated when features of
ence in accuracy between the two modalities in characterizing both branch- and main-duct types are present (Tanaka et al,
cystic pancreatic lesions (Visser et al, 2007), CT is frequently 2012).
requested. The white paper stratifies lesions into surveillance It is largely the mucin produced by the tumor that is identi-
frequencies mostly by size, indicating that among lesions lacking fied at imaging rather than the neoplastic epithelium itself.
solid elements in asymptomatic patients, only those greater than However, visible solid mural nodules and enhancing (in any
3 cm not clearly representing a benign SCA should undergo phase) solid components, when present, may actually represent
further invasive workup. The International Consensus Guide- the tumor. Presence of invasive cancer and high-grade dysplasia
lines puts more emphasis on two groups of mostly imaging has been associated with these features, as well as with
features: “high-risk stigmata,” including main duct caliber
greater than 9 mm and enhancing solid component; “worrisome
features,” including main-duct 5- to 9-mm caliber; abrupt
change in duct caliber with distal gland atrophy; nonenhancing
mural nodules; and size greater than 3 cm. Only lesions without
any of these imaging features in patients also without any of the
specified clinical features (obstructive jaundice, pancreatitis) are
placed into imaging surveillance. One potential problem in
applying this approach is that agreement on the presence of
certain of the imaging features may not be solidly repeatable
among interpreting radiologists (Do et al, 2014). Although the
two guidelines have made a strong contribution to thinking
about management of these lesions, neither has gained universal
acceptance as yet, and particularly large centers with specialty
expertise use their own combination of clinical judgment and
imaging data to guide management decisions.
A B
C D
FIGURE 18.69. Intraductal papillary mucinous neoplasm. A to D, Diffuse involvement of the main (white arrows) and branch (black arrows) pan-
creatic ducts with invasive adenocarcinoma. B, No evidence of vascular encasement is found, as shown on the normal-appearing portal vein (arrows),
and none was found at surgery or at pathology examination.
A
FIGURE 18.71. Serous cystadenoma of the pancreatic head shown
in the portal phase.
arterial) phase gradually increasing over time (Baek et al, to encase them. This is a major distinguishing feature useful for
2010). After resection, patients should be followed by imaging diagnosis (Fig. 18.76). Detection of metastatic disease to the
because late metastases can occur. pancreas requires a high index of suspicion, because primary
pancreatic carcinomas of ductal origin are far more common.
OTHER CYSTIC PANCREATIC LESIONS. Cystic masses may also be When clinical suspicion is present, the study can be tailored
secondary to degeneration of previously solid masses. Neuro- to optimize the likelihood of detection. In a patient with
endocrine cancers may become necrotic and present with cystic renal carcinoma, hypervascular metastases to the pancreas may
degeneration (Fig. 18.74) (see Chapter 65). Mucinous tumors be detected on routine scanning or triphasic examination
may invade adjacent structures and present as cystic masses (Fig. 18.77).
(Fig. 18.75).
Acinar Cell Carcinoma of the Pancreas (See Chapter 59)
Metastatic Disease to the Pancreas (See Chapter 64) Acinar cell carcinoma is predominantly a tumor of the elderly
A pathology review (Adsay et al, 2004) of surgical and autopsy man, with peak incidence in the 60s and many more men
cases showed the most common primary malignancies meta- affected than women. Accounting for approximately 1% of all
static to the pancreas were lung carcinomas, gastrointestinal pancreatic tumors, acinar cell carcinoma of the pancreas is
carcinomas, and lymphomas. These are usually found in defined as a carcinoma of the exocrine pancreas exhibiting
patients with widely disseminated disease. As at other sites in
the body, pancreatic lymphoma tends not to occlude vessels but
FIGURE 18.73. Papillary epithelial neoplasm of the pancreas with FIGURE 18.74. Pancreatic neuroendocrine neoplasm with cystic
calcification in portal venous phase. degeneration in the portal venous phase.
A B
FIGURE 18.75. Intraductal papillary mucinous tumor with invasive mucinous adenocarcinoma. A, Large multicystic tumor extends into the papilla.
B, Computed tomography shows that the mass also invades into the duodenum and stomach.
354 PART 2 DIAGNOSTIC TECHNIQUES
pancreatic enzyme production by the neoplastic cells (Cubilla islet-cell tumors contain calcification (Buetow et al, 1995b;
& Fitzgerald, 1975; Morohoshi et al, 1983). They have a char- Eelkema et al, 1984). In a more recent series (Chiou et al,
acteristic microscopic appearance of a relatively circumscribed 2004), tumor diameters ranged from 3.3 to 18 cm, with an
periphery and minimal desmoplastic stroma within the tumor, overall mean size of 7.2 cm. Most of these tumors were
with cells arranged in nests and cords. The tumor is most hypodense with respect to normal pancreatic parenchyma,
common in the head, neck, and uncinate process of the pancreas although some showed hypervascular enhancement on the early
but may arise in any portion of the gland (Holen et al, 2002; arterial phase, some of which persisted into the portal venous
Klimstra et al, 1992). Initial symptoms include abdominal pain phase.
or fullness, postprandial vomiting, and jaundice. Some patients
may be asymptomatic, and the mass may be detected inciden- Inflammatory Diseases of the Pancreas
tally. Serum tumor markers may be normal, or there may be Pancreatitis (See Chapters 54 to 58)
mild elevation of serum α-fetoprotein, CEA, and CA 19-9. The most common cystic mass of the pancreas is not a malig-
CT features include a well-defined tumor with a thin, nancy but rather a complication of acute or chronic pancreatitis.
enhancing capsule and central necrosis, which may contain Fluid collections occur in approximately 50% of patients with
areas of internal calcification (Fig. 18.78). Such calcification moderate to severe pancreatitis. Of these, approximately 50%
may be a useful feature in distinguishing this entity because only resolve spontaneously within 6 weeks (Baron & Morgan, 1997;
2% of ductal adenocarcinomas and 22% of nonfunctioning Byrne et al, 2002), and 10% to 15% may progress to pseudo-
cyst formation after developing a capsule. Pseudocyst formation
is more common in patients with chronic pancreatitis and may
occur in 20% to 40% of these patients.
A B
FIGURE 18.77. Renal cell carcinoma metastatic to pancreas. A, Computed tomographic angiogram of the pancreas shows hypervascular pan-
creatic metastases (arrows) from renal carcinoma. B, Portal venous phase imaging shows far fewer masses.
Chapter 18 Computed tomography of the liver, biliary tract, and pancreas 355
Common causes of pancreatitis include alcohol, gallstones, retroperitoneum; this may dissect retroperitoneal planes and
idiopathic hypertriglyceridemia, drugs, pancreas divisum, resolve spontaneously 50% of the time. An acute pseudocyst is
trauma, and endoscopic retrograde cholangiopancreatography defined as a collection of pancreatic juice confined by a
(Baron & Morgan, 1997). Clinical presentation includes nausea, nonepithelialized wall of granulation tissue that occurs as a
vomiting, and epigastric pain. Serum amylase, frequently used result of acute pancreatitis (Baron & Morgan, 1997) and
to monitor pancreatitis, may be normal in acute pancreatitis requires at least 4 weeks to form (Fig. 18.81). It is character-
and elevated in nonpancreatitic conditions. Elevation of the ized by the presence of a well-defined wall and may contain
serum lipase may support the diagnosis of acute pancreatitis. internal septations.
Mild acute pancreatitis may appear on CT scan as enlarge-
ment of the pancreas with loss of definition of the borders of Lymphoplasmacytic (Autoimmune) Pancreatitis
the pancreas. Depending on the part of the pancreas involved, (See Chapter 59)
there may be thickening of the right or left anterior pararenal Lymphoplasmacytic pancreatitis, also known as autoimmune
fascia or diffuse thickening of adjacent fascial planes (Figs. pancreatitis (Kawaguchi et al, 1991; Kim et al, 2004b; Yoshida
18.79 and 18.80). Acute fluid collections associated with pan- et al, 1995), was first described as a “primary inflammatory
creatitis are enzyme-rich collections, which lack a defined wall. sclerosis of the pancreas” (Sarles et al, 1961). It is characterized
Pancreatic fluid collections may present as an acute by a mixed inflammatory infiltrate about pancreatic ducts and
fluid collection interspersed with pancreatic parenchyma ductules, combined with obliterative phlebitis (Hardacre et al,
without a defined wall. The fluid collection may be well cir- 2003). It is now recognized as the pancreatic manifestation of
cumscribed, or it may infiltrate throughout the pancreas and a more systemic disease process known as immunoglobulin G4
(IgG4)-related sclerosing disease (Vlachou et al, 2011). Men
are affected at least twice as frequently as women. The clinical
presentation can be identical to that of pancreatic adenocarci-
noma, with abdominal pain, jaundice, weight loss, and elevated
levels of CEA or CA 19-9. Elevation of pancreatic enzymes is
not a prominent feature of this entity, with mild elevation in
serum amylase or lipase levels most commonly reported. Ele-
vated levels of IgG and hypergammaglobulinemia are reported
in 37% to 76% of patients with autoimmune pancreatitis (Kim
et al, 2004b). IgG4 in particular is often elevated, as are other
autoantibodies, such as rheumatoid factor and antinuclear
antibody. Patients may also present with fluctuating obstructive
jaundice without pain (Kamisawa et al, 2007).
At imaging, three patterns of involvement have been recog-
nized: diffuse, focal, and more recently multifocal (Kajiwara
et al, 2008). Diffuse disease (Fig. 18.82) is most common, in
which a diffusely enlarged “sausage-like” gland is noted with
loss of the lobular contour and pancreatic clefts. Focal disease
is less common, manifesting as a focal mass, particularly in the
FIGURE 18.79. Pancreatitis involving the body and tail of the pan- head, often resembling ductal adenocarcinoma but with vari-
creas. Note the loss of fat planes to the spleen and in the left anterior ably present milder upstream main-duct dilation. In focal and
pararenal space. multifocal forms, the affected area(s) of the gland typically
FIGURE 18.80. Severe pancreatitis obliterates tissue planes in a FIGURE 18.81. Pancreatic pseudocyst in portal venous phase. The
patient after gastrectomy. patient also has adenopathy from an islet cell tumor.
356 PART 2 DIAGNOSTIC TECHNIQUES
appear hypoattenuating on CT, with decreased enhancement gallbladder wall (Kawamoto et al, 2004; Takahashi et al, 2008).
and sometimes moderate delayed enhancement likely due to Involvement of the kidneys is also common, manifesting as
fibrosis (Vlachou et al, 2011). A capsule-like hypoattenuating hypoattenuating round or wedge-shaped cortical nodules,
rind or “halo” about the gland is common at affected areas, as peripheral cortical lesions, and renal pelvic lesions; less com-
is narrowing of peripancreatic veins. The main pancreatic duct monly involved organs include lymph nodes and the retroperi-
typically is narrow and irregular in affected regions. Calcifica- toneum (Vlachou et al, 2011).
tion and peripancreatic stranding/fluid collections are rare. It is often not possible to distinguish by imaging the focal
Because the disease is part of a multisystem spectrum of form of lymphoplasmacytic pancreatitis (with localized stenosis
involvement, imaging also may demonstrate thickening and/or of the main pancreatic duct and upstream duct dilation) from
narrowing of the wall of the CBD, intrahepatic biliary tree, and pancreatic adenocarcinoma, but because the disease typically
responds well to a trial of corticosteroids, rapid clinical and
imaging response may help establish the diagnosis. If this step
is omitted and IgG4 levels are either not obtained or negative,
the diagnosis may require laparotomy (Learn et al, 2011).
Groove Pancreatitis
Groove pancreatitis affects the groove between the pancreatic
head, duodenum, and the CBD and was first described by
Becker and named by Stolte and colleagues (Becker, 1973;
Stolte et al, 1982). This can be extremely difficult to distinguish
from groove pancreatic carcinoma, as patients are seen initially
with abdominal pain and vomiting secondary to duodenal
stenosis. This represents chronic pancreatitis that occurs with a
platelike mass between the head of the pancreas and the duo-
denum, and it may cause intrahepatic and extrahepatic biliary
duct dilation. Duodenal stenosis may be associated with wall
thickening and cystlike lesions in the duodenal wall or in the
groove area (Gabata et al, 2003; Lauffer et al, 1999; Trianto-
poulou et al, 2009) (Fig. 18.83). Pancreatic duct dilation is
much less common than bile duct dilation, and distinguishing
FIGURE 18.82. Lymphoplasmacytic pancreatitis causing diffuse groove pancreatitis from groove pancreatic carcinoma is done
pancreatic enlargement. from a biopsy.
A B
C D
FIGURE 18.83. Groove pancreatitis. Images A to D show paraampullary duodenal wall cysts with extension to the pancreas along with cystic
dilation of the pancreatic duct. At pathology examination, no malignancy was found. The duodenal wall showed fibrosis and chronic inflammation,
and the adjacent pancreas showed focal chronic pancreatitis. The gallbladder showed changes of chronic cholecystitis.
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CHAPTER 19
Magnetic resonance imaging of the liver, biliary
tract, and pancreas
Scott R. Gerst and Richard Kinh Gian Do
Magnetic resonance imaging (MRI) is a cross-sectional multi- tissues. Differences in T1 and T2 times intrinsic to various soft
planar imaging technique (Fig. 19.1). MRI uses magnetic fields tissues can be exploited to improve image contrast and diag-
and radiofrequency pulses to generate images with outstanding nostic accuracy. For example, free water, which has a long T1
tissue contrast and excellent spatial resolution. The principles relaxation, is low signal on standard T1-weighted imaging and
of nuclear magnetic resonance were first described in the 1940s markedly high signal on T2-weighted imaging. Thus so-called
by Bloch and colleagues (1946) and Purcell and colleagues heavily T2-weighted imaging sequences, such as those used in
(1946) as a method for in vitro chemical analysis. Several MR cholangiopancreatography, highlight high water content
decades later, Damadian (1971) and Lauterbur (1973) applied structures, such as bile and pancreatic ducts, while reducing
some of these basic principles to design MRI to allow in vivo the signals of other organs.
imaging. Today, MRI is used extensively as a medical imaging Diffusion-weighted MRI (DWI) is an alternative tissue con-
tool throughout the body to visualize and distinguish normal trast mechanism that produces images dependent on the local
and pathologic tissue. magnitude of water diffusion. DWI of the liver may be used to
help detect focal hepatic lesions, especially metastases, and may
PRINCIPLES OF MAGNETIC also be used to assess changes in the liver parenchyma, such as
RESONANCE IMAGING liver fibrosis. Tremendous interest in this sequence first arose
due to its increased sensitivity to early changes in the brain after
MRI harnesses the signal available from the magnetic moment a cerebrovascular accident compared with more traditional T1-
or spin present in certain nuclei, including hydrogen atoms. or T2-weighted imaging. Applications for DWI in body imaging,
When placed in a large static magnetic field, the nuclei align initially hampered by hardware and software limitations, were
themselves in a parallel or antiparallel direction to the field and addressed in the mid-2000s. With new advances in receiver coil
also rotate or spin at a precise frequency termed the Larmor design, improved gradient coils used to acquire images, and
frequency. This frequency depends on the specific type of nuclei motion correction through respiratory or navigator techniques,
imaged and the strength of the magnetic field. The most com- DWI has flourished as a functional imaging sequence in hepa-
monly imaged nucleus in clinical practice is hydrogen (H1) topancreatobiliary imaging (Taouli et al, 2010).
because of its great abundance in the human body, mostly in
the form of water. Other nuclei that may be imaged by MRI MAGNETIC RESONANCE IMAGING SAFETY
include phosphorus (P31), sodium (Na23), and carbon (C13).
When unperturbed in a static magnetic field, nuclei with MRI is safe for most patients. However, physicians and
magnetic spins are in equilibrium: An almost an equal number patients should be aware of some important considerations,
of nuclei are in an “up” (parallel) or “down” (antiparallel) such as MR contrast safety, and the risk of interactions
alignment. The slight difference between the two states creates between the patient (including their implants) with the strong
a net magnetic moment. A measurable signal is generated from static magnetic field of the scanner as well as the RF field
the magnetic moment after excitation by a radiofrequency (RF) used to generate images. The magnetic field interactions are
pulse at the resonance Larmor frequency. This signal is gener- potentially dangerous by causing the motion of ferromagnetic
ated as the excited nuclei in the body return to equilibrium, aneurysm clips or causing electronic malfunctioning of cardiac
releasing energy in the form of an electromagnetic field that is pacing devices and defibrillators. Many MRI facilities have
captured by a receiver coil. The strength of this emitted signal screening programs in place to address potentially contraindi-
determines the signal intensity (SI) of a tissue. The precise cated devices, under new MRI safety guidelines proposed by
tissue SI depends on several factors, including longitudinal the American College of Radiology (Expert Panel on MR
relaxation (T1), transverse relaxation (T2), proton density Safety, 2013). However, referring physicians should be aware
(essentially the number of nuclei present), and flow. Some of of their local imaging centers’ approach to MRI safety, such
these factors can be manipulated (e.g., through T1 and T2 as their ability to scan patients with MR-conditional or
weighing) to create images highlighting various soft tissue MR-unsafe pacemakers, for example.
properties. MRI has a role in patients with minimal or mild renal insuf-
All tissues have an intrinsic T1 value for relaxation along the ficiency. Iodinated contrast used in CT is associated with a risk
longitudinal magnetic axis, which varies between 200 and 800 of contrast-induced nephropathy; however, administration of
milliseconds. T2 time, or transverse relaxation, is a measure of intravenous gadolinium contrast agents in patients with severe
signal loss perpendicular to the long axis of the magnetic field renal insufficiency carries a risk of nephrogenic systemic fibrosis
and typically varies between 20 and 200 millisecconds for most (NSF). NSF is a serious and potentially fatal complication
358
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 359
C
FIGURE 19.1. Multiplanar T2-weighted images through the liver in a patient with multiple hepatic metastases. A, Axial image. B, Sagittal image.
C, Coronal image. A variety of techniques can be used to obtain these images. Note that fluid-containing structures, including small bowel (curved
arrow, A), gallbladder, biliary tree, and pancreatic duct (arrow, C), are bright.
related to free gadolinium deposition within soft tissues and an important role in imaging benign disorders, as well as com-
organs, with resulting scleroderma-like fibrosis. The exact prehensive evaluation of malignancies of the biliary system
causal mechanism of NSF remains unknown, but the risk of (Mandelia et al, 2013; Singh et al, 2014; Vaishali et al, 2004).
NSF increases in patients with a glomerular filtration rate Heavily T2-weighted images are used to provide an overview
(GFR) less than 30 mL/min, and particularly in patients with of biliary and pancreatic ductal anatomy, removing the signal
severe, end-stage disease (GFR < 15 mL/min). In addition, of surrounding structures. Excellent diagnostic-quality images
linear agents with lower thermodynamic stability carry a greater are obtainable, with high sensitivity and specificity for evalua-
risk than others. If available, more stable, lower-risk macrocy- tion of ductal dilatation, strictures, and intraductal abnormali-
clic agents can be used in patients with a GFR less than 30 mL/ ties (Hekimoglu et al, 2008; Palmucci et al, 2010a; Palmucci
min. Gadolinium contrast usage in patients with a GFR less et al, 2010b; Sandrasegaran et al, 2010). Cross-sectional
than 15 mL/min should only be performed if essential, after images and maximum intensity projection images (Fig. 19.2)
careful evaluation of risks versus benefits, and with consultation are produced with current MRCP techniques, and projection
with a nephrologist, if available. Since NSF was initially images are similar to direct contrast-enhanced cholangiograms
described, the rapid international investigation, dissemination obtained with either endoscopic retrograde cholangiopancrea-
of information, and swift adjustment to policy have led to a tography (ERCP) or percutaneous transhepatic cholangiogra-
precipitous drop of reported NSF cases. In multiple countries, phy (PTC; see Chapter 18). MRCP is noninvasive, eliminating
NSF has essentially disappeared since 2009 (Bennett et al, the potential morbidity associated with ERCP or PTC (Zhong
2012; Grobner, 2006; Idee et al, 2014). et al, 2004).
The basic principle of MRCP is to use T2-weighted imaging
MAGNETIC RESONANCE IMAGING to highlight stationary or slowly moving fluid, including bile, as
CHOLANGIOPANCREATOGRAPHY high in signal intensity; surrounding tissues, including retroperi-
toneal fat and the solid visceral organs, with shorter T2 values,
MR cholangiopancreatography (MRCP) is an imaging tech- are markedly reduced in signal. In addition to heavilyT2-weighted
nique used to evaluate the bile and pancreatic ducts and plays sequences, MRCP protocols also include routine intermediate
360 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 19.2. Mixed main- and branch-duct intraductal papillary mucinous neoplasm (IPMN) of the pancreatic tail. A, Coronal T2 image. A lesion
with high T2 signal indicating cystic contents involves the pancreatic tail and shows multiple thin septations (arrow). B, Coronal three-dimensional
maximum intensity projection T2-weighted magnetic resonance cholangiopancreatography image. The multiseptated cystic pancreatic tail mass is
apparent (arrow). C, Axial T2 image. Multiple septations are apparent with dilated main pancreatic duct (star). Incidental note is made of a right renal
cyst with thin septations (open circle). D, Axial T1-weighted fat saturation image postintravenous gadolinium contrast. The numerous septations
enhance within the lesion (arrow). Some components appeared nodular, and the lesion was resected. Histopathology revealed an IPMN with a focus
of noninvasive mucinous cancer.
T2-weighted sequences and T1-weighted sequences to evaluate enhancement patterns between benign and malignant liver
surrounding structures. MR-specific techniques for obtaining lesions have been well reported and are discussed in individual
cholangiographic images include breath-hold, as well as respira- entities later.
tory and navigator gated techniques, which can generate images Several new hepatobiliary-specific contrast agents have been
in a patient during free breathing. developed to add additional functional information compared
with traditional ECF contrast agents. These hepatobiliary spe-
MAGNETIC RESONANCE IMAGING cific contrast agents are taken up to varying degrees by function-
CONTRAST AGENTS ing hepatocellular tissue and are excreted in bile as well as
through the kidneys. Hepatobiliary specific agents include
MRI contrast agents work primarily by altering the intrinsic T1 mangafodipir trisodium, gadobenate dimeglumine, and gadox-
relaxation times of various soft tissues where contrast accumu- etic acid (Gd-EOB-DTPA). Both gadobenate dimeglumine
lates. In the hepatobiliary system, MRI contrast agents can (MultiHance; Bracco Imaging, Cranbury Township, NJ) and
improve the detection of liver lesions and improve the charac- gadolinium-ethoxybenzyl-diethylenetriamine pentaacetic acid
terization of focal liver abnormalities. MRI contrast agents for (Eovist/Primovist; Bayer Healthcare, Wayne, NJ) have been
hepatobiliary imaging are divided into two basic categories: approved in the United States. These contrast agents are all
extracellular fluid contrast (ECF) agents, and those with addi- administered intravenously, although the dose and pharmaco-
tional hepatobiliary excretion. In the past, the most commonly kinetics are different. These two agents are sometimes referred
used contrast agents were the ECF agents, such as gadopen- to as combination agents because of their dual capacity for
tetate dimeglumine (gadolinium diethylenetriaminepentaacetic imaging both in the dynamic phase (as done routinely with ECF
acid [Gd-DTPA]), which is distributed within the intravascular agents) and in the delayed, hepatocyte-specific phase. These
compartment initially and rapidly diffuses through the extra- agents provide comprehensive information about the hepatic
vascular space, similar to the action of iodinated contrast agents parenchyma, bile ducts, and liver vasculature (Burke et al,
in computed tomography (CT; see Chapter 18). Differences in 2013; Seale et al, 2009).
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 361
NORMAL HEPATIC APPEARANCE ON or focal. The pattern of fatty liver is related to regional differ-
MAGNETIC RESONANCE IMAGING ences in perfusion. It may be difficult to distinguish focal fat
from focal hepatic lesions on CT because both appear low in
MRI is routinely used to evaluate diffuse and focal liver abnor- attenuation. Additionally, focal fatty sparing may appear similar
malities. With liver MRI, a combination of precontrast T1, T2, to an enhancing neoplasm on contrast-enhanced CT. Although
and DWI sequences are used. Normal hepatic parenchyma is geographic margins and location may aid in the diagnosis, this
brighter (hyperintense) than the spleen on T1-weighted images, is more readily distinguished on MRI due to different signal
whereas on T2-weighted images, the spleen is relatively brighter characteristics. T1-weighted in-phase and out-of-phase imaging
than the liver (Fig. 19.3). Although most hepatic lesions are allows differentiation of signals from fat and water when they
low in signal intensity on T1-weighted images, they have more are present in the same voxel, as it exploits minute differences
variable intensity on T2-weighted images, with cysts and hem- in resonance frequencies between fat and water protons (Fig.
angiomas having the highest T2 signal intensity in general. 19.4). Using fast gradient-echo techniques, fat and water
Precontrast and postcontrast T1-weighted imaging is also per- protons that share the same voxel will be imaged both “in phase”
formed to assess enhancement patterns of the liver parenchyma or 180 degrees “out of phase.” Tissues that have relatively equal
and liver lesions. If a hepatobiliary contrast agent is used, addi- quantities of fat and water will appear dark on the out-of-phase
tional delayed hepatobiliary phase images are acquired. sequence because the signals from fat and water are “opposed
in phase” and can cancel each other out (Boll et al, 2009;
DIFFUSE HEPATIC DISEASE Springer et al, 2010). Areas of fatty sparing will remain hyper-
intense relative to the surrounding fatty liver on out-of-phase
Fatty Liver imaging. On standard T1-weighted imaging, areas of focal fat
Fat may accumulate within hepatocytes for many reasons, can show increased signal. The appearance on T2-weighted
including alcohol intake, diabetes, medications, and obesity (see images depends on the type of sequence acquired and whether
Chapters 71 and 100). Hepatic steatosis may be diffuse, patchy, fat saturation is used. The ability of MRI to exploit those signal
A B
C
FIGURE 19.3. Normal hepatic magnetic resonance image. A, T1-weighted spin-echo image. The liver is brighter (hyperintense) relative to the signal
of the spleen. There are normal flow voids that appear as dark areas in the visualized vessels (straight arrow, intrahepatic portion of the inferior vena
cava; curved arrow, aorta). B, T2-weighted fast spin-echo image. Because of reversal of the liver/spleen contrast, the normal spleen is brighter than
the liver. Note the flow voids within the vessels (straight arrow, intrahepatic portion of the inferior vena cava; curved arrow, aorta). C, Postcontrast
T1-weighted gradient-echo image. Normal enhancement in the liver and spleen is evident, and the parenchyma of both is about equal in this phase
of the injection. All the vessels are bright as a result of the T1 shortening effect of gadolinium (straight arrow, intrahepatic portion of the inferior vena
cava; curved arrow, aorta).
362 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
E
FIGURE 19.4. Focal fat within the liver. A, Non–contrast-enhanced computed tomography image in a young adult with history of testicular cancer
shows heterogeneous regions of low attenuation in the right hepatic lobe (arrows). B, T1-weighted in-phase image at the same level now shows
signal abnormality in this region. C, T1-weighted out-of-phase image shows geographic areas (arrow) that have lost signal. On the out-of-phase
images, a black line “India ink effect” surrounds tissue interfaces. D, T1-weighted fat saturation precontrast image also shows mild signal loss in this
area (arrow). E, T1-weighted fat saturation postcontrast image. The area in question has normal vascularity coursing through it; no mass was
present—the typical appearance of fatty infiltration.
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 363
A B
C D
E F
G
FIGURE 19.5. Iron deposition. A, T1-weighted in-phase gradient-echo image (echo time [TE] 4.8) shows abnormal liver/spleen contrast. The liver
is homogeneously darker than the spleen from preferential deposition of iron within the hepatic parenchyma. This is a pediatric patient who had
undergone numerous transfusions while undergoing therapy for cancer. Note the difference from Figure 19.X. B, T1-weighted out-of-phase gradient-
echo image (TE 2.2) shows the liver/spleen contrast reverses, with the liver being brighter than spleen. This is opposite from Figure 19.X and shows
iron deposition disease within the liver. C, Axial T2-weighted fast spin-echo sequence shows marked low T2 signal within both liver and spleen. D-G,
Using T2-weighted multigradient-echo technique, there is progressive signal loss in the liver. This type of multiecho imaging allows estimation of iron
quantification using computer software.
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 365
A B
FIGURE 19.6. Hepatic cysts associated with polycystic kidney disease. A, Axial T2-weighted image at the level of the kidneys shows bilaterally
enlarged kidneys with multiple hyperintense cysts. Little normal renal parenchyma is present at this level, and multiple small hepatic cysts (arrow)
are seen. B, Coronal T2-weighted images through the kidneys show similar findings of enlarged kidneys containing multiple cysts (black arrows),
and small hepatic cysts are identified (white arrow).
decrease over time, may all offer clues to suggest the diagnosis, Hepatic Adenoma
but biopsy may be necessary for confirmation, depending on Hepatocellular adenomas (HCAs) (see Chapter 90A) also are
the clinical picture (Ridge et al, 2014). benign liver lesions, but unlike FNH, are associated with com-
plications, including abdominal pain, bleeding, and rarely,
Focal Nodular Hyperplasia malignant degeneration. HCAs are strongly associated with oral
Focal nodular hyperplasia (FNH; see Chapter 90A) is the contraceptive or steroid use and are more common in women
second most common benign tumor of the liver after heman- of childbearing age. Newer low-dose oral contraceptives have
gioma. Pathologically, FNH contains all the elements of normal a less strong association with HCAs. Although HCA may be
liver and may have a central fibrous scar, which shows delayed large at presentation, they are increasingly incidentally discov-
enhancement, and is surrounded by hepatocytes and small bile ered and often less than 4 cm in diameter (Grazioli et al, 2012).
ducts (see Chapter 89). FNH has been associated with oral Hemorrhage may be life threatening if it extends into the peri-
contraceptive use (Scalori, 2002) as well as chemotherapy in toneum. Although imaging characteristics vary, a combination
the pediatric age group (Do et al, 2011; Sudour et al, 2009). of features, including enhancement characteristics, intralesional
Most FNH are isointense to normal liver parenchyma on T1- lipid, and hypointensity on delayed hepatobiliary phase imaging,
and T2-weighted images, and a few are mildly T1 hypointense may help increase diagnostic confidence (Mohajer et al, 2012).
or minimally hyperintense on T2-weighted images (Fig. 19.8A Nonetheless, small adenomas without hemorrhage may be dif-
and B). When discussing relative T1 and T2 signal, a normal ficult to differentiate from FNH without a central scar and from
background liver parenchyma is assumed. In a liver with iron well-differentiated HCC.
deposition, which diffusely lowers the signal intensity of the Recently, distinct genetic subtypes of adenomas have been
liver parenchyma, T1 and T2 relative hyperintensity can be described and show differing behaviors, histopathology, and
expected. This may be seen, for example, in pediatric oncologic imaging features. These include inflammatory, hepatocyte
patients who have concomitant iron deposition (Do et al, nuclear factor-1α (HNF-1α–mutated), and β-catenin–mutated
2011). Frequently, FNH is visualized by displacement of the HCAs (see Chapter 89). Of note, some adenomas may be both
normal hepatic vasculature, and classic FNH shows strong β-catenin mutated and inflammatory. A group remains unclas-
arterial peak enhancement following administration of an intra- sified and encompasses other HCAs without any genetic abnor-
venous contrast agent, with lack of washout in portal venous or malities (Grazioli et al, 2013). Inflammatory HCA, the most
late dynamic phase imaging. common subtype (30% to 50% of HCAs) typically seen in
A common feature of FNH is the presence of a central scar. women with a history of oral contraceptive use, is generally
This distinguishing feature is hypointense on T1-weighted hypointense on T1 images, hyperintense on T2, and frequently
images and hyperintense on T2-weighted images with enhance- heterogeneous. They usually show moderate arterial enhance-
ment on delayed imaging beginning at approximately 3 minutes ment, persistent dynamic phase enhancement, and variable
by using ECF contrast agents (Fig. 19.8C) (Karam et al, uptake in delayed hepatobiliary phase (Grazioli et al, 2013).
2010). The presence of enhancement, similar to or higher- The enhancement pattern may reflect a mix of poorly function-
than-normal parenchyma, during the delayed hepatobiliary ing hepatocytes, arterioles without accompanying veins,
phase with a hepatocyte-specific contrast agent is expected for inflamed bile ducts, and dilated sinusoids. On MRI, small
the majority of FNHs. Of note, with the hepatobiliary agent amounts of intralesional lipid may be seen. A small percentage
gadoxetate disodium, a central scar, if present, does not usually of these HCA show contrast washout in late dynamic phases,
enhance relative to the hepatocytes present in this lesion. whereas others retain contrast similar to hemangiomas. Delayed
366 PART 2 DIAGNOSTIC TECHNIQUES
A B C
D E F
FIGURE 19.7. Hepatic hemangioma undergoing sclerosis. A, Heavily T2-weighted image (echo time [TE] 150) shows a mass (m) that is hyperintense
to hepatic parenchyma with well-defined margins. B, Precontrast T1-weighted fat saturation image at the same level shows the mass to be low
signal compared with background parenchyma. C, T1-weighted postcontrast image in early portal venous phase shows peripheral nodular enhance-
ment within this mass (arrows). Portions of the lesion fail to show enhancement during this phase. D, Equilibrium phase T1-weighted image post-
contrast shows the lesion has partially filled in toward the central portion. This constellation of findings is typical for hepatic hemangioma.
E-F, The same lesion 5 years later on T1-weighted postcontrast scans in portal venous and equilibrium phase imaging shows less avid enhancement
and has shown slight size decrease, consistent with developing sclerosis. Sclerosing hemangiomas may show size decrease with less avid enhance-
ment, associated capsular retraction, and lower T2 signal than nonsclerosed hemangiomas.
peripheral rim enhancement in hepatobiliary phase may also be malignant degeneration. They show moderate, often heteroge-
seen (Grazioli et al, 2013). neous arterial phase enhancement, which may persist but is
Hepatocyte nuclear factor-1α mutated HCAs (30% to 35% variable in late dynamic and delayed phases. Although T1
of HCAs) are almost exclusively seen in women and often show hypointensity and T2 hyperintensity are common, it is often
large amounts of intralesional lipid. They enhance less avidly heterogeneous. These lesions show diffuse glutamine synthetase
in arterial phase than inflammatory HCA and typically are expression from upregulation, although it may be heteroge-
homogeneously low in signal on delayed hepatobiliary phase. neous. This is in contradistinction to FNH, which shows map-
They may also remain low signal in portal venous or equilib- like glutamine synthetase expression distribution adjacent to
rium dynamic phases, but that may be due to the opposed- hepatic veins (Agarwal et al, 2014; Balabaud et al, 2013; Grazi-
phase property of postcontrast T1-weighted imaging (Grazioli oli et al, 2013).
et al, 2013). Unclassified HCA (10% of HCAs) have no specific genetic
β-Catenin–mutated HCAs (10% to 15% of HCAs) are asso- or histopathologic abnormalities. No specific imaging features
ciated with glycogen storage disease, androgen use, and have a have been identified for these lesions, although experience
male predilection; they also have a higher chance of undergoing remains limited due to their infrequent diagnosis.
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 367
A B
C D
FIGURE 19.8. Focal nodular hyperplasia (FNH). A, T2-weighted image shows a mass that is isointense to hepatic parenchyma (arrows). Centrally,
within this mass is a linear, hyperintense focus (arrowhead). B, A precontrast, T1-weighted gradient-echo image shows the mass (arrows) to be
mildly hypointense to liver. C, Arterial dominant phase T1-weighted gradient-echo sequence shows that the mass enhances intensely with respect
to hepatic parenchyma (arrows). The central focus, which was bright on the T2-weighted images, does not show enhancement on this phase of the
injection (arrowhead). D, Postcontrast equilibrium phase image shows the mass to be isointense to background hepatic parenchyma. The central
portion of scar shows delayed enhancement (arrowhead) characteristic of FNH.
Hepatic Abscess/Infection lesions, including hemangiomas or focal fat, may appear similar
CT is generally the modality of choice in recent postoperative to metastases when imaged with CT or ultrasound. In general,
patients in whom there is a clinical suspicion of a hepatic metastases are mildly hypointense on T1-weighted images and
abscess (see Chapter 72). Patients with more atypical symptoms are mildly hyperintense on T2-weighted images. Unless they are
may present a diagnostic dilemma. Although some patients necrotic, mucinous, or cystic, metastases are not as bright on
show symptoms suggesting abscesses, others do not, but T2-weighted images as hemangiomas or cysts and often become
patients suspicious for abscesses or bile leaks may be imaged less conspicuous with greater (longer echo time [TE]) T2
with MRI. Abscesses are usually hyperintense on T2-weighted weighting. A number of metastases are hypervascular and best
images with an irregular rim of intermediate signal intensity seen on arterial phase imaging, such as those arising from a
surrounding a hyperintense outer rim. Abscesses are generally primary neuroendocrine tumor, renal cell carcinoma, or intra-
hypointense on T1-weighted images, unless they have hemor- hepatic metastases from hepatocellular carcinoma. Most
rhage or proteinaceous debris within them. After administration metastases, however, are hypovascular and tend to have less
of contrast material, the rim enhances, whereas the central well-defined borders after contrast enhancement than other
portion does not. The imaging findings may overlap with malig- benign lesions (Fig. 19.9). During contrast administration,
nancies, including gallbladder cancer. Infected cystic hepatic metastases often show early peripheral marginal enhancement.
lesions also may occur, such as parasitic echinococcal infec- These peripheral rims may wash out and appear hypointense on
tions. Echinococcal cysts are typically multiloculated with inter- delayed images (Fig. 19.10). Larger metastases tend to have a
nal thin-walled daughter cysts, and typically show no internal thick irregular rim of enhancement representing viable tumor
enhancement. A peripheral low T1 and T2 signal rim, as well with areas of central necrosis. Multiple studies have demon-
as correlation with a history of possible exposure, may provide strated superior accuracy of hepatobiliary agent contrast-
added clues to the diagnosis (see Chapter 74) (Qian et al, enhanced MRI over contrast-enhanced CT (Lafaro et al, 2013).
2013). Both ECF and hepatobiliary agent contrast-enhanced MRI has
shown higher sensitivity and specificity than CT–positron-emis-
Hepatic Metastases sion tomography (PET) imaging as well, particularly for small
The liver is the most common site for the hematogenous spread (<1 cm) lesions, and hepatobiliary contrast-enhanced MRI
of malignant neoplasms (see Chapters 92 to 94). Other hepatic combined with PET imaging may offer added benefit (Donati
368 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 19.9. Hepatic metastasis from colorectal carcinoma. A, T1-weighted image shows a low signal intensity metastasis (arrow) within segment
IVB of the liver. B, T2-weighted image shows the mass is mildly brighter than background hepatic parenchyma. C, Post–contrast-enhanced,
T1-weighted fat saturation image shows the lesion as centrally hypointense, in contrast to the normal surrounding hepatic parenchyma, with minimal
areas of marginal enhancement. D, Fused computed tomography/fluorodeoxyglucose–positron-emission tomography image confirms avid tracer
uptake within the lesion, consistent with active tumor. Note the differences in appearance from hemangioma (see Fig. 19.7).
et al, 2010; Maegerlein et al, 2015; Seo et al, 2011). Arterial of disease, progressing from benign to malignant, which occurs
phase imaging may also provide anatomic detail preoperatively; in response to hepatic parenchymal damage and scarring (Lee
however, CT angiography offers improved spatial resolution et al, 2012). The advantage of MRI in the evaluation of HCC
over MRI. is that areas of carcinoma show differences in signal intensity,
diffusion, blood pool, and functional hepatocyte enhancement
Hepatocellular Carcinoma and growth compared with regenerative or dysplastic nodules,
The diagnosis of HCC (see Chapter 91) on CT and ultrasound or background cirrhotic parenchyma. MRI also has an advan-
can be challenging. It is often associated with cirrhosis and tage over other modalities in assessing vascular invasion.
parenchymal heterogeneity (Fig. 19.11), increasing the diffi- Although HCC generally is hypointense on T1-weighted
culty in distinguishing focal hepatic lesions. Cirrhotic livers and hyperintense on T2-weighted images, and shows arterial
show both nodular hepatic contour and parenchymal multi- phase hyperenhancement with delayed dynamic phase washout,
nodular change. These nodules represent a spectrum, from signal intensity may be variable (Silva et al, 2009), particularly
regenerative or dysplastic nodules to HCC. These nodular for early HCC measuring less than 2 cm (Rhee et al, 2012).
lesions are generally thought to constitute a multistep spectrum On T2-weighted images, larger, more poorly differentiated
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 369
A B
C D
FIGURE 19.10. Hepatic metastasis from breast carcinoma. A, T2-weighted image shows a small lesion within the liver (straight arrow) that is mildly
hyperintense. Portal lymphadenopathy also is present (curved arrow). B, Pre-contrast-enhanced, T1-weighted gradient-echo image shows a well-
defined mass (arrow) that is hypointense to liver. C, T1-weighted gradient-echo image after the administration of contrast shows the peripheral portion
that enhanced irregularly during the arterial dominant phase (not shown) beginning to wash out, suggesting an early target appearance (arrow). D,
Delayed postcontrast gradient-echo image shows continued filling of the central portion of this lesion; the periphery has washed out (arrow).
A B
FIGURE 19.11. Liver with cirrhotic configuration. A, T1-weighted spin-echo image at the level of the portal vein shows hypertrophy of the left lobe
and caudate with atrophy of the right lobe of the liver. B, T2-weighted image of the liver at the same level shows mildly heterogeneous signal in the
atrophied right lobe, making exclusion of an underlying mass difficult. Note also the focal hepatic scarring (arrow).
370 PART 2 DIAGNOSTIC TECHNIQUES
A B
FIGURE 19.12. Large hepatocellular carcinoma showing the mosaic pattern. A, T1-weighted image shows a large heterogeneous mass (m) in the
liver. Note the hypertrophied left hepatic lobe and caudate. B, T2-weighted image also shows the mass (m) to be heterogeneous, with islands of
tissue that are hyperintense with respect to other portions of the same mass. This pattern is known as the mosaic pattern, and it can be seen in
hepatocellular carcinoma, especially when the lesion is large.
A B
FIGURE 19.13. Hepatocellular carcinoma containing intracellular lipid. A, T1-weighted in-phase gradient-echo image shows a mass in the liver
that is darker than normal parenchyma, with a small internal area of brighter signal (arrow). B, T1-weighted out-of-phase gradient-echo image shows
the same area (arrow) has lost signal, which is consistent with an admixture of fat and water-containing tissue.
HCCs may be heterogeneous due to areas of necrosis (Fig. hyperenhance, they tend to be more homogeneous and isoin-
19.12). Areas of heterogeneity may indicate moderate to poorly tense to background liver parenchyma during the equilibrium
differentiated tumors (Witjes et al, 2012). HCC may show high phase, often show low T2 signal, and are variable on delayed
T1 signal (Fig. 19.13) (Basaran et al, 2005), and lesions with hepatobiliary phase imaging (Cruite et al, 2010). In HCC,
intracellular lipid show signal loss on out-of-phase T1-weighted hepatocyte contrast agents generally show hypointensity in
imaging. Intracellular lipid may be an important clue to small delayed hepatobiliary phase imaging compared with surround-
HCCs without typical enhancement patterns, as early HCC are ing liver in the vast majority of cases, with a small percentage
sometimes hypovascular in arterial phase (Rhee et al, 2012). showing variable internal uptake, which may reflect either the
Contrast washout in portal venous or later dynamic phase grade of tumor differentiation or specific enzyme production
MRI, as well as heterogeneous enhancement, has been associ- and tumor receptors. (Cruite et al, 2010) Rarely, well-
ated with moderate to poorly differentiated tumors; a higher differentiated HCC may show tracer concentration in delayed
percentage of well-differentiated tumors may not demonstrate hepatobiliary phase with areas of increased signal intensity.
washout (Okamoto et al, 2012; Tan et al, 2011; Witjes et al, Due to the complexity of imaging features and overlap, as
2012). In addition to washout, peritumoral capsules, which are well as multimodality availability, there have been organized
low in signal intensity on the arterial dominant phase and efforts to improve report standardization and communication
enhance later, are also associated with microvascular invasion, regarding imaging findings, as well as recommendations regard-
an important feature with clinical significance (Witjes et al, ing surveillance imaging and screening. The American Associa-
2012). These are distinguishing features in contrast to benign tion for the Study of Liver Diseases (AASLD) issued revised
or dysplastic nodules. Although dysplastic nodules may also recommendations in 2010, recommending HCC screening for
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 371
patients at risk with ultrasound (US) every 6 months combined Although extracellular lipid is typical in HAMLs, they often
with serum α-fetoprotein (AFP). MRI imaging has an emphasis show brisk, avidly enhancing soft tissue components with
on arterial phase hyperenhancement and washout, with biopsy washout, which overlaps with other liver malignancies, such as
improving sensitivity for indeterminate lesions (Tan et al, hepatocellular carcinoma. HAML is generally considered a
2011). The Liver Imaging Reporting and Data System (LI- benign, solitary tumor comprising three elements: smooth
RADS), an initiative supported by the American College of muscle, thick-walled blood vessels, and mature adipose tissue
Radiology, as well as the Liver and Intestinal Organ Transplant (Cai et al, 2013), although they can also present without fat
Committee (OPTN) have also issued guidelines regarding (Butte et al, 2011). Limited data suggest a well demarcated,
HCC classification. LI-RADS was revised in 2014 to better lipid-containing tumor with a thin peripheral enhancing rim,
incorporate OPTN and AASLD guidelines regarding growth lack of peritumoral capsule, and an early draining vein that may
and lesion detection on screening ultrasound. Ancillary fea- offer clues to the diagnosis, particularly in patients without cir-
tures, including nodule-in-nodule or mosaic appearance, intra- rhosis or elevated serum AFP (Fig. 19.14) (Cai et al, 2013; Du
lesional fat, diffusion restriction, and perilesional or coronal et al, 2012). Surgical excision remains preferable, as there have
enhancement, for example, are also incorporated into the been reports of HAML hemorrhage and capsular rupture, as
LI-RADS imaging interpretation algorithm (http://nrdr.acr.org/ well as venous obstruction or Budd-Chiari syndrome from mass
lirads/). Although continued revisions are inevitable, consensus effect. Furthermore, pathologic analysis remains essential for
guidelines will encourage report standardization, improve com- diagnostic confirmation; immunohistochemical stains for
munication, and ultimately improve decision making. Agree- markers may offer increased accuracy (Du et al, 2012).
ment among readers using newer algorithms tends to be
moderate to substantial for expert readers but lower among Mesenchymal Tumors
novices, suggesting implementation of criteria may require a Rarely, tumors of mesenchymal origin, including hepatic angio-
learning curve (Davenport et al, 2014). sarcoma (HAS), leiomyosarcoma, and fibrous histiocytoma,
may be present within the liver (Anderson et al, 2009). The
Fibrolamellar Carcinoma MRI appearance of these tumors is nonspecific; they are gener-
Fibrolamellar HCC (FLHCC), a rare variant, occurs in young ally of low intensity on T1-weighted images and hyperintense
adults, and is distinct from conventional HCC on multiple on T2-weighted images, with heterogeneous enhancement.
levels, including molecular and clinical differences (see Chapter HAS typically shows hyperenhancement, often peripheral, but
91). The average age at presentation is 25 years, and the pres- sometimes central and irregular, with progressive fill-in on more
ence of nodal metastases is common (Ganeshan et al, 2014). delayed phases following blood pool. Although similar to cav-
FLHCC may have a central scar, and these scars tend to be ernous hemangiomas, HAS may also show centrifugal or
low in signal intensity on T1-weighted and T2-weighted images “reverse” enhancement patterns and show greater degrees of
due to fibrous changes. FNH also may have a central scar, variance and heterogeneity, with more disordered peripheral
although FNH scars generally show increased T2 signal; enhancement than nodular, discontinuous, clump-like enhance-
however, it is not always a reliable differentiating feature (Gane- ment typically seen in benign hemangiomas. HAS is typically
shan et al, 2014; Kim et al, 2009). FLHCC may show early multiple, of varying size, involving both hepatic lobes, and
heterogeneous enhancement with variable washout and may rapidly growing, as median survival has been reported as less
show partial hepatocyte agent concentration in delayed hepa- than 6 months (Huang et al, 2014; Pickhardt et al, 2015).
tocyte phase imaging (Meyers et al, 2011). Metastatic disease
is also common at presentation, both in the abdomen and chest, Epithelioid Hemangioendothelioma
with adenopathy being prominent (>2 cm) in a majority of Epithelioid hemangioendothelioma (EH) is a rare tumor of
cases (Do et al, 2014). adults that should be distinguished from infantile hemangioen-
dothelioma, which occurs in infants and children. The progno-
LESS COMMON HEPATIC TUMORS sis is better for EH than for other parenchymal tumors, such
as sarcoma, although extrahepatic metastases do occur. EH is
Lymphoma generally low in signal intensity on T1-weighted images and
Non-Hodgkin lymphoma accounts for most hepatic lympho- hyperintense on T2-weighted images but not as hyperintense
mas. MRI shows masses of varying size, which are generally as hemangiomas. They also may show a distinct target sign on
low in signal intensity on T1-weighted images and hyperintense T1- and T2-weighted images (Economopoulos et al, 2008).
on T2-weighted images (Coenegrachts et al, 2005; Rizzi et al, After Gd-DTPA administration, an irregular nodular and con-
2001), but not as great as with other benign hepatic lesions, centric enhancement may be seen. Capsular retraction also may
such as hemangiomas or cysts. This difference in signal inten- be seen with EH, helping to elucidate the diagnosis (Lin et al,
sity makes it relatively easy to determine the malignant nature 2010) (see Chapter 89).
of the lesion but not the specific tumor type. Lymphoma may
be relatively hypoenhancing in early dynamic phases, with Biliary Cystadenoma and Biliary Cystadenocarcinomas
isointensity in later phases (Coenegrachts et al, 2005). The Biliary cystadenomas and biliary cystadenocarcinomas are rare
imaging characteristics of lymphoma overlap with other malig- tumors of the liver that present as a predominantly cystic mass
nant hepatic lesions. containing enhancing septations (Fig. 19.15; see Chapters 89
and 90B). These lesions may be of low, intermediate, or
Angiomyolipoma increased signal on T1-weighted images, depending on the
Hepatic angiomyolipoma (HAML) is an uncommon tumor, protein or hemorrhagic content within the mass, and they are
more frequent in females, which currently presents a diagnostic usually hyperintense on T2-weighted sequences. Enhancing
challenge for imaging diagnosis (see Chapters 89 and 90). mural or internal irregular soft tissue nodularity, as well as
372 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 19.14. Angiomyolipoma. A, T1-weighted in-phase image shows a high-signal right hepatic mass (arrow). B, T1-weighted out-of-phase
image shows low signal at its margin due to chemical shift artifact between the mass and surrounding liver, confirming the presence of bulk fat.
C, Axial T2-weighted image with fat saturation shows the mass is dark. D, Axial T1-wieghted fat saturation image shows the mass is dark as well.
internal hemorrhage, has been shown in to be more often asso- high T2 signal thickening of the gallbladder wall, with early and
ciated with cystadenocarcinomas; however, differentiation may prolonged heterogeneous enhancement, often in patients with
not be possible (Arnaoutakis et al, 2015; Qian et al, 2013; multiple gallstones (Tan et al, 2013). Cholelithiasis is a predis-
Wang et al, 2012). Communication with the biliary ductal posing condition. Evidence of liver invasion and spread to
system on delayed hepatobiliary phase imaging with hepatocyte regional lymph nodes also may be identified with MRI, which
contrast agents has been reported, helping to differentiate these is optimal for evaluation of these lesions because of its out-
tumors from nonneoplastic simple hepatic cysts. (Billington standing tissue contrast, ability to image directly in multiple
et al, 2012; Marrone et al, 2011). Infectious cysts may also planes (Dai et al, 2009; Sikora et al, 2006), with DWI offering
communicate with the biliary tree, however, such as with added sensitivity and specificity for the primary tumor as well
complex cysts from echinococcal disease. as nodal or hepatic metastatic disease (Tan et al, 2013). Fluo-
rodeoxyglucose (FDG) PET imaging may also provide
BILIARY TUMORS improved sensitivity and specificity for nodal or distant meta-
static disease (Lee et al, 2010).
Gallbladder Carcinoma
MRI offers improved characterization of gallbladder cancer Bile Duct Cancer
compared with other modalities. However, its differentiation Bile duct tumors (see Chapters 50, 51, and 59) are well
from inflammatory conditions, which may occur concurrently, depicted on MRI and may be intrahepatic, hilar, or extrahe-
may be difficult (see Chapters 33 and 49). As opposed to the patic, with a mass-forming appearance or as periductal infil-
inflammatory associated wall thickening with maintained trating or papillary intraductal morphologies (Chung et al,
mucosal and submucosal layers, with differential enhancement, 2009). Tumors may show focal nodular thickening along
gallbladder cancer typically shows irregular intermediate to ductal walls or be discrete intrahepatic masses. Central hilar
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 373
A B
C
FIGURE 19.15. Biliary cystadenoma. A, Coronal T2-weighted image shows a lobulated mass (m) in close proximity to the left hepatic duct (arrow-
head). B, Projection image in the coronal oblique plane shows the well-defined hyperintense mass to be in continuity with a mildly dilated left-sided
biliary radicle (straight arrow). The normal right-sided biliary radicle (curved arrow) is easily seen with this technique. C, Postcontrast, T1-weighted
gradient-echo image shows no enhancement within this mass (m).
cholangiocarcinomas are the most common and are generally capsular retraction as well as vascular encasement, typically
associated with biliary ductal dilation. Bile duct tumors may without tumor thrombus (Chung et al, 2009). Smaller tumors
be seen as intermediate, mildly increased T2 signal (Fig. may show early, more uniform arterial enhancement, particu-
19.16), however, less so than the surrounding biliary dilata- larly when less than 4 cm in size (Kim et al, 2011). Intraductal
tion. The level of obstruction and continuity of the tumor with papillary neoplasm of the bile duct is an uncommon subtype of
the vasculature are well evaluated with MRI (Peporte et al, bile duct cancer with characteristics similar to pancreatic intra-
2013), although CT angiography with multiphasic imaging ductal mucinous neoplasms. The majority of tumors occur near
offers improved spatial resolution and similar accuracy to MRI the hilum or in extrahepatic ducts, and the clinical outcomes
to assess vascular involvement, and exceeds MRI accuracy are better than conventional bile duct cancers (Rocha et al,
when assessing for nodal and distant metastases (Aljiffry et al, 2012).
2009). Focused assessment of ductal, portal venous, and
hepatic arterial involvement is performed in staging and pre- BENIGN DISEASES OF THE BILIARY TRACT
operative imaging.
Peripheral, mass-forming intrahepatic cholangiocarcinomas Cholelithiasis and Choledocholithiasis
occur in approximately 10% of cases and generally have high Gallstones are well identified on T2-weighted images and on
T2 signals, lobulated heterogeneous masses with peripheral MRCP sequences (Fig. 19.18; see Chapters 32, 33, and 36).
enhancement, and gradual centripetal fill-in (Fig. 19.17) They usually appear as low signal intensity structures in a
(Hennedige et al, 2014, Kang et al, 2012) (see Chapter 50). fluid-filled gallbladder. Ultrasound is usually the modality of
Satellite lesions are common within the liver, and these lesions choice in the evaluation of uncomplicated cholelithiasis or cho-
tend to show low signal intensity on delayed hepatocyte imaging lecystitis due to its high sensitivity and lower cost, but choledo-
phase (Chung et al, 2009; Kim et al, 2011; Peporte et al, cholithiasis is more effectively imaged by MRI (Johnson et al,
2013). Intrahepatic cholangiocarcinomas may show adjacent 2010; Samaraee et al, 2009). Coronal T2-weighted imaging,
374 PART 2 DIAGNOSTIC TECHNIQUES
A B
C
FIGURE 19.16. Hilar mass. A, Axial T2-weighted image shows dilatation of the left hepatic duct and a low to intermediate–intensity mass expand-
ing the right hepatic duct (arrow). B, T1-weighted late arterial phase postcontrast image shows early enhancement of the tumor (arrow). C, Portal
venous phase postcontrast T1-weighted imaging shows the mass (arrow) is hypoenhancing to liver. Biopsy of a more superior intrahepatic mass in
this patient with cirrhosis showed poorly differentiated hepatocellular carcinoma. Extension into the biliary ducts with ductal expansion and obstruc-
tion is an uncommon finding in hepatocellular carcinoma (HCC). Although HCC and cholangiocarcinoma may exist simultaneously as two distinct
tumors, a distinct subtype of mixed HCC-cholangiocarcinoma is increasingly recognized.
performed routinely with MRI, readily identifies common duct have been described (Lee et al, 2009; Todani et al, 1977): type
stones (Fig. 19.19). MRCP can also be obtained to evaluate I has been subdivided into A, B, and C, in addition to types II,
whether retained stones are present after cholecystectomy, III, IVa, IVb, and V. Recently, there have been advocates for
although clips may limit examinations in the perioperative time dropping the numeric classification system, instead using a
period. If no stones are present on MRCP, this may obviate the more descriptive, clinically meaningful nomenclature (Visser
need for ERCP. et al, 2004). MRI is well suited not only to diagnose these cysts,
but also to classify the type of cyst. Not only can 3D MR chol-
Choledochal Cysts angiograms depict the normal and abnormal anatomy, but
Choledochal cysts (see Chapter 46) represent dilatation of the direct coronal imaging and delayed scans post–hepatocyte-
extrahepatic bile ducts with possible associated intrahepatic specific gadolinium-based contrast agents can be obtained for
biliary duct dilatation. This entity is a relatively uncommon further evaluation (Gupta et al, 2010).
congenital anomaly that usually presents before 10 years of age.
The classic triad includes a palpable mass, abdominal pain, and Postoperative Biliary Complications
jaundice. Cysts may be associated with chronic inflammation Complications from surgical procedures include bile leaks,
and increase the risk for cholangiocarcinoma. Five types of cysts abscess formation, and biliary strictures (see Chapters 27 and
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 375
A B C
D E F
FIGURE 19.17. Mass forming intrahepatic cholangiocarcinoma. A, T1-weighted in-phase gradient-echo image shows a peripheral hypointense
mass (m) with capsular retraction. B, A T2-weighted fat saturation image shows increased signal intensity within the mass. C, Diffusion-weighted
image shows restricted diffusion within the mass, which is brighter than liver. D, T1-weighted fat saturation post–contrast-enhanced image in late
arterial phase shows peripheral enhancement. E, T1-weighted post–contrast-enhanced image in late portal venous phase shows only partial filling
of the mass. F, T1-weighted post–contrast-enhanced image in late portal venous phase at a separate level shows an additional satellite lesion (arrow),
smaller in size with marginal enhancement, typical of intrahepatic metastasis.
A B
FIGURE 19.18. Choledocholithiasis. A, Coronal T2-weighted single-shot fast spin-echo image through the common duct in a patient after chole-
cystectomy shows multiple stones within the common bile duct. Note the distal stone impacted at the level of the ampulla (arrow). B, Axial T2-weighted
image with the same technique also shows a stone, surrounded by bile, in the distal common bile duct (arrow).
376 PART 2 DIAGNOSTIC TECHNIQUES
PANCREAS
Solid Tumors of the Pancreas
Pancreatic solid tumors include both neoplastic and nonneo-
plastic origins (see Chapter 59). Although MRI characteristics
alone may help predict etiologies, there may be imaging-feature
overlap between entities. Imaging characteristics combined
with clinical presentation and demographic data often guide
therapy and predict the diagnosis. Neoplastic etiologies include
tumors arising in the pancreas, such as adenocarcinoma, solid
pseudopapillary tumor, neuroendocrine tumors, or pancreatic
lymphoma. Metastases, lymphomas, and other rare tumors
may involve the pancreas (Low et al, 2011). In addition to
enhancement characteristics, such as early arterial enhance-
ment in neuroendocrine tumors, precontrast signal character-
istics, such as hemorrhage with increased T1 signal in solid
A pseudopapillary tumors, may provide clues to the diagnosis.
Nonneoplastic etiologies include focal pancreatitis, accessory
spleen, focal fat, congenital anomalies, and other rare etiolo-
gies. Intrapancreatic splenic tissue shows signal intensity and
enhancement characteristics paralleling that of spleen on all
MRI sequences. Focal pancreatitis may mimic pancreatic ade-
nocarcinoma; however, restricted diffusion on DWI is typically
seen in adenocarcinoma (Fattahi et al, 2009; Kartalis et al,
2009), compared with focal pancreatitis. Focal pancreatitis may
also cause irregular narrowing of the main pancreatic duct, as
opposed to the abrupt cutoff and upstream dilatation with
associated parenchymal atrophy noted in adenocarcinoma
(Low et al, 2011; Siddiqi et al, 2007).
Pancreatic Cancer
Pancreatic adenocarcinoma (see Chapters 59 and 62) is well
B evaluated on MRI and MRCP. T2, diffusion-weighted, and
dynamic contrast-enhanced T1-weighted MRI sequences are
FIGURE 19.19. Afferent loop syndrome. A, Coronal T2-weighted particularly helpful to characterize pancreatic cancer and stage
sequence in a patient after pancreaticoduodenectomy for pancreatic patients (Tamm et al, 2012). MRI is generally thought to be
carcinoma. The patient has a hepaticojejunostomy with a patent anas-
highly accurate in assessing for vascular invasion or encasement
tomosis (white arrow). The afferent loop is markedly dilated (black arrow)
compared with other loops of bowel. No mechanical obstruction was
(tumor surrounds >50% of the vessel circumference), local-
noted. B, Axial T2-weighted image through the level of the anastomosis regional tumor extension, and liver metastases (Tamm et al,
(arrow) shows the site to be patent without evidence of a stricture. The 2012), although recent data have suggested MRI may under-
afferent loop is dilated. estimate tumor size (Hall et al, 2013; Legrand et al, 2015).
Similar to other modalities, accuracy is limited for assessment
of lymph node metastases with MRI techniques. Pancreatic
30). Although using other imaging modalities in the immediate cancer subtypes may be predicted based on imaging features,
postoperative setting to assess for bile leaks and abscesses may patient demographics, and clinical presentation, particularly
be prudent, MRI is uniquely suited for the assessment of the neuroendocrine tumors; however, there is overlap in the imaging
postoperative biliary tract. Bile duct injuries after surgery can appearance and location of solid and cystic neoplasms. Prelimi-
be caused by a number of things, but these may all lead to the nary data suggest grade of tumor enhancement may correlate
same result—a stricture at the anastomotic site. MRCP is with tumor grade in adenocarcinomas (Lauenstein et al, 2010).
uniquely suited for addressing this problem. Surgical clips near
the anastomosis may create streak artifacts during CT scan- Cystic Lesions of the Pancreas
ning, but currently used clips are less problematic for MRI. Detection of pancreatic cystic lesions (see Chapter 60) has
MRI has multiplanar capabilities and superior tissue contrast, increased in recent years with increased imaging and improved
and MRCP sequences can minimize susceptibility to artifacts spatial resolution. They are increasingly found incidentally.
to allow improved visualization of the region of the anastomosis Benign lesions may also progress to malignant lesions over
and improved diagnostic confidence (see Fig. 19.19). More time. Diagnostic possibilities include benign lesions, such as
recently, hepatocyte contrast agents also allow delayed hepato- pseudocysts, serous cystadenomas, and true epithelial cysts; to
Chapter 19 Magnetic resonance imaging of the liver, biliary tract, and pancreas 377
benign lesions with potential for malignant degeneration, such to have a higher association with malignancy; their presence
as intraductal mucinous or parenchymal mucinous cystic neo- may warrant surgical excision (Kim et al, 2014). Evaluation
plasms; to malignant lesions, such as rare cystic or necrotic after contrast administration helps assess cyst wall irregularity
adenocarcinomas or cystic neuroendocrine tumors (Kucera or enhancement of soft tissue components. Molecular analysis
et al, 2012). Multiple imaging modalities may be used to iden- of cyst contents to assess for genetic mutations or gene silencing
tify and characterize pancreatic cystic lesions, including ultra- associated with IPMN may offer improved accuracy in diag-
sound, CT, and MRI. nostic workup (Freeny et al, 2014).
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CHAPTER 20
Direct cholangiography: approaches, techniques, and
current role
Robert H. Siegelbaum and Robin B. Mendelsohn
DIRECT CHOLANGIOGRAPHY OVERVIEW the gallbladder. The first report of PTC was by Huard and
Do-Xuan-Hop in 1937, who performed cholangiography with
Direct cholangiography, the introduction of contrast medium the suboptimal contrast agent Lipiodol. The use of transhe-
into the biliary system, can be performed under fluoroscopic patic cholangiography as a diagnostic tool gained popularity
guidance percutaneously, endoscopically, or intraoperatively 15 years later, after Carter and Saypol’s (1952) discussion of
via surgically placed catheters. The nonoperative techniques are PTC with the use of a water-soluble contrast agent. In the
percutaneous transhepatic cholangiography (PTC) and endo- ensuing years, many investigators (Flemma & Shingleton,
scopic retrograde cholangiopancreatography (ERCP). Cur- 1966; Glenn et al, 1962; Mujahed & Evans, 1966; Seldinger,
rently, noninvasive magnetic resonance imaging (MRI) and 1966; Shaldon et al, 1962; Weicher, 1964) described a variety
contrast-enhanced computed tomography (CECT) have virtu- of different methodologic details, including the use of sheathed
ally eliminated the indications and need for direct cholangiog- or unsheathed needles of various sizes and different puncture
raphy (Bakhal et al, 2009; Miller et al, 2007; Stroszczynski & sites with varying directions of puncture. The procedure
Hünerbein, 2005) (see Chapters 18 and 19). Today, ERCP and remained associated with a significant risk of bile peritonitis,
PTC are typically performed only as part of a planned inter- especially in obstructed biliary systems, and less frequently,
ventional procedure, such as biliary drainage, stent placement, hemorrhage. The use of fine needle technique was developed
stone extraction, or stricture dilation (see Chapters 29 and 30). at Chiba University and was first presented by Ohto and
Imaging evaluation of the biliary tree with magnetic reso- Tsuchiya (1969), and later by Tsuchiya (1969). Numerous
nance cholangiopancreatography (MRCP) or CECT is nonin- additional reports have also described decreased complications
vasive, does not require sedation, and is generally regarded as with fine needle transhepatic access, and the fine needle tech-
safe. Imaging protocols with multiplanar reconstruction allow nique has been generally accepted as the standard (Benjamin
a large field of view that enables visualization of the entire et al, 1978; Ferrucci et al, 1976; Fraser et al, 1978; Gold &
biliary tree and pancreatic duct (Fig. 20.1). Reconstructed Price, 1980; Harbin et al, 1980; Hinde et al, 1977; Jain et al,
three-dimensional data sets can be displayed in an appearance 1977; Pereiras et al, 1977).
similar to a diagnostic cholangiogram, with the added benefit Transhepatic cholangiography has essentially been sup-
of being able to rotate the images to further delineate the planted by noninvasive imaging techniques for the evaluation
anatomy of the bile duct and pancreatic duct. In comparison, of the biliary tree. In 1985, Kadir reported that less than 5%
injection of contrast dye under fluoroscopic guidance is limited of patients referred for evaluation of biliary disease required
to visualization of structures in direct continuity with the opaci- concomitant drainage procedures. With continued advance-
fied, nonisolated segments of the biliary tree (Fig. 20.2). While ment of cross-sectional imaging techniques, in particular
performing direct cholangiography with PTC, simultaneous MRCP (see Chapter 19) (Park et al, 2004; Romagnuolo et al,
cross-sectional imaging may be required to ensure that the 2003; Simone et al, 2004; Vaishali et al, 2004; Zhong et al,
entire biliary tree has been opacified, even with multiple per- 2003), percutaneous fluoroscopic imaging of the biliary tree is
cutaneous puncture sites and injections. Cross-sectional typically only performed as part of a planned radiologic inter-
imaging of the liver can be performed in a fluoroscopy room ventional procedure.
with rotational angiography or by direct CT imaging if there is Imaging evaluation of the biliary tree with MRCP or CECT
an in-line CT scanner. In addition, MRCP and CECT typically is noninvasive, does not require sedation, and is generally
provide superior diagnostic accuracy when compared with PTC regarded as safe (see Chapters 18 and 19). With direct puncture
or ERCP, allowing visualization of the bile duct wall, structures and contrast injection in the biliary tree, only bile ducts in
contiguous to the biliary tree (such as cysts and neoplasms), continuity with the punctured duct are visualized. Multiple
and structures adjacent to the liver. percutaneous punctures may be required to visualize the entire
biliary tree in the presence of bile duct isolation (see Fig. 20.2).
Even with multiple transhepatic bile duct punctures, CT
PERCUTANEOUS TRANSHEPATIC imaging performed at the time of the procedure can be helpful
CHOLANGIOGRAPHY to ensure that the biliary tree has been completely assessed.
Alternatively, MRI and CECT can image the entire biliary
History system and can demonstrate the presence and severity of bile
The first report of fluoroscopic imaging of the biliary tree was duct isolation (see Fig. 20.1). Furthermore, by also visualizing
presented by Burckhardt and Müller in 1921, who performed the bile duct wall, liver, and surrounding structures, additional
cholecystocholangiography through percutaneous puncture of anatomic information is provided with MRI or CECT.
378
Chapter 20 Direct cholangiography: approaches, techniques, and current role 379
Procedure
Although not always present in modern fluoroscopy suites,
PTC is ideally performed on a tilting fluoroscopic table. As the
specific gravity of contrast material is greater than that of bile,
less contrast dye is typically required to fully delineate the
biliary tree when the table is tilted.
FIGURE 20.1. Magnetic resonance cholangiopancreatography. Three- Right-Sided Puncture
dimensional maximum intensity projection image showing marked dilata-
tion of the intrahepatic and extrahepatic biliary tree, as well as the After the patient has been prepared and draped in a sterile
pancreatic duct, in a patient with a head of pancreas mass. fashion, a puncture site is selected in the right midaxillary line,
typically one or two interspaces below the costophrenic angle.
Puncture sites are generally kept below the ninth intercostal
space to avoid inadvertent entry into the pleural space. One
percent lidocaine is infused subcutaneously, and a small derma-
totomy is made with a No. 11 scalpel. A 21- or 22-gauge, 15- to
20-cm Chiba-style needle is advanced under fluoroscopic guid-
ance superior to the closest rib to the target puncture site, to
avoid laceration of an intercostal vessel. Real-time ultrasound
guidance can be helpful for the initial puncture in the presence
of bile duct dilatation (Covey & Brown, 2008). The puncture
site and direction are chosen based on evaluation of the patient’s
cross-sectional imaging studies (Fig. 20.3A and B).
Care should be taken to avoid puncture of the gallbladder
or extrahepatic bile duct. A small amount of water-soluble
contrast agent is injected while slowly withdrawing the needle
until a bile duct is identified. Injection of contrast agent into a
bile duct has the appearance of oil being dropped in water.
Inadvertent opacification of a vascular structure is recognized
by the rapid clearance of the contrast agent. If a bile duct is not
entered during withdrawal of the needle, the needle is reintro-
duced in a slightly different direction. It is generally recom-
mended not to withdraw the needle completely from the liver,
to minimize the number of punctures through the liver capsule.
When opacification of the biliary tree is challenging, particu-
larly in the case of a nondilated biliary tree, the same puncture
FIGURE 20.2. Hilar cholangiocarcinoma involving first-order right and site may be used multiple times prior to selecting a new percu-
left hepatic ducts. Separate needle punctures were required to fill the taneous access site. If successful puncture of a bile duct is
right and left ducts. unlikely from that site after multiple attempts, a new site should
be chosen. In patients with biliary obstruction, gentle injection
of 10 mL of iodinated contrast is typically sufficient for bile
Preprocedural Preparation duct opacification. A larger volume of contrast material is typi-
Ideally, all patients should undergo cross-sectional imaging cally required in nonobstructed systems. When the bile ducts
(CECT or MRI) prior to PTC. This imaging is particularly are visualized, fluoroscopic images should be acquired and
important in patients who have undergone prior liver resection. stored in multiple projections to identify specific portions of the
MRI or CECT are the imaging modalities of choice due to their biliary tree and to completely delineate abnormal findings, if
diagnostic accuracy in depicting the level of obstruction, posi- present.
tion of the liver, portal vein patency, the relationship of the liver
and bile ducts to other structures, and presence of tumors or Left-Sided Puncture
lobar atrophy, all of which could greatly facilitate successful There is considerable variation in size and anatomic position
puncture. of the left lateral segments of the liver, and careful review of
380 PART 2 DIAGNOSTIC TECHNIQUES
LOGIQ
preprocedural cross-sectional imaging is recommended to
E9 select an optimal puncture site. Although left-sided punctures
can be performed through the right liver via an anterior axillary
line approach to the segment IV bile ducts, the generally pre-
21 ferred method is a subxiphoid approach to a bile duct in
segment II or segment III. As in punctures of right sided bile
ducts, percutaneous access to the biliary tree can be simplified
by using real-time ultrasound guidance in the presence of
dilated bile ducts (Covey & Brown, 2008).
Pitfalls in Interpretation
Lack of Opacification
Failure to inject adequate volume of contrast agent can result
in false interpretation of the level of obstruction. This pitfall
can occur in the setting of complete obstruction and can be
B
recognized by the presence of a hazy margin at the level of the
FIGURE 20.3. Real-time ultrasound guidance can be helpful for the apparent (false) obstruction (Fig. 20.4) (Kittredge & Baer,
initial puncture in the presence of bile duct dilatation. A, Color Doppler 1975). In high bile duct obstruction, especially when associated
image of the left liver revealing a dilated segment III bile duct. B, Static with variant anatomy, isolated segments of the biliary tree can
grayscale ultrasound image taken during puncture of the dilated bile duct be visualized only by direct puncture. If the wrong bile duct is
with an echogenic 21-gauge needle.
selected, or if puncture of an additional bile duct is needed but
A B
FIGURE 20.4. Ampullary carcinoma. A, With the patient supine, contrast pools proximally, giving a false impression of a high bile duct obstruction.
The spurious nature of the level is suggested by the hazy inferior margin to the contrast column. B, With the patient sitting semierect, the contrast
pools at the true point of obstruction, which is sharply defined.
Chapter 20 Direct cholangiography: approaches, techniques, and current role 381
not performed, the diagnosis of bile duct injuries and bile leaks that ERCP, MRCP, and endoscopic ultrasound have compa-
can be missed. rable sensitivity and specificity in the diagnosis of common bile
duct (CBD) stones. With newer diagnostic imaging technolo-
Ductal Dilatation gies, however, ERCP has evolved into a predominantly thera-
The absence of bile duct dilatation does not exclude the pres- peutic procedure. They stated that avoidance of unnecessary
ence of clinically significant biliary obstruction. Disorders such ERCPs is the best way to reduce the number of complications
as sclerosing cholangitis, acquired immunodeficiency syn- and that endoscopists performing ERCPs should have appro-
drome, and chemotherapy-induced biliary sclerosis can present priate training and expertise. In 2005, the American Society of
with bile duct fibrosis, impeding the ability of the bile ducts to Gastrointestinal Endoscopy published guidelines, stating that
become dilated. Conversely, bile duct dilatation does not based on expert opinion, ERCP is primarily a therapeutic pro-
always imply the presence of an obstructed biliary system. For cedure for the management of pancreaticobiliary disorders
example, dilatation that may be seen in patients with Caroli (Adler et al, 2005). Therefore ERCP is rarely performed
disease, or choledochal cysts, can have the radiographic appear- without a therapeutic component.
ance of bile duct dilation without the presence of obstruction.
Technique
Complications Most ERCPs are performed as outpatient procedures in a hos-
Serious complications of PTC are rare and occur in approxi- pital setting, although they can be performed in ambulatory
mately 3% of patients (Harbin et al, 1980). The most common centers as well. Given that ERCP is a complex procedure,
major complications are bile leak (1% to 2%), sepsis (2% to requiring special equipment and training, the risks and benefits
3%), and hemorrhage (0.2% to 0.4%). Other rare complica- of the procedure must be heavily considered prior to proceed-
tions include pneumothorax, biliothorax, injury to the colon ing. Patients should be alert, oriented, and able to give informed
related to the puncture, and abscess formation. Puncture below consent. In the rare cases where patients are unable to give
the ninth intercostal space will clearly decrease the incidence informed consent, the next of kin can provide consent. Patient
of pleural and lung complications. The risk of infectious com- age and clinical picture are important. Elderly patients can
plications such as sepsis and abscess formation can be mitigated safely undergo ERCP; they have the same risks of bleeding and
with proper antibiotic coverage. Care should be taken to not perforation as younger patients and actually have a lower risk
overdistend the biliary tree, as opacification and incomplete of pancreatitis (Badalov et al, 2009).
drainage of the biliary tree can be a source of cholangitis (Covey Once consent is obtained, the patient is brought into a room
& Brown, 2008), particularly in the presence of bile duct with a C-arm for availability of fluoroscopy during the proce-
isolation. dure. Intravenous sedation is given under monitored control.
In the past, drug combinations of narcotics, such as meperidine
and droperidol, and benzodiazepines, such as midazolam or
ENDOSCOPIC RETROGRADE diazepam, were used. More recently, this has been replaced by
CHOLANGIOPANCREATOGRAPHY propofol, a short-acting sedative and amnestic with a rapid
recovery profile. Studies have shown that propofol is more
History effective than sedation with midazolam, is safe, and is associ-
Endoscopic retrograde cholangiopancreatography (ERCP) (see ated with a faster postprocedure recovery (Fanti et al, 2004;
Chapter 29) was first described in 1968 (McCune et al, 1968) Wehrman et al, 1999). In some centers, general anesthesia may
and rapidly became accepted as an important diagnostic modal- be used if the endoscopic procedure is expected to be difficult,
ity for patients with hepatobiliary and pancreatic diseases the patient has significant comorbid medical conditions, or if
(Cotton, 1977; Cotton et al, 1972; Freeney, 1988; Oi et al, there are any signs of functional or mechanical intestinal
1970). Over the last 4 decades, multiple advances in technology obstruction. Oxygen is administered by nasal cannula to avoid
and training have enhanced and expanded the scope of ERCP. hypoxemia, which has been described in 40% of patients under-
The improvement of the side-viewing duodenoscope with an going ERCP (Woods et al, 1989). The patient’s electrocardio-
elevator helped facilitate cannulation of the papilla of Vater gram, blood pressure, oxygen saturation, and overall condition
(Kasugai et al, 1971; Ogoshi et al, 1970; Takagi et al, 1970). are continually monitored throughout the procedure by a dedi-
In addition, the development of therapeutic applications cated nurse. Antibiotics are not given routinely for diagnostic
through ERCP, including sphincterotomy (Classen et al, 1975; procedures. All endoscopic equipment used for this procedure,
Cotton et al, 1976; Kawai et al 1974) and stenting (Laurence including the endoscopes, is either chemically disinfected or gas
et al, 1980; Soehendra et al, 1980), has evolved ERCP from a sterilized.
diagnostic into a therapeutic procedure. ERCP is considered to The patient is placed in a semiprone position with special
be an advanced procedure, requiring skills more difficult to positioning of the arms, to help optimize access to the ampulla
learn than routine endoscopic procedures, and is offered as an of Vater. A side-viewing duodenoscope is used to afford excel-
additional year of training beyond the standard gastroenterol- lent visualization of the ampulla of Vater. In patients with a
ogy fellowship. Billroth II type gastrojejunostomy, a standard forward-viewing
upper endoscope or pediatric colonoscope may be needed to
Indications successfully approach the ampulla. An initial endoscopic evalu-
With the exception of a few scenarios, diagnostic ERCP has ation of the stomach and duodenum is performed before can-
largely been replaced by noninvasive imaging techniques. In nulation of the ampulla. The ampulla is usually located in the
2002, the National Institutes of Health sponsored a consensus second portion of the duodenum but, in rare instances, may be
conference on ERCP and issued a statement proposing the found more proximal or distal. It is usually easily identified,
indications for ERCP (Cohen et al, 2002). They concluded although, in some cases, it may be distorted due to malignancy
382 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 20.5. Pancreatic duct stent placement. A, Wire placement into the pancreatic duct. B, Contrast injection to confirm position in pancreatic
duct. C, Placement of a 5-Fr × 5-cm pancreatic duct stent with a full external pigtail and a single internal flap. D, Endoscopic view of 5-Fr pancreatic
duct stent.
or edema from pancreatitis, hidden behind a fold, or within a motility can be controlled by bolus injections of 0.25 to 1 mg
diverticulum. The orifice of the CBD is usually located on the of intravenous glucagon. If the pancreatic duct is inadvertently
left upper corner of the ampulla. In most patients, the CBD cannulated, placement of a pancreatic duct stent may help can-
and main pancreatic duct share a common channel. In a minor- nulation by both blocking the pancreatic duct orifice as well as
ity of patients, the orifices are separate. The minor papilla is by providing more information to the endoscopist about the
located about 1 to 2 cm above the major papilla. The CBD is angle of the bile duct, especially in cases of distorted anatomy
selectively cannulated with either a cannula or sphincterotome. (Fig. 20.5) (Goldberg et al, 2005). Another technique involves
Studies have shown that access to the biliary tree is easier and placing a guidewire into the pancreatic duct, which adds more
faster with a sphincterotome compared with a cannula (Kara- information about the optimal angle to approach cannulation
manolis et al, 2005; Laasch et al, 2003; Rossos et al, 1993). (Fig. 20.6). The studies are limited, but this technique
More recently, some endoscopists have been using guidewire- does not appear to increase the risk of post-ERCP pancreatitis
assisted cannulation. It remains controversial whether insertion (Draganov et al, 2005; Saad, 2004). Other more invasive
of a guidewire, as opposed to the more conventional technique maneuvers, including precut sphincterotomy with or without
of contrast injection, should be the preferred technique to pancreatic duct stent placement, may also improve success rate
access the bile ducts. A guidewire does not produce the hydro- but is associated with an increased risk of complications, includ-
static pressure associated with contrast injection and decreases ing bleeding, perforation, and pancreatitis, even in experienced
the risk of trauma to the pancreatic duct, thereby theoretically hands (Harewood et al, 2002).
decreasing the risk of post-ERCP pancreatitis. The data, Duodenal diverticula are common and almost always are
however, are mixed. A recent meta-analysis looking at 12 ran- located near the papilla in the descending duodenum. Although
domized trials with 3450 patients concluded that wire-guided usually asymptomatic, diverticula have been shown to be asso-
technique had a higher cannulation success rate (84% vs. 77%) ciated with choledocholithiasis. Periampullary diverticula
and a lower risk of post-ERCP pancreatitis (3.5% vs. 6.7%) may make cannulation more difficult, but the data are mixed
(Tse et al, 2013). However, a prospective trial with 1249 (Rajnakova et al, 2003; Tham & Kelly, 2004).
patients showed no significant difference in post-ERCP pancre- In patients with surgically altered anatomy, ERCP may be
atitis in the guidewire group (5.2%) compared with the contrast quite challenging. In patients with a Billroth II gastrojejunos-
injection group (4.4%) (Mariani et al, 2012). tomy, success rates for bile duct cannulation are much lower
In the event of a difficult cannulation, there are techniques (Forbes et al, 1984). The papilla is found in the afferent limb,
to help facilitate access to the bile duct. Excess duodenal which may be difficult to traverse. In addition, the orientation
Chapter 20 Direct cholangiography: approaches, techniques, and current role 383
A B C
FIGURE 20.6. Guidewire placement in pancreatic duct to facilitate bile duct cannulation. A, Wire placement into pancreatic duct. B, This provided
more information to the endoscopist about the angle of the bile duct, and the cannulatome was adjusted under fluoroscopic guidance. C, Contrast
injection confirmed position in common bile duct.
Pancreatography
Imaging the pancreatic duct can be an important adjunct to
cholangiography during ERCP. Strictures, stones, and other FIGURE 20.7. Pancreas divisum. The cannula is in the major papillary
obstructing lesions can be identified. Most recommend guide- orifice, and contrast injection opacifies the proximal portion of the major
wire cannulation of the pancreatic duct over contrast injection pancreatic duct (Wirsung). Injection through the minor papillae allows
as this produces less hydrostatic pressure in the duct, possibly opacification of the duct of Santorini and the distal duct of Wirsung.
decreasing the risk of post-ERCP pancreatitis. In general, the
pancreatic duct is about 20 cm in length and variable in caliber.
With increasing age comes progressive atrophy and fibrosis of
the pancreas. The diameter of the main pancreatic duct also Cholangioscopy and Pancreatoscopy
increases with age, although one study found no difference in Cholangioscopy and pancreatoscopy involve using miniature
pancreatic duct length among patients younger than 40 years endoscopes through the channel of the duodenoscope, allowing
compared with older patients. Duct diameter throughout the direct visualization of the bile and pancreatic ducts, respec-
pancreas was significantly greater, however, in patients older tively. A new skill set is necessary to perform these procedures,
than 40 years (Anand et al, 1989). given that this technique uses two different endoscopes. Diag-
Anatomic variations, such as pancreas divisum (Fig. 20.7), nostic cholangioscopy may be used to evaluate indeterminate
also may be identified on a pancreatogram (see Chapter 2). This biliary strictures and filling defects. Similarly, diagnostic pan-
abnormality has been described in 7.5% of ERCP procedures creatoscopy may be used to evaluate pancreatic strictures and
and can be confirmed by cannulation of the main pancreatic intraductal papillary mucinous neoplasms. Studies have shown
duct through the orifice in the minor papilla (Bernard et al, that it is an accurate diagnostic tool for patients with pancreati-
1990). cobiliary disorders (Fukuda et al, 2005; Itoi et al, 2010; Yamao
384 PART 2 DIAGNOSTIC TECHNIQUES
et al, 2003). One prospective multicenter study of 87 patients et al, 1985), and a meta-analysis showed no significant differ-
reported that endoscopists were able to distinguish benign from ence in post-ERCP pancreatitis among different contrast media
malignant indeterminate biliary lesions 92.1% of the time with (George et al, 2004).
cholangioscopy with visualization alone (Osanai et al, 2013). Although it remains unclear whether these mechanisms
Complications of cholangiopancreatoscopy include bacteremia, work independently or in conjunction, recent data have helped
bleeding, and pancreatitis. One retrospective study reported to elucidate both patient- and procedure-related risk factors
that complications of cholangiopancreatoscopy are increased that are independently associated with post-ERCP pancreatitis.
compared with ERCP alone and are associated with a much These risk factors are additive (Freeman et al, 2001). Patient-
higher risk of cholangitis (Sethi et al, 2011). related factors include younger age, female sex, normal serum
bilirubin, recurrent pancreatitis, history of post-ERCP pancre-
Complications atitis, and sphincter of Oddi dysfunction. Procedure-related
Complications of ERCP include those associated with endo- factors include difficult cannulation, pancreatic duct injection,
scopic procedures in general as well as those specific to ERCP. precut sphincterotomy, pancreatic sphincterotomy, minor
Incidence rates of complications vary in the literature. A sys- papilla sphincterotomy, balloon sphincteroplasty, ampullec-
tematic survey of prospective studies reviewed 21 studies with tomy, and sphincter of Oddi manometry. One study showed
16,855 patients and reported a specific complication rate of that trainee participation was an independent risk factor (Cheng
6.9% and a mortality rate of 0.33% (Andriulli et al, 2007). The et al, 2006). Most studies, however, have not shown a correla-
experience of the endoscopist and case volume also has an tion between case volume and rates of pancreatitis (Freeman
impact on the complication rate. In a study conducted in et al, 2001; Loperfido et al, 1998; Testoni et al, 2010).
Austria, endoscopists performing more that 50 ERCP proce- Specific techniques and measures to decrease the risk of
dures per year were compared with those performing fewer than pancreatitis have been studied. The risk is reduced by minimiz-
50 per year. Those in the higher case-volume group had a ing the number of attempts of cannulation, avoiding pancreatic
significantly higher success rate (86.9% vs. 80.3%; P < .001) duct cannulation if not necessary, and by avoiding overdisten-
and a lower overall complication rate (10.2% vs. 13.6%; P = sion or “acinarization” of the pancreatic duct by minimizing
.007) (Kapral et al, 2008). the volume of contrast medium into the pancreatic duct.
Placement of a temporary pancreatic duct stent may also
Pancreatitis reduce the risk. One meta-analysis demonstrated that the use
The most common complication of ERCP is pancreatitis, with of pancreatic duct stents in high-risk patients decreased the rate
reported incidences ranging from 1% to 40%, but most fre- of post-ERCP pancreatitis by about two thirds (Singh et al,
quently reported around 3% to 5% (Andriulli et al, 2007; 2004). Their use is not routinely recommended but is reserved
Cheng et al, 2006; Christensen et al, 2004; Freeman et al for high-risk patients. Studies have shown a benefit of pancre-
2001; Loperfido et al, 1998) (see Chapter 54). The incidence atic duct stents in biliary sphincterotomy for sphincter of Oddi
of post-ERCP pancreatitis in children is quite low, about 2.5% dysfunction, precut sphincterotomy, balloon sphincteroplasty,
in one study (Iqbal et al, 2008). The consensus classification endoscopic ampullectomy, and difficult cannulation (Fazel
defined post-ERCP pancreatitis as the clinical picture of new et al, 2003; Freeman et al, 2004; Singh et al, 2004).
or worsened abdominal pain with amylase at least three times Many pharmacologic agents have been studied. A recent
normal at 24 hours after the procedure and requiring hospital- systematic review included 85 randomized clinical trials and 28
ization (Cotton et al, 1991). They further defined it as mild if meta-analyses evaluating pharmacologic prevention of post-
hospitalization is 2 to 3 days, moderate if hospitalization is 4 ERCP pancreatitis. They concluded that rectal nonsteroidal
to 10 days, and severe if hospitalization is more than 10 days, antiinflammatory drugs (NSAIDs) were beneficial, especially in
if there is a pseudocyst or hemorrhagic pancreatitis, or if an high-risk patients. Data on bolus-administered somatostatin,
intervention is required. Post-ERCP pancreatitis should be dis- sublingual nitroglycerin, and some protease inhibitors were
tinguished from transient asymptomatic hyperamylasemia, considered promising, but confirmatory studies are necessary
which occurs in 40% to 75% of cases and disappears within 1 (Kubiliun et al, 2015).
to 2 days (Classen & Demling, 1975; Okuno et al, 1985). Most NSAIDs inhibit prostaglandin synthesis, phospholipase A2
cases of post-ERCP pancreatitis are mild and usually resolve in activity, and neutrophil/endothelial cell attachment, which are
a few days with conservative measures of bowel rest and intra- all thought to play a major role in the pathogenesis of pancre-
venous fluids. The management is the same as for pancreatitis atitis, and thus may have a role in post-ERCP pancreatitis
from other causes. prevention. A meta-analysis that included 10 randomized con-
There have been multiple potential mechanisms proposed trolled trials with a total of 2269 patients concluded that
to explain the pathogenesis of post-ERCP pancreatitis. Mechan- NSAID use decreased the risk of post-ERCP pancreatitis (risk
ical injury to the pancreatic duct from manipulation of the ratio, 0.57; 95% confidence interval [CI], 0.38 to 0.86; P =
papilla, instrumentation of the pancreatic duct, or injection of .007) (Ding et al, 2012). However, these studies were extremely
the pancreatic duct likely plays a role (Johnson et al, 1997). heterogeneous in regard to type of NSAID as well as to route
Similarly, thermal injury from electrocautery leading to edema and timing of administration. A randomized, placebo-
and possible obstruction of the duct has been invoked (Ratani controlled, double-blind clinical trial of high-risk patients
et al, 1999). Hydrostatic pressure from contrast injection showed that patients who received rectal indomethacin imme-
leading to injury is also likely a component. The contrast itself diately after the procedure were less likely to develop post-
theoretically may cause a chemical or allergic injury. However, ERCP pancreatitis than the control group (9.2% vs. 16.9%;
the use of nonionic contrast medium of low osmolarity has P = .0005) and were less likely to develop moderate to severe
shown no advantage over the less expensive ionic contrast pancreatitis (4.4% vs. 8.8%; P = .03) (Elmunzer et al, 2012).
medium in preventing ERCP-related pancreatitis (Hannigan A meta-analysis that specifically looked at studies of rectal
Chapter 20 Direct cholangiography: approaches, techniques, and current role 385
indomethacin included four studies with 1470 patients showed (25%; P = .012) (Hao et al, 2009). In both studies, however,
that the rate of pancreatitis was significantly lower using indo- the consensus definition for pancreatitis was not used, which
methacin compared with placebo (odds ratio, 0.49; CI, 0.34 to may account for the high rates of pancreatitis in the control
.71; P = .0002) (Yaghoobi et al, 2013). A network meta-analysis groups. One recent randomized controlled trial of 300 patients
compared rectal indomethacin to pancreatic duct stenting and showed that the combination of rectal indomethacin and sub-
concluded that rectal indomethacin alone was superior to pan- lingual nitroglycerin was superior to rectal indomethacin alone
creatic duct stenting in post-ERCP prevention (odds ratio, at prevention of post-ERCP pancreatitis (6.7% vs. 15.3%; P =
0.48; 95% CI, 0.26 to 0.87) (Akbar et al, 2013). The European .016) (Sotoudehmanesh et al, 2014). More studies are needed
Society of Gastrointestinal Endoscopy guidelines recommend to further clarify the benefit of nitroglycerin in post-ERCP
routine prophylactic use of rectal NSAIDs immediately before pancreatitis.
or after ERCP in all patients without a contraindication Protease inhibitors, such as gabexate mesylate, nafamostat
(Dumonceau et al, 2014). mesylate, and ulinastatin, have been investigated, given that
Somatostatin and its analogue octreotide inhibit pancreatic activation of proteolytic enzymes likely contributes to the
secretions, decrease sphincter of Oddi pressure, modulate pathogenesis of pancreatitis. A meta-analysis of 18 studies with
cytokines, and lead to apoptosis of pancreatic acinar cells, and a total of 4966 patients showed a significant, yet small, risk
therefore may be protective against post-ERCP pancreatitis. reduction in post-ERCP pancreatitis with the protease inhibi-
They have been studied extensively with conflicting results. tors (Seta & Noguchi, 2011). They stated there was no solid
One meta-analysis included seven homogeneous high-quality evidence to support their use at this time. A recent pilot study
studies involving 3130 patients and concluded that somatosta- investigated whether aggressive periprocedural hydration
tin administered as a bolus was effective in prevention of post- reduced the risk of post-ERCP pancreatitis and found that
ERCP pancreatitis (Rudin et al, 2007). A more recent none of the patients in the aggressive hydration group devel-
meta-analysis looked at 17 studies with a total of 3818 patients oped pancreatitis compared with 17% of patients in the stan-
and found that somatostatin and high-dose octreotide pre- dard hydration group (Buxbaum et al, 2014). Larger studies
vented post-ERCP pancreatitis if given over 12 hours or in are needed to corroborate these findings. Many other agents
bolus form (Omata et al, 2010). Subsequent randomized trials have been investigated, including secretin, corticosteroids, allo-
have yielded mixed results. One double-blinded, placebo- purinol, and topical epinephrine, with conflicting results, and
controlled, randomized study involved 391 patients in three are not recommended at this time.
hospitals. Patients were randomized to receive 3 mg of soma-
tostatin in 500 mL normal saline infused for 12 hours, starting Infection
30 minutes before the ERCP or 500 mL normal saline infused A serious complication of ERCP is the development of post-
for 12 hours, starting 30 minutes before the ERCP. They procedure infectious complications, most commonly cholangi-
found a significantly lower risk of pancreatitis in the soma- tis and cholecystitis. In a systematic survey of 21 prospective
tostatin group (3.6% vs. 9.6% in the placebo group; P = .02) studies with 16,855 patients, the incidence of infectious com-
(Lee et al, 2008). Another study involved 133 patients who plications was 1.4% (Andriulli et al, 2007).
were randomized to a bolus of somatostatin infusion before Cholangitis most commonly occurs when there is failed or
ERCP, followed by continuous infusion for 12 hours, a bolus incomplete biliary drainage. The risk is increased in patients
of somatostatin before ERCP only, and placebo alone; no sig- with hilar obstruction and sclerosing cholangitis, given the
nificant differences were found among the three groups (Chan increased risk of incomplete drainage (Bangarulingam et al,
et al, 2008). A recent randomized trial of 510 patients ran- 2009; Rerknimitr et al, 2004). Other risk factors include jaun-
domized to an intravenous bolus of 250 µg of somatostatin dice, small endoscopy center, and delay in performing ERCP
prior to cannulation, followed by a 4-hour continuous infusion (Loperfido et al, 1998; Navaneethan et al, 2013). Treatment
of the drug at 250 µg/hr, or placebo with normal saline showed involves supportive care with antibiotics and decompression of
no significant difference in rates of post-ERCP pancreatitis the obstruction. Studies have shown that prophylactic antibiot-
(Concepcion et al, 2014). In addition, when pancreatitis has ics significantly reduce the frequency of procedure-related bac-
developed, the use of somatostatin does not improve its clini- teremia but have not shown a difference in rates of cholangitis
cal course (Phillip et al, 1985). Future research is necessary to (Sauter et al, 1990). Two meta-analyses failed to demonstrate
elucidate the role of somatostatin in prevention of post-ERCP a benefit of giving routine prophylactic antibiotics (Bai et al,
pancreatitis. 2009; Harris et al, 1999). Antibiotics added to the injected
Nitroglycerin acts as a smooth muscle relaxant and subse- radiographic contrast medium are also of no benefit (Jendrze-
quently may decrease sphincter of Oddi pressures, thereby jewski et al, 1980).
decreasing the risk of post-ERCP pancreatitis. Only three out It has also been found that endoscopic instruments used in
of seven randomized controlled studies showed that nitroglyc- ERCP can be the source of serious infections (Earnshaw et al,
erin was effective, but two of the three positive studies used 1985). Salmonella species are the most common organisms
sublingual nitroglycerin (Kubiliun et al, 2015). One compared transmitted by contaminated endoscopes (Axon, 1991), and for
2 mg sublingual nitroglycerin given 5 minutes prior to endos- this reason, it is imperative to ensure that the endoscopic equip-
copy with placebo in 186 patients and found a lower incidence ment used for ERCP is adequately disinfected or sterilized.
of pancreatitis in the nitroglycerin group (7/90 vs. 17/96; P <
.05) (Sudhindran et al, 2001). The second one enrolled 74 Bleeding
patients and randomly assigned them to 5 mg sublingual glyc- Bleeding is a rare complication of diagnostic ERCP and is
eryl trinitrate versus 100 mg vitamin C, 5 minutes prior to the most commonly seen with sphincterotomy. Risk factors for
ERCP. They found a significant difference in post-ERCP pan- postsphincterotomy bleeding include bleeding during the
creatitis in the study group (7.9%) compared with placebo procedure, concomitant thrombocytopenia or coagulopathy,
386 PART 2 DIAGNOSTIC TECHNIQUES
anticoagulation started within 3 days of the sphincterotomy, confluence (Figs. 20.10 and 20.11B). A right sectoral duct
and low case volume of the endoscopist (Freeman et al, 1996). crosses to the left to join the left hepatic duct in 28% of cases,
Rarely, there may be a Mallory-Weiss tear from scope trauma according to Healey and Schroy (1953); in 22%, this is the
or submucosal hemorrhage from manipulation of the papilla posterior sectoral duct (see Figs. 20.9B and 20.11B), and in
(Loperfido et al, 1998). There have been case reports of intra- 6%, this is the anterior duct (see Figs. 20.9C and 20.11D).
peritoneal hemorrhage from injury to abdominal vessels, liver, Occasionally, a right sectoral or segmental duct, posterior more
and spleen (Lo et al, 1994; Wu & Katon, 1993). often than anterior, courses inferiorly and enters the common
hepatic duct directly (Fig. 20.12). The confluence of the right
Perforation and left ducts takes the form of a trifurcation rather than a
The most common type of perforation associated with ERCP bifurcation in 12% of cases according to Couinaud (1957; see
is retroperitoneal perforation and is usually associated with Fig. 20.9A).
sphincterotomy, with an incidence ranging from 0.5% to 2.1% In the left lobe, the superior and inferior lateral segment
(Cotton et al, 1991). In their systematic survey of 21 prospec- ducts, segments II and III, unite in the line of, or to the right
tive studies with 16,855 patients, Loperfido and colleagues
(1998) reported 101 perforations (0.6%) and 10 deaths from
perforation (0.06%). Free bowel wall perforation is quite rare
and is usually associated with a structural abnormality such as TABLE 20.1 Segmental Nomenclature
a stricture or Billroth II gastrectomy (Wilkinson et al, 1994). I Caudate lobe
The management of the perforation depends on the size, II Left lateral superior segment
location, and clinical picture. Free bowel wall perforations III Left lateral inferior segment
usually require surgery. Use of endoscopic clips for the treat- IV Left medial segment or quadrate lobe
ment of duodenal perforations has also been reported V Right anterior inferior segment
(Katsinelos et al, 2005; Solomon et al, 2012). VI Right posterior inferior segment
VII Right posterior superior segment
DIRECT CHOLANGIOGRAPHY AND VIII Right anterior superior segment
PANCREATOGRAPHY BY PERCUTANEOUS
TRANSHEPATIC CHOLANGIOGRAPHY OR
ENDOSCOPIC RETROGRADE RPSD
CHOLANGIOPANCREATOGRAPHY RHD
LHD
The anatomy of the bile ducts is discussed in Chapter 2. LHD
Knowledge of the common variations of ductal branching is
essential for accurate interpretations of cholangiograms, and CHD
these are shown in Figures 20.8 and 20.9; segmental nomen-
RASD Sectoral
clature is summarized in Table 20.1. In the right lobe, the
duct
posterior segments lie more laterally than the anterior seg- A D
ments, so that the most lateral ducts on a cholangiogram are
usually segments VI inferiorly and VII superiorly. The posterior RPSD
sectoral duct is often recognizable by an arched course near the
RHD
II
RPSD LHD
III
VII VIII
II RASD
IV
I B E
VI
V IV III RHD
RPSD
II
RASD LHD
IV III
RHD
LHD
CHD
RASD
FIGURE 20.8. Standard intrahepatic ductal anatomy. The seg-
ments are numbered according to Couinaud’s description (see Table C F
20.1). CHD, Common hepatic duct; LHD, left hepatic duct; RASD, right FIGURE 20.9. Variations of perihilar ductal anatomy. CHD, Com-
anterior sectoral duct; RHD, right hepatic duct; RPSD, right posterior mon hepatic duct; LHD, left hepatic duct; RASD, right anterior sectoral
sectoral duct. duct; RHD, right hepatic duct; RPSD, right posterior sectoral duct.
Chapter 20 Direct cholangiography: approaches, techniques, and current role 387
Interpretations
FIGURE 20.10. Hilar cholangiocarcinoma involving first-order right Because of its inherent weakness of only allowing visualization
hepatic duct, proximal common hepatic duct, and faintly opacified left of the bile duct lumen, the main problem with the use of direct
hepatic duct (arrowhead). Note the characteristic arched course of the cholangiography is its lack of specificity. There are few, if any,
right posterior sectoral duct (arrow). pathognomonic radiologic findings. Many disease entities, from
benign to malignant, overlap greatly in their cholangiographic
appearances. The combination of history, blood markers, asso-
ciated radiologic findings, and clinical scenario can often sig-
TABLE 20.2 Average Duct Diameters Measured Directly from
nificantly narrow the differential diagnosis. However, it must
50 Normal Percutaneous Transhepatic Cholangiography be stressed strongly that because the cholangiographic appear-
Examinations ance of many biliary diseases may be indistinguishable, biopsy
Duct Diameter (mm) is often required to rule out malignancy or to confirm suspected
Right hepatic = 4.7 diagnosis.
Left hepatic = 5.2
Bile Leaks
Common hepatic = 6.5
Bile leaks are seen as sites of free extravasation of contrast
Common bile = 7.6
agent at a site of bile duct injury. Injury may be secondary to
From Okuda K, et al: Frequency of intrahepatic arteriovenous fistula as a sequela to percutaneous trauma, but most commonly it is iatrogenic in nature. Associ-
needle puncture of the liver, Gastroenterology 74:1204–1207, 1978.
ated bilomas may be seen at the point of bile leak. Diagnosis
of bile leak can usually be made by noninvasive imaging
techniques such as ultrasound, CT or MRI, but because the
of, the umbilical fissure in 92% of cases. In the latter instance, intrahepatic bile ducts are usually not dilated, a bile leak may
the quadrate lobe, segment IV, may drain wholly or partially not be evident on imaging. Cholescintography with techne-
into the segment II duct. Rarely, segment II and III ducts join tium 99m–hepatic iminodiacetic acid (HIDA scan) may be
at or close to the confluence (see Figs. 20.9E and 20.11C), and useful for diagnosis when the other imaging modalities are
segment IV drains directly into the common hepatic duct in inconclusive. ERCP can diagnose bile duct leaks effectively
1% of cases (see Fig. 20.9F) (Healey & Schroy, 1953). but is usually reserved for cases when a therapeutic interven-
The caudate ducts are often difficult to identify. Usually two tion is anticipated.
or three ducts drain most commonly into the right posterior
sectoral duct, right hepatic duct, or left hepatic duct (Healey Filling Defects
& Schroy, 1953). The recognizable caudate ducts are usually a Air Bubbles, Blood Clots, Calculi, Primary and Secondary Bile
few centimeters long and drain downward or to the right. Duct Cancers, and Parasitic Diseases
The left hepatic duct (average length, 17 mm) is consider- Air bubbles, although confusing, most commonly declare
ably longer than the right hepatic duct (average length, 9 mm) themselves by their perfectly circular shape and their distribu-
and has a longer extrahepatic course. The normal diameters of tion to nondependent structures. Blood clots in the bile duct
the main bile ducts as measured at PTC are shown in Table are seen more frequently with PTC than with ERCP. Hemobi-
20.2. These figures are greater than the true duct dimensions lia can sometimes take more than 48 hours to resolve, and when
because of some distension produced by direct cholangiogra- it is more severe, it can be castlike and may mask other filling
phy, together with considerable magnification occurring on any defects (see Chapter 125).
fluoroscopic “spot film.” The magnification is of the order of Calculous disease (see Chapters 36 and 39) remains the
40% (Nichols & Burhenne, 1984) and affects all structures in most common filling defect in the biliary system. Distinguishing
the image, including calculi, tubes, and strictures. characteristics of gallstones and primary bile duct calculi
388 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 20.11. Postcholecystectomy strictures graded according to Bismuth. A, Grade I (>2 cm from the confluence of the right and left hepatic
ducts; arrowheads): Calculi lie above and below the stricture (arrow). B, Grade II (<2 cm from the confluence): There has been a previous hepato-
jejunostomy; the right posterior sectoral duct (arrowhead) has an exaggerated arched course and enters the left hepatic duct as a normal variant.
C, Grade III (the confluence is involved by stricture, but the right and left hepatic ducts are not completely separated): Ducts of segment II (white
arrow) and segment III (black arrow) join the confluence independently as a normal variant. D, Grade IV (the right and left ducts are separated by
the stricture): The right anterior sectoral duct (A) is draining into the left hepatic duct (L), which is separated from the right posterior sectoral duct (P)
by the stricture (arrows).
include a faceted appearance and disposition to move to gravity- more unusual causes of cholangiographic filling defects (Riopel,
dependent positions. Calculi may be seen as discrete filling 1997).
defects (Figs. 20.15 and 20.16) or castlike structures filling Parasitic infections, such as hydatid disease (see Chapter 74)
entire ducts, as occurs in recurrent pyogenic cholangitis, cystic and infections with Ascaris lumbricoides or Clonorchis sinensis (see
diseases of the bile ducts, or even proximal to strictures of any Chapter 45), are diseases with worldwide distribution that can
etiology. Impacted calculi may be difficult to differentiate from also present cholangiographically as intraductal filling defects.
strictures or tumors. A proportion of hepatic hydatid cysts (5% to 10%) rupture into
Primary bile duct cancer (see Chapter 51), specifically papil- the bile ducts and may simulate choledocholithiasis. Calcified
lary cholangiocarcinomas, can also present as cholangiographic cysts are easy to recognize on radiographs, and daughter cysts
filling defects (Fig. 20.17). T-shaped filling defects may also be can cause biliary obstruction. When the calcified cyst is not
detected (Fig. 20.18 ) (Torok & Gores, 2001), and papillary obvious, biliary strictures with obstruction may be noted on
bile duct cancers may cause filling defects as a result of mucin cholangiogram. The biliary ducts can show considerable irregu-
production (Fig. 20.19). Other malignancies, including mela- larities in caliber and extensive displacement of the intrahepatic
noma and intraductal metastases, such as colon cancer, are also branches secondary to the mass effect of a large hydatid cyst
Chapter 20 Direct cholangiography: approaches, techniques, and current role 389
FIGURE 20.16. Benign stricture of the right hepatic duct (arrow) with
multiple ductal calculi proximal to it. The hepatojejunostomy is partially
strictured.
FIGURE 20.18. “Golf tee” appearance of a papillary bile duct cancer FIGURE 20.19. Nasobiliary cholangiogram opacifying left hepatic
(arrow) involving the common hepatic duct. ducts. Main left hepatic duct contains a small mucin-secreting papillary
cholangiocarcinoma (arrow). The mucin results in expansion of the
common bile duct below the tumor and appears as strandlike filling
defects. (Courtesy Dr. A. Speer.)
Chapter 20 Direct cholangiography: approaches, techniques, and current role 391
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preliminary report, Ann Surg 167:752–756, 1968. Seldinger SI: Percutaneous transhepatic cholangiography, Acta Radiol
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2010. 1001, 2013.
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Endoscopy 45(8):605–618, 2013.
CHAPTER 21
Diagnostic angiography in hepatobiliary and
pancreatic disease: indications
Hooman Yarmohammadi
392
Chapter 21 Diagnostic angiography in hepatobiliary and pancreatic disease: indications 393
hepatic” artery in older works. Separate origins of segment IVA, confluence, but it may also enter the SMV either at or just
usually from the LHA, and segment IVB from the RHA are caudal to the confluence. The coronary vein most often drains
frequently identified. Also, a branch from the segment IV artery into the cephalic aspect of the main portal vein just beyond the
is often seen extending outside of the liver, supplying the confluence of the SMV and splenic vein. The number and
falciform ligament. Recognition of this vessel is important when location of veins draining the pancreas is variable. Multiple
embolization, chemoembolization, or radioembolization are small, unnamed veins drain directly into the splenic vein. Typi-
conducted to avoid nontarget embolization. cally, the anterior-superior pancreaticoduodenal vein drains
The RHA conventionally divides into an anterior (ventral) directly into the portal vein, and the posterior-superior pancre-
and a posterior (dorsal) branch. The anterior branch usually is aticoduodenal vein drains into the SMV. The inferior pancre-
more vertically oriented and supplies segments V and VIII. The aticoduodenal veins drain into the SMV at the caudal margin
posterior branch is usually more horizontally oriented and of the pancreas, and the portal vein courses obliquely cephalad
supplies segments VI and VII. More than one projection is from near the midline toward the liver, where it divides to
usually required to ascertain with certainty which is the anterior supply the right and left lobes. This division, as well as the
branch and which the posterior branch. In the right anterior division into segmental branches, is variable and must be
oblique projection, the anterior branch moves medially and the delineated when clinically relevant for each individual patient.
posterior branch moves laterally when compared with the
posteroanterior projection. The entire segmental arterial supply ANGIOGRAPHY INDICATIONS
to the liver should be accounted for before hepatic arterial
therapy (see Chapters 96 and 99), major hepatic resection, As mentioned earlier in this chapter, historic indications
partial hepatectomy (see Chapter 103), or living-donor liver for performing diagnostic catheter angiography have been
transplantation (see Chapters 104 and 117). replaced by multidetector computed tomography angiography
The arterial supply to the pancreas is somewhat variable. (MDCTA), including visceral angiography to assess the resect-
The most consistent supply is to the pancreatic head, through ability of pancreatic and biliary tract tumors by demonstrating
an arcade formed by the inferior pancreaticoduodenal branch presence or absence of vascular invasion; angiography for
of the SMA to the anterior- and posterior-superior pancreati- diagnosis of a hepatic mass, such as differentiating a cavernous
coduodenal branches of the GDA (Fig. 21.3). The transverse hemangioma from a hepatocellular carcinoma; and preopera-
pancreatic artery runs along the middle portion of the long axis tive arterial mapping of the arterial anatomy of the liver prior
of the pancreas and may take origin from the arterial arcade in to major hepatic resection. MDCTA provides higher sensitivity
the head of the pancreas, directly from the GDA, or as a branch and diagnostic accuracy for these indications. On rare occa-
of the dorsal pancreatic artery, which variably originates from sions, there is a specific piece of critical anatomic information
the CHA or the splenic artery (Fig. 21.4). A number of small that cannot be ascertained with certainty by MDCTA, such as
branches from the splenic artery supply the pancreatic body the origin and course of the artery to segment IV prior to a
and tail, but the number and location of these arteries vary and living-donor partial hepatectomy. In this circumstance, catheter
must be identified in each individual patient when clinically angiography can be useful to answer the question.
relevant. On extremely rare occasions, large tumors are identified on
cross-sectional imaging, but the organ of origin cannot be
Venous Anatomy determined. The majority of these are large sarcomas of the
The splenic vein and superior mesenteric vein (SMV) join retroperitoneum, but excluding a pancreatic source may be
to form the main portal vein (see Chapter 2). The inferior difficult. A similar situation can occur with large right adrenal
mesenteric vein usually enters the splenic adjacent to the or renal tumors blending with the hepatic parenchyma. In these
GDA
RGA
PSPD
DP
ASPD
TP
A B
FIGURE 21.5 Extrahepatic perfusion detected with C-arm computed tomography (CCT). A, Selective cystic arteriogram shows the gallbladder and
several branches extending medially (arrow). B, CCT performed during contrast injection of the cystic artery confirms aberrant perfusion of the
duodenum (arrowheads). (Courtesy Daniel Sze, Stanford University.)
396 PART 2 DIAGNOSTIC TECHNIQUES
Two techniques are used to perform splenic embolization: Obviously, the contribution of the embolization to these com-
the first is occlusion of the proximal splenic artery with coils or plications may be difficult to distinguish from sequelae of the
Amplatzer plugs (AGA Medical, Plymouth, MN), and the underlying traumatic injury.
second is selective small intrasplenic arterial embolization with Iatrogenic injury to the hepatic artery is suspected when a
a gelatin sponge or coils. Collaterals through the short gastric biliary drainage tube puts out blood following placement, or
arteries and the gastroepiploic arcade usually maintain splenic melena secondary to hemobilia develops in the patient follow-
viability following occlusion of the proximal splenic artery. ing an intervention through the hepatic parenchyma. CT in
Intrasplenic embolization generally results in a variable degree these patients may or may not reveal an abnormality, and
of splenic infarction, depending upon the size of the artery patients should undergo hepatic arteriography when a clinical
occluded, as intrasplenic arteries have no significant collateral suspicion of a hepatic arterial injury exists. Patients with iatro-
routes. Both techniques have equivalent rates of major infarc- genic injuries usually have a single, discrete bleeding source that
tions and infections requiring splenectomy (Ekeh et al, 2013). can be addressed with superselective embolization techniques.
Distal splenic embolization is associated with higher rates of Complications related to the embolization procedure tend to
infarction; however, these infarctions are limited to the seg- be lower when compared with patients who have had blunt
ments just distal to the site of embolization with questionable trauma, as the traumatic injury to the liver is less extensive.
clinical relevance. In summary, the current literature is incon-
clusive regarding whether the proximal or distal embolization Pancreas Bleeding
should be used. Minor complications including fever, pleural Bleeding is more commonly encountered in patients with
effusion, and partial splenic infarction have been reported in as pancreatitis (see Chapter 56) or pancreatic surgery (see Chap-
many as 34% of patients. Major complications including ters 66 and 67). Posttrauma bleeding from the pancreas is not
splenic abscesses, splenic infarction, splenic atrophy, and post- common. Hemorrhage can occur in the retroperitoneum, or it
procedure bleeding have been observed in 14% of patients may extend from the retroperitoneum into the peritoneal cavity
(Ekeh et al, 2013). or into the gastrointestinal tract via communication with the
pancreatic duct (hemosuccus pancreaticus). Vascular complica-
Hepatic Bleeding tions are seen in 25% of patients suffering from pancreatitis and
Hemorrhage from the liver may be encountered from blunt or are usually arterial in origin. Proteolytic enzymes coupled with
penetrating trauma (see Chapter 122) but is most commonly intense inflammation can erode small arterial branches and
due to an iatrogenic injury related to a biopsy (see Chapter 22) create foci of extravasation or create small pseudoaneurysms.
or percutaneous transhepatic biliary drainage (PTBD) (see Although this complication is encountered in only 2% to 5%
Chapters 30 and 52). Arteriographic findings indicating a of cases, it may be life threatening. Pseudocysts may erode small
source of hemorrhage include extravasation, pseudoaneurysm arterial branches, leading to hemorrhage within the pseudocyst,
formation, and/or arteriovenous fistula (see Chapter 124). or it may erode into larger arterial branches and create a large
Superselective catheterization by using coaxial microcatheters pseudoaneurysm (Fig. 21.6). These pseudoaneurysms are most
to deposit coil-spring emboli both distal and proximal to the frequently identified in the splenic artery or its branches (60%
area of injury is the preferred technique for embolization when to 65%), followed by the GDA (20% to 25%), pancreaticoduo-
a discrete bleeding site can be identified. In contrast to the denal arteries (10% to 15%), hepatic artery (5% to 10%), and
spleen, a rich collateral network exists in the hepatic arterial left gastric artery (2% to 5%) (Aswani et al, 2015; Kirby et al,
bed, making proximal occlusion of the offending artery ineffec- 2008).
tive in many cases. For more diffuse injuries with multiple MDCT has been reported to have 90% sensitivity in detect-
bleeding sites secondary to blunt trauma, using particulate ing pseudoaneurysms in patients with acute pancreatitis;
embolization with a gelatin sponge may be a useful adjunct. however, tiny aneurysms in the intrapancreatic arteries may
As with blunt splenic injuries, nonoperative management not be visible (Hyare et al, 2006). When a patient has clinical
has become the preferred method of management of hemody- evidence of significant hemorrhage, or a CT scan reveals a
namically stable patients. The success rate of this management pseudoaneurysm, arteriography followed by embolization is
exceeds 90% (Christmas et al, 2005). Two main indications for indicated. When the bleeding site is identified angiographically,
hepatic angioembolization are primary hemostatic control in a it can be controlled with embolotherapy in as many as 88% of
hemodynamically stable patient that has radiographic evidence patients (Mansueto et al, 2007).
of active arterial hemorrhage and adjunctive hemostatic control Angiography and embolization are feasible and safe in treat-
following surgical exploration and packing of a hepatic paren- ment of hemorrhagic complications following pancreatic surgery
chymal injury with evidence of continued bleeding or hemody- (Casadei et al, 2014; Yekebas et al, 2007). Yekebas and col-
namic instability. Additionally, patients who are seen with leagues (2007) reported significant hemorrhage in 5.7% of 1669
hemodynamic instability who can be successfully resuscitated consecutive patients following partial or total pancreatectomy.
can be treated effectively with transcatheter embolization (Mis- In a more recent study, Casadei and colleagues (2014) reported
selbeck et al, 2009). The yield of arteriography in identifying significant hemorrhage in 9.8% of 182 patients following pan-
an arterial injury amenable to embolization is higher when the creatic resection for pancreatic and periampullary diseases.
CT scan suggests a vascular injury. Bleeding may manifest clinically as gastrointestinal hemorrhage,
Complications following embolization of a hepatic arterial retroperitoneal or intraperitoneal bleeding, or bleeding through
injury secondary to blunt trauma are relatively frequent percutaneous or surgically placed drains. When a pancreatico-
(Letoublon et al, 2011). In a retrospective study, Letoublon jejunal anastomosis has been created, disruption of the anasto-
and colleagues reported a 70% liver complication rate. These mosis may lead to false localization of the bleeding site.
complications include hepatic ischemia, infarction, hepatic Specifically, an extraluminal bleeding site may drain into the
failure, gallbladder ischemia, bile leak, and abscess formation. bowel through the dehisced anastomosis, or bleeding from the
Chapter 21 Diagnostic angiography in hepatobiliary and pancreatic disease: indications 397
A B
C
FIGURE 21.6 Pseudoaneurysm secondary to pancreatitis treated with coil embolization. A, Contrast-enhanced computed tomography reveals a
pseudoaneurysm in the pancreatic head (arrow). B, Selective gastroduodenal arteriogram reveals the pseudoaneurysm (arrow) taking origin from a
branch of the anterior-superior pancreaticoduodenal artery. C, The pseudoaneurysm is occluded with coils (arrowheads).
bowel at the anastomosis may extend outside the lumen to cause but may be suggested by CT. If the underlying etiology is
an intraperitoneal hematoma or hemorrhage through a drain. compression of the splenic vein, percutaneous transhepatic
Angiography can be extremely useful in the diagnosis and stenting of the splenic vein may be potentially useful.
treatment of these patients. In 25 of 43 patients undergoing
angiography to diagnose and treat postpancreatectomy hemor- Diagnosis of Arterial Occlusive Disease
rhage, a bleeding site was located and embolized with an 80% Many arterial disorders that involve the primary branches of
success rate in controlling the hemorrhage (Yekebas et al, the celiac trunk, as well as the SMA, can be assessed adequately
2007). The relatively low rate of positive angiograms may be with MDCT or MRA. However, delineation of pathology in
explained by the high incidence of venous bleeding encountered smaller branches, such as with vasculitis, or subtle pathologic
in the postpancreatectomy patient. Regional portal hyperten- changes may require the increased morphologic detail afforded
sion develops in many of these patients as a result of splenic or by catheter angiography.
superior mesenteric venous compression or occlusion second- Arterial occlusive disease as a result of atherosclerosis and
ary either to the underlying pathology or a surgical complica- compression of the celiac axis by a median arcuate ligament are
tion. Venous extravasation is rarely identified by arteriography common diseases that do not generally influence the conduct
398 PART 2 DIAGNOSTIC TECHNIQUES
of hepatobiliary or pancreatic surgery. The principle exception Treatment of Visceral Arterial Aneurysms
is in the performance of orthotopic liver transplantation (OLT), Visceral artery aneurysms are rare entities that involve the
when preservation of brisk hepatic arterial flow is essential. In celiac, splenic, superior mesenteric, or inferior mesenteric
that circumstance, the inflow must be corrected either by surgi- arteries and their branches (see Chapter 124). The prevalence
cal or endovascular interventions. Another potential area of of visceral artery aneurysm is 0.1% to 2% (Hemp & Sabri,
concern is pancreaticoduodenectomy, particularly in jaundiced 2015; Tulsyan et al, 2007). True aneurysms involve all three
patients. In this situation, sacrifice of the GDA is required, vessel walls and are usually atherosclerotic or developmental
which interrupts the retrograde arterial flow from the SMA to in origin and differ from those encountered in pancreatic
the liver and could result in hepatic ischemia and necrosis. inflammatory disease, which are typically pseudoaneurysms.
Likewise, fibromuscular dysplasia may rarely involve the SMA, Depending on the size and location of the aneurysm, mortal-
but associated clinical sequelae are extremely uncommon. The ity from rupture ranges from 25% to 100% (Cordova &
SMA may also be compromised in very rare circumstances by Sumpio, 2013).
a median arcuate ligament. The splenic artery is the most common affected artery,
followed by the hepatic artery. Splenic artery aneurysms in
Diagnosis and Treatment of Arterial Stenosis women of childbearing age are of particular concern because
Hepatic arterial anastomotic stenoses are observed in as many of their propensity to rupture during childbirth. Most splenic
as 11% to 12% of patients following OLT (see Chapters 116 aneurysms are saccular and located in the mid to distal segment
and 120) (Duffy et al, 2009; Kim et al, 2012). Although these of the artery (Nosher et al, 2006). The rate of rupture ranges
stenoses are usually detected by surveillance duplex ultrasound from 3% to 20% (Lagana et al, 2006). Endovascular treatment
and confirmed with MDCTA, catheter angiography is often of splenic artery aneurysms depends on the tortuosity and
performed to improve morphologic delineation and assess the location of the aneurysm. Stent placement is used for more
degree of stenosis in preparation for endovascular treatment proximal disease and distal disease in a tortuous vessel is usually
(Vaidya et al, 2007). Stenosis of the hepatic artery anastomosis treated with coil embolization (Hemp & Sabri, 2015).
usually leads to allograft dysfunction, and stenoses of the Traditionally, surgical resection or ligation of the visceral
hepatic artery may also be more diffuse (Fig. 21.7). Severe aneurysms was the gold standard of therapy; however, endovas-
stenosis may lead to hepatic artery thrombosis. The hepatic cular treatments have largely replaced open resection. Large
artery supplies the bile duct, and the bile duct has been ren- studies have reported technical success rates ranging from 89%
dered devoid of collateral arterial supply during donor hepatec- to 98% (Hemp & Sabri, 2015; Sachdev et al, 2006; Tulsyan
tomy. Arterial insufficiency typically leads to biliary strictures et al, 2007). Endovascular treatments are associated with
and to potentially diffuse biliary ductal infarction. Hepatic shorter hospital stay, when compared with surgical repair: 3.8
artery thrombosis may lead to irretrievable allograft damage versus 12 days, respectively.
and may necessitate retransplantation. When a hepatic arterial
stenosis is identified before advanced biliary injury, endovascu- Diagnosis of Vasculitis
lar therapy with either balloon angioplasty and/or stent place- Vasculitis
ment is warranted. Vasculitides that involve the hepatic arterial system may require
the spatial resolution provided by catheter angiography for
definitive diagnosis, because the characteristic microaneurysms
and areas of arterial narrowing may not be apparent by MDCT.
The most common vasculitis with hepatic involvement is
polyarteritis nodosa, which may not lead to symptoms despite
involvement of the visceral arteries, although pancreatitis,
cholecystitis, and hepatic dysfunction may be observed.
Arterial abnormalities in the liver have also been identified
in patients with systemic lupus erythematosus and Wegener
granulomatosis. In most patients, the underlying diagnosis is
apparent, and the angiographic findings do not represent a
diagnostic dilemma.
Hereditary Hemorrhagic Telangiectasia depicting the malformations shunting hepatic arterial blood
Hereditary hemorrhagic telangiectasia (HHT) also known as into the hepatic venous system (Fig. 21.9) (Memeo et al, 2008).
Osler-Weber-Rendu syndrome, is an autosomal dominant vascular Although this disorder has been treated with transcatheter
disease, characterized by telangiectasias of the skin and mucous techniques, embolotherapy has currently fallen out of vogue
membranes. HHT is also associated with arteriovenous malfor- because of the risk of precipitating hepatic failure. OLT is
mations in the pulmonary and hepatic circulation that may be curative if high-output cardiac failure develops in the patient.
life-threatening. Diagnosis is usually based on family history
and clinical criteria. Cross-sectional imaging, including ultra- Peliosis Hepatitis
sound, CT or MRI, plays a fundamental role in detecting vis- Peliosis is an abnormality of the reticuloendothelial system that
ceral involvement in HHT. The hepatic arterial malformations is most commonly encountered in the liver (peliosis hepatis)
that shunt blood into the hepatic venous system may be initially (see Chapter 89). Pathologically, it is characterized by blood-
noted on a cross-sectional imaging study, but the findings may filled cystic spaces that range in size from a few millimeters to
be nonspecific. Catheter angiography can be diagnostic by almost a centimeter. This abnormality has been associated with
human immunodeficiency virus infection as well as with the use
of certain drugs, including immunosuppressives, antimetabo-
lites, and oral contraceptives. Although usually benign, it has
been associated with spontaneous massive hemorrhage and
therefore may be encountered angiographically during the
investigation of hepatic bleeding (Choi et al, 2009). Angio-
graphically (Fig. 21.10), the lesions are easily visible as a dis-
organized collection of amorphous channels not dissimilar to
those observed in HHT or hemangioma; however, the lack of
shunting to the hepatic venous system distinguishes it from
HHT, and the absence of sharp definition with persistence into
the late venous phase distinguishes it from hemangioma.
Localization of Functional Pancreatic Neuroendocrine
Tumors (See Chapter 65)
Calcium stimulation arteriography was developed and described
in 1991 (Doppman et al, 1991). Although unnecessary when
imaging can confidently detect the offending pancreatic lesion,
it is an extremely useful adjunct when the location of the lesion
cannot be defined with confidence (Fig. 21.11). When 1 mL of
10% calcium gluconate is injected into an artery supplying the
FIGURE 21.8 Segmental arterial mediolysis (SAM). Abdominal aorto- pancreas, tumor cells degranulate and release insulin into the
gram reveals a dissection with a small aneurysm in the celiac artery portal venous circulation. Sequential blood samples obtained
(arrow) as well as undulating irregularity of the common hepatic artery from the hepatic vein will demonstrate a significant rise in the
(arrowhead) typical of SAM. concentration of insulin when the portion of the pancreas
A B
FIGURE 21.9 Hereditary hemorrhagic telangiectasia (HHT). A, Selective hepatic arteriogram shows disorganized and dilated intrahepatic vessels
typical of HHT. Coils are being placed preoperatively for impending liver transplantation. B, Slightly later in the sequence, early opacification of the
hepatic vein is visible (arrowheads).
400 PART 2 DIAGNOSTIC TECHNIQUES
containing the tumor is injected. By sequentially injecting the determining the approximate areas of pancreatic arterial supply.
arterial supplies to different regions of the pancreas, it is pos- In the article by Guettier and colleagues (2009), calcium stimu-
sible to ascertain the location of the tumor. The GDA supplies lation arteriography was the most sensitive technique for local-
the head of the pancreas, the SMA supplies the head and izing surgically proven insulinomas, with an accuracy of 84%,
uncinate process, and the splenic artery supplies the body a false-negative rate of 11%, and a false-positive rate of 4%.
and tail. The origin of small branches supplying the pancreas Percutaneous transhepatic sampling of the splenic, superior
from the splenic artery and CHA are important to note in mesenteric, and portal venous system can be performed to
diagnose occult neuroendocrine tumors of the pancreas. This
may be done in conjunction with calcium stimulation as
described earlier, or it may be performed without stimulation
because of the higher concentration of the hormone when
obtained directly or adjacent to the venous tributary.
Insulinomas
Greater than 90% of insulinomas are single, benign tumors for
which surgical resection is curative. These tumors are the most
common tumors originating from the islets of Langerhans (see
Chapter 65). The most effective method of diagnosing these
tumors is a combination of dual-phase thin-section CT scan and
RIGHT endoscopic ultrasonography (EUS) (Jackson, 2005). Advances
in imaging technology have improved the sensitivity of CT and
MRI to greater than 80% and 70%, respectively (Nikfarjam
et al, 2008). The sensitivity of EUS in detecting and localizing
insulinomas ranges from 82% to 94% (McLean, 2004).
Gastrinomas
Gastrin-secreting tumors are the cause of Zollinger-Ellison
syndrome and in approximately one-third of the cases occur in
association with multiple endocrine neoplasia (MEN) type 1.
Fifty percent of gastrinomas occur in the pancreas, with the
FIGURE 21.10 Peliosis hepatitis. Multiple small contrast collections duodenum being the most common extrapancreatic location.
can be seen within the hepatic parenchyma. This patient had spontane- Approximately 60% to 90% of gastrinomas are malignant.
ous hemorrhage that created displacement of the hepatic parenchyma When a sporadic gastrinoma is identified, surgical resection is
(arrowheads). indicated. The role of surgery in patients with MEN type 1 is
A B
FIGURE 21.11 Insulinoma. A, Selective gastroduodenal arteriogram shows no definite abnormality during the arterial phase. B, A subtle area of
hypervascularity is identified during the capillary phase, possibly representing an insulinoma (arrowheads). This was confirmed as the region of tumor
by calcium stimulation with venous sampling.
Chapter 21 Diagnostic angiography in hepatobiliary and pancreatic disease: indications 401
A B
FIGURE 21.12 Arterial portography in a patient with cavernous transformation of the main portal vein. A, Venous phase of superior mesenteric
arterial injection shows the superior mesenteric vein (arrow) and cavernous transformation of the main portal vein. B, Venous phase of splenic arterial
injection from the same patient shows the splenic vein (arrow).
more controversial because of multiplicity of tumors and lack trunks and their primary branches in the vast majority of
of an established survival benefit. patients. Cross-sectional imaging can accurately depict the
The diagnosis and location of a gastrinoma can be estab- relationship of a mass in the pancreas to both the splenic and
lished with a combination of somatostatin receptor scintigraphy superior mesenteric veins. It also has the advantage of simulta-
and EUS in approximately 90% of patients. When an occult neous opacification of all of the venous structures. However, in
gastrinoma is encountered, angiography has been used for certain clinical situations, it is desirable to visualize the venous
localization. The principles are identical to the localization of structures with a higher level of clarity. These situations include
insulinomas; however, secretin has been used in addition to planning of percutaneous venous intervention in situations
calcium gluconate as the stimulating agent. Sensitivities of where occlusions are suspected or occasionally to plan a surgi-
arterial stimulation venous sampling (ASVS) in the detection cal portosystemic shunt.
of gastrinomas have ranged from 70% to 100% (Cohen et al, The most common technique to visualize the splanchnic
1997; Turner et al, 2002). vein is transarterial portography, in which selective splenic and
Angiographically, gastrinomas are less hypervascular and superior mesenteric arteriograms are performed with delayed
more difficult to detect in comparison to insulinomas. Sensitiv- imaging into the venous phase, depicting the splenic and supe-
ity of angiography alone without ASVS is less than 50%. rior mesenteric veins, respectively (Fig. 21.12). When detailed
Moreover, the 50% extrapancreatic location makes detection visualization of the venous anatomy is required, a higher dose
more difficult, often requiring superselective catheterization to of contrast media can be used for the arterial injection, increas-
evaluate the duodenum. ing the clarity of venous opacification.
When an extremely detailed evaluation is required, a com-
Glucagonoma bination of transarterial portography during MDCT can be
Glucagonomas may occur sporadically or may be associated performed (Fig. 21.13). The increased contrast sensitivity of the
with MEN type 1. These tumors are usually larger than gastri- MDCT coupled with multiplanar and 3D reconstruction allows
nomas or insulinomas at presentation; therefore localization can visualization of the veins that cannot be achieved by any other
generally be achieved with cross-sectional imaging or EUS. single technique. This is particularly useful in the presence of
Equchi and colleagues (2012) reported eight patients with portal vein occlusion, when a complex venous reconstruction
pancreatic hypervascular tumor and elevated serum glucagon or bypass is being considered.
level that glucagonomas were successfully localized using ASVS. Direct venography of the splanchnic veins can be achieved
by three routes: transjugular, transhepatic, and transsplenic. In the
Venographic Technique transjugular approach, a catheter is placed into the jugular vein
MDCT, magnetic resonance venography, and ultrasound are and advanced into a hepatic vein. Free and wedged hepatic
usually sufficient for depiction of the major visceral venous pressures can be obtained through this catheter. Using these
402 PART 2 DIAGNOSTIC TECHNIQUES
403
404 PART 2 DIAGNOSTIC TECHNIQUES
Either alone, or through a guiding needle, a 25 to 20 gauge are commonly placed in formalin. Occasionally, specimens may
needle is advanced into the target lesion, and real-time (ultra- be sent “fresh” to pathology in saline or on saline-soaked gauze
sound [US], fluoroscopy, MR or CT fluoroscopy) or inter- for special studies. Because cells placed in saline eventually
rupted imaging (conventional CT or MRI) is performed to undergo cell lysis related to osmotic shifts of saline into the cell,
guide and assess needle position (Billich et al, 2008). a specimen in saline needs to be fixed or frozen within a few
Fine needles come in a variety of tip designs. Many physi- hours to avoid deterioration of the tissue sample. Tissue also
cians use a Chiba-style needle, in which the needle tip and inner may be snap frozen for future studies. The preferred method
stylet are beveled. Our preference is a Westcott-style needle: In for processing tissue may vary from institution to institution,
addition to a beveled tip, it has a notch in the sidewall of the and the preference of the pathologists reviewing the material
needle just proximal to the tip; this facilitates the operator’s should be determined before initiating a biopsy. For core biop-
ability to choose more precisely the location from which the sies obtained to evaluate organ parenchyma, compared with
cells will be aspirated. side-notch needles, end-cut needles may yield more diagnostic
When needle position has been confirmed, the needle is samples in terms of number of portal triads or glomeruli (Con-
attached to a disposable syringe. The plunger of the syringe is stantin et al, 2010). In the setting of organ dysfunction or
retracted to apply suction while the needle is moved back and failure, no touch preparation is required; specimens are sent in
forth within the lesion to obtain a sample. The needle is with- formalin or saline, depending on the indication and the prefer-
drawn after suction is released, and the specimen is deposited ence of the pathologist.
on a glass slide. Smears are made from the biopsy specimen, As mentioned earlier, many authors advocate performing
and these may be used for immediate analysis (e.g., Diff-Quik) both fine needle and core biopsy to maximize the diagnostic
or fixed in ethanol for immunohistochemical stains. The resid- yield of every given biopsy (Sigel et al, 2011; Stewart et al,
ual material within the syringe and needle is rinsed in a cell- 2002). Core biopsy may be particularly useful to distinguish a
preserving solution for preparation of a cell block. The solution well-differentiated HCC from nodular regeneration in the
used for the cell block should be selected based on the sus- setting of cirrhosis (see Chapter 76) and in confirmation of
pected diagnosis, the need for special studies, and preference benign diagnoses, including hemangioma, adenoma, and focal
of the cytopathologist. For cases in which non-Hodgkin’s lym- nodular hyperplasia (Kulesza et al, 2004; Kuo et al, 2004) (see
phoma is suspected, a specimen for flow cytometry may be Chapter 90A), although recent literature describes findings that
prepared by rinsing the needle and syringe in a nutrient-rich may increase the diagnostic accuracy of fine needle biopsy for
culture medium (e.g., Roswell Park Memorial Institute HCC versus cirrhotic nodules (Geramizadeh et al, 2012). Yang
medium). When infection is suspected, material can be set and colleagues (2004) described an interesting method of dis-
aside for culture. tinguishing well-differentiated HCC from benign hepatic
In the ideal situation, an on-site cytopathologist or cytotech- lesions by using the physical features of the smear from the fine
nologist can provide an immediate interpretation of the sample; needle aspirates; namely, the smear in malignant lesions will
this has been shown to increase the sensitivity of the biopsy, appear finely granular, whereas a benign lesion would produce
shorten the procedure time, and minimize the number of passes fragments of rigid fine needle cores. The authors attribute this
required to obtain a diagnostic specimen (Nasuti et al, 2002; to the reticulin status of the tissue.
Tsou et al, 2009).
IMAGING GUIDANCE
Core Biopsy
The technique for localizing a lesion is identical for fine needle Ultrasound
and core biopsies. To obtain a good core sample, a target lesion Ultrasound (see Chapter 15) is commonly used to guide per-
should ideally be at least 1 cm in maximum dimension, although cutaneous biopsies of the liver because it is widely available,
we have found that useful core biopsy material can be obtained inexpensive, and portable. US may be used at the bedside or
from even smaller lesions. Because of the typically larger needle in patients in whom CT guidance is impractical. Lesions larger
size (14 to 20 gauge) used to perform a core biopsy, care should than 1 cm are often visible, and US allows real-time visualiza-
be taken to minimize the possibility of traversing medium-sized tion of the needle while it courses from the skin into the lesion.
arteries, which lack the muscular wall of larger arteries and have This is especially helpful in small lesions that move with respira-
an increased tendency to bleed; traversing the colon can result tion and are difficult to target with interrupted imaging modali-
in peritonitis or abscess. Core biopsy needles come in a variety ties. Visualization of smaller-caliber needles may be difficult,
of sizes and styles, including biopsy “guns” and cutting needles although many manufacturers make needles specially designed
that obtain histologic samples manually as the needle is passed to enhance visibility with US.
back and forth within the lesion. Another advantage of US guidance is the capability of mul-
To confirm adequacy of the specimen, a touch preparation tiplanar imaging and the absence of ionizing radiation—a
may be prepared on a glass slide for immediate evaluation by benefit to both the patient and the operator. This is particularly
a cytopathologist or cytotechnologist. Before placement in for- useful in finding a route to lesions at the hepatic dome that
malin or saline, the core of tissue is placed on a glass slide and avoids aerated lung and eliminates the risk of causing pneumo-
gently moved over the slide to allow some cells to collect on thorax. Because CT provides a two-dimensional image,
the surface. Care should be taken to avoid excessive vigorous complex triangulation often is required to accomplish the same
touch preparations, because this has been shown to deplete the result. Doppler imaging is occasionally helpful in performing a
cellularity and DNA content of the specimen (Rekhtman et al, biopsy by enhancing the localization of small lesions. US con-
2015). In addition to the tissue sample, material that is suitable trast agents may help identify the most viable regions of a
for cytology is often collected at the same time, and this tumor. Limitations of US include interoperator variability and
increases the diagnostic yield of the procedure. Core samples poor transmission through air, fat, and bone, which limits the
Chapter 22 Percutaneous biopsy 405
visualization of some lesions. Additionally, patients who are for endoluminal biopsy, when satisfactory decompression of the
sedated for biopsy may not be able to cooperate with breathing biliary tree has been achieved. Biopsy forceps or brush-biopsy
instructions necessary to facilitate visualization of some masses, catheters can be used through the existing tract to obtain tissue
including small lesions or those high in the hepatic dome. samples of suspicious areas (Fig. 22.2). The sensitivity of
forceps biopsy is in the range of 40% to 80%, higher than that
Computed Tomography of brush biopsy, which is in the range of 30% to 60%. Specific-
Computed tomography (see Chapter 18) is a common modality ity for each approaches 98% (Govil et al, 2002; Stewart et al,
for guiding percutaneous biopsies because it provides superb 2001; Weber et al, 2008), and sensitivity is highest for intra-
anatomic detail, which gives the operator the ability to plan a ductal lesions and when biopsy is done in conjunction with
path from skin to lesion using the safest approach, clearly visu- choledochoscopy to provide direct visualization of the lesion
alizing interposed structures. CT is the imaging modality of (Ponchon et al, 1996). Combining forceps and brush biopsy of
choice for biopsies of the lung, pancreas, adrenal glands, the bile duct may provide superior results to either alone.
abdominal and retroperitoneal lymph nodes, and bone and liver Kulaksiz and colleagues (2011), noted sensitivity of brushing
lesions that are not well visualized with US or when biopsy is alone of 49%, forceps alone of 69%, and combined of 80%;
performed by operators who are not skilled with US. specificity for malignancy was 100%. However, a recent report
of a new percutaneous forceps biopsy technique cites sensitivity
Computed Tomographic Fluoroscopy of 93.3%, specificity of 100%, positive predictive value of
Many manufacturers now offer CT fluoroscopy as an option 100%, and negative predictive value of 70%; overall accuracy
on diagnostic scanners. This produces CT images in near real was 94.2% (Patel et al, 2015).
time. It does expose the operator to ionizing radiation and Alternatively, after the biliary tree is opacified, a direct per-
requires that the operator wear lead, as with conventional fluo- cutaneous needle biopsy of a bile duct lesion may be targeted
roscopy, but it is preferred by some physicians, owing to with fluoroscopy using a transhepatic approach (Chawla et al,
decreased time between needle manipulation and image 1989) (see Chapter 30). This technique is most useful for
availability. intrinsic bile duct lesions but may also be used to diagnose
lesions adjacent to the bile duct. With this technique, contrast
Cone-Beam Computed Tomography is injected into an indwelling biliary drainage catheter to delin-
Cone-beam computed tomography (CBCT), also sometimes eate the targeted bile duct abnormality. A needle is advanced
referred to as C-arm CT, uses a flat-panel X-ray detector that through the anterior abdomen to the lesion, and a specimen is
rotates around the patient; the X-rays are divergent, forming a obtained. Confirmation of accurate needle position is made by
cone. Images can be reconstructed in multiple planes, and obtaining oblique fluoroscopic images and by real-time fluoros-
three-dimensional reconstruction can be performed and rotated copy, when the needle is seen to move the duct or the indwell-
in multiple planes. The soft tissue resolution is not comparable ing catheter or both (Fig. 22.3). Fluoroscopy may also be useful
to conventional CT for abdominal and pelvic soft tissue, but to guide percutaneous biopsy of lung nodules and for nontar-
the resolution for lung and bone is adequate for biopsy guid- geted transvenous biopsies of the liver or kidney.
ance. Further, available biopsy path–planning and needle-
navigation software may assist the operator with needle Positron-Emission Tomography
placement (Floridi et al, 2014). Occasionally, a lesion is only well demonstrated by 18F-
fluorodeoxyglucose (FDG) PET imaging. In these cases, it is
Magnetic Resonance Imaging possible to use PET and CT to guide accurate needle place-
Biopsies guided by MRI (see Chapter 19) have been made ment. Certain lesions may also have varying FDG avidity; PET
possible by the advent of open-bore MRI systems that provide guidance allows the most hypermetabolic portion of a lesion to
access to patients during imaging and the availability of nonfer- be targeted. Operators should be mindful of the patient as a
rous biopsy needles and monitoring equipment. The superior source of radiation; the major source of radiation to the opera-
contrast resolution of MR allows targeting lesions that are dif- tor during PET-guided interventions was found to be the time
ficult to visualize with US and noncontrast CT, and the ability spent in close proximity to the patient (Ryan et al, 2013) (see
of MRI to image in any plane enhances the targeting of lesions Chapter 17).
that are not safe to approach or easy to access in the axial plane
(Stattaus et al, 2008) (Fig. 22.1). Owing to high cost and Other Guidance
limited availability, as well as a relative paucity of MRI- New technology is under development that allows fusion of
compatible biopsy needles, MR-guided biopsies are generally multiple modalities. For example, CT and MRI scans can be
reserved for patients whose lesion cannot be seen or targeted overlaid with real-time US images to achieve the clarity of the
with US or CT. In addition, it is necessary to ensure that non- one imaging modality and the real-time visualization capabili-
ferromagnetic, MRI-compatible equipment is on hand and that ties of the other. PET images (see Chapter 17) also can be fused
the patient is able to undergo MRI fluoroscopy. to demonstrate sites of highest metabolic activity. Additionally,
Fluoroscopy is useful for guiding bile duct biopsies. Benign robotic guidance systems have been piloted in an effort to opti-
and malignant biliary strictures (see Chapters 42 and 51) often mize speed and accuracy of needle placement.
have similar cholangiographic appearances and rarely can be
distinguished based on imaging alone (Corvera et al, 2005; BIOPSY OF SPECIFIC SITES
Hadjis et al, 1985). Lesions originating within the duct may be
sampled by either an endoluminal (see Chapter 29) or a direct Liver Biopsy
percutaneous approach (see Chapter 30). Percutaneous tran- Percutaneous liver biopsy is performed to determine the nature
shepatic biliary drainage allows direct access to the biliary tract of focal liver masses, the cause and extent of cirrhosis, or the
406 PART 2 DIAGNOSTIC TECHNIQUES
A B
C D
FIGURE 22.1. Magnetic resonance (MR)-guided percutaneous liver biopsy. A, Axial T1 MR after contrast administration shows a focal lesion in
segment IV in a patient with hepatitis B. B, Noncontrast computed tomography in the same patient at the same level failed to show the lesion. C,
The lesion was hypermetabolic on fluorodeoxyglucose positron-emission tomography. D, biopsy was successfully performed using MR guidance in
the sagittal plane to avoid the risk of pneumothorax. The biopsy specimen confirmed the diagnosis of hepatocellular carcinoma.
cause of liver dysfunction (see Chapters 76 and 89). Modern diagnoses should be considered in all solitary liver lesions,
cross-sectional imaging techniques, including US, CT, and unless they are known to be new in the setting of a known
MRI, allow percutaneous biopsy of both small and deep lesions cancer or in patients at risk for primary HCC.
to be performed on an outpatient basis with minimal morbidity. HCC may also be diagnosed based on imaging and clinical
With current techniques, almost any liver lesion can be targeted criteria (see Chapter 91). According to the American Associa-
percutaneously; many liver lesions larger than 5 mm are suit- tion for the Study of Liver Diseases (AASLD) guidelines, in
able for biopsy (Yu et al, 2001). Fine needle biopsy of liver patients with cirrhosis, liver lesions identified on screening US
lesions has a sensitivity of 69% to 97% (Ohlsson et al, 2002). that are larger than 1 cm may be diagnosed as HCC based on
a single CT or MR imaging study demonstrating classic find-
Focal Liver Lesions ings of arterial enhancement and portal venous or delayed-
Focal liver lesions may be solitary or multiple. For a solitary phase washout (Bruix & Sherman, 2011); the National
lesion, several benign conditions—cyst, hemangioma, focal Comprehensive Cancer Network guidelines are the same for
nodular hyperplasia, and adenoma—often can be diagnosed lesions 2 cm and larger, but for lesions 1 to 2 cm in size, they
confidently by high-quality cross-sectional imaging, obviating advise that two concordant imaging studies are necessary to
the need for biopsy (Gibbs et al, 2004; Hussain et al, 2004; confirm a diagnosis of HCC (Benson et al, 2009). When the
Kim et al, 2004) (see Chapters 15, 18, and 19). These diagnosis of HCC is considered, and these criteria are not met,
Chapter 22 Percutaneous biopsy 407
Transvenous Biopsy
Transjugular liver biopsy is a useful alternative to percutaneous
biopsy in patients with coagulopathy or when hepatic venous
pressure measurements are required (Behrens & Ferral, 2012;
Garcia-Compean & Cortes, 2004). Although transvenous
biopsy is seemingly more invasive than percutaneous biopsy,
the risk of significant bleeding in patients with coagulopathy is
minimized using a transvenous approach, because bleeding
B from the biopsy site tracks back into the venous circulation and
FIGURE 22.2. Biliary brush biopsy. A, Transhepatic cholangiogram
not into the abdominal cavity as can happen with percutaneous
shows a high bile duct stricture (arrow) Prior brush biopsy was nondi- biopsies. Proper technique to avoid puncture of the liver capsule
agnostic. B, A brush (curved arrow) was advanced to the stricture and is crucial to optimize safety.
used to obtain a specimen for cytology. The specimen was diagnostic In this technique, a venous sheath is introduced into a
of cholangiocarcinoma. hepatic vein, most commonly the right hepatic vein, typically
from a right internal jugular approach. Pressure measure-
ments may be obtained to evaluate the source (presinusoidal,
biopsy may be required. Smaller, encapsulated tumors are more sinusoidal, or postsinusoidal) and degree of portal hyperten-
likely to be well differentiated, and tissue cores may be required sion. A biopsy needle is introduced through the sheath into
to distinguish a well-differentiated tumor from normal or cir- the liver parenchyma to obtain histologic samples (Fig. 22.4).
rhotic liver. Because of the risk of tumor seeding (Chaudhry Care must be taken to avoid performing the biopsy in too
et al, 2004; Durand et al, 2007; Perkins, 2007), when a cura- peripheral an area of liver, because this increases the risk that
tive treatment is possible, biopsy for HCC should be performed the liver capsule will be punctured and that peritoneal hemor-
only after consultation with a hepatobiliary surgeon and after rhage will result.
referencing the most current imaging and clinical criteria. The Transvenous biopsy is only used for nontargeted parenchy-
AASLD position paper on liver biopsy reinforces caution based mal biopsy; it cannot be used for biopsy of a focal lesion.
on concern for needle-track seeding, sampling error, and, based Transvenous biopsy of the kidney also has been reported and
on a paper by Saborido and colleagues (2005), possible may be useful for evaluation of renal dysfunction in coagulo-
increased rate of recurrence posttransplant, although only in pathic patients (Misra et al, 2008). This may be particularly
408 PART 2 DIAGNOSTIC TECHNIQUES
A B
C
FIGURE 22.3. Percutaneous bile duct biopsy. A, Transhepatic cholangiogram shows a high bile duct stricture (marked by the clamp) of uncertain
etiology. B, Under fluoroscopic guidance, a 22 gauge needle was used to target the stricture. C, Oblique imaging confirmed the position of the
needle at the site of the bile duct stricture.
convenient in coagulopathic patients who require both paren- adenomas occur in 5% of individuals (Abecassis et al, 1985;
chymal hepatic and renal biopsies. Libe et al, 2002). Adrenal biopsy can often be avoided,
because MRI or adrenal protocol CT can sometimes distin-
Biopsy of Other Organs guish between an adenoma and a metastasis (Davarpanah &
Adrenal Biopsy Israel, 2014; National Institutes of Health, 2002). In some
The adrenal gland is a common site of metastatic disease. cases, the mass remains indeterminate, and biopsy is indi-
This gland also is the site of many benign neoplasms, and cated. Because of the posterior approach used for all left and
Chapter 22 Percutaneous biopsy 409
Pancreas Biopsy
Despite the best efforts of clinicians and advances in imaging,
most patients with pancreatic cancer still initially present with
unresectable disease (see Chapter 59). Needle biopsy may be
requested for tissue diagnosis so that treatment can be initiated,
and it is essential to evaluate the preprocedure imaging carefully
to determine the safest approach. Increasingly, endoscopic
ultrasound (EUS) has become an excellent alternative to per-
cutaneous biopsy (see Chapter 16). In cases where in which
EUS-guided biopsy is not feasible or adequate material is not
obtained, percutaneous biopsy may still be necessary. An ante-
rior approach to the pancreas may be difficult because of inter-
posed colon, spleen, or mesenteric vessels, which we would
prefer not to traverse. We often prefer a posterior, transcaval
approach (Sofocleous et al, 2004) or a transhepatic approach,
particularly for lesions in the head or uncinate process
(Fig. 22.6).
A B
C D
FIGURE 22.5. Adrenal biopsy. A, Transhepatic right adrenal mass (arrows) biopsy eliminates the risk of pneumothorax. B, Coronal reformat of a
contrast enhanced computed tomography shows a right adrenal mass (arrows). C, With the patient positioned prone, there is interposition of lung
between the skin and adrenal mass (arrows). D, With the patient in a right-side-down position, there is no need to traverse aerated lung for biopsy
of the adrenal mass (arrows).
Mediastinal biopsies are usually performed using CT guidance. a tyrosine kinase inhibitor compared with chemotherapy in
The size of the needle used and type of specimen acquired vary nonsmokers or former light smokers (Mok et al, 2009). Patients
depending on the clinical indication. Diagnostic rates for needle with adenocarcinoma and an EGFR mutation were also shown
biopsy of malignant lung lesions have been reported as greater to do better when a tyrosine kinase inhibitor was used as main-
than 90% (Swischuk et al, 1998). Lung biopsy may be useful tenance after first-line treatment rather than as second-line
to provide material in the setting of metastatic disease, primary therapy (Wang et al, 2011). The KRAS and ALK mutations
malignancy, and/or infection. Personalized medicine is already have also been shown to influence response to treatment (Eber-
making its mark in primary lung cancer. Not long ago, all cases hard et al, 2005; Kwak et al, 2010).
of non–small-cell lung cancers were treated in a similar fashion.
However, recent studies have shown that histologic subtype and Bone Biopsy
certain molecular alterations influence the response to various Bone biopsies are often done using CT guidance. MRI and
chemotherapies and targeted agents (Moreira et al, 2012; fluoroscopy may also be used. More recently, operators have
Travis et al, 2010). For example, bevacizumab, a humanized described excellent results using CBCT with needle-guiding
monoclonal antibody targeted at endothelial growth factor, is software (Tselikas et al, 2015). Bone biopsies are typically per-
contraindicated in patients with squamous cell lung carcinoma formed using larger needles (11 to 15 gauge) than those used
due to increased risk of pulmonary hemorrhage (Johnson et al, for organ or soft tissue. Purely lytic lesions are the exception,
2004). Patients with adenocarcinoma also respond better to the because small-caliber needles will often suffice to document
antifolate agent pemetrexed than those with squamous carci- metastases and are able to penetrate bone in the setting of
noma (Scagliotti et al, 2008), and patients with adenocarci- cortical destruction. For surgical candidates, the biopsy path
noma and an epidermal growth factor receptor gene (EGFR) should be discussed with the surgeon to ensure that violating
mutation have been shown to have a better response to an uninvolved compartment does not compromise a planned
Chapter 22 Percutaneous biopsy 411
CONCLUSION
B Percutaneous needle biopsy is a well-established and safe diag-
nostic tool, and it is an important instrument in the diagnosis
of tumors, for determining the cause of organ dysfunction
staging, and for documenting recurrent or metastatic disease.
Increasingly, needle biopsy is essential to provide material for
genetic analysis. Complications occur infrequently, and most
are easily treated or self-limiting. Tract seeding has been
reported but occurs infrequently. There is no such thing as a
“negative” biopsy (Phillips et al, 1998). If a diagnosis of malig-
nancy is not made, a specific benign diagnosis needs to be
confirmed. If nonspecific findings are evident on cytology,
including inflammatory or reactive changes, fibrous tissue, or
normal site tissue, or, if atypical cells are present, another
biopsy should be performed, or the lesion should be closely
followed up, depending on the pretest probability of disease.
The role of biopsy in patient management is evolving in
tandem with the development of associated fields, including
functional and molecular imaging. Until biopsies are no longer
necessary, every effort should be made to keep morbidity low
and diagnostic rates high.
C
References are available at expertconsult.com.
FIGURE 22.7. Hemorrhage complicating liver biopsy. A, Contrast-
enhanced computed tomographic scan 5 days after liver biopsy shows
a large subcapsular hematoma (curved arrow) with active extravasation
of contrast from the liver mass (curved arrow). B, Angiography shows
active extravasation (curved arrow) from peripheral segment VIII artery
that was successfully embolized with stainless steel coils (C).
Chapter 22 Percutaneous biopsy 412.e1
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412.e2 PART 2 DIAGNOSTIC TECHNIQUES
Rekhtman N, et al: Depletion of core needle biopsy cellularity and Stewart CJ, et al: Comparison of fine needle aspiration cytology and
DNA content as a result of vigorous touch preparations, Arch Pathol needle core biopsy in the diagnosis of radiologically detected abdom-
Lab Med 139(7):907–912, 2015. inal lesions, J Clin Pathol 55(2):93–97, 2002.
Rockey DC, et al; American Association for the Study of Liver Disease: Stigliano R, et al: Seeding following percutaneous diagnostic and thera-
Liver biopsy, Hepatology 49(3):1017–1044, 2009. peutic approaches for hepatocellular carcinoma. What is the risk and
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management of a patient with an acute abdomen: a case report with Cancer Treat Rev 33(5):437–447, 2007.
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2001.
CHAPTER 23
Intraoperative diagnostic techniques
Kelly M. Collins and M. B. Majella Doyle
413
414 PART 2 DIAGNOSTIC TECHNIQUES
Biliary Disease
LHD Evaluation of the Biliary Tree
As laparoscopic cholecystectomy has become the standard of
care for gallbladder disease, the use of laparoscopic US during
this procedure has emerged as an alternative to cholangiogra-
phy (see Chapters 35 and 36). Laparoscopic US is recom-
mended as the primary screening modality for evaluating bile
duct calculi because of its safety, efficiency, and overall cost-
effectiveness (Machi et al, 1999). IOUS is at least as good as
PV cholangiography, if not better, at detecting stones during lapa-
roscopic cholecystectomy (Catheline et al, 1999; Siperstein
et al, 1999; Tranter & Thompson, 2003). Laparoscopic US, in
particular, has the added advantage of reducing the risk of
biliary and vascular injury. Perry and associates (2008) reported
on the use of laparoscopic US in a prospective study performed
FIGURE 23.1. Intraoperative ultrasound view of a tumor (arrows) at between 1995 and 2005. Laparoscopic US was performed in
the base of segment IV. The confluence of the right and left portal venous 236 (60%) of 396 laparoscopic cholecystectomies performed
branches is shown (PV). Dilation of the left hepatic duct (LHD) is indi- for cholelithiasis. US had a positive predictive value of 100%,
cated and suggests possible involvement by tumor. a negative predictive value of 99.6%, a sensitivity of 92.3%, and
a specificity of 100% for detecting CBD stones (Perry et al,
2008). However, proficiency with IOUS requires some time to
biliary structures. Intraoperative transducers appropriate for develop, which may explain why it is not used more liberally
liver surgery include high-frequency (6 to 10 MHz) T-shaped for biliary disease.
linear- or curvilinear-array transducers. These probes provide Laparoscopic US is a useful adjunct for staging gallbladder
excellent high-resolution images and are capable of identifying carcinoma and cholangiocarcinoma (see Chapters 49 to 51).
lesions as small as approximately 1 to 2 mm in size at depths Sonographic findings not only reveal subtle liver metastases but
of penetration of approximately 10 to 12 cm. Transducers with may help to define the local extent of these tumors and their
color flow Doppler imaging enable further discrimination of relationship to the ductal system. Doppler and color flow
tumors and normal hepatic vasculature. images may help distinguish biliary sludge from polyps and
Techniques for IOUS continue to evolve. Particular atten- other intraluminal tumors. Other applications of laparoscopic
tion must be given to port placement when IOUS will be US include evaluating biliary strictures and malignant biliary
performed laparoscopically (see Chapter 105). Typically, no obstructions in the planning of surgical reconstructions, such
coupling gel is required because the natural surface moisture as biliary bypass procedures. These approaches and others are
of the liver provides adequate acoustic coupling. The trans- summarized in a review by Berber and Siperstein (2004).
ducer is initially held in a transverse position, and the survey
of the liver begins by first identifying the confluence of the right Technical Considerations
and left portal pedicles. Next, all segmental pedicles on the The biliary tree and gallbladder are imaged best from a right
right are visualized, followed by identifying those on the left. subcostal port or from the periumbilical port. Sonographic
Each hepatic vein is visualized by scanning peripherally and examination of the gallbladder is approached through the liver
then by traversing toward the vena cava. It is easiest to identify by using a 5- or 7-MHz transducer. A nasogastric or orogastric
the hepatic veins by placing the transducer cranially, in a tube should be placed for decompression. The bile ducts can
midline position and angled toward the heart. Only light pres- be visualized through a compressed duodenum or gastric
sure should be applied to the liver. The confluence of the left antrum using a 7-MHz transducer, but placing the transducer
and middle vein has a characteristic appearance and should be directly on the ducts should be avoided because reverberation
observed in all sonographic examinations. If the entire liver artifact limits its sensitivity. Color flow images are helpful for
is to be scanned—for example, to search for metastases— distinguishing the common bile duct (CBD) from the portal
sequential overlapping sagittal strokes are made sweeping from vein, for identifying the insertion of cystic duct into the CBD,
superior to inferior, beginning at the most lateral margin of and for identifying any aberrant biliary anatomy.
segment II and traveling toward the right. More focal scanning
can be used to localize impalpable lesions situated deep within Pancreatic Disease
the liver parenchyma. Special care must be taken when imaging Evaluation of the Pancreas
the superior portion of the right liver, the posterior subdia- The principal application of IOUS for pancreatic disease is
phragmatic bare area, and surface lesions, such as hamartomas, during staging laparoscopy (SL) in patients with pancreatic
as these areas are particularly challenging to completely visual- malignancy. Its utility lies in demonstrating vascular invasion,
ize. Once the lesion has been delineated and measured, photo- liver metastases, and the degree of resectability. Approxi-
graphic documentation should be obtained and saved. mately 20% to 35% of patients deemed resectable based on
Chapter 23 Intraoperative diagnostic techniques 415
5 mm
5 mm
10 mm
Hasson
FIGURE 23.4. Examination of the liver. A blunt 10-mm instrument is
used in conjunction with a 5-mm grasper.
FIGURE 23.7. Lesser sac. The “gastric pillar” (dashed arrow) and
hepatic artery (solid arrow) are shown.
BOX 23.4 Steps for Laparoscopic Ultrasound BOX 23.5 Criteria for Clinical Risk Score to Determine Risks for
Insertion of laparoscopic ultrasound probe Extrahepatic Disease
Examination of liver: left lateral segment, right lobe Lymph node–positive tumor
Transverse scan of hepatoduodenal ligament Disease-free interval between primary and detection of metastasis:
Identification of superior mesenteric artery, portal vein, splenic vein <12 mo
Examination of pancreas Number of hepatic tumors: >1 (based on preoperative imaging)
Assessment of tumor Carcinoembryonic antigen: >200 ng/mL within 1 mo of surgery
Size of the largest hepatic tumor: >5 cm
From Minnard EA, et al: Laparoscopic ultrasound enhances standard laparoscopy in the staging
of pancreatic cancer, Ann Surg 228:182–187, 1998. From Jarnagin WR, et al: A clinical scoring system predicts the yield of diagnostic laparoscopy in
patients with potentially resectable hepatic colorectal metastases, Cancer 91:1121–1128, 2001b.
for other laparoscopic procedures and include hemorrhage,
visceral perforation, and infection. A misconception is that
suspected malignancy precludes staging laparoscopic examina- criteria) hepatobiliary malignancy. Laparoscopy was performed
tion. An early report raised concern about “port-site” tumor in 401 patients between 1997 and 2001; 291 (73%) cases were
implants 2 weeks after laparoscopy in a patient with malignant considered complete, 88 (22%) incomplete, and 22 (5.5%)
ascites (Dobronte et al, 1978); this concern was also expressed were considered failures. Unresectable disease was discovered
by later studies in the 1990s, which reported rates of port-site at the time of laparoscopy in 84 cases, for an overall incidence
recurrence ranging from 0.8% to 2% (Curet, 2004; Nieveen of 21%. Sixty-nine patients had unresectable disease identified
van Dijkum et al, 1999; Pearlstone et al, 1999). Shoup and during open exploration, for an overall false-negative rate of
colleagues (2002) examined this question in a series of 1650 22%. This high false-negative rate was attributed primarily to
diagnostic laparoscopic procedures, in which 4299 trocars were failure to identify lymph node metastases or to detect vascular
inserted. The overall rate of port-site recurrence was 0.8% (13 invasion.
cases); 5 of those occurred in patients with local disease; the Laparoscopy is most accurate for identifying peritoneal
remaining 8 occurred in patients with documented metastatic deposits (80% accuracy) and hepatic disease (63% accuracy);
disease. The findings of this study suggest that recurrence is a it is least accurate for identifying nodal metastases (7% accu-
marker of more advanced disease rather than being an event racy) and vascular invasion (18% accuracy) (D’Angelica et al,
resulting from the laparoscopy. Overall, Shoup and associates 2003). Factors that can improve the yield of laparoscopy
concluded that SL can be performed safely in the setting of include the surgeon’s preoperative judgment regarding the like-
presumed malignancy (Shoup et al, 2002; Shoup et al, 2004). lihood of resectability, the completeness of laparoscopic staging
This concept has been confirmed by others, including Velanov- examinations, the addition of laparoscopic ultrasound, and the
ich (2004), who demonstrated that the incidence of port-site primary diagnosis. The yield was highest with gallbladder ade-
recurrence (3%) is equivalent to that of wound recurrence in nocarcinoma and cholangiocarcinoma and lowest with colorec-
patients who had an exploratory laparotomy alone (3.9%). tal metastases (Callery et al, 1997; D’Angelica et al, 2003; John
et al, 1994).
Staging Laparoscopy for Potentially Resectable Disease Laparoscopic staging can be used in the evaluation of
Hepatobiliary Malignancy colorectal metastases (Rahusen et al, 1999) (see Chapter 92).
Determination of resectability of hepatobiliary malignancy Approximately one half of all patients with new diagnoses of
begins with CT or MRI; however, laparoscopy plays an essen- colorectal cancer will subsequently develop liver metastases, yet
tial role in detecting occult disease (Jarnagin et al, 2001a; only 20% are candidates for curative hepatic resection. Most
Jeffers et al, 1988; Lightdale, 1982; Torzilli et al, 2002). authors agree that hepatic cirrhosis, extrahepatic tumor spread,
Roughly 20% to 25% of patients initially believed to have and significant bilobar disease are relative contraindications for
resectable disease will harbor occult disease detected by lapa- hepatic resection. In a large series of patients with colorectal
roscopy that precludes curative resection and thereby can be metastases identified as resection candidates who underwent
spared laparotomy (Conlon et al, 2003; Weber et al, 2002). SL with IOUS, Thaler (2005) reported that a change in the
In addition to the quality of the preoperative imaging, the preoperatively determined plan occurred in 67% (46/69) of
yield of laparoscopy depends on the underlying disease and the patients. Of those in whom resection was considered impossi-
quality of preoperative imaging. For example, hilar cholangio- ble, 18 were untreatable altogether, and 28 patients had alterna-
carcinoma rarely gives rise to peritoneal disease; however, it is tive treatments (i.e., regional therapy or a palliative hepatic
often unresectable due to local tumor extension and/or vascular arterial infusion pump) (Thaler et al, 2005). Of 36 patients in
involvement, which is difficult to determine laparoscopically. whom radiofrequency ablation was planned, 14 had procedures
The yield of laparoscopy is therefore lower than for other diag- altered by SL/IOUS (Thaler et al, 2005).
noses, such as gallbladder cancer, which frequently results in In an effort to improve the yield of SL for hepatic colorectal
peritoneal disease. metastases, a study used a clinical risk score (CRS) to try to
In HCCs, laparoscopy can be used to evaluate for cirrhosis determine which patients are more likely to have disease that
and aid in determining resectability. Weitz and colleagues (2004), is occult on preoperative imaging. The CRS uses five clinical
in a study of patients with HCC who underwent SL, found that parameters: Each is shown as an independent predictor of
22% of patients were spared nontherapeutic laparotomy. The outcome after resection, and each criterion is assigned 1 point.
reported yield of SL over the past 10 years ranges from 16% to Forty-two percent of patients with a CRS greater than 2 had
57% (Gaujoux & Allen, 2010) (see Chapter 91). unresectable disease detected at laparoscopy versus none of the
In a prospective analysis, D’Angelica and colleagues (2003) patients with CRSs of zero to 1 (Box 23.5) (Grobmyer et al,
studied the use of SL in patients with resectable (by radiologic 2004; Jarnagin et al, 2001b). The score was validated by Mann
420 PART 2 DIAGNOSTIC TECHNIQUES
Pancreatic
mass on CT
Resectable Unresectable
Laparoscopic
staging ± LUS Localized Metastatic
disease disease
Open Appropriate
exploration therapy No mets Mets
Chemotherapy Chemotherapy
/radiotherapy
FIGURE 23.10. Use of laparoscopic staging in the management of adenocarcinoma of the pancreas. CT, Computed tomography; mets, metastases;
LUS, laparoscopic ultrasound.
and colleagues (2007) in a study of 200 patients with colorectal 2. For locally advanced unresectable pancreatic cancer without
metastases who underwent SL. The CRS predicted the likeli- radiographic evidence of distant metastasis, SL may be used
hood of finding incurable disease (P < .001) and predicted to rule out subclinical metastatic disease to optimize treat-
curability determined by laparoscopy (P < .001). Laparoscopy ment selection (Callery et al, 2009).
did not change the management of any patient with a CRS of Cuschieri and colleagues first reported their experience
zero or 1; however, it did alter the course of patients with a using SL for pancreatic malignancy in 1988. In this report,
score of 2 to 3 (18/129 patients affected) and a score of 4 to 5 laparoscopic examinations demonstrated that 42 (57%) of 73
(21/40 patients affected) (Mann et al, 2007). Using such a risk patients had unresectable disease, mainly because of peritoneal
scoring system to help guide the addition of laparoscopy to or omental metastases. Since these early papers, laparoscopy
higher-risk patients should improve the overall yield from has been refined and is now comparable to open exploration in
laparoscopy. defining resectability. Other groups have reported similar find-
ings. Warshaw and colleagues (1990) compared CT, MRI,
Pancreatic and Periampullary Malignancy angiography, and laparoscopy in 88 patients and found that CT
Our approach for the staging of pancreatic adenocarcinoma is failed to show peritoneal disease in 22 cases discovered at lapa-
illustrated in Figure 23.10. A minority of patients (20% to roscopy. MRI conferred no further benefit, and laparoscopy
35%) with pancreatic and periampullary malignancies (see had a sensitivity of 96%, having understaged 1 patient. This
Chapters 62 and 63) are suitable candidates for curative resec- same group reported that 39 patients (44%) were spared a
tion (Conlon & Brennan, 2000; Conlon & Minnard, 1997; laparotomy because of metastases discovered at laparoscopy
Jimenez et al, 2000). Similar to the management of hepa- not seen on spiral CT. SL was performed as a day-case proce-
tobiliary malignancies, initial diagnostic evaluation begins with dure, further reducing inpatient hospital time. Reddy and asso-
high-resolution contrast-enhanced CT. Imaging studies can ciates (1999) confirmed these findings in a later report; 29%
predict resectability in 57% to 88% of cases (Contreras et al, were spared further intervention. A more recent prospective
2009; Freeny, 2001; Mayo et al, 2009; Pisters et al, 2001). study (Doran et al, 2004) reported outcomes of 239 patients
Other useful imaging modalities that may augment CT eva with pancreatic cancer who were submitted to SL; of these, 190
luations include MRI, ERCP, EUS, and positron-emission were considered to have resectable disease based on CT find-
tomography. ings. After SL, roughly 15% of patients were spared a lapa-
The Society of Surgical Oncology guidelines from the 2009 rotomy. This estimate likely reflects advancements in
consensus statement regarding the pretreatment assessment of high-resolution imaging, but it also demonstrates that, despite
pancreatic cancer state the following regarding the use of refinements in imaging techniques, peritoneal disease is not
laparoscopy: easily revealed on CT.
1. For apparent resectable pancreatic cancer, SL should be As imaging has improved, the yield of laparoscopy has been
used selectively on the basis of clinical parameters that opti- challenged. In 1996, Conlon reported the Memorial Sloan Ket-
mize yield. These include pancreas head tumors of greater tering experience. In a review of 115 patients between the years
than 3 cm, tumors of the pancreas body and tail, equivocal of 1992 and 1994 deemed resectable based on imaging, 38%
findings on a CT scan, and high cancer antigen 19-9 levels had findings at the time of SL that precluded resection (Box
(>100 U/mL). 23.6) (Conlon, 1996). However, in an updated review of their
Chapter 23 Intraoperative diagnostic techniques 421
Flum DR, et al: Bile duct injury during cholecystectomy and survival
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CHAPTER 24
Intraoperative and immediate
postoperative management
Mary Fischer, Vittoria Arslan-Carlon, and Jose Melendez
423
424 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
are modifiable risk factors. Detailed evaluation and correction this noninvasive test to the LRCRI (Hwang et al, 2015). The
of all modifiable risk factors combined with best practice 2014 American College of Cardiology/American Heart Associa-
guidelines are our best choices to help avoid the most prevent- tion (ACC/AHA) guidelines on perioperative cardiovascular
able complications. Medical guidelines have rapid turnover, evaluation and care for noncardiac surgery are an excellent
with medical reversal a reality, and staying current to apply framework for evaluating cardiac risk in the perioperative
evidence-based practice is recognizing that the correct “scien- period for patients with clinical risk factors (Fleischer et al,
tific answer” may shift over time (Neuman et al, 2014; Prasad 2014).
et al, 2013). Not only is the patient population becoming older Cardiac functional status can be expressed in metabolic
with ever expanding comorbidities, but improvements in the equivalents or simply the inability to perform various activities
medical management of some chronic illnesses mean that the such as climbing two flights of stairs or walking four blocks
implications of such illnesses may be quite different today than (Eagle et al, 2002; Girish et al, 2001). Over the years, periop-
years past. Select patients might be better served having hepatic erative management has shifted from treating coronary obstruc-
surgery at a major medical center where the multidisciplinary tion with coronary revascularization toward medical therapy
care team provides optimum preparation of patients as well as aiming at prevention of myocardial oxygen supply and demand-
the ability and availability to minimize the impact on patients ing mismatch and coronary plaque stabilization. Today
when adverse events occur (Fong et al, 2005; Nathan et al, preoperative cardiac testing, cardiac stenting, and coronary
2009). revascularization are only performed for the same indications
as the nonoperative setting (Neuman et al, 2014).
Cardiac Evaluation The risks and benefits of continuing perioperative medical
Although the perioperative event rate has declined as a conse- management are complex. Perioperative β-blockade (PBB) has
quence of better anesthetic and surgical techniques, periopera- been shown to reduce the incidence of perioperative ischemic
tive cardiac complications remain a significant problem. The events and MI in patients with coronary artery disease but
first step in preoperative care is an adequate identification of confers questionable benefit and possible harm in patients
patients at risk for perioperative cardiac events. Clinical history, without coronary artery disease (Goldman, 2001; Lindenauer
physical examination, and review of a baseline electrocardio- et al, 2005). In 2008, the PeriOperative Ischemic Study Evalu-
gram usually provide enough data to estimate cardiac risk. ation (POISE) trial completely transformed the premise of
Estimation of a stable patient’s cardiac risk can be derived from PBB, finding PBB stroke morbidity outweighed any PMCE
the Lee Revised Cardiac Risk Index (LRCRI), a simple index prevention (Devereaux et al, 2006). POISE confirmed what
that identifies six independent risk factors to provide the risk clinical anesthesiologists had experienced increased intraopera-
of a cardiac complication in percent (Lee et al, 1999). The risk tive hypotension and bradycardia in low-risk patients with
of a perioperative major cardiac event (PMCE), defined as newly initiated PBB. PBB guidelines revisions followed rapidly
cardiac death, myocardial infarction (MI), or pulmonary edema in 2009. The guidelines recommend continuation of β-blockers
within 30 days postoperative, is the summation of an individual for patients who are already on them, the initiation of PBB for
patient’s risk and functional capacity and the cardiac stress high-risk patients, but not to initiate PBB in low-risk patients
related to the surgery. There are active cardiac conditions that in the perioperative period. β-Blockers should still be used to
may lead to cancellation of the procedure, unless the surgery is manage acute hypertension and tachycardia perioperatively in
emergent, but most PMCE risk is silent, and the LRCRI has patients at risk for myocardial supply and demand imbalance.
shown only moderate predictive performance (Ford et al, Similarly, balancing the risk-to-benefit ratio of dual antiplatelet
2010). The absence of coronary computed tomographic angi- therapy or aspirin interruption and the risk of stent thrombosis
ography findings of coronary artery disease confers low PMCE versus continuation and the risk of bleeding is challenging
risk regardless of clinical risk, and some have suggested adding (Newsome et al, 2008). The POISE-2 trial showed that
Chapter 24 Intraoperative and immediate postoperative management 425
perioperative aspirin did not reduce PCME at 30 days but did or dypsnea may benefit from this test of cardiopulmonary
increase perioperative bleeding (Devereaux et al, 2014). Only reserve to determine complication risk (Snowden et al, 2010).
a small number of patients in this trial had coronary stenting, Although it seems reasonable to assume that fitter patients will
and patients with a bare-metal stent for less than 6 weeks or a have better outcome, a recent study suggested that cardiopul-
drug-eluting stent for less than 1 year were excluded. monary exercise testing should not be used as a barrier to
Communication among the patient’s cardiologist, surgeon, patients undergoing liver surgery (Declan et al, 2014). Potential
and anesthesiologist is essential for the management of patients interventions to reduce PPCs include smoking cessation, pre-
with active or quiescent coronary artery disease. At our institu- operative exercise training, early mobilization, postoperative
tion, the medical consult takes into account both the ACC/ parental nutrition, and optimal treatment of pain (Smetana
AHA patient’s number of clinical factors (does the patient have et al, 2006).
active cardiac condition?; planned surgery, low or high risk?; Although obesity presents the anesthesiologist with signifi-
good functional capacity?; further testing required?) and the cant challenges, obesity per se is not a significant risk factor for
LRCRI (high-risk type of surgery?; history of ischemic heart PPCs and should not be used to deny a patient hepatic surgery.
disease?; history of congestive heart failure?; history of cerebro- There are two subsets of obese patients: One group is “the
vascular disease?; diabetes mellitus [insulin dependent]?; renal metabolically healthy but obese”; the other group is the “meta-
insufficiency [creatinine > 2]?), to determine if the patient is at bolically unhealthy but obese” (Glance et al, 2010). When an
acceptable risk to proceed to the planned surgery or if there is obese patient has three or more of the following criteria—
the need for further testing prior to surgery or pharmacologic abdominal obesity, increased trigycerides, decreased high-
intervention perioperatively (Neuman et al, 2014). density lipoprotein, elevated cholesterol, hypertension, and
The elderly patient will also have a geriatric assessment to glucose intolerance—the patient has a 2.5 increased incidence
test cognitive function, fall risk, and risk of postoperative of PPCs (Neligan & Fleischer, 2006). Obese patients are at risk
delirium. This assessment also includes advice on medications of suffering from a number of respiratory derangements,
to be used with caution and nonpharmacologic strategies to including obstructive sleep apnea (OSA), obesity-hypoventilation
reduce delirium and analgesics while the patient is in the syndrome, and restrictive impairment. The increase in body
hospital. mass also results in increased oxygen consumption and carbon
In hepatobiliary patients with a history of alcohol abuse, dioxide production. With these issues in mind, it is not surpris-
cardiac assessment needs to stress the evaluation of myocon- ing that acute PPCs are twice as likely in OSA patients (Dindo
tractile function. Two basic patterns of alcohol-induced cardio- et al, 2003). Many patients with OSA are undiagnosed, but
myopathy have been shown: left ventricular dilation with there is a strong relationship between obesity and OSA. The
impaired systolic function and left ventricular hypertrophy with ASA addressed this issue with practice guidelines, including
diminished compliance and normal or increased contractile assessment of patients for possible OSA before surgery and
performance. careful postoperative monitoring for those suspected to be at
risk (Gross, et al, 2006). It is unclear whether screening for
Pulmonary Evaluation OSA will affect surgical morbidity, but it is reasonable to ques-
Despite steady advances in care, patients with respiratory tion obese patients about symptoms that may suggest sleep
disease are still at increased risk for postoperative pulmonary apnea prior to liver surgery. At our institution, all obese patients
complications (PPCs). PPCs continue to rival cardiovascular are given the STOP (Snoring, Tiredness, Observed apnea, high
complications in frequency and severity after hepatic surgery blood Pressure)-Bang (Body mass index, Age, Neck circumfer-
(Kingham et al, 2014). ence, and gender) questionnaire (Chung et al, 2012). Given the
There are many limitations of studies that examine risk association of obesity and OSA with multiple medical
factors for PPCs, but there are some consistent patterns. Impor- conditions—increased risk of venous stasis, pulmonary embo-
tant risk factors for PPCs are the presence of pulmonary disease, lism, hypertension, cerebral vascular accidents, cardiomyopathy,
cigarette smoking, low preoperative arterial oxygen saturation, arrythmias, and ischemic heart disease—the anesthesiologist is
acute respiratory infection during the previous month, age, in a position to have an informed discussion with the patient
preoperative anemia, site of surgery (with upper abdominal, about the increased risk of morbidity and mortality and work
especially near the diaphragm, or intrathoracic surgery being the with other members of the patient’s care team to determine
highest risk), surgery duration of at least 2 hours, and emergency whether any interventions should be initiated before surgery in
surgery (Canet et al, 2010; Warner, 2000). Despite the increased an effort to minimize the risk of complications (Gupta et al,
risk of PPCs in patients with preexisting pulmonary disease, no 2001). Polysomonography is the gold standard for diagnosis of
prohibitive level of pulmonary function has been established for OSA, but it is expensive and a limited resource. The most
which surgery is contraindicated. Neither abnormal pulmonary reasonable approach is to check room air-pulse oximetry. If the
function testing or arterial blood gas analysis are useful in patient has an oxygen saturation level less than 96%, further
predicting risk. Thus these tests are only justified as part of an evaluation is warranted. A 2-week period of continuous positive
effort to optimize preoperative pulmonary status, either with an airway pressure (CPAP) therapy has been shown to be effective
immediate perioperative course of systemic corticosteroids or in correcting abnormal ventilatory drive and improving cardiac
antibiotics, or to advise if surgery should be delayed (McAlister function (Loadsman et al, 2001).
et al, 2003). Submaximal cardiopulmonary exercise testing is a After liver resection, the risk of venous thromboembolism
noninvasive objective test that measures a patient’s anaerobic (deep vein thrombosis, pulmonary embolus) is not insignificant
threshold. Poor functional capacity and especially low anaerobic and is higher in the obese patient. Prophylaxis is not routine
threshold has been associated with a high risk of postoperative for these patients after major hepatectomy due to the concern
complications and death (Older et al, 1999). This test is expen- that the risk of bleeding may outweigh the benefit of pharma-
sive; however, patients with low subjective functional capacity cologic prophylaxis, as well as the misconception that after
426 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
anesthetic volatile hepatotoxicity is not a significant concern concentration is little changed after passage through the liver
(Elliot et al, 1993). and depend on the intrinsic clearance (liver size, total enzyme
capacity) of the liver. The elimination of drugs with a low-
Hemodynamics extraction rate (benzodiazepines) depends more on the meta-
Volatile anesthetics reduce HBF in a dose-dependent fashion bolic capacity of the liver and less on the hepatic blood flow.
by affecting cardiac output and systemic pressure. Isoflurane In patients with impaired liver function, such drugs experience
has been considered the agent of choice in cases in which a prolonged length of activity with no increase in peak levels.
preservation of splanchnic blood flow is required. Liver blood The safety of IV anesthestic agents and muscle relaxants is
flow and the hepatic artery buffer response are maintained uncontested, yet, increasingly, anesthesiologists prefer agents
better in the presence of isoflurane than with any other volatile that are not influenced by liver function or using multiple drugs
anesthetic agent (Berendes et al, 1996a). In addition, isoflurane for the same effect despite liver dysfunction. Although the use
is shown to attenuate the increases in hepatic oxygen consump- of opioids is appropriate during liver surgery and the manage-
tion associated with surgery and liver manipulation. Desflurane ment is similar to other abdominal surgery, remifentanil, a short
is shown to have no deleterious effects on liver function and rapidly acting opioid, given by continual infusion and metabo-
hepatocyte integrity. Desflurane anesthesia is associated with lized by plasma esterases, is gaining in popularity over fentanyl.
significantly greater gut blood flow than equipotent isoflurane. The muscle relaxants atracurium and cisatracurium both
This difference cannot be explained by systemic hemodynamics undergo Hoffman degradation and ester hydrolysis, of which
alone. There is no difference in total hepatic flow between neither is dependent on liver function. Dexmedetomidine, an
isoflurane and desflurane groups, however, implying that an α2-agonist, and ketamine do depend on hepatic function;
intact hepatic arterial supply buffers response with desflurane however, perioperatively, their weak analgesic effects decrease
(O’Riordan et al, 1997). Sevoflurane seems to be similar to the minimum alveolar concentration of volatile vapors and the
isoflurane and desflurane with a few exceptions. Indocyanine postoperative opioid requirements (De Kock et al, 2001; Lin
green clearance is better preserved during sevoflurane anesthe- et al, 2014).
sia. Sevoflurane seems similar to isoflurane in its effect on
regional hepatic blood flow (Ebert et al, 1995). Epidural Anesthesia (EDA)
Nitrous oxide is used extensively in patients with hepatic Hepatic resection is performed under general anesthesia with
disease. It is not shown to contribute to hepatic disease exac- or without thoracic epidural block. The epidural block may be
erbation (Lampe et al, 1990). The sympathomimetic effects of used intraoperatively or solely to provide postoperative analge-
nitrous oxide decreases HBF. sia. Its benefit-to-risk ratio is controversial due to the role the
liver plays in the postoperative coagulation cascade (Matot
Intravenous Anesthetics and Muscle Relaxants et al, 2002) and the possibility that EDA may drive increased
Inhaled anesthetics supply all the aspects needed for anesthesia fluid therapy and transfusion (Page et al, 2008). Studies do not
in one package, but today most anesthesiologists choose mul- support the routine use of EDA and epidural analgesia (EPA),
tiple drugs to reach their goals: immobility, amnesia, suppres- rather than general anesthesia and parenteral analgesia, to
sion of autonomic reflexes, muscle relaxation, and analgesia. prevent postoperative mortality (Park et al, 2001; Rigg et al,
Over the last several decades, dramatic advances have been 2002; Wijeysundera et al, 2008). Nonetheless, enthusiasts
made in IV anesthesia, with the result that total IV anesthesia point out that there may be several other advantages to regional
is now a workable alternative to the traditional inhalation anesthesia, especially when combined with postoperative EPA:
anesthetic. Anesthesiologists using multiple drugs take advan- better pain control, attenuation of the stress response, decreased
tage of the interactions of drugs with different mechanisms of requirement of volatile anesthetics, and a reduction in the need
action but similar therapeutic effects. The therapeutic goal of for perioperative opioids.
the anesthetic can often be achieved with less toxicity and faster Perhaps the strongest arguments for the use of thoracic EDA
recovery than when the individual drugs are used alone in for liver surgery is its possible modulation of the immune
higher doses. response and its possible effect on tissue microperfusion (Sinis-
The liver plays a major role in biotransformation, the process calchi et al, 2015). Preclinical data, animal studies, and retro-
through which drugs are broken down into metabolites that can spective reviews demonstrate the potential for a decreased
be more easily eliminated. The main mechanisms that affect recurrence rate in some cancer types. Animal studies have
hepatic elimination of a drug are changes in HBF and changes shown that EDA could have an important role in modifying
in the ability of the liver cells to biotransform a drug for excre- tissue microperfusion and protecting tissue from ischemic
tion. These two mechanisms, hepatocyte function and HBF, damage, regardless of the effects on hemodynamics. The notion
have an important role in the choice of anesthetics for patients that anesthesiologists may be able to impact the short-term and
undergoing hepatobiliary surgery because even small changes long-term outcome for a cancer patient simply by incorporating
in liver function or blood flow can change the concentrations regional anesthesia is appealing, although unproven, and more
of drugs and their metabolites. High-extraction drugs (ket- prospective randomized research is needed.
amine, flumazenil, morphine, fentanyl, sufentanil, lidocaine)
are directly related to liver blood flow and essentially cleared SPECIAL ANESTHETIC CONSIDERATIONS
as they pass through the liver. Protein binding, enzymatic
induction, intrahepatic shunting, and the effect of anesthetics Anesthesia for Hepatectomy
on liver blood flow may affect the elimination of drugs with a For hepatic resection, a relationship between extent of intraop-
high-extraction rate. Reductions in metabolic clearance result erative blood loss and mortality and morbidity has been con-
in increases of peak drug level with minimal change in the sistently shown (see Chapter 103). To minimize blood loss, it
elimination half-life. Low-extraction drugs are those whose is common anesthesia practice to perform liver resections with
Chapter 24 Intraoperative and immediate postoperative management 429
and the use of dynamic parameters of fluid responsiveness allow blockade, systemic hemodynamics, or even the circulating
the use of protocolized GDT strategies. Functional hemody- effects of local anesthetics. Splanchnic veins, with their higher
namic parameters provide a numeric representation of the density of α-adrenergic receptors, play the main role in main-
patient’s fluid responsiveness and are more reliable than using taining a ratio between stressed (Vs) and unstressed blood
standard static parameters, such as blood pressure, heart rate, volume (Vu) (Gelman, 2008). Vu is hemodynamically inactive,
urine output, or even CVP (Auler et al, 2008). A recent meta- but when venoconstriction changes it, this is equivalent to a
analysis supports GDT for patients having abdominal surgery, transfusion of a significant amount of blood. Controlled ventila-
to improve postoperative recovery and decrease complication tion and EDA both decrease venous return (VR) and must be
rates (Pearse et al, 2014). Liver surgery exposes patients to associated with an increase in Vs to maintain hemodynamics.
periods of cardiovascular insufficiency, either because of Decreased Vs and VR can be restored by fluid infusion to fill
anesthesia-induced loss of vasomotor tone and baroreceptor up the increased venous capacity or by an α-agonist to increase
responsiveness or because of blood loss and mechanical sympathetic tone of the compliant veins, which robs from Vu
obstruction to blood flow. In all cases, stroke volume will fall to give to Vs. The clinical advantage of using a vasopressor is
as well as global oxygen delivery to the tissues. GDT is targeted that it maintains tissue blood flow but avoids fluid infusion.
to detect hypovolemia and hypoperfusion early (at or before However, a clinician who practices LCVP should realize that
anesthetic induction) to be proactive to avoid hypoperfusion. this approach might decrease the margin of safety. Low Vu per
Early proactive GDT may compromise the effectiveness of se is not harmful. Up to 1000 mL of blood may be lost without
LCVP on decreased blood loss. Although most liver surgery change in standard hemodynamic parameters. However, beyond
does not result in profound tissue hypoperfusion, some degree this point, when the mobilization of blood from Vu to Vs is
of hypoperfusion does occur with the Pringle technique, adding approximately complete, even minor reduced VR, whether by
tissue perfusion injury before resuscitation. There is presently the Pringle technique, vena caval compression, or blood loss,
no approved treatment for ischemia reperfusion injury (IRI), can quickly lead to hemodynamic deterioration. Vasopressors
the inflammation that occurs when blood flow is returned to during LCVP-assisted liver surgery are certainly justified;
healthy liver tissue after diseased tissue has been surgically however, it may delay recognizing dangerous hypovolemia.
removed. IRI can harm the vascular barrier, in particular the On the other hand, if fluid is infused to counteract the
endothelial glycocalyx (Chappell et al, 2014), and results in hemodynamic effects of EPA this may lead to excessive hydra-
part from the deposition of complement, a protein that kills tion and increased packed RBC transfusion after hepatectomy
liver cells and impairs regeneration (Chappell et al, 2014). (Page et al, 2009). The liver is the only organ to have regional
Because surgery also creates a cytokine storm, the combination blood flow monitored by the autonomic nervous system, and
of relative hypoperfusion and immune modulation will alter the whether the effects of an epidural on perfusion pressure may
microcirculation, causing subclinical damage. Whether GDT be reversed by vasopressors is unclear, as well as the influence
for liver surgery can rescue patients from this insult is unknown. of EDA on fluid balance.
GDT has been shown to be effective when combined in an
enhanced recovery after liver surgery (ERAS) program (Hughes Air Embolus
et al, 2014; Jones et al 2013). A recent randomized trial for The goal of keeping a low central pressure to minimize back
hepatic surgery at our institution showed intraoperative GDT bleeding from the liver sinusoids during transection must be
was a safe technique, allowed for less intraoperative fluid, but counterbalanced by a central pressure that minimizes the risk
did not influence overall 30-day morbidity. The optimal peri- of air entrainment. The risk of intraoperative air emboli is likely
operative fluid resuscitation strategy for liver resections remains to increase under LCVP anesthesia. Elimination of nitrogen
undefined. from the anesthetic gas mixture is necessary to permit expira-
tory nitrogen monitoring for air emboli. Restriction of nitrous
Low Central Venous Pressure: Epidural Anesthesia oxide in the gas mixture prevents the diffusion-mediated
EDA may be used to provide LCVP conditions during hepatic increase in the size of circulating air. Transesophageal echocar-
surgery (Feltracco et al, 2008; Jones et al, 2013). Despite many diography can be used to monitor air emboli, but this technol-
animal and human studies, the effects of thoracic EDA on HBF ogy is sensitive and overdiagnoses clinically insignificant events.
are not entirely clear. An early study using the indocyanine At our institution, during open hepatectomy, surgical and
green plasma disappearance rate revealed that EDA resulted in anesthesia vigilance and communication are the keys to detect
a decrease in mean arterial pressure and HBF (Kennedy et al, and treat air emboli. With surgical watchfulness and rapid
1971). Another study using indocyanine green and EDA con- occlusion of open venous channels, and our monitoring of
cluded that maintaining normotension with volume infusion end-tidal carbon dioxide and hemodynamics, LCVP anesthesia
does not reverse its hemodynamic effect; however, the decrease results in a low incidence of clinically significant air emboli.
in flow is reversed by dopamine (Tanaka et al, 1997). Patients
treated with norepinephrine to compensate for the EDA- Bloodless Surgery: Blood Conservation, Transfusion
induced decrease in arterial blood pressure had an additional The anesthesiologist not only has a pivotal role in reducing
marked decrease in HBF (Meierhenrich et al, 2009). blood loss during hepatic surgery but also contributes to intra-
Subsequently, these studies have been shown to oversimplify operative blood conservation and controls transfusion protocol.
the numerous factors affecting HBF: hemodynamics, auto- Transfusion-free surgery, better known to the public as blood-
nomic nervous system, circulating neurohumoral agents, and less surgery, can only be achieved by the application of blood
local metabolites (adenosine). Today it is accepted that this management techniques to decrease allogeneic transfusion.
multiplicity of regulatory mechanisms provide overlapping The three pillars of blood conservation are (1) build up the
controls to maintain tissue perfusion (Siniscalchi et al, 2015). patient’s own blood, (2) reduce blood loss, and (3) recycle the
EDA can interfere with all these factors either by sympathetic patient’s own blood (Spahn & Goodnough, 2013). The liver
Chapter 24 Intraoperative and immediate postoperative management 431
anesthesiologist should be familiar with recycling techniques, (Kooby et al, 2003). Patients receiving only autologous blood
intraoperative RBC salvage and hemodilution, maneuvers that or spared-blood transfusion from ANH also did not have better
may contribute to reduced allogeneic RBC transfusion in disease-free survival (Correa-Gallego et al, 2015; Kooby et al,
major liver surgery. Autologous RBC salvage (intraoperative 2003). Postoperative complications, especially infectious and
autotransfusion) involves recovery of the patient’s shed blood other tumor-related factors, such as tumor-infiltrating lympho-
from a surgical wound, washing or filtering, and reinfusion of cytes, are more dominant determinants of long-term cancer
the blood into the patient. Hepatectomies often are performed survival (Khan et al, 2014). The magnitude of operative blood
for cancer. Cell salvage had been excluded in oncologic surgery loss during resection of HCC was found to be a predictor of
because of the concern for potential dissemination of cancer recurrence and survival rates; however, the blood loss was
cells, but the availability of leukocyte-depleting filters allows its found to be related to tumor characteristics and extent of
use during cancer surgery. Another transfusion-sparing tech- surgery (Katz et al, 2009). RBC transfusions are indisputably
nique is acute normovolemic hemodilution (ANH). ANH is a associated with an increase in mortality and morbidity in liver
recycling technique that can be performed intraoperatively by surgery; however, transfusion may be a surrogate marker of one
the anesthesiologist. Blood is removed from the patient after or more other variables that is more directly related to the
induction and replaced with crystalloid or colloid fluid. The complication.
removed blood is stored at room temperature in the operating
room and is returned to the patient at the conclusion of the Minimally Invasive Liver Resection
operation. Two randomized studies of ANH in major hepatic Anesthesiologists continually adjust strategies as innovative
resection showed a significant reduction in the percentage of surgical techniques evolve. The benefits of laparoscopic liver
patients requiring allogeneic RBC transfusion (Jarnagin et al, resection (LLR) have been associated with less blood loss and
2008; Matot et al, 2002). Tolerance of normovolemic anemia earlier postoperative recovery (Ito et al, 2008), although all of
is important, and care must be taken not to confuse the the comparisons reported are retrospective and therefore asso-
momentary helpful effect of RBC transfusion on hypotension ciated with a huge selection bias. Pneumoperitoneum induces
and hypovolemia with an outcome benefit. A restrictive predictable pulmonary and renal responses as well as phasic
approach to blood transfusion with a threshold of 7 g/dL has hemodynamic changes. Intraperitoneal insufflation and head-up
been shown to reduce blood use and not cause harm in criti- tilt result in impairment of HBF secondary to decreases in
cally ill patients (Holst et al, 2014), as well as in liver resection cardiac output (Berendes et al, 1996b; Eleftheriadis et al,
patients (Wehry et al, 2015). 1996). In well-selected patients, the consequences of these
In a recent review, Kingham and colleagues reported that changes are not relevant. However, the challenges of the effect
transfusions have decreased by 50% over 2 decades, but peri- of pneumoperitoneum, positioning, and mechanical ventilation
operative blood loss and transfusion remain associated with on cardiopulmonary function in addition to longer surgical time
morbidity. Cannon and colleagues (2013) specifically showed may not be the correct choice for every patient. Before position-
that transfusion with packed RBCs was associated with post- ing, the patient should be prepared the same as for an open
operative complications in patients undergoing hepatectomy. case, including the ability to do large-volume transfusion in
The correlation of transfusion with complications should not case inadvertent major vessel bleeding occurs. A protocol
be interpreted as a direct cause and effect relationship; instead, should be in place as well as a fully open instrument tray and
what is important is the fact that patients having liver surgery equipment available in case the robot must be undocked emer-
receiving very few units of blood transfusion nevertheless gently to convert to open surgery. It is important that the
have higher complication rates (Kooby et al, 2003). There are anesthesiologist and surgeon have a discussion before the start
increased infectious complications in those transfused: The of the laparoscopic or robotic liver case because the risk versus
more transfusions that are done, the higher the rate of total benefit of LCVP-assisted hepatic resection is less clear.
complications and infectious complications (Page et al, 2009). The pneumoperitoneum compresses the portal vein, reduces
The cause is not known, but one possible mechanism proposed portal blood flow, and seems to reduce hepatic back bleeding
is “transfusion-related immunomodulation” (Vamvakas et al, during transection. Decreasing blood loss for open resection is
2014). Patients who have received a blood transfusion stored based on keeping the radius of an inadvertent venous injury
29 days or more have twice the rate of infections. A hypothesis small and the pressure head low so that less blood will be lost
is that as stored RBCs break down, they release cytokines that through the opening. However, retractions can tort vessels and
can lower immune function (Vamvakas, 2002). One could actually stent them open during LLR. Fluid management is
hypothesize that by reducing transfusion, complications would complicated by compromised hemodynamics resulting from
also be reduced. A prospective trial of ANH reduced RBC positioning and decreased lung compliance. Renal parenchyma
transfusion but did not reduce morbidity (Jarnagin et al, 2008). and venous compressions during pneumoperitoneum are the
Most liver surgery is performed for cancer, and studies have etiology of oliguria during LLR. The effects are reversible
examined the association of cancer progression and RBC and usually cause no harm. Yet, many anesthesiologists prefer
transfusion for primary and metastatic cancer. Because it was to optimize intravascular volume to minimize the effects of
reported in the journal Anesthesiology that blood transfusion in intraabdominal pressure (IAP) on renal and cardiac function.
rats promoted cancer progression (Atzil et al, 2008), there has The issue of gas embolism (GE) during LLR is still debated.
been a perception that an anesthesiologist’s choice to transfuse Some authors consider it little or no problem, and some con-
RBCs can influence long-term survival. Human studies have sider it a real threat to patient safety (Min et al, 2007). The
not supported animal studies. A retrospective reivew of 1300 debate centers on the theory that GE occurs when the IAP
hepatectomy patients with metastatic colorectal cancer reported exceeds CVP (Eriksson et al, 2011). The opposite situation,
the major effect on survival is in the immediate postoperative when CVP exceeds IAP, does not prevent GE because it can
period, but transfusion did not predict long-term survival occur irrespective of whether CVP is greater or less than IAP
432 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
may ameliorate the first two mechanisms but not the third, and Particular attention must be paid to anesthetic elimination
significant decrements in pulmonary function may still be and residual drug effect, especially sedative, analgesic, and
observed after laparoscopic surgery. neuromuscular blockers, in posthepatectomy patients who have
ACPs play a key role in the prevention of PPCs. Preoperative altered drug pharmacodynamics and pharmacokinetics. In a
preparation, intraoperative management, and immediate post- recent prospective cohort study, the use of intermediate-acting
operative care can have a major impact on the occurrence of neuromuscular blocking agents was associated with postopera-
this morbidity. It has long been known that the induction of tive desaturation (90%) and reintubation, regardless of train-
general anesthesia, both total IV anesthesia and inhaled anes- of-four monitoring and use of reversal agents (Grosse-Sundrup
thesia, decreases lung volume and promotes dependent zone et al, 2012). In a cohort of 33,769 surgical cases, planned
atelectasis (Putensen et al, 2009; Serpa Neto et al, 2012). To reintubation within the first 3 days after surgery was associated
improve oxygenation, ACPs apply a high tidal volume (TV) and with a 72-fold increased risk of in-hospital mortality (Brueck-
high fraction of inspired oxygen (FiO2). High FiO2 via absorp- mann et al, 2013).
tion atelectasis has also been linked to the development of The findings of a recent systematic review and meta-analysis
atelectasis during the postoperative period (Edmark et al, suggest that the use of early CPAP for the prevention of hypox-
2003). After liver surgery, like all abdominal surgery, this emia after abdominal surgery may reduce the incidence of
impaired oxygenation caused by intraoperative atelectasis per- PPCs compared with just supplemental oxygen (Ferreyra et al,
sists for days after the surgical procedure (Duggan et al, 2005). 2008).
An association, but not a causal effect, of atelectasis and PPC Anticipated respiratory compromise after liver surgery in
has been reported (Milic-Emili et al, 2007). There is experi- patients without an epidural may preclude early extubation,
mental work that links atelectatic areas of the lung to transloca- especially in combination with any baseline abnormality in gas
tion and increased bacterial growth, providing an optimal nidus exchange. If a patient must be placed on mechanical ventila-
for infection (Van Kaam et al, 2004). Regardless of the etiology, tion, diaphragmatic weakness, atrophy, and respiratory muscle
PPCs increase 30-day mortality (Canet et al, 2010). fatigue can occur within hours. Similar to all muscles, complete
The use of high TV (10 to 15 mL/kg) ventilation, encour- rest can lead to diaphragm atrophy, and modes that allow
aged to prevent atelectasis, results in high peak ventilatory patient triggering, such as assist-control ventilation are neces-
airway pressure, which has been shown to be associated with sary to maintain diaphragm muscle function (Powers et al,
acute lung injury (Fernandez-Perez, et al, 2009). Low TV 2008).
ventilation (TV 6 to 8 mL/kg ideal body weight) with positive
end-expiratory pressure (PEEP) (6 to 8 mm H2O) and recruit- Venous Thromboembolism
ment maneuvers every 30 minutes (lung protective ventilation) Patients having cancer surgery have a moderate risk for venous
has demonstrated reduced mortality in patients with acute thromboembolism (VTE) (Agnelli et al, 2006; Alcalay et al,
respiratory distress syndrome and decreased PPCs in patients 2006; Catheline et al, 2000). Guidelines recommend low-
at risk of PPCs after abdominal surgery (Futier et al, 2013). molecular-weight heparin for patients undergoing general
Yet, most anesthesiologists decrease TVs without the addition surgery procedures with at least moderate (3%) risk of VTE, if
of PEEP or respiratory maneuvers (likely because of their the risk of bleeding does not negate the risk of VTE (Gould
effects on hemodynamics), which in a large retrospective cohort et al, 2012). After major hepatectomy, the concern for postop-
may have lead to increased mortality (Levin et al, 2014). The erative bleeding, combined with an erroneous presumption of
authors speculated that this was increased atelectasis from protection due to the coagulopathy, often preclude the use of
lower TV ventilation. Lung protective ventilation is being routine prophylaxis despite evidence to the contrary (Tzeng
proposed as a standard of care to be bundled into ERAS or et al, 2012). In a recent retrospective review at our institution,
perioptimal care to further decrease the incidence of PPCs and postoperative VTE occurred in 2.6% of patients and was
serve as a measure of the quality and safety of care. The liver independently associated with higher postoperative interna-
ACP must weigh the evidence for lung protective ventilation tional normalized ratio (INR) and LWMH had no relationship
and the effect of high PEEP and respiratory maneuvers on to VTE incidence or bleeding complications (Nathan et al,
decreased venous return or liver congestion on a patient-by- 2013). Patients with more extensive liver resections and higher
patient basis. operative blood loss had a higher incidence of VTE. Despite an
Postoperative respiratory failure is most commonly defined elevated INR and lower platelet count, a patient having major
as the need for mechanical ventilation for more than 48 hours liver cancer surgery is in a normocoagulable or even a hyper-
or unplanned postoperative reintubation. The nature and coagulable state and at risk for venous thromboembolism; yet
magnitude of the preexisting respiratory conditions determine there is no consensus of opinion for pharamacologic prophylaxis
the effect of a given standard anesthetic on respiratory function. (Barton et al, 2013).
The ACP plays a key role in the prevention of respiratory
muscle-related PPCs. In patients with obstructive lung disease, Liver Dysfunction (See Chapters 79 to 81)
high airway resistance favors deep slow respiration, which may Jaundice
not be possible in patients with large abdominal incisions. The Liver regeneration after partial hepatectomy involves rapid cell
treatment of this pain with opioids will reduce minute ventila- division of 24 to 72 hours and can be characterized by signifi-
tion and respiratory drive. A meta-analysis of patients undergo- cant changes in cellular phosphorus metabolism (Zakian et al,
ing thoracic and abdominal surgery showed that the odds of 2005). Standard therapy for posthepatic resection should
developing postoperative pneumonia was reduced nearly 50% include the supplementation of IV fluids with potassium phos-
in patients receiving epidural versus IV analgesia, fueling the phate (30 to 40 mmol/day).
controversy of this choice in patients after liver resection Mild jaundice in the early postoperative period after partial
(Popping et al, 2008). hepatectomy is relatively common, particularly in patients who
434 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
undergo a major resection and who have a transient, self- surgery, by itself, is generally unimportant clinically. Even in
limited hyperbilirubinemia in the first few days after operation, the presence of severe hypoalbuminemia, albumin infusion is
which may be exacerbated by hematoma reabsorption and of no beneficial effect. The medical management of ascites
hemolysis of transfused blood. emphasizes bed rest and sodium restriction. If a spontaneous
The portal circulation is valveless: Changes in pressure are diuresis does not occur, therapy is begun with the aldosterone
transmitted across the entire portal circulation, with the large antagonist spironolactone. In patients with ascites, electrolyte
sinusiodal area of the normal liver offering very little resistance abnormalities (hyponatremia, hyperkalemia, hypochloremia,
to portal flow. After hepatic resection, there will be increased and hypokalemia) and contraction alkalosis are commonly
resistance to portal flow until the liver regenerates. Usually, this encountered as a result of the primary process and medical
increase in portal pressure is of little consequence. If the size therapy. If ascites is refractory to medical management, para-
or the health of the remaining liver is not adequate to carry out centesis may offer temporary palliation. If life-threatening
the metabolic functions of the liver, the patient may experience complications such as cardiac or respiratory compromise occur,
small-for-size syndrome, characterized by coagulopathy, cho- these patients require transfer to the intensive care unit.
lestasis, hyperbilirubinemia, and ascites. For these patients, it
is important to maintain HBF and perfusion pressure to avoid Renal Dysfunction
hepatic artery thrombosis, hepatic artery vasospasm, or portal After hepatobiliary surgery, one may encounter rapidly progres-
vein thrombosis. sive renal failure, although this is uncommon (Correa-Gallego
Progressive jaundice that does not resolve portends a more et al, 2015; Melendez et al, 1998) after routine resections. This
significant problem. One suggested definition of postoperative postoperative acute renal failure (ARF) generally resolves when
hepatic insufficiency is a peak bilirubin greater than 7 mg/dL. not correlated with liver failure or multiorgan dysfunction. The
In a cohort of 1059 noncirrhotic patients undergoing hepatic principal differential diagnoses include acute tubular necrosis,
resection, a postoperative bilirubin greater than 7 mg/dL was prerenal azotemia, and hepatorenal syndrome. Postoperative
associated with a 30% chance of dying of hepatic insufficiency renal clinical dysfunction is associated with perioperative trans-
(Mullen et al, 2006). However, in the same cohort, 70% sur- fusions, LOS, other major complications, 30- and 90-day
vived, highlighting the importance of identifying any correctable mortality, larger resections, and age (Correa-Gallego et al,
problem that may be contributing to the hyperbilirubinemia, 2015; Kim et al, 2014).
such as a bile duct injury at the time of surgery, a bile leak, Recently, using a large national database, procedure-specific
infection, or vascular embarrassment to the functioning liver. risk of perioperative acute kidney injury (AKI) for patients
Endoscopic retrograde cholangiopancreatography or imaging undergoing intraabdominal surgery was evaluated (Kim et al,
studies will help in the diagnosis. 2014). The results demonstrated that among patients undergo-
ing intraabdominal surgery, the risk of severe AKI varies con-
Coagulation siderably, depending on the specific procedure. Hepatobiliary
The half-life of coagulation factors is 6 hours, so coagulation procedures (liver and pancreas, elective and emergent) had a
factor deficiency is likely to evolve rapidly. After routine liver 1.8 % incidence of ARF with an adjusted risk of 1%. The
resections, a transient and self-limited prolongation of pro- authors hypothesized that AKI may be a spectrum of diseases
thrombin time or INR occurs commonly and usually resolves with different causes and consequences that depend on the
without the need for transfusion of fresh frozen plasma (FFP) clinical context in which it occurs. A retrospective review in a
or administration of other agents. Patients undergoing major similar time period, as in the report by Kim and colleagues
liver resection have higher peak postoperative INR (median, (2014), evaluated severe clinical AKI following LCVP-assisted
1.6) and lower nadir platelet count (median, 148,000) within liver resection. Clinically relevant AKI was rare (<1%) and
7 days than patients undergoing lesser procedures (Nathan resolved in half of these patients during a short follow-up period
et al, 2013). Routine parenteral administration of vitamin K (Correa-Gallego et al, 2015). These results are mirrored by
(10 mg/day) commonly corrects the coagulation abnormalities analysis of postoperative morbidity after liver resections (Virani
within 48 hours. More rapid correction may be accomplished et al, 2007). Whereas Kim only had severe end points (creati-
by FFP but is rarely needed unless the INR exceeds 2 or if nine >2, dialysis) to analyze, and may have underestimated the
there are otherwise concerns of ongoing postoperative blood incidence of clinically significant AKI defined by the RIFLE
loss (Martin et al, 2003). If coagulopathy persists, dysfibrino- (Risk, Injury, Failure, Loss of kidney function, and End-stage
genemia should be entertained. kidney disease) criteria, this review analyzed laboratory data
and was able to apply the RIFLE criteria to the incidence
Ascites of biochemical AKI (Correa-Gallego et al, 2015). Although
Ascites (see Chapter 81) manifests as a result of several factors: biochemically defined renal dysfunction was a relatively
(1) impaired albumin and protein synthesis; (2) increased common event (16%) in patients undergoing LCVP-assisted
hydrostatic pressure in hepatic sinusoids and splanchnic capil- liver resection, it was a transient phenomenon, and its clinical
laries; (3) overproduction of hepatic and splanchnic lymph, significance was limited. These results are mirrored by analysis
leading to a transudation of lymph into the peritoneal space; of postoperative morbidity after liver resections (Virani et al,
(4) limited or reduced reabsorption of water and protein by 2007).
peritoneal lymphatics; (5) sodium retention by the kidney There is no standard definition of ARF, but common criteria
secondary to hyperaldosteronism, increased sympathetic stimu- are either biochemical (a rise in serum creatinine of 50 μmol/l,
lation, and alterations in metabolism of prostaglandins and or of 50% from baseline, or beyond a set level, for example,
kinins; and (6) impaired renal water excretion, partially >500 μmol/l), or clinical (oliguria with urine output <400 ml/
owing to increased concentrations of antidiuretic hormone. The day), a combination of both, or the need for renal replacement.
decreased serum albumin 1 to 2 weeks after hepatobiliary A recent development is the RIFLE classification, which seeks
Chapter 24 Intraoperative and immediate postoperative management 435
to standardize definitions of ARF based on a combination of group of anesthesiologists, surgeons, and surgical scientists that
biochemical and urine output criteria. recommend optimal postoperative pain management that is
The incidence of biochemical bARF is not in and of itself specific for different surgical procedures, as well as arguments
an argument against the use of LCVP anesthesia for liver resec- for and against the invasiveness of the analgesic technique and
tions. Some permissive, clinically relevant renal dysfunction is the consequences of pain on outcome (Neugebauer et al,
a very uncommon event in this patient population, and it is 2007). Hepatic surgery is not represented, and what operation
consistent with published literature regarding other types of is transferable is unclear.
major operations (Bihorac et al, 2013). The evidence does not The most commonly used incisions are subcostal or midline,
support LCVP-assisted liver surgery increasing the incidence with significant cephalic retraction of the chest wall. Therefore
of significant AKI. the patient’s pain is more similar to a postthoracotomy patient’s
pain. For postoperative pain after liver surgery, acute pain treat-
Glucose Metabolism ment services primarily offer thoracic EPA with dilute local
Glucose deprivation leads to hepatic glycogenolysis to maintain anesthetics, with the premise that neuraxial delivery of drug will
normoglycemia. After glycogen stores in the liver are exhausted result in equivalent or improved analgesia at doses much lower
(12 to 24 hours), the liver must synthesize glucose from than would be required by systemic delivery. Although thoracic
other substrates (gluconeogenesis). The hormones, insulin, EPA provides superior pain relief for thoracoabdominal opera-
glucagon, and epinephrine are important modulators of these tions (Joshi et al, 2008) and reduces PPCs (Popping et al,
processes. On balance, the postoperative patient would seem 2008), the risk versus benefit of an indwelling catheter with
to be prone to hypoglycemia secondary to diminished glycogen EDA for liver operations is debatable because of possible
reserves, increased insulin levels, and impaired gluconeogenesis, changes in postoperative coagulation. In addition, the number
but dangerous hypoglycemia is rare, and its presence must raise one complication following hepatectomy is abdominal infec-
the suspicion of acute hepatic failure. In most resections, iso- tions, with PPCs less common than thoracic surgery and result-
tonic saline solutions without dextrose can be used during the ing more from the act of surgery (pleural effusion or bile leak)
first 12 to 24 hours after resection, following which routine than the patient’s comorbidity. An elevated INR or decreased
dextrose solutions should be ordered and glucose levels platelet count can influence the timing of the removal of the
monitored. catheter because of a theoretical risk of spinal hematoma (Sinis-
calchi et al, 2015). In recent years, bloodless hepatic surgery,
Analgesia the known hypercoagulable state despite elevated INR and
After hepatic resection, most patients are extubated in the decreased platelet counts, and the safety of an indwelling cath-
operating room. Until recently, it was tacitly assumed that eter in other surgeries in patients who undergo anticoagulation
postoperative pain was essentially the pain of inflammation postoperatively allows reevaluating the modern age risk versus
plus, perhaps, some direct pain from cutting nerves. Subse- benefit in patients undergoing liver resection. There are no
quently, it has been demonstrated that there are important clinical guidelines as to the safety of epidural use in the patient
differences between pain from surgery and pain from inflam- for liver surgery. The guidelines for the placement and removal
mation (Brennan, 2005). More important from a clinical per- of neuraxial analgesia in patients with coagulation defects out-
spective, some drugs are effective to treat either surgery pain or lined by the American Society of Regional Anesthesia (ASRA)
inflammation, such as opioids, whereas others are unique to the apply to hepatic resection as well (Apfelbaum et al, 2012).
setting. A better understanding of the pain pathways and the Recently, basic science and retrospective reviews have sug-
concerted effort by ERAS to shorten and uncomplicate hospital gested that the anesthetic management during cancer surgery
stay, especially in the older patient, has drawn attention to the may influence the patient’s long-term survival. There are several
success of multimodality analgesia. Postoperative pain manage- multicenter prospective trials underway to examine whether the
ment has evolved considerably from the use of parental or use of regional anesthesia can truly decrease cancer recurrence.
neuraxial opioid monotherapy to multimodal opioid-sparing What is perhaps the most intriguing and an immediate hypoth-
analgesia. Today’s menu includes nonsteroidal antiinflammatory esis for liver surgery is whether EDA can improve immune
drugs/cyclooxygenase-2 inhibitors, local anesthetics, N-methyl- function and increase resistance to postoperative infection.
D-aspartate antagonists, α2-antagonists, thoracic epidural Surgical stress and pain may induce lymphocyte depletion,
catheters, IV patient-controlled analgesia, and catheters for the which may be associated with the risk of postoperative infec-
incisional wound (White & Kehlet, 2010). tious complications. Although circulating cytokines related to
Although opioids have stood the test of time to anchor monocyte activation and phenotype alterations are not influ-
postoperative pain, these drugs, whether infused epidurally or enced by postoperative pain reduction compared with systemic
parentally, are not without adverse effects; consequently, tar- opioid treatment, there has been evidence in animals that EPA
geted multimodality opioid-sparing analgesic algorithms are influences lymphocyte distribution, increases the postoperative
being proposed. These algorithms may not be safe for patients CD4/CD8 ratio and B cells, and decreases natural killer cells.
having hepatic surgery; instead, choices must be based on an This preservation of immunity has not been shown in human
individual basis, given the liver’s role in drug biotransformation studies (Cata et al, 2013) (see Chapter 11). EDA combined
and coagulation. with EPA has been shown to significantly reduce the amount
of postoperative inflammatory response of patients by altering
Epidural Analgesia the circulating leucocyte surface molecules CD11b and CD62L
The ASA postoperative evidenced-based pain management (L-selectin), which are known to be more sensitive markers of
guidelines are generalized and can be confusing when adapted the early detection of postoperative stress response inflamma-
to liver surgery. The web-based PROSPECT (Procedure- tory markers (Chloropoulou et al, 2013). If there is an attenu-
SPECific Postoperative Pain ManagemenT) is a collaborative ated neutrophil adhesive capability by EDA/EPA, and if this
436 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
improves patient resistance to infection, this may be more better pain relief, avoidance of polypharmacy, and good nutri-
important for liver surgery than for other types of surgery tion, but from a prevention or therapeutic point of view, there
because of the role that the liver plays in the immune and is no one target for decreasing the incidence after surgery.
inflammatory process. Ketamine is an anesthetic that has been used for 50 years, and
new research has shown that even in low doses intraoperatively,
Intraabdominal Infection in addition to regular anesthesia during surgery, it may reduce
Abdominal infections are the most common complication of the risk of delirium (Khan et al, 2015).
modern liver surgery (Kingham et al, 2014). Postoperative Encephalopathy is usually graded using the West Haven
complications in cancer patients with liver resections have been criteria for encephlopathy (Ferenci, 2013). This tries to semi-
shown to reduce disease-free survival and disease-specific sur- quantitate the grading of a patient’s mental status, as it pro-
vival (Ito et al, 2008). The mechanism is unknown, but peri- gresses from a trivial lack of awareness to lethargy, confusion,
operative inflammation and infection are a current theory. and coma. Clinically, a sudden change in a patient’s mental
Postoperative bilirubin, blood loss, transfusion, major hepatec- status or the onset of asterixis, a flapping tremor related to loss
tomy, and hepatectomy combined with a colon resection have of extensor tone, is a sign of hepatic insufficiency and should
all been shown to be associated with complications. Complica- precipitate a search for the cause and the start of therapy for
tions, especially infections, are powerful predictors and a pos- hepatic encephalopathy. Any number of perioperative factors,
sible cause of adverse disease-specific survival (Correa-Gallego including gastrointestinal bleeding, infection, drugs, diet, and
et al, 2015; Ito et al, 2008). A common condition causing a dehydration can precipitate hepatic encephalopathy (Sladen,
low-flow state to the liver is sepsis. Biliary manipulation and 2008). The exact pathogenesis of hepatic encephalopathy is
placement of biliary stents, culture-positive bile, retained gall- unknown. Accumulation of endogenous ammonia is associated
stones, ascites, blood loss, and transfusion all may predispose with the onset of encephalopathy and has been suggested as
to abdominal infection. Patients undergoing hepatic resection causative; however, it is only a marker of disordered protein
for hilar cholangiocarcinoma are at particular risk for postop- metabolism. In an acidic milieu, ammonia gains a hydrogen ion
erative infective complications. Preventing a hospital-acquired to become ionized ammonium (NH4+), which cannot cross lipid
infection is always better than treatment. membranes and enters the central nervous system (CNS). In
Initial treatment of abdominal infections falls under the an alkalotic milieu, ammonium loses the hydrogen ion to
domain of the interventional radiology. Ultrasound and CT are become ammonia, which, as it is nonionized, freely crosses lipid
used to locate collections that are then drained percutaneously, membranes and enters the CNS. Ammonia plays an important
often without sequelae (see Chapter 27). Radioisotopes that role in the development of cerebral edema because astrocytes
attach to white blood cells and glucose and can display high take up ammonia produced by bacteria in the bowel and convert
metabolic demand (biologic imaging) are on the horizon to be it into glutamine, which has considerable osmotic activity.
used in the future for identifying an abdominal collection. Ammonia also causes additional changes in neurotransmitter
synthesis and release, mitochondrial function, and neuronal
Delirium: Encephalopathy oxidative stress (Norenberg et al, 2014). Standard therapy is
Delirium (temporary inability to focus attention and think designed to reduce levels of ammonia and other potentially
clearly) occurs in one out of five older patients who undergo toxic metabolites. Metabolic alkalosis associated with potas-
major surgery. Delirium is associated with a slower recovery sium chloride should be corrected. Decreasing absorption of
and a poorer outcome, and a vicious circle may be initiated gut protein by using oral lactulose or rifaximin is preferred to
(delirium, physical restraint, and medication to treat delirium; dietary protein restriction, which may complicate wound
postoperative complications; then more delirium). Our hospital healing (Mas et al, 2003).
has a daily protection and intervention program based on early-
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CHAPTER 25
Perioperative critical care in
hepatopancreatobiliary patients
Louis P. Voigt, Stephen M. Pastores, and Neil A. Halpern
437
438 PART 3 ANESTHETIC MANAGEMENT, PRE- AND POSTOPERATIVE CARE
CTP 5-15 + + + + + −
MELD 6-40 − − − + + +
CTP, Child-Turcot-Pugh; MELD, Model for End-stage Liver Disease; PT-INR, prothrombin time–international normalized ratio.
surgery and may not confer postoperative resistance to warfarin extrahepatic procedures in patients with HPS is associated with
(Woods et al, 2007). increased perioperative risk (Mazzeo et al, 2004). A preopera-
Recent studies and analyses have failed to establish a clear tive partial pressure of oxygen in arterial blood (PaO2) of
correlation between an increased risk of hemorrhage and a 50 mm Hg or a macroaggregated albumin scan quantification
prolonged PT or activated partial thromboplastin time (aPTT) shunt fraction of 20% or higher is associated with prohibitive
(Tripodi & Mannucci, 2011). In the absence of bleeding, mortality rates from cardiorespiratory complications (Arguedas
routine fresh frozen plasma (FFP) transfusions to correct pro- et al, 2003).
longed PT-INR and aPTT are no longer advocated because of Portopulmonary hypertension is an integral component of
better understanding of the coagulation paradigm in liver cir- HPS and predisposes to intraoperative cardiac arrhythmias and
rhosis (Monroe & Hoffman, 2009; Northup & Caldwell, 2013). cardiac arrest (Porres-Aguilar et al, 2012). Mortality of porto-
However, the final decision by the perioperative team is often pulmonary hypertension is high, with 1- and 5-year survival
individualized. Excessive FFP transfusions can lead to volume rates of 54% and 14%, respectively (Swanson et al, 2008).
overload and may exacerbate ascites. Human recombinant acti- Portopulmonary hypertension is often asymptomatic and dif-
vated factor VIIa (rFVIIa) or prothrombin complex concentrate ficult to diagnose. Right side of the heart catheterization helps
is an effective alternative to plasma in patients with acute hem- to determine the various causes of pulmonary hypertension and
orrhage (Pabinger et al, 2008; Romero-Castro et al, 2004), but is the best diagnostic tool for portopulmonary hypertension
their use has not been rigorously tested. Administration of (Krowka et al, 2006). Elective surgery under general anesthesia
cryoprecipitate is advocated when serum fibrinogen levels are in patients with severe HPS-associated pulmonary hyperten-
less than 100 mg/dL in the presence of bleeding (Anderson sion should be deferred until the pulmonary hypertension is
et al, 2013). Data on the benefits of fibrinogen concentrates are controlled with vasodilator agents.
limited to trauma and massive hemorrhage (Fenger-Eriksen
et al, 2008). Transfusion of platelets is recommended before Electrolytes
invasive procedures for moderate thrombocytopenia of less Electrolyte abnormalities are frequent in patients with active
than 50,000/µL (Johansson, 2009; Rebulla, 2001). Adjunctive alcohol use and chronic liver diseases. Hyponatremia is attrib-
desmopressin may be considered as rescue therapy for refrac- uted to an impaired ability to excrete free water and occurs
tory hemorrhage, particularly when AKI is present, but con- in the setting of severe ascites, hepatic encephalopathy, SBP,
flicting results persist about its benefits in chronic liver disease and hepatorenal syndrome (Angeli & Merkel, 2008). The
(Shah et al, 2014). causes of hyponatremia should be elucidated and addressed
through various strategies, such as correction of fluid deficit
Cardiovascular and Respiratory Parameters or fluid restriction, and cautious and transient use of
Repiratory alkalosis tends to develop in patients with chronic vasopressin-2 (V2)-receptor antagonists, such as conivaptan,
liver disease. Increased abdominal girth in the setting of tense satavaptan, and lixivaptan (Kwo, 2014). Other electrolyte
ascites can lead to restrictive ventilatory defect with reduced imbalances (hypokalemia, hypomagnesemia, and hypophos-
FRC, and hypoxia and paracentesis may lead to improvement phatemia) can result from the use of loop diuretics, chronic
in respiratory parameters (Gupta et al, 2000). Patients with respiratory alkalosis, or malnutrition and should be corrected
cirrhosis also are at risk for coronary artery disease because of before surgery to limit cardiac arrhythmias, peritonitis, and
a high prevalence of cigarette smoking and diabetes mellitus hepatic encephalopathy.
(Dam et al, 2013; Hickman & MacDonald, 2007). Cirrhotic
patients typically have a hyperdynamic hemodynamic profile Infection
similar to the systemic inflammatory response syndrome (SIRS) Patients with cirrhosis are at increased risk for infection, par-
with high cardiac output and vasodilatation of the pulmonary, ticularly SBP (Khan et al, 2009). In patients with cirrhosis,
splanchnic, and peripheral beds (Cazzaniga et al, 2009; Moller infections increase mortality fourfold with a median mortality
& Henriksen, 2008). Patients with alcoholic liver disease and rate of 38% (30% within 1 month after infection, whereas
iron overload are predisposed to cardiomyopathy and cardiac another 30% die within 1 year) (Arvaniti et al, 2010). Risk
arrhythmias (Moller & Henriksen, 2008). factors for SBP include gastrointestinal hemorrhage, metabolic
alkalosis, dehydration, hyponatremia, and a high MELD score
Hepatopulmonary Syndrome and (Obstein et al, 2007). SBP carries an increased mortality rate,
Portopulmonary Hypertension which can be worsened by age, renal dysfunction, bacteremia,
Hepatopulmonary syndrome (HPS) is relatively common in and elevated MELD score (Cho et al, 2007; Khan et al, 2009;
advanced cirrhosis and is often associated with portopulmonary Nobre et al, 2008). SBP can be confirmed by a diagnostic
hypertension as a result of alterations in the pulmonary vascu- paracentesis, especially in the setting of large-volume ascites
lature by various toxins that accumulate and bypass the cir- (Kuiper et al, 2007). If SBP is present, elective surgery should
rhotic liver (Ho, 2008) (see Chapter 79). Signs and symptoms be deferred until the infection has been adequately controlled.
of HPS include hypoxemia, platypnea, orthodeoxia, clubbing, Prophylactic intestinal decontamination with quinolones can
and spider angiomata (Singh & Sager, 2009). Transthoracic prevent SBP in high-risk patients, such as those in whom GI
echocardiography with agitated saline or bubble contrast allows hemorrhage develops, or who have a low protein level in the
identification of intrapulmonary and right-to-left intracardiac ascitic fluid (Loomba et al, 2009; Terg et al, 2008).
shunts indicative of HPS (Rodriquez-Roisin et al, 2005). The
severity of HPS can be quantified with a tagged, macroaggre- Surgical Procedures
gated albumin lung perfusion scan and arterial blood gas analy- The complexity of the surgical procedure influences outcomes
sis. HPS worsens the overall prognosis of liver cirrhosis (see Chapters 24, 77, and 103D). Timing of the surgery and
(Fauconnet et al, 2013). General anesthesia for hepatic and perioperative management should factor in the nature of the
440 PART 3 ANESTHETIC MANAGEMENT, PRE- AND POSTOPERATIVE CARE
surgical procedures, the administration of anesthetic agents, they are not metabolized through the hepatic or renal system
the severity of the cirrhosis, and occasionally the degree of (Hoetzel et al, 2012). Isoflurane and sevoflurane remain the
acuity and the causes of the liver disease. Emergent surgery preferred inhalational anesthetic agents in patients with liver
and unscheduled laparotomy for trauma carry a high mortality disease because they undergo less hepatic metabolism (Nishi-
(Demetriades et al, 2004; Georgiou et al, 2009). Cholecystec- yama et al, 2004). Of the two agents, isoflurane is more fre-
tomy and surgical repair of umbilical and inguinal hernia were quently selected because of its minimal effects on hepatic blood
associated with the lowest morbidity and mortality risk, flow, whereas enflurane and halothane are not used because of
whereas pancreatic surgery, cardiovascular, and trauma surgery the high risk of hepatotoxicity (Berendes et al, 1996).
correlated with the highest (De Goede et al, 2012). The mor- Most narcotic, sedative, and analgesic agents are extensively
bidity and mortality rates of cardiovascular operations, open metabolized in the liver, and their half-life is often altered in
cholecystectomy, hysterectomy, nephrectomy, and transure- patients with chronic liver disease (Bosilkovska et al, 2012).
thral resection of the prostate are also higher in comparison Cirrhosis delays the elimination of alfentanil, whereas the
to laparoscopic and elective interventions (Csikesz et al, metabolism of fentanyl, sufentanil, and remifentanil does not
2009; Filsouf et al, 2007; Pavlidis et al, 2009; Shaheen et al, seem to be affected (Delco et al, 2005). Decreased protein
2009). binding and increased volumes of distribution hinder the clear-
ance of midazolam in cirrhotic patients (Verbeeck, 2008). IV
Assessment for Pancreatobiliary Surgery remifentanil is favored for induction because of rapid onset and
Surgery for gallbladder bile duct, and pancreatic cancer remains elimination. Propofol is also increasingly preferred versus mid-
very challenging and requires experienced surgical and anes- azolam for sedation during surgical or endoscopic procedures
thesiology teams. During the past four decades, the mortality because of shorter recovery time, better pharmacokinetics,
associated with standardized Kausch-Whipple pancreaticoduo- and less propensity to exacerbate subclinical encephalopathy
denectomy for adenocarcinoma of the pancreatic head has dra- (Khamaysi et al, 2011). In general, opioids are avoided or their
matically improved (Richter et al, 2003) (see Chapters 66 and use is limited intraoperatively.
67). However, postoperative complications are frequent and
include cardiopulmonary events, fistula, delayed gastric empty- Management of Mechanical Ventilation
ing, sepsis, and bleeding (Schmidt et al, 2004). From a ventilatory perspective, cirrhosis is a relative contrain-
Predictive models of postoperative morbidity based on the dication to the use of carbon dioxide during exploratory lapa-
estimation of physiologic ability and surgical stress score in roscopy. Low to moderate VT is advocated even in the absence
pancreatic surgery are associated with mixed results (Deyle of acute lung injury/acute respiratory distress syndrome because
et al, 2011; Hashimoto et al, 2010). Other scoring systems larger VT may cause abdominal hypertension, worsen respira-
allow preoperative risk stratification, prediction of major com- tory alkalosis, lead to barotrauma, reduce ventricular preload,
plications associated with pancreaticoduodenectomy, and and result in systemic hypotension and multiorgan injury
careful patient selection. The Preoperative Pancreatic Resec- (Determann et al, 2010). Patients with chronic liver disease are
tion (PREPARE) score is based on several variables, such as at increased risk of hypoxemia because of diffusion abnormali-
systolic blood pressure, heart rate, hemoglobin level, albumin ties, ventilation-perfusion mismatch, and decreased FRC
level, the American Society of Anesthesiologists category, elec- (Polverino et al, 2014). Muscle relaxants and inhaled anesthetic
tive versus emergent surgery, and disease of pancreatic origin agents may reduce the oxygen debt. Surgery is contraindicated
or not. The PREPARE score is quite accurate in identifying in cases of uncontrolled portopulmonary hypertension because
low-, intermediate-, and high-risk patients for pancreatic of high mortality rates (Kawut et al, 2005).
surgery (Uzunoglu et al, 2014). Other predictors of postopera-
tive outcome include texture of the pancreas, pancreatic duct Fluid/Blood Loss and Hemodynamic Parameters
diameter, and operative blood loss (Braga et al, 2011). Careful patient selection, attention to the volume of hepatic
tissue resected, and reduction in intraoperative blood loss con-
INTRAOPERATIVE MANAGEMENT tribute to improved perioperative morbidity and mortality.
Decreased effective circulatory volume is frequently present,
The core components of the intraoperative care of patients with despite the presence of total body fluid overload (Cazzaniga
cirrhosis include careful selection of anesthetic, narcotic, and et al, 2009). The initial periods of surgery may be associated
sedative agents; management of mechanical ventilation; main- with significant fluid shifts resulting from the removal of ascites
tenance of adequate intravascular volume in the setting of hem- when the peritoneal cavity is accessed. Surgery may also be
orrhage and fluid shift/loss; glucose control and correction of complicated by excessive intraoperative hemorrhage resulting
electrolyte disorders; improved surgical techniques; avoidance from the presence of portal hypertension and coagulopathy.
of hypothermia; and adjustment to blood losses in the setting Thromboelastography has been advocated as a guide for the
of relative anemia and coagulopathy (see Chapter 24). intraoperative monitoring and therapy of coagulopathy (Lud-
dington, 2005). The administration of IV fluids in the immedi-
Selection of Anesthetic, Narcotic, and Sedative Agents ate preoperative period may reduce the hemodynamic alterations
The choices and doses of anesthetics, muscle relaxants, anal- and prevent complications related to hypovolemia, such as
gesics, and sedatives should account for the degree of impair- hepatic encephalopathy and postoperative AKI. Large volumes
ment in hepatic synthetic function and clearance (Hoetzel et al, of blood products or IV fluids are sometimes necessary to
2012). Endotracheal intubation and induction are achieved maintain hemodynamic stability. Colloid solutions such as
in patients with liver disease similar to that in the general albumin (with vasoconstrictors) should be administered to
population. Atracurium and cisatracurium are the preferred minimize the risks of worsening portal hypertension and volume
neuromuscular blocking agents to facilitate intubation because overload (Appenrod et al, 2008).
Chapter 25 Perioperative critical care in hepatopancreatobiliary patients 441
Anesthetic techniques aimed at maintaining a low central Hepatic cirrhosis increases the risk for AKI, sepsis, ICU
venous pressure (CVP) during hepatic resection are associated admission, and postoperative mortality, particularly when asso-
with a reduction in blood loss, renal failure, and mortality ciated with alcohol dependence, hepatic encephalopathy, and
(Melendez et al, 1998). Alternatively, stroke volume variation GI hemorrhage (Lin et al, 2013). High MELD score, admis-
is an alternative strategy to CVP monitoring because it is a sion to the ICU, and need for mechanical ventilation and con-
useful indicator of intraoperative blood loss, and it can safely tinuous renal replacement therapy are predictors of increased
guide the administration of IV fluid during hepatic resection length of stay and both short- and long-term mortality
(Dunki-Jacobs et al, 2014; Harimoto et al, 2013). Intraopera- (Bahirwani, 2013; Cholongitas et al, 2009; Levesque et al,
tive blood transfusion is a harbinger of morbidity and mortality 2014). Among cirrhotic patients admitted to the ICU, sequen-
in patients undergoing hepatic resections (Neeff et al, 2014). tial organ failure assessment and MELD scores were more
Increased blood loss during surgical resection of hepatocellular accurate in predicting mortality, and those with failure of three
carcinoma is an independent predictor of cancer recurrence or more organs had a 90% mortality rate (Cholongitas et al,
and mortality (Katz et al, 2009). 2006). The three main risk factors for postoperative mortality
are older age, high MELD score of 20 or greater, and American
Correction of Electrolyte Abnormalities Society of Anesthesiologists class IV and V (Teh et al, 2007).
Correction of electrolyte abnormalities is important to prevent
arrhythmias and hemodynamic compromise. Compared with Postoperative Hepatic Failure
the general population, acute hypocalcemia during massive Hepatic failure, often manifested as encephalopathy, hyperbili-
blood transfusion is more frequent in patients with chronic liver rubinemia, and coagulopathy, can lead to acute respiratory
disease and is the result of high citrate load (Chung et al, failure, renal failure with/without hepatorenal syndrome, and
2012). Administration of IV calcium should be considered in bleeding in the setting of thrombocytopenia and acquired coag-
the setting of intraoperative hemorrhage and hypotension ulation defect. Several postoperative criteria have been used in
because it helps maintain vascular muscle tone and may predicting hepatic failure and mortality. The 50-50 criteria, a
enhance hemostasis. Intraoperative and postoperative serum combination of prothrombin time of less than 50% (or PT-INR
levels of potassium, calcium, magnesium, and phosphorus > 1.7) and serum bilirubin greater than 50 µmol/L (or > 2.9 mg/
should be monitored, and abnormalities should be promptly dL), has been validated as an excellent predictor of death on
corrected (Hayter et al, 2012). days 3 and 5 for patients admitted to the ICU for postoperative
liver failure following hepatic resection (Balzan et al, 2005;
Improved Surgical Techniques Paugam-Burtz et al, 2009). The Mullen criteria (bilirubin peak
During the past decade, advances in surgical techniques for > 7 mg/dL on postoperative days 1 to 7) were found to be more
hepatic surgery have resulted in significant improvement in accurate than the 50-50 criteria in predicting death from hepatic
postoperative outcomes (Rowe et al, 2009; Schiffman et al, failure after liver resection (Filicori et al, 2012). Encephalopa-
2015; Vavra et al, 2014) (see Chapter 103). Reduction in intra- thy and hyperbilirubinemia warrant avoidance of hepatotoxic
operative blood loss, ischemic preconditioning with intermit- medications, use of small incremental doses of analgesics and
tent portal triad clamping, and other techniques that allow other medications to achieve desired therapeutic effects, and
preservation of a larger volume of hepatic parenchyma are the administration of lactulose and stool softeners (Wright & Jalan,
primary contributing factors to these favorable outcomes, par- 2007). N-acetylcysteine does not offer any survival benefit in
ticularly at high-volume centers (Aragon & Solomon, 2012; the management of hepatic failure after liver resection (Robin-
Heizmann et al, 2008). However, the benefits of ischemic pre- son et al, 2013). Liver transplantation may be necessary but
conditioning could not be demonstrated in recent randomized transient supportive care with liver assist devices remains elusive
controlled trials and meta-analyses (O’Neill et al, 2013;Ye et al, (Schilsky, 2011; Sussman et al, 2009) (see Chapter 79).
2014; Zhu et al, 2014).
In regard to pancreatic surgery, pylorus-preserving pancre-
Fluid Management and Abdominal
aticoduodenectomy does not differ in intermediate- and long- Compartment Syndrome
term outcomes from the classic Whipple procedure as surgical Patients with cirrhosis are prone to postoperative hypotension,
treatment of pancreatic carcinoma (Diener et al, 2014; Tran vasodilation, and a hyperdynamic state of SIRS as well as portal
et al, 2004). However, a pylorus-preserving procedure offers hypertension (Cazzaniga et al, 2009). Surgical procedures can
significant advantages, such as shorter operative time and hos- cause significant fluid shifts, and ascites may occur even in
pital length of stay, reduced blood loss and blood transfusions, stable patients with cirrhosis without documented preoperative
decreased incidence of delayed gastric emptying, and more portal hypertension. Judicious administration of IV fluids may
enduring impact on long-term functional and nutritional status preserve renal function and prevent ascites (Cholongitas et al,
(Niedergethmann et al, 2006) (see Chapter 66). 2006). Oliguria is frequently caused by reaccumulation of
ascites at the expense of the intravascular space and is indicative
POSTOPERATIVE MANAGEMENT of the need for IV colloids and vasopressor agents (e.g.,
norepinephrine, terlipressin), rather than diuretics or α-
Despite careful planning, cautious patient selection, and judi- adrenoreceptor agonists such as midodrine (Appenrodt et al,
cious intraoperative monitoring and management, some patients 2008; Belcher et al, 2013).
experience hepatic failure, the most alarming postoperative The development of tense ascites predisposes to
complication. Patients with chronic liver diseases are also sus- surgical wound dehiscence, AKI, peritonitis, and abdominal
ceptible to other postoperative complications, such as abdomi- compartment syndrome. Abdominal compartment syndrome is
nal compartment syndrome, fluid derangements, and venous characterized by an acute and progressive elevation of the
thromboembolism (VTE). intraabdominal pressure to more than 20 mm Hg in association
442 PART 3 ANESTHETIC MANAGEMENT, PRE- AND POSTOPERATIVE CARE
after recent studies and analyses have indicated no clear correla- Early enteral nutrition is advocated after liver resection
tion between an increased risk of hemorrhage and a prolonged because of a perceived decrease in postoperative complications
PT or aPTT (Tripodi & Mannucci, 2011). Moreover, FFP (Richter et al, 2006). Compared with enteral nutrition, paren-
transfusion may lead to volume overload and does not correct teral nutrition for 7 days before planned hepatectomy in patients
coagulation defect or decrease the risk of bleeding (Tinmouth, with liver cirrhosis and continued for 7 days afterward was
2012; Tripodi et al, 2012). The routine use of rFVIIa in acute associated with fewer septic complications and a lower mortal-
variceal hemorrhage is controversial (Bendtsen et al, 2014; ity rate (Fan et al, 1994). In reality, the benefits and recom-
Bosch et al, 2008). Data on the successful use of four-factor mended route of nutritional support after hepatopancreatobiliary
prothrombin and fibrinogen complex in patients with liver cir- surgery are debatable because of conflicting results from a few
rhosis and postoperative hemorrhage are lacking. randomized trials and systematic review (Fan et al, 1994;
Koretz et al, 2012). At present, no specific guidelines or recom-
Sedative and Pain Management and mendations are available, even during liver regeneration or in
Hepatic Encephalopathy instances of acute pancreatitis (Poropat et al, 2015).
In patients with cirrhosis, sedative and narcotic agents undergo
increased volume of distribution, slow hepatic metabolism, and Postoperative Care after Pancreaticoduodenectomy
delay elimination (Delco et al, 2005). Advanced cirrhosis is Postoperative complications of the Kausch-Whipple procedure,
often associated with renal dysfunction, which increases the such as anastomotic leak, fistula, and abdominal collections,
risks of adverse events, and the doses of sedative and analgesic are relatively frequent and vary with the type of pancreaticoen-
medications should be adjusted to prevent an exacerbation of teric anastomosis, pancreatic texture and intraoperative blood
hepatic encephalopathy and other complications (Verbeeck, transfusion (Fathy et al, 2008) (see Chapters 27 and 66).
2008). Inappropriate use of narcotics and sedatives can lead to Abdominal sepsis is relatively common, and pneumonia,
atelectasis, aspiration, and postoperative pneumonia by impair- abdominal abscess, and multiorgan dysfunction syndrome
ing respiratory drive and by delaying extubation or triggering (MODS) in the setting of hemorrhage are the main contribu-
reintubation. tors to the relatively low mortality rate of 2% to 5% (Satoi et al,
Among the narcotic agents available, remifentanil is pre- 2006). Early recognition is the most important component in
ferred because of its limited hepatic metabolism (Uchida the successful management of pancreatic leak, and in the
et al, 2011). Continuous epidural analgesia is frequently absence of sepsis, hemorrhage, or MODS, most cases are
avoided because of concerns about coagulopathy, thrombocy- managed expectantly on the surgical wards (Ho et al, 2005).
topenia, and the increased risk of hematoma. In a small Imaging studies are sometimes indicated, and a few patients
series, patient-controlled analgesia has been found to be a may require IV antibiotics, blood transfusion, and close drain-
safe and effective method of managing pain after hepatic age. Surgical exploration and prognosis are often dictated by
resection (Roy et al, 2006). Propofol is a better choice than the degree of destruction and inflammation of the retroperito-
benzodiazepines for sedation because of its shorter recovery neum (Ho et al, 2005).
time, which may allow more reliable serial neurologic assess- As many as 18% of patients may require ICU admission for
ment (Khamaysi et al, 2011). Although data are limited, dex- postoperative complications of pancreaticoduodenectomy.
medetomidine is a potential alternative to IV propofol because Delayed admission to the ICU for septic shock with multiorgan
of rapid onset and offset of the drug (Wang et al, 2014). failure and hemorrhage carries a mortality rate of close to 20%
Nonsteroidal antiinflammatory agents should be used spar- (Welsch et al, 2011). Prophylactic octreotide has no impact on
ingly because of the potential for peptic ulceration, fluid the rates of pancreatic fistula or total complications after pan-
retention from inhibition of renal prostaglandin synthesis, creaticoduodenectomy (Yeo et al, 2000). However, the periop-
precipitation of hepatorenal syndrome, and bleeding due to erative use of pasireotide was associated with significant
antiplatelet activity, gastrointestinal irritation, and renal failure decrease in postoperative pancreatic fistula, leak, or abscess
(Bosilkovska et al, 2012; Dwyer et al, 2014). (Allen et al, 2014).
Hepatic encephalopathy warrants assessment and treatment
of infections and administration of oral lactulose or lactitol Venous Thromboembolism Prophylaxis
suppository (Wright & Jalan, 2007). Second-line agents for the Compared with the general population, patients with cirrhosis
treatment of hepatic encephalopathy include oral antibiotics are at higher risk of bleeding because of anemia, thrombocyto-
such as neomycin, metronidazole, and rifaximin (Al Sibae & penia, and the inability of the liver to produce procoagulants in
McGuire, 2009). response to the stress of bleeding. Yet these patients manage to
strike a fine balance between prothrombotic and anticoagulat-
Liver Regeneration, Hyperglycemia, and Nutrition ing proteins and other endogenous products (Senzolo et al,
Hypophosphatemia is a frequent occurrence in the early days 2009). Severe thrombocytopenia rather than coagulopathy is
after hepatectomy and should be corrected, accordingly (George the most significant risk factor for bleeding after invasive pro-
& Shiu, 1992). Failure to develop hypophosphatemia is a cedures (Giannini et al, 2010; Rockey et al, 2009).
marker of postoperative hepatic insufficiency and mortality In patients with liver cirrhosis and with noncirrhotic chronic
(Squires et al, 2014). Liver regeneration is a protracted com- liver disease, the risks of VTE are relatively higher (Sogaard et al,
pensatory process of hepatocytes replication that can be assessed 2009). Postoperative VTE may occur in the setting of low serum
by magnetic resonance spectroscopic imaging (Fausto et al, albumin, despite thrombocytopenia and coagulopathy (Dabbagh
2006; Zakian et al, 2005) (see Chapter 6). Early postoperative et al, 2010; Northup et al, 2006). In postoperative patients with
hyperglycemia after pancreaticoduodenectomy increases the cirrhosis at moderate risk for VTE (i.e., Caprini score < 5 and
risk of infectious complications, delayed gastric emptying, and Rogers score < 10), early ambulation and mechanical thrombo-
reoperation (Eshuis et al, 2011). prophylaxis with intermittent pneumatic compression devices
444 PART 3 ANESTHETIC MANAGEMENT, PRE- AND POSTOPERATIVE CARE
and/or graduated compression stockings, are favored particu- (Gould et al, 2012). Although renal impairment must be con-
larly in the early perioperative period, when the consequences of sidered when choosing the type of heparin for VTE, a recent
bleeding are potentially severe (Gould et al, 2012). meta-analysis showed no meaningful differences in the inci-
Pharmacologic thromboprophylaxis with unfractionated dence of heparin-induced thrombocytopenia and/or thrombosis
heparin or low-molecular-weight heparins (LMWH) is appro- between LMWH and unfractionated heparin (Morris et al,
priate when the risk of bleeding subsides (Barclay et al, 2013). 2007).
Periodic surveillance with venous compression ultrasound and
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CHAPTER 26
Preoperative and postoperative nutrition in
hepatobiliary surgery
Farzad Alemi, D. Owen Young, and William S. Helton
445
446 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
intestine (Sun et al, 2014) and Kupffer cells of the liver (Billiar
Vitamin E et al, 1988). These observations show that hepatocellular func-
Vitamin E has the ability to scavenge intermediate peroxyl tion before and after HPB operations can be potentially modu-
radicals and therefore interrupt the chain reactions of lipid lated by the administration of specific nutrients and vitamins
peroxidation (Birlouez-Aragon et al, 2003), and it is the most (Helton, 1994) and provide a potential opportunity whereby
important inhibitor of the free-radical chain reaction of lipid the hepatobiliary surgeon might influence patient outcomes by
peroxidation. Studies in rodents show that supplemental nutritional means. ω3FAs have also been implicated in the
vitamin E significantly attenuates liver I/R injury and hepatic maintenance of postoperative hepatic function by increasing
lipid peroxidation (Sugino et al, 1989). In vitro, physiologic liver perfusion. A meta-analysis of 21 randomized controlled
concentrations of vitamin E inhibit lipopolysaccharide- trials showed perioperative administration of ω3FAs to signifi-
stimulated TNF secretion by Kupffer cells, suggesting that cantly reduce hospital stay, infections, and liver functions tests
subnormal tissue or plasma levels of vitamin E may potentiate (Li et al, 2014).
macrophage cytokine release (McClain et al, 1994).
Plasma levels of vitamin E decrease significantly in the first Obstructive Jaundice
hours after surgery. A significant reduction in the levels of liver Patients with jaundice often have anorexia and weight loss
α-tocopherol, an active form of vitamin E, was observed during because of decreased oral intake coupled with malabsorption.
the first hour of reperfusion in a rat model of liver ischemia Approximately 45% to 70% of patients with obstructive jaun-
(Maderazo et al, 1990, 1991). Obstructive jaundice often is dice are seen with malnutrition as evidenced by greater than
associated with endotoxemia, which leads to Kupffer cell pro- 10% weight loss, albumin less than 3 g/dL, decreased triceps
duction of oxygen-free radicals and nitric oxide, which inhibit skin fold, and impaired delayed hypersensitivity reactivity
protein synthesis (Curran et al, 1990). Endotoxemia also (Foschi et al, 1986). The primary nutritional deficit resulting
reduces endogenous levels of the antioxidants glutathione, from obstructive jaundice is malabsorption of fat and fat-
vitamin E, and coenzyme Q (Marubayashi et al, 1986). soluble vitamins. In addition, there is loss of trace minerals,
Vitamin E has a variety of protective effects on the hepato- such as phosphate, calcium, magnesium, and zinc, because of
biliary system. It attenuates endotoxemia (Powell et al, 1991), salt formation from unabsorbed dietary fat (Shronts, 1988).
hepatocellular membrane lipid peroxidation, and cellular Biliary sepsis in patients with obstructive jaundice contrib-
damage after I/R injury (Lee & Clemens, 1992). Large doses utes to malnutrition by shifting protein synthesis from anabolic
of enterally administered vitamin E inhibit the release of TNF protein synthesis to acute-phase protein synthesis (O’Neill
in animal models of infection (Bulger et al, 1997). Under these et al, 1997). This reprioritization of protein synthesis occurs as
conditions, vitamin E supplementation improves survival after a result of endotoxin-stimulated Kupffer cell production of
a septic challenge (Yoshikawa et al, 1984). α-Tocopherol has TNF, IL-6, eicosanoids, and other inflammatory mediators that
also shown protective effects against warm and cold I/R injury directly inhibit protein synthesis (see Chapter 43). Because of
(Eum et al, 2002; Gondolesi et al, 2002). These animal studies these derangements, some authors have advocated preoperative
show a protective effect of vitamin E on liver function and biliary decompression (PBD) in patients undergoing HPB
survival during conditions commonly encountered in patients surgery. However, multicenter trials and Cochrane analysis
undergoing HPB surgery. Despite this evidence, no clinical have demonstrated no evidence to support or refute routine
trials have demonstrated a beneficial effect of vitamin E in biliary drainage and stenting in patients with malignant pancre-
patients undergoing HPB surgery. aticobiliary diseases awaiting surgery (Mumtaz et al, 2007;
Wang et al, 2008) (see Chapters 29, 30, 51, and 52). On the
Vitamin C other hand, PBD should probably be performed in patients
Ascorbic acid (vitamin C) is required as a cofactor for many undergoing extended hepatectomy for hilar cholangiocarci-
enzymes involved in the scavenging of free radicals. Vitamin C noma, if the future liver remnant volume is estimated to be less
deficiency is evident in 50% of patients with alcoholic liver than or equal to 30% (see Chapter 108). To reverse the cata-
disease (Muller, 1995) and is probably even higher in alcoholics bolic effects of chronic endotoxemia and restore hepatic protein
who smoke. Vitamin C recycles α-tocopherol and is intimately synthesis, patients with biliary infection should be treated with
linked to vitamin E’s ability to quench free radical–mediated biliary decompression for at least 4 weeks before major HPB
cellular damage (Sardesai, 1995). The simultaneous adminis- surgery to allow hepatocytes to recover their protein synthetic
tration of ascorbate and α-tocopherol is more effective in inhib- capacity.
iting oxidation than either alone (Niki et al, 1995). The
synergistic protective effects of vitamin C and vitamin E in Cirrhosis and Liver Failure
preventing lipid peroxidation and cellular damage suggest that Patients with cirrhosis have multiple hormonal and metabolic
these vitamins should be administered together for maximal alterations (see Chapter 79). These changes cause loss of fat
potential benefit (Bulger & Helton, 1998). A prospective ran- and muscle mass, growth failure, glucose intolerance, hyperin-
domized study in patients undergoing liver resection by using sulinemia, insulin resistance, increased plasma glucagon and
an infusion containing 10 mg α-tocopherol acetate and 1 g catecholamines, elevated serum free fatty acids, elevated glyc-
ascorbate administered before reperfusion demonstrated less erol, hypoproteinemia, hyperammonemia, hypophosphatemia,
plasma lipid peroxidation and acute liver damage and fewer and alterations in plasma and cerebrospinal fluid amino-acid
postoperative complications (Cerwenka et al, 1999). profiles (Achord, 1987; Henriksen et al, 1985; Petrides & De
Fronzo, 1989; Riggio et al, 1984). These metabolic aberrations
Omega-3 Fatty Acids lead to altered metabolism of fat, protein, and carbohydrate. In
The administration of fish oils rich in omega-3 fatty acids addition, there is an increase in skeletal muscle proteolysis for
(ω3FAs) can influence cytokine and prostanoid release by the energy provision, which leads to eventual muscle wasting. In
Chapter 26 Preoperative and postoperative nutrition in hepatobiliary surgery 447
The effects of fasting and feeding on liver allograft function upon chronic pancreatitis, are at risk for profound malnutrition
after cold preservation and reperfusion are complex and incom- and metabolic derangement because of the catabolic effects of
pletely understood. No guidelines currently exist to support critical illness and sepsis (see Chapters 55 and 56). Despite
specific feeding regimens or NS guidelines for liver transplant these collective risks, patients with severe acute pancreatitis are
donors. However, using the principles of pharmaconutrition, best managed with oral and/or enteral nutrition (EN) (Bakker
there is the potential to modulate the response of liver grafts to et al, 2014). A detailed discussion of nutritional support for
I/R. patients with acute pancreatitis is covered in Chapter 54.
steatorrhea can lead to significant weight loss, malnutrition, of vitamin A, D, E, and K either orally or through a feeding
vitamin deficiencies, poor quality of life, and delays in therapy tube.
(Klapdor et al, 2012). In one study, one third of patients with
chronic pancreatitis admitted for medical rehabilitation had a Pain
body mass index (BMI) less than 20 kg/m2, and one fourth had Patients with pancreatic disease often experience severe
profound steatorrhea (Armbrecht, 2001). Deficits in fat-soluble abdominal pain because of involvement of the celiac plexus by
vitamins (A, D, E, and K) are common in patients with both tumor, pancreatic duct obstruction, and/or pancreatitis. When
jaundice and PEI. Multiple studies have reported that patients abdominal pain is exacerbated by oral intake, patients will
with chronic pancreatitis and pancreatic cancer are also vitamin avoid food intake or modify their diet, which contributes to a
D deficient (Cho et al, 2013; Klapdor et al, 2012). Further- malnourished state (Rasmussen et al, 2013). In many cases,
more, patients with serum 25-hydroxyvitamin D-25(OH)D patients unconsciously avoid certain foods, such as those con-
levels less than 20 ng/mL have a worse prognosis when com- taining fat, which during time leads to weight loss. Patients
pared with those with levels greater than 20 ng/mL (Cho et al, taking large doses of narcotics to control their pain may also
2013). have alterations in GI motility and obstipation that also lead
to reduced food intake.
Biliary Obstruction
Biliary obstruction in patients with pancreatic head disease can Cancer-Related Effects on Metabolism
be associated with nutritional deficits, which are corrected once Direct adverse effects of cancers on nutrition and metabolism
obstruction is relieved either surgically or by nonoperative have been known to exist for years but are poorly understood.
means, such as endoscopic stenting or percutaneous drainage The mechanism(s) by which pancreatic cancer induces cachexia
(see Chapter 8). Patients with recent-onset obstructive jaundice are largely unknown but believed to be modulated, in part,
who are not profoundly malnourished and candidates for major through activation of proinflammatory mediators that stimulate
abdominal operation do not necessarily require preoperative systemic inflammation, the magnitude of which is associated
biliary decompression (PBD). In fact, PBD is to be discouraged with poor prognosis (Fearon et al, 2006; McMillan et al, 2009,
in such patients because it substantially increases the incidence 2013) (see Chapter 11). Protein malabsorption coupled with
of postoperative infectious complications (Mezhir et al, 2009). increased catabolism leads to weight loss and impaired immune
On the other hand, patients with long-standing obstructive surveillance by decreasing lymphocyte counts, ILs, helper T
jaundice associated with profound malnutrition will most likely cells, and T-cell blastogenesis (Kanda et al, 2011). Peripancre-
benefit from a period of nutritional repletion before undergoing atic tissues and tumors also stimulate the release of TNF-α,
major abdominal surgery. This is true for patients undergoing which plays a pivotal role in cachexia and catabolism (Todorov
any type of HPB operation. Such patients are best managed et al, 1996).
with endoscopic PBD as part of a comprehensive nutritional A combination of factors—exocrine insufficiency, tumor
repletion program. Unfortunately, endoscopic drainage is effects, pain, alcohol use—leading to malnutrition in patients
sometimes unsuccessful and requires percutaneous transhe- with pancreatic disease has a detrimental effect on patient out-
patic biliary decompression (PTBD). When this is the case, a comes and treatment. The degree of malnutrition, as measured
rendezvous procedure should be performed to convert the by weight alone, is often more than 25% of preillness weight
PTBD to an internal endoscopic stent either immediately or as (Wigmore et al, 1997). Others have observed that more than
soon as the patient is medically stable so that bile flows back 80% of patients are cachectic at diagnosis; this proportion
into the duodenum (see Chapters 29 and 30). Bile refeeding increases while the disease progresses (Tisdale, 2003) and is
into the proximal small bowel is an important issue, because associated with poor prognosis (Bachmann et al, 2008). These
prolonged PBD that occurs with either complete biliary obstruc- metabolic and nutritional responses negatively impact treat-
tion or with biliary disconnection from a bile duct injury will ment plans and can often delay resection, chemotherapy, and
lead to metabolic derangement and malnutrition because exces- lead to progressive deterioration in performance status.
sive losses of bile can lead to dehydration, metabolic acidosis,
progressive loss of biliary protein, and malabsorption. Refeed- Malnutrition and Pancreatic Resection
ing bile into the small bowel improves the digestion and absorp- Pancreatic resection is associated with a relatively high inci-
tion of fat and reduces the volume of hepatic bile output dence of perioperative morbidity (see Chapters 27 and 66).
through the enterohepatic recirculation of bile salts. Most While strategies have evolved to minimize and effectively
patients can tolerate bolus infusion of bile into their small bowel manage the typical complications following pancreatic resec-
of 150 mL or less every 4 hours, and they can be taught to do tion, such as pancreatic fistula and infection, optimization of
this on their own at home. But if a patient has a feeding jeju- perioperative nutritional status has remained a challenging
nostomy or gastrojejunostomy tube, it is preferable to provide endeavor. Postoperative complications following pancreatic
bile refeeding in a continuous manner. An alternative to enteric operations, particularly PD, frequently exacerbate a preopera-
bile refeeding is to provide oral bile salts in the form of urso- tive chronic malabsorption state and weight loss (Sanford et al,
deoxycholic acid (300 mg, four times daily) to form micelles 2014). Furthermore, neoadjuvant chemotherapy can worsen an
for fat absorption (Tripathy et al, 1996). already marginal preoperative nutritional state and subject an
Malnourished patients with complete biliary obstruction or already malnourished patient to additional risk at the time of
disconnection may require specialized semielemental diets to operation (Attar et al, 2012; Bozzetti et al, 2009). Some have
avoid fat malabsorption. Diets rich in medium-chain triglycer- reported that preventing weight loss during neoadjuvant che-
ides (MCTs) are preferred over diets containing long-chain motherapy is associated with better overall survival (Naumann
triglycerides. These patients are also at risk for fat-soluble et al, 2013). This fact underscores the importance of screening
vitamin deficiency and should be offered water-soluble forms and identifying patients with PC who are at nutritional risk and
450 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
taking steps to restore and prevent weight loss before operation 2013). Patients with chylous leaks are at increased risk for
(Sanford et al, 2014). postoperative malnutrition not only because low-fat diets
The indications for pancreatic resection are evolving to provide fewer calories and are nonpalatable, but also because
include more elderly patients with benign and premalignant of protein losses stemming from externally drained chyle. After
diseases such as intraductal papillary mucinous neoplasms. In dietary modification, chyle leaks are usually self limited and
one review, close to 50% of patients undergoing PD in a geri- resolve without the need for further surgical intervention.
atric population did so for benign disease (Sanford et al, 2014). Chylous ascites is significantly associated with early enteral
Because patients are living longer following PD, the necessity feeding following PD (Kuboki et al, 2013). Even though there
to properly manage postoperative nutritional side effects is of is no further morbidity or mortality once conservative manage-
utmost importance. This is illustrated by the observation that ment is initiated, chylous ascites is associated with prolonged
1 in 3 patients identified with nutritional risk after a PD for abdominal drainage and decreased likelihood of hospital dis-
benign disease were dead within 5 years, compared with only charge within 10 days postoperatively (Hilal et al, 2013).
1 in 14 patients without nutritional risk (Sanford et al, 2014).
Recent trials have shown that as many as 88% of preoperative Delayed Gastric Emptying
patients are at medium to high risk of malnutrition (La Torre The most frequent complication following PD is DGE, which
et al, 2013). These data underscore the importance of identify- significantly delays the resumption and tolerance of adequate
ing patients at nutritional risk so that nutritional repletion strat- oral nutrition and exacerbates any preoperative malnourished
egies can be initiated before operative intervention. state. DGE significantly prolongs hospitalization and is associ-
ated with increased postoperative morbidity and mortality
Nutritional Implications of Pancreatic Resection (Hu et al, 2014). The exact etiology of DGE following PD is
Malnourished patients undergoing HPB surgery have increased incompletely understood and likely multifactorial. One cause is
risk for intraabdominal and systemic complications and thought to be related to disruption of the migrating motor
decreased survival (Windsor, 1993). Nutritional deficits lead to complex that originates from the gastric pacemaker. A meta-
impaired wound healing, increased susceptibility to infections, analysis demonstrated that the most likely cause of DGE was
and increased bleeding as a result of capillary wall fragility and a postoperative complication (Hu et al, 2014), in particular
impaired clotting (Kanda et al, 2011). Preoperative malnutri- postoperative pancreatic fistulas and/or abdominal fluid collec-
tion has been shown to be an independent predictor of morbid- tions (Hashimoto et al, 2010; Liu et al, 2014). Patients with
ity in patients undergoing PD and results in a significantly significant DGE often require prolonged nasogastric decom-
higher rate of complications and fourfold longer hospitalization pression and may not have return of normal gastric emptying
(La Torre et al, 2013). Severely malnourished patients under- for weeks or months. When this happens (on average in 20%
going distal pancreatectomy have a 6.0 to 8.8 times increased of patients), patients are best served with a nasoenteric tube
risk for postoperative complications (Sierzega et al, 2007). It is placed distal to the gastrojejunal anastomosis alone or with
intuitive to think that correction of nutritional deficits will lead concomitant percutaneous gastric decompression when persis-
to improved outcomes or mitigate risk. Unfortunately, there is tent emesis occurs. Studies have reported that routine postop-
a paucity of good prospective clinical trial data to support this erative EN both exacerbates (Martignoni et al, 2000) and
contention. One prospective clinical trial showed that preopera- alleviates DGE (Zhu et al, 2013). Many surgeons have used a
tive nutritional support for 7 days decreased complications in variety of mechanisms and techniques to counteract this com-
malnourished patients identified to have high preoperative plication, including preoperative NS, intraoperative placement
nutritional risk who subsequently underwent abdominal surgery of jejunostomy feeding tubes, or postoperative placement of
(Jie et al, 2012). Hence, early nutritional assessment has impli- nasojejunal (NJ) feeding tubes. Zhu demonstrated significant
cations for reducing complications and overall hospital stay decrease in DGE after initiation of early EN via an NJ tube
(Kruizenga et al, 2005). feed and hypothesized that the mechanical effects of the NJ
Like GI surgery, pancreatic resection is fraught with the tube and its presence across the gastrojejunostomy helped
typical complications of infection and ileus. However, a PD or gastric and intestinal motility (Zhu et al, 2013). Others have
distal pancreatectomy also harbors specific subsets of complica- argued that NJ feeding tubes should be placed only if patients
tions that are unique to pancreatic surgery, including pancreatic do not resume adequate oral intake by postoperative day 7.
fistula, delayed gastric emptying (DGE), and chylous ascites. More than one meta-analysis however, failed to identify any
Although these high rates of complications are likely the result particular operative technique or process of care that reduces
of a variety of factors, the interplay between them and nutri- the incidence of DGE (Hu et al, 2014; Wu et al, 2014).
tional status (both preoperatively and postoperatively) must be
appreciated and addressed (Zhu et al, 2013). Pancreatic Fistula
The most dreaded complication of a pancreatic resection is
Chylous Ascites pancreatic fistula (PF). Although there are a multitude of
The incidence of chyle leak after a pancreatic resection occurs factors contributing to PF, including surgical technique, gland
in as many as 11% of operations (Hilal et al, 2013). Chyle leaks texture, pancreatic duct size, and stent placement (Kanda et al,
are treated with simple dietary modification, which includes 2011), its incidence and severity is still associated with malnu-
transition to a low-fat or no-fat diet or a diet enriched with trition. Nutritional risk was the only independent risk factor
MCTs, which shifts the burden of fat digestion away from the identified by Sierzega et al (2007) to be associated with a PF
lymphatic plexus. Some surgeons prefer the institution of PN for patients following distal pancreatectomy. Others have
and administration of somatostatin analogues to further assist reported that patients who are overweight (BMI >25 kg/m2)
with treatment and hasten resolution of the fistula, although actually tended to have increased rates of PF after distal
the evidence to support this practice is weak (Kuboki et al, pancreatectomy (Sledzianowski, 2005). This observation is
Chapter 26 Preoperative and postoperative nutrition in hepatobiliary surgery 451
supported by Kanda and colleagues (2011), who found that jaundice, and altered stool pattern, which may indicate fat
patients with low BMI tended to have infrequent rates of PF. malabsorption and steatorrhea. There are a variety of ways to
The authors hypothesized that weight loss is related to the assess preoperative nutritional status.
amount of peripancreatic fat and that the resultant changes to
pancreatic gland texture as a result of malnutrition may con- Anthropometric Measurements
tribute to the eventual fistula rates in distal resections. On the Anthropometric tests have the benefit of objectivity, rapidity,
other hand, Sanford and colleagues (2014) reported that and ease of interpretation. A variety of anthropometric mea-
patients older than 65 years with a high Nutritional Risk Score surements have been tested with respect to degree and risk of
(NRS) were at risk for postoperative PF following a PD, malnutrition, such as mid arm circumference and triceps skin-
whereas those younger than 65 years were not. This latter study fold thickness (Durnin & Womersley, 1974). Although these
suggests that it is not just nutritional risk but rather an interac- modes of assessment are cheap and easy to perform, they are
tion between age and nutritional risk that predisposes to PF. rarely, if ever, used for NA in patients undergoing HPB opera-
More studies are necessary to better define the relationship tions. Others have used surrogates of muscle wasting, such as
between nutritional status and PF. hand-grip strength, to assess protein-energy malnutrition
(Alvares-da-Silva et al, 2005). These assessments have largely
IDENTIFICATION OF PATIENTS AT RISK FOR been demonstrated to be incompletely characteristic of nutri-
POSTOPERATIVE COMPLICATIONS tional state, although they can be used in conjunction with
other scoring systems to provide a clinical picture of
Great efforts have been made to develop scoring systems or nutrition.
methods of nutritional assessment (NA) that identify patients
at risk for perioperative morbidity and mortality HPB opera- Bioelectrical Impedance
tions. The ideal test for preoperative NA should incorporate Changes in body cell mass can serve as a marker for nutritional
measures for quantifying the severity of malnutrition and deple- status and measured using bioelectrical impedance (BEI)
tion of lean body mass as well as estimating the magnitude of (Pirlich et al, 2000). BEI directly measures the impedance to
metabolic stress that would be induced by surgical interven- an alternating current within the body. Different body compart-
tions (Schiesser et al, 2009). ments, including body cell mass, body fat, and lean body mass,
NA should begin preoperatively and continue throughout a can be separately measured and used to define a patient’s
patient’s course of treatment. A thorough NA includes: (1) nutritional state. BEI has been shown to reliably predict sur-
clinical and dietary history; (2) physical examination with vival and surgical morbidity in patients undergoing GI opera-
assessment of muscle mass and strength; (3) evaluation of tions (Schiesser et al, 2009).
serum albumin, prealbumin, and C-reactive protein; (4) mea-
surement of vitamin and mineral deficits; and (5) determination Sarcopenia
of nutrient requirements (Box 26.3). Historic questions should BMI is widely used in patient risk models. However, BMI fails
focus on the patient’s nutritional intake and habits, the degree to account for the diversity of body composition; patients of
and rate of weight loss during the previous month, and 6 the same BMI may differ significantly in composition of lean
months (Windsor, 1993), use of alcohol, length of time with muscle and fat mass. A relative dearth of lean muscle mass,
called sarcopenia, is associated with functional impairments,
physical disability, perioperative complications, prolonged hos-
BOX 26.3 Nutritional Assessment pital length of stay following abdominal operations, and poorer
Clinical Evaluation long-term outcomes in cancer patients (Harimoto et al, 2013;
Dietary and medical history Janssen et al, 2002; Lieffers et al, 2012; Tan et al, 2009; van
Physical activity Vledder et al, 2012). The term sarcopenia was originally used
Weight loss during past 6 months to describe age-related declines in muscle mass (Rosenberg,
1989) but is increasingly recognized as an independent risk
Physical Examination factor for poor survival in patients with cancer regardless of
Body weight their age. Sarcopenia should not be confused with cachexia,
Skin changes which is marked by weight loss and muscle wasting over a rela-
Ascites tively short time period. Sarcopenia develops during a long
Muscle mass and strength
period of time and, in the elderly, is not associated with weight
Objective Evaluation loss (Walrand et al, 2011). Thus many patients who fall into a
Bioelectical impendance analysis normal range for weight and BMI may have unrecognized
Dual-energy x-ray absorptiometry sarcopenia and be at risk for perioperative complications and
Computed tomography muscle mass analysis poor outcomes. Many obese patients may not appear to be
malnourished but have significant occult depletion of their skel-
Protein Synthetic Function etal muscle mass, putting them at particularly high risk for
Albumin, transferrin postoperative complications because excess weight coupled
Prealbumin, prothrombin time with reduced muscle mass leads to impaired mobility, poor
C-reactive protein respiratory function, and prolonged rehabilitation (Lieffers
et al, 2012). Patients who are both obese and sarcopenic are
Vitamin, Mineral, Trace Element Deficits
Vitamins A, D, E, K, B6, niacin, folate, B12 now categorized with “sarcopenic obesity.” Sarcopenic obesity
Thiamine, magnesium, potassium, zinc, iron, phosphorus has been reported as one of the most powerful independent
predictors of poor survival for patients with cancer and is
452 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
associated with impaired functional status, decreased ability to obtainable through simple blood tests. The rapidity and ease
tolerate chemotherapy, and surgery and other invasive therapies of measurement have led to the use of serum markers in predic-
(Martin et al, 2014; Prado et al, 2008). Because the prevalence tive models to facilitate rapid surgical judgment and therapeutic
of obesity continues to rise, recognition of occult sarcopenia by decisions.
diagnostic imaging is an increasingly important method that
should be used to identify patients at nutritional risk. Albumin
The pathophysiology of sarcopenia is not well understood. Serum albumin has been extensively studied as a marker for
It is unclear if significant loss of muscle mass is a natural and nutritional status, and low levels have been shown to be a sensi-
immutable consequence of aging in some individuals or if ther- tive predictor of adverse surgical outcomes (Billingsley et al,
apeutic or lifestyle interventions can slow or reverse it (Walrand 2003; Gibbs et al, 1999; Lai et al, 2011). Gibbs analyzed more
et al, 2011). Age-related sarcopenia is thought to result from than 50,000 surgical patients and demonstrated a significant
factors related to muscle cell senescence and extrinsic factors increase in surgical morbidity and mortality (especially sepsis
such as decreases in growth hormone and insulin-like growth and infections) with worsening hypoalbuminemia (Gibbs et al,
factor-1 (Kalyani et al, 2014). Sarcopenia results in preferential 1999). In HPB surgery, serum albumin has been studied as a
atrophy of type II skeletal muscle fibers, resulting in a relative marker of perioperative risk. Used in conjunction with other
loss of muscle strength over endurance. Cancer, autoimmune markers of malnutrition, albumin was found to be predictive of
diseases, human immunodeficiency virus infection, cirrhosis, mortality after PD (Venkat, 2011). In liver surgery, serum
and endocrine dysfunction are among the many chronic disease albumin is harder to interpret as a nutritional marker in patients
states that can lead to rapid muscle loss. Poor nutrition, altera- with cirrhosis, given its correlation with intrinsic liver function
tions in hormonal and other signaling pathways, as well as (Piquet et al, 2006). Likewise, with liver transplant, some have
inflammatory factors and cytokines are thought to be the prin- suggested a correlation between preoperative serum albumin
cipal mechanisms behind the development of sarcopenia in the and posttransplant complications (Fusai et al, 2006). However,
chronically ill (Kalyani et al, 2014; McMillan et al, 2009). serum albumin should not be used as a sole prognosticator
Several techniques have been used to identify the presence of nutritional status, given its relationship as an acute-phase
and magnitude of sarcopenia. The most clinically applicable reactant.
method uses computed tomography (CT) imaging to estimate
lean muscle mass (Janssen et al, 2002; Mourtzakis et al, 2008). Prealbumin
The method estimates lean muscle mass by measuring the area Also known as transthyretin, prealbumin is synthesized by the
of the psoas muscle of a single CT image at the L3 level nor- liver and serves as a transport protein. Unlike albumin, which
malized for height (total psoas area [mm2]/height [m2]). Patients has a half-life of approximately 20 days, prealbumin is rapidly
are sarcopenic if these values are less than 385 mm2/m2 in processed and is thought to be a better indicator of nutritional
women or less than 545 mm2/m2 in men. In retrospective status, given its half-life of 48 hours. As such, short-term fluc-
studies based on CT imaging, sarcopenic patients who under- tuations of nutritional standing can be more accurately assessed
went liver transplantation, liver resection of primary liver using serum prealbumin rather than albumin (Beck et al, 2002).
cancers, or colorectal metastases and pancreas resection had Unfortunately, like albumin, prealbumin is also an acute-phase
increased perioperative complications, increased postoperative reactant, and its measurement can vary with chronic disease
mortality, and worse overall and recurrence-free survival states. Huang et al (2012) studied the outcomes of liver resec-
(Englesbe et al, 2010; Harimoto et al, 2013; Itoh et al, 2014; tion in Child-Pugh Class A patients and found that serum pre-
Peng et al, 2012; Valero et al, 2015; van Vledder et al, 2012; albumin was significantly correlated with postoperative liver
Voron et al, 2015). A study in patients with liver transplants failure. Whether this relationship was the result of nutritional
found that serum albumin and Model for End-Stage Liver depletion or intrinsic liver disease remains unknown.
Disease (MELD) score correlated poorly with sarcopenia,
underscoring the fact that traditional measures of poor nutrition Nutritional Scoring Systems
may underestimate risk in these patients (Englesbe et al, 2010). Given the limitations of anthropometric and biochemical
Some studies have identified sarcopenia as an independent assays, more accurate methods of NA have incorporated key
risk factor for mortality in patients with cirrhosis (Meza-Junco features of both to create predictive nutritional scoring systems.
et al, 2013; Montano-Loza et al, 2011; Montano-Loza, 2014). Although a number of different schemas exist, the more fre-
In one study of cirrhotics, 70% of those who underwent tran- quently used include the Nutritional Risk Index (NRI), NRS,
sjugular intrahepatic portosystemic stenting had reversal of their Subjective Global Assessment (SGA), Malnutrition Universal
sarcopenia, which correlated with a lower mortality compared Screening Tool (MUST), and Glasgow Prognostic Score
with those whose sarcopenia did not improve or worsened (GPS).
(9.8% vs. 43.5%) (Tsien et al, 2013) (see Chapter 79). Others
have reported that exercise combined with supplemental protein Nutritional Risk Index
or amino acids can reverse sarcopenia in the elderly (Evans et al, Developed by the Veteran’s Affair Total Parenteral Nutrition
2014; Yang et al, 2012). These observations provide support for Group, the NRI (Box 26.4) calculates a risk score based on
the practice of prescribing exercise along with supplemental serum albumin and the ratio of present to usual weight. Its use
protein in patients identified to be sarcopenic prior to subjecting as a scoring system to reflect nutritional risk and predict adverse
them to HPB operations (Evans et al, 2014). outcomes has been validated (Cohendy et al 1999). The NRI
is simple to use and can define a high-risk subgroup of patients
Serum Biochemical Markers with obstructive jaundice considered for operation. In one
Although no single laboratory value is by itself indicative of study, patients with obstructive jaundice and a NRI less than
nutritional insufficiency, many have the benefit of being easily 83.5 were found to have a significant increased risk for
Chapter 26 Preoperative and postoperative nutrition in hepatobiliary surgery 453
Absent: Score 0 Normal nutritional status Absent: Score 0 Normal nutritional requirements
Mild: Score 1 Weight loss >5% in 3 mo or food intake Mild: Score 1 Hip fracture,* chronic patients, in
below 50%-85% of normal requirement particular with acute complications:
in preceding week cirrhosis, COPD,* chronic
hemodialysis, diabetes, oncology
Moderate: Score 2 Weight loss >5% in 2 mo or BMI 18.5-20.5 Moderate: Score Major abdominal surgery,* stroke,*
+ impaired general condition or food 2 severe pneumonia, hematologic
intake 25%-60% of normal requirement malignancy
in preceding week
Severe: Score 3 Weight loss >5% in 1 mo (>15% in 3 mo) Severe: Score 3 Head injury,* bone marrow
or BMI <18.5% + impaired general transplantation* Intensive care
condition or food intake 0%-25% of patients (APACHE >10)
normal requirement in preceding week
Score: + Score: = Total Score
Age: If ≥70 years, add 1 to total score above: = age-adjusted total score
Score ≥3: The patient is nutritionally at risk, and a nutritional care plan is initiated.
Score <3: Weekly rescreening of the patient. If the patient, e.g., is scheduled for a major operation, a preventive nutritional care plan is
considered to avoid the associated risk status.
*indicates that a trial directly supports the categorization of patients with that diagnosis. From Kondrup J, et al: Nutritional risk screening (NRS 2002): a new method based on an analysis of controlled
clinical trials, Clin Nutr 22(3):321. e36, 2003.
APACHE, Acute Physiology and Chronic Health Evaluation; BMI, body mass index; COPD, chronic obstructive pulmonary disease.
were present: BMI greater than 18.5 kg/m2, albumin less than
BOX 26.4 Nutritional Risk Index
3.0 g/dL, or mean weight loss greater than 10% of total body
Nutritional risk index = (1.519 × serum albumin [g/dL]) + (41.7 × weight in the preceding 6 months (Sanford et al, 2014). In
present weight [kg]/usual body weight* [kg]) geriatric patients, severe nutritional risk was independently
>100: Not malnourished
associated with significantly poorer survival on both univariate
97.5-100: Mild malnourishment
and multivariate analysis. Using these guidelines, geriatric
83.5-97.5: Moderate malnourishment
<83.5: Severe malnourishment patients with severe nutritional risk who underwent PD for
benign or premalignant indications had significantly decreased
*Usual weight is defined as the stable weight 6 mo or more before illness. overall 5-year survival compared with their nongeriatric coun-
terparts (65% vs. 93%, P < .001) (Sanford et al, 2014). The
authors concluded that patients with benign disease and low
postoperative death and longer duration of hospital stay but not NRS should be offered nonoperative therapy or no therapy
an increased complication rate (Clugston et al, 2006). Shinkawa until their NRS improves to a level that predicts a more favor-
and colleagues (2013) reviewed a series of more than 60 able outcome following operation.
patients undergoing PD and demonstrated the NRI to be an
independent risk factor for surgical-site infection on multivari- Subjective Global Assessment
ate analysis. The SGA analyzes patient-reported facets of nutritional health
to provide a NA (Detsky et al, 1987). The elements used in
Nutritional Risk Score the SGA include changes in dietary intake, weight loss, func-
First developed as a screening methodology by the European tional capacity, signs of muscle wasting, lower extremity edema,
Society of Parenteral and Enteral Nutrition in 2002, the NRS and GI symptoms. Severity of malnutrition is scored by a
(Table 26.1) encompasses patient age, food intake in the week trained examiner and used to classify perioperative risk. The
before surgery, weight loss, BMI, and severity of underlying SGA is a widely used assessment tool and has the advantage of
disease (Kondrup et al, 2003). The NRS has proved to be reli- not being influenced by fluid retention or ascites (Gunsar et al,
able and reproducible in retrospective analysis of more than 2006). However, the SGA has the disadvantage of subjectivity
100 controlled nutrition trials (Schiesser et al, 2008). When and interobserver variability, which is related to the memory of
analyzed prospectively in a cohort of more than 600 patients the patient and training of the examiner. When used in combi-
undergoing GI surgery, the NRS maintained an ability to iden- nation with other NA tools or biochemical markers of nutrition,
tify those deemed as malnourished with significantly more com- the SGA was able to predict patients who experienced postop-
plications as well as longer hospital stays (Schiesser et al, 2008). erative pancreatic surgery complications ranging from 82% to
The NRS has been adapted to preoperatively stratify geriatric 90% of instances (La Torre et al, 2013).
patients by the American College of Surgeons National Surgical
Quality Improvement Program. Preoperative screening is rec- Malnutrition Universal Screening Tool
ommended for geriatric and cancer patients using serum The MUST score is highly consistent with SGA scores to
albumin, BMI, and weight loss (Chow et al, 2012). Severe identify patients at nutritional risk (Loh et al, 2012). The
nutritional risk was shown to increase the risk of perioperative MUST is calculated by using BMI, weight loss, and an acute
morbidity and mortality when any of the following features illness component lasting longer than 5 days, during which the
454 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
Unplanned weight
BMI kg/m2 Score loss in past 3-6 months If patient is acutely ill and
>20 (>30 obese) =0 there has been or is likely to
% Score be no nutritional intake
18.5-20 =1
<18.5 =2 <5 =0 for >5 days
5-10 =1 Score 2
>10 =2
If unable to obtain height and weight, see Acute disease effect is unlikely to
reverse for alternative measurements and apply outside hospital. See “MUST”
use of subjective criteria Step 4 Explanatory Booklet for further
Overall risk of malnutrition information
FIGURE 26.1. Malnutrition Universal Screening Tool (MUST). BMI, Body mass index.
BOX 26.5 Glasgow Prognostic Score BOX 26.6 General Guidelines for Postoperative Nutritional
CRP level (>1.0 mg/dL) and hypoalbuminemia (<3.5 g/dL) = 2 points Support
CRP level (>1.0 mg/dL) or hypoalbuminemia (<3.5 g/dL) = 1 point Oral route > enteral > PICC > TPN
CRP level (<1.0 mg/dL) and normoalbuminemia (>3.5 g/dL) = 0 point kcal: 25-30 kcal/kg/day
Nitrogen: 1-1.5 g/kg/day
CRP, C-reactive protein.
Glucose: ≤5 mg/kg/min
Fat calories: ≤30% of total calories
patient is likely to have no nutritional intake (Fig. 26.1). Unlike PICC, Percutaneous indwelling central catheter; TPN, total parenteral nutrition.
NRI or SGA, the MUST is simple to use, can be performed
rapidly (usually <5 minutes), and is less expensive (Tu et al,
2012). When compared with SGA, MUST has good predictive BOX 26.7 Management of Perioperative Nutrition Complications
ability for perioperative mortality, hospital cost, and length of Management of Perioperative Nutritional Complications
stay (Kyle et al, 2006). Loh and colleagues (2012) demon- Anorexia: appetite stimulants
strated that three quarters of patients had a high calculated risk Chylous ascites: low-fat diet/medium-chain triglycerides
of malnutrition despite normal BMI because of recent weight Delayed gastric emptying: frequent, small meals; jejunostomy tube
loss. This study emphasizes the importance of unintentional feeds; TPN
weight loss, which was found to be the only significant predictor Pancreatic insufficiency: pancreatic enzymes
of adverse outcomes. La Torre et al (2013) reported a cohort Intraluminal bile deficiency: bile refeeding, oral ursodeoxycholic acid
of 143 patients who underwent pancreatic surgery for malig- TPN, total parenteral nutrition.
nancy and used MUST for nutritional screening. They identi-
fied that patients deemed to have high risk of malnutrition by
MUST had a fivefold higher surgical-site infection rate, four- procedure. An analysis of more than 120 patients with advanced
fold longer postoperative hospital course, and a morbidity rate PC demonstrated a significant association between median
of 53% compared with patients at low nutritional risk. Malnu- overall survival and GPS; patients scoring 2 points had an
trition defined by MUST was an independent predictor of overall survival of 1.8 months compared with 8.3 months for
overall morbidity. patients with 0 points (Martin et al, 2014). Although the exact
interplay between nutrition and systemic inflammation as mea-
Glasgow Prognostic Score sured by GPS is incompletely understood, it appears to be a
The GPS (Box 26.5) was created to quantify the magnitude of good measure of outcome in patients undergoing HPB surgery.
the systemic inflammatory response seen with malignancy and
was introduced initially as a marker of survival. The GPS clas- NUTRITIONAL SUPPORT OF
sifies patients with 0, 1, or 2 points depending on the presence PATIENTS UNDERGOING
of hypoalbuminemia (<35 g/L) or elevated C-reactive protein
(>10 mg/L) (Forrest et al, 2003). The GPS has been shown to
HEPATOPANCREATOBILIARY SURGERY
be predictive of poor survival in patients with cancer and is The primary goal for NS in patients before and after HPB
strongly associated with malnutrition, increased weight loss, surgery is to restore health and function as quickly as possible
increased perioperative morbidity, and poor performance status (Boxes 26.6 and 26.7). There are three principal ways to
(McMillan et al, 2013). Glen and colleagues (2006) demon- achieve this goal. The first is to enable patients to resume oral
strated the GPS to be a significant predictor of survival intake as soon as possible; this is facilitated by the use of
(independent of tumor-nodes-metastasis stage) for those enhanced recovery after surgery (ERAS) protocols. The second
patients with inoperable PC who underwent a palliative bypass is to support and/or restore normal digestion and intestinal
Chapter 26 Preoperative and postoperative nutrition in hepatobiliary surgery 455
absorption. The third is to identify nutritional deficits preop- Heidegger et al, 2007). In a few situations, specially formulated
eratively and to correct them. No data support the routine use diets may be beneficial for patients with hepatobiliary disease
of NS in well-nourished patients undergoing HPB surgery. In or PEI. For example, patients with diarrhea caused by malab-
fact, prospective, randomized trials have shown that the admin- sorption of fat may have improved tolerance to feeds with a diet
istration of PN to well-nourished patients undergoing surgery enriched with MCTs, which do not require micelle formation
is associated with a higher incidence of postoperative complica- for absorption or processing. In theory, dampening the proin-
tions (Brennan et al, 1994; Buzby, 1991). Conversely, patients flammatory response to illness and operation by administration
who are profoundly malnourished or deficient in specific vita- of water-soluble fatty acids alone or in combination with high
mins probably benefit from preoperative and postoperative NS doses of antioxidants has the potential to improve patient out-
(Buzby, 1991; Evans et al 2014; Halliday et al, 1988). comes (Braga et al, 2012; Ok et al, 2003; Persson et al, 2005).
The majority of patients with HPB disease who are malnour- Clinical evidence to support this theory is beginning to emerge,
ished do not require specialized NS to correct their nutritional but additional study is necessary to identify which patients are
deficits because, in most circumstances, their malnutrition is most likely to benefit (Wu et al, 2012).
the consequence of inadequate caloric intake during prolonged
periods of time, rather than maldigestion and malabsorption or Parenteral Nutrition
specific vitamin deficiency. Correction of malnutrition in these In the rare event when a patient fails to meet their total nutri-
patients only requires supplying sufficient quantity of appropri- tional needs by combined oral and enteral routes, the addition
ate substrate (fat, protein, and carbohydrate) (Klein, et al, of PN is appropriate. When this is the case, the initiation of PN
1997). There are no consensus guidelines supporting a certain should wait until at least 7 to 10 days after surgery to avoid
length of time of nutritional repletion to achieve a certain level adverse consequences (Casaer et al, 2011; Heidegger et al,
of risk reduction of operative complications. Experts recom- 2007; Marik, 2011; Martindale et al, 2009). The increased
mend at least 7 days and preferably 2 to 3 weeks of oral nutri- infectious complications and costs associated with PN mandate
tional repletion in patients who have profound malnutrition or that it is used only in patients with anatomic abnormalities of
until such time that the serum prealbumin rises to a normal the GI tract in whom EN is not feasible or fails (Braunschweig
range (Evans et al, 2014; Jie et al, 2012; Klein et al, 1999). et al, 2001; Heyland et al, 2003; Kreymann et al, 2006; Mar-
tindale et al, 2009; Meier et al, 2006; Plauth et al, 2006;
Routes of Feeding Weimann et al, 2006). High-quality studies have not found
There are several ways to provide patients NS preoperatively routine PN to be beneficial to patients undergoing HPB opera-
and postoperatively. Most common and physiologic is an oral tions in the first 2 weeks postoperatively (Bengmark, 2012).
diet tailored to the patient’s needs. If the patient is unable to Prolonged PN can cause hepatocellular steatosis and choles-
consume an oral diet or meet their estimated caloric needs tatic liver dysfunction (Bauer and Kiehntopf, 2014). In pancre-
orally, a nasogastric or nasoduodenal feeding tube should be atic surgery, routine postoperative PN after PD is associated
placed, even in the presence of known esophageal varices. If with increased morbidity (Brennan et al, 1994; Gianotti et al,
the patient is unable or unwilling to accept a nasoenteric feeding 2000). It is important that when PN is used, patients must not
tube, placing a feeding jejunostomy or gastrostomy tube using be given excess calories (e.g., they should receive <30 kcal/kg/
laparoscopic, interventional radiologic, or percutaneous endo- day), and glycemic control (serum glucose 100 to 150) should
scopic approaches should be considered. Profoundly malnour- be maintained with insulin.
ished patients with malabsorption who experience diarrhea in
response to enteral feeding can receive partial EN with the Enteral and Parenteral Nutrition
balance of calories, protein, fat, trace elements, and vitamins Some clinicians have tried a combination of EN and PN to
administered by the peripheral IV route until their intestinal more quickly meet patients’ estimated total caloric needs. Zhu
digestive and absorptive capacity adapts and allows them to a nd colleagues (2013) reported their outcomes comparing
tolerate higher amounts of EN (Kondrup et al, 2003). post-PD patients who were administered as combination EN
The physiologic beneficial effects of EN over PN are main- and PN with those who only received PN in the postoperative
tenance of intestinal immunity and gut integrity, prevention of period. Compared with the PN-only group, the combination
intestinal microbial translocation, reduced postoperative infec- group had a significant decrease in complications, hospital stay,
tions and sepsis, and less expense (Hilal et al, 2013; Kuboki and infections. Moreover, PD-specific complications such as
et al, 2013; Zhu et al, 2013). However, jejunal feeding can DGE and hyperglycemia were also reduced.
contribute to and/or exacerbate post-PD DGE. Martignoni and
colleagues (2000) showed a significant increase in nasogastric
Nutritional Support as Part of Enhanced Recovery after
intubation and prolonged hospital stay with postoperative Surgery Programs
jejunal EN. Perioperative feeding regimens have changed substantially
An enteral formula should be chosen based on the patient’s during the last decade with the advent of ERAS (Kehlet, 1997).
ability to digest and absorb nutrients. For most patients, a ERAS is a multimodal and multidisciplinary management
standard enteral diet is sufficient. The general guidelines for pathway whose goal is to more quickly restore health and func-
feeding listed in Box 26.6 are sufficient for most patients. There tion to patients by mitigating the catabolic stress response to
is no clinical evidence to support the administration of super- operation. A central tenet of ERAS is to limit preoperative
physiologic amounts of substrate (e.g., more than 5 mg/kg/min fasting and restore oral intake as soon as possible postopera-
of glucose or more than 2 g protein/kg/day. Conversely, there tively. Current ERAS guidelines recommend (grade A evi-
is evidence to suggest that “overfeeding” malnourished patients, dence) the use of preoperative oral carbohydrate supplementation
particular with carbohydrates and/or with diets rich in omega-6 2 to 3 hours before anesthesia (Lassen et al, 2012; Viganò et al,
fatty acids may be associated with harm (Buzby et al, 1988; 2012; Weimann, et al, 2006). This practice has been shown to
456 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
reduce psychological and physiologic stress, improve glycemic surgery or transplantation (Evans et al, 2014; Langer et al,
control during and after surgery, reduce skeletal muscle prote- 2012). Nevertheless, many believe that there is value to the
olysis and weakness, restore bowel motility, and reduce DGE administration of oral IMN and supplements to all patients
after PD (Viganò et al, 2012). The feasibility, safety, and utility undergoing high-risk surgery (Evans et al, 2014; Martindale
of ERAS in patients undergoing HPB operations has recently et al, 2009), and many centers using ERAS protocols incorpo-
been established and leads to reduced morbidity and shorter rate IMN as part of a multimodal perioperative care plan
hospital length of stay (Balzano et al, 2008; Braga et al; 2014; (Burden et al, 2012).
Coolsen et al 2013; Gerritsen A et al, 2014; Hendry et al 2010;
Hughes et al, 2014; Jones et al, 2013; Kagedan et al, 2015; Vitamins
Lassen et al, 2012; Revie et al 2012; Wong-Lun-Hing et al, Vitamins are considered to be essential components of periop-
2014). Although some ERAS programs have included the erative nutrition. Vitamin D, for instance, has been noted to be
administration of an immune-enhancing dietary supplement for deficient in three quarters of patients with pancreatic cancer at
5 to 7 days preoperatively, the value of such dietary supple- diagnosis, and this deficiency is associated with poor survival
ments to patients undergoing HPB operations within the (Cho et al, 2013). A 2005 placebo-controlled double-blind
context of an ERAS program have not been established. study of 47 patients who underwent partial liver resection dem-
The majority of patients managed within an ERAS protocol onstrated that the group receiving infusions containing vitamin
who do not experience a major complication, have rapid return E had a significantly shorter length of stay in the intensive care
of bowel function and tolerate ingestion of a normal diet within unit (ICU) and showed improvement in aspartate aminotrans-
24 to 48 hours of surgery independent of the type of operation ferase, alanine aminotransferase, and glutamic dehydrogenase
(Hughes et al, 2014; Kagedan et al, 2014, Revie et al, 2012; van (Bartels et al, 2004). Vitamin C is clinically important in peri-
Dam et al, 2008). Conversely, patients who fall off of an ERAS operative healing (Cevikel et al, 2008). Patients who are active
pathway, (e.g., do not tolerate an oral diet within a few days of smokers have significant reductions in total body and circulat-
surgery) usually have an underlying major complication, such as ing vitamin C and should receive preoperative supplementa-
liver failure, intraabdominal collection, fistula, or systemic infec- tion. In the perioperative period, vitamin C concentrations are
tion. In a systematic review of the literature, Kagedan et al significantly reduced and can fall even further with prolonged
(2015) reported on 10 ERAS studies in patients undergoing PD. hospitalization and complications (Fukushima et al, 2010).
Nasogastric tubes were discontinued either at the end of opera- This decrease in vitamin C can adversely affect other compo-
tion or on the first postoperative day. In the majority of studies, nents of perioperative recovery, such as muscle weakness,
patients were allowed access to and tolerated solid food on the fatigue, and physical performance (Lukaski, 2004). Although
first or second postoperative day. A systematic review of five randomized clinical trials have yet to show that preoperative
feeding routes after PD concluded that an oral diet is the pre- administration of vitamins A, D, E, and C reduce perioperative
ferred route of feeding and that there is no evidence to support morbidity, it makes physiologic sense to do so and is safe (Evans
routine EN or PN after PD (Gerritsen et al, 2013). Lassen et al et al, 2014). When considering the fact that vitamins are cheap,
(2012) observed that it was safe to allow patients undergoing safe, and readily available, and that patients undergoing HPB
major upper GI surgery, including all types of HPB surgery, to operations are at risk for oxygen radical–mediated injury, it is
eat normal food at will beginning on the first day after surgery. reasonable to consider administration of vitamins E and C for
ERAS regimens in patients undergoing liver surgery routinely several days preoperatively in patients at risk for postoperative
allow patients a regular diet at will beginning the night of surgery complications.
(Coolsen et al, 2012; Dunne et al, 2014; Hughes et al, 2014;
Jones et al, 2013; van Dam et al, 2008). These studies demon- Probiotics and Synbiotics
strate that patients undergoing PD or liver resection do not need A recent area of interest within NS science is the use of both
prolonged gastric decompression, nor do they have to wait for prebiotics and probiotics (synbiotics) in combination with EN
return of bowel function to tolerate an oral diet. However, there to enhance GI immunity. A prospective, randomized, double-
are patients who will not tolerate early oral feeding. Unfortu- blind trial treated postoperative liver transplant recipients with
nately, there is no reliable way to identify these patients. Never- EN and a combination of lactic acid bacteria and fiber, and it
theless, until new clinical studies demonstrate that an early reduced bacterial infection rates from 48% to 3% following
postoperative oral diet is harmful, patients should be allowed to liver transplantation (Rayes et al, 2005). This resulted in
eat normal food at will shortly after major HPB operations. shorter ICU and overall hospital stays and duration of antibiotic
treatment. Zhang et al (2013) retrospectively reviewed 67 post
Immune-Modulating Nutrition liver transplant recipients who took probiotics and fiber and
The potential benefit of administering immune-modulating showed a significant reduction in infection rate from 30% to
nutrition (IMN) and antioxidants to patients undergoing HPB 9%, compared with controls. Sugawara and colleagues (2006)
surgery is controversial, although of increasing interest (Evans randomly assigned more than 100 patients who underwent
et al, 2014). Several meta-analyses concluded that specialized hepatic resection for biliary cancers to preoperative and post-
oral supplements enriched with ω3FAs, arginine, and gluta- operative synbiotics or standard postoperative supplements and
mine given orally for 7 to 14 days preoperatively reduced the found that the symbiotic group had a lower incidence of post-
risk of postoperative complications, particularly infection, fol- operative infectious complications (12% vs. 30%).
lowing upper GI surgery (Braga et al, 2013; Burden et al, 2012;
Marik et al, 2010, Marimuthu et al, 2012). ω3FAs adminis- Appetite Stimulants
tered parenterally preoperatively have also been shown to One strategy to improve perioperative malnutrition has used
decrease levels of IL-6 and TNF in patients undergoing hepa- dietary stimulants. The most common approach is through the
tectomy for HCC (Wu et al, 2012). Other reviews have reported administration of oral megestrol acetate (MA), a derivative of
no conclusive evidence to support the use of IMN in GI tract progesterone. The mechanism by which MA increases appetite
Chapter 26 Preoperative and postoperative nutrition in hepatobiliary surgery 457
postoperative day. Almost all patients are able to tolerate a full much difficulty or patient discomfort. The routine use of PN
regular diet within 5 days. Malnourished patients being consid- in malnourished patients undergoing liver transplantation
ered for elective liver resection should receive nutritional reple- (Reilly et al, 1990) is no longer considered appropriate
tion preoperatively and postoperatively by the oral and/or because the majority of patients can be fed EN successfully
enteral route. and safely by a nasoduodenal or NJ tube within hours after
It is strongly recommended that patients not receive hyper- transplantation (Mehta et al, 1995; Sekido et al, 2003). In
tonic glucose infusions in the immediate (<6 hours) postopera- several studies, early initiation of EN after operation (<24
tive period because this can interfere with the liver’s preferential hours) was associated with a postoperative infection rate that
use of fatty acids for energy and hepatic regeneration. If NS is was lower than expected (Hasse et al, 1995; Martin et al,
desired within hours after liver resection, and it is anticipated 1993; Mehta et al, 1995; Wicks et al, 1994). In a prospective,
that the patient will not be able to take an oral diet (e.g., in the randomized study reported by Hasse and colleagues (1995),
event they are intubated), then intraoperative placement of a patients receiving EN had no viral infections in the first 2
nasoduodenal or jejunal tube should be considered. postoperative weeks. Bacterial and overall infection rates also
Several prospective randomized clinical trials have reported were decreased in the EN group (14% vs. 29%, and 21% vs.
that the administration of PN enriched with BCAAs is of 41%, respectively). Postoperative liver transplant patients fed
benefit to patients undergoing liver resection. Fan and col- immediately via the enteral route also have a decreased inci-
leagues (1994) showed a benefit of preoperative and postopera- dence of postoperative ileus (5% vs. 28%; P < .01) and started
tive BCAA-enriched PN in cirrhotic patients undergoing an oral diet much sooner (8 days vs. 12 days; P = .07) than
elective liver resection for HCC. The PN-supplemented group patients given PN (Mehta et al, 1995). BCAA supplementa-
had reduced septic complications compared with controls tion has been shown to improve metabolic and nutritional
(17% vs. 37%), less deterioration of liver function, and less abnormalities in the early posttransplant period by increasing
ascites. Postoperative mortality in the PN group was also 45% albumin synthesis and improving liver function (Yoshida et al,
less than in the control group. In two other studies, Okabayashi 2012).
and colleagues (2008, 2011) reported that oral supplementa-
tion with carbohydrate- and BCAA-enriched nutrients reduced Pancreatic Cancer
postoperative complications and improved postoperative The most common presenting conditions of patients with pan-
quality of life in patients with chronic liver disease undergoing creatic head cancers (see Chapter 62) are PEI and steatorrhea.
hepatic resection for HCC. There are no data to support the Sikkens et al (2014) reported the prevalence of PEI was 66%
use of BCAAs in patients without liver disease who undergo in a cohort of pancreas cancer patients, which increased to 92%
liver resection. after 2 months. Fortunately, this nutritional deficiency can be
easily corrected with pancreatic enzyme replacement therapy,
Liver Transplantation which should be taken with every meal and snack (Domínguez-
Clinical and experimental observations show that nutrition Muñoz, 2011; Sikkens et al, 2010). Even in cases of surgical
plays an extremely important role in just about all aspects of or medical futility, relief of exocrine insufficiency can signifi-
liver transplantation (see Chapter 112). The status of the cantly palliate symptoms and improve quality of life. Pancreatic
donor, the function of the transplanted liver, the overall health head cancers can also lead to biliary obstruction. As neoadju-
of the recipient, the rejection process, the absorption and vant chemotherapy is more frequently used as part of a multi-
metabolism of immunosuppressive drugs, and a variety of disciplinary treatment approach for pancreatic cancer, enteric
metabolic pathways are influenced by nutrients and how they flow of bile is preferable and can be achieved with use of endo-
are administered. Clinical observations show that malnour- scopic stenting or percutaneous drainage and refeeding. In fact,
ished patients undergoing liver transplantation have a signifi- many chemotherapeutic agents cannot be administered safely
cantly poorer outcome than well-nourished patients (Porayko in the setting of biliary obstruction.
et al, 1991). They have an incidence of infectious morbidity
and 3-month mortality rates twice that of well-nourished SUMMARY
patients undergoing liver transplant (Harrison et al, 1997).
Pretransplant nutritional status and disease severity are inde- Careful attention must be paid to the HPB patient’s overall
pendently associated with infectious episodes during hospital- clinical condition, inadequacy of diet, degree of malnutrition,
ization (Meril et al, 2009). Degree of malnutrition also metabolic derangements, and impaired digestion and absorp-
correlates significantly with days spent in the ICU, days spent tion to determine the appropriate level and type of NS. Inap-
mechanically ventilated, and length of hospital stay, and also propriate nutritional support, particularly the provision of
correlates significantly with mortality after transplantation excess calories via PN and poor glycemic control, are poten-
(Meril et al, 2009; Pikul et al, 1994). tially harmful. Increasing evidence shows that specific nutrients
Patients awaiting transplantation who are malnourished administered under specific conditions to select patients can
should receive aggressive nutritional counseling and support modulate metabolic events in patients with hepatobiliary
(Cabré & Gassull, 2001; Hasse et al, 1995; Mehta et al, 1995). disease undergoing operation. Before prescribing nutritional
Nutritional supplements, including vitamins, should be taken therapy to a patient, a clinician or dietician with experience and
in an effort to attenuate further nutritional deficits and to expertise in liver metabolism should be consulted to evaluate
replenish losses. Patients who ingest inadequate amounts of the patient, provide nutritional recommendations, and monitor
calories should be fed EN via a soft nasal feeding tube. In the patient’s course.
contrast to what most people and physicians believe, these
tubes are well tolerated and can be used for months without References are available at expertconsult.com.
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1369, 2009. tion in patients undergoing pancreaticoduodenectomy, World J Gas-
Yang Y, et al: Resistance exercise enhances myofibrillar protein synthe- troenterol 19(35):5889–5896, 2013.
sis with graded intakes of whey protein in older men, Br J Nutr
108:1780–1788, 2012.
CHAPTER 27
Postoperative complications requiring intervention:
diagnosis and management
Stephen B. Solomon, James F. Griffin, Matthew J. Weiss, and Franz Edward Boas
OVERVIEW the surgical mortality from 25% to less than 2% at some high-
volume centers, whereas morbidity has remained essentially
During the last 2 decades, the number of complex pancreatic unchanged (Cameron & He, 2015) (see Chapter 66). The
and hepatic resections performed in the United States has reported morbidity and mortality following pancreatic resection
steadily increased along with a significant decrease in associated in several large series reported since 2000 is presented in Table
perioperative mortality (Allen, 2007; Cameron & He, 2015; 27.1. For pancreaticoduodenectomy (PD), overall periopera-
Dimick et al, 2004; Jarnagin et al, 2002; Nathan et al, 2012; tive mortality ranges from 1.6% to 9%, whereas reported mor-
Winter et al, 2006). This is due in part to a trend toward surgi- bidity ranges from 35% to 45% (Büchler et al, 2000; Cameron
cal specialization and centralization of care at high-volume & He, 2015; Mezhir et al, 2009; Muscari et al, 2006; Winter
institutions, where the inverse volume-outcomes relationship et al, 2006).
has been well described for many complex procedures (Finks Pancreatic resection is associated with a host of complica-
et al, 2011; Nathan et al, 2009; Stitzenberg et al, 2009; Valero tions, many of which are procedure specific and occur at the
et al, 2015). Despite the observed decrease in postoperative operative site (hemorrhage, leak, obstruction), whereas others
mortality, morbidity has remained essentially unchanged, with occur remotely as a consequence of major surgery rather than
most large series reporting a 35% to 45% major complication the specific type of surgery (deep venous thrombosis, cardiac
rate following either pancreatic or hepatic resection (Cameron arrhythmia, pneumonia). This chapter is primarily concerned
& He, 2015; Kneuertz et al, 2012; Nathan et al, 2009; Vin with the most common severe complications directly related to
et al, 2008). the technical aspects of the operation itself. In the case of pan-
This widening gap between morbidity and mortality implies creatic resection, this includes delayed gastric emptying (DGE),
an improved ability to manage postoperative complications intraabdominal fluid collection or abscess, pancreatic fistula,
when they occur, thereby rescuing patients who previously and postoperative hemorrhage. The reported frequencies of
would have died (Bassi et al, 2001; Sohn, 2003). This is par- these complications are listed in The reported frequencies for
tially due to earlier and more effective detection based on famil- these complications in several large series since 2000 are pre-
iarity with procedure-specific complications and advances in sented in Table 27.2 and a comprehensive list of complications
high-quality imaging. Another reason is the shift in management from the Johns Hopkins series (Winter et al, 2006) is presented
from operative reexploration to interventional and endoscopic in Table 27.3.
techniques that are effective with much less added morbidity
(Sohn, 2003; Vin et al, 2008). Interventional radiologists now
Defining and Grading Complications
make up an indispensible part of the multidisciplinary team After Pancreatectomy
caring for patients undergoing complex hepatopancreatobiliary Postoperative complications are notoriously difficult to study
procedures and their expertise in the minimally invasive treat- due to the inconsistent definitions and imprecise terminology
ment of anastomotic leaks, intraabdominal abscesses, and post- used to designate them (see Chapter 66). Before the formal
operative bleeding is responsible for significantly improved definition of postoperative pancreatic fistula (POPF) (Bassi
patient outcomes (Mezhir, 2013; Sohn, 2003). et al, 2005), pancreatic leaks, fistulae, and intraabdominal
This chapter will provide an overview of the most commonly abscesses were indicative of this problem (Mezhir, 2013). They
reported postoperative complications associated with major comprise three overlapping manifestations of the same underly-
pancreatic and hepatic resections, including a review of the ing issue, which is breakdown and leakage at the pancreatic
current definitions and grading systems used for reporting. It anastomosis (or pancreatic closure site for distal and central
will then provide a detailed discussion of the appropriate man- pancreatectomies). For example, an intraabdominal fluid col-
agement of each complication according to the most current lection requiring drain placement could reasonably be reported
literature and with an emphasis on interventional techniques. as an abscess. If the drainage was studied and found to be
amylase rich, it could be considered a leak. If drainage from
PANCREATECTOMY the leak persisted during a period of time, it could also be
considered a fistula. However, the absence of any standardized,
Before the 1980s, the high morbidity and mortality rates associ- quantifiable measures for reliably differentiating these from
ated with pancreatic resection led many surgeons to all but one another meant that the same complication could be
abandon the procedure. Since that time, significant improve- reported in three different ways. This inconsistency in reporting
ments in surgical technique and postoperative care have reduced was demonstrated by Bassi and colleagues (2004), who
459
460 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
Pancreaticoduodenectomy
Büchler et al, 2000 1993-1999 331 127 (38) 7 (2)
Muscari et al, 2006 1995-1999 300 117 (39) 28 (9)
Winter et al, 2006 1970-2006 1175 415 (35) 26 (2)
Mezhir et al, 2009* 2000-2005 340 147 (43) 9 (3)
Braga et al, 2011 2002-2010 700 432 (67) 27 (4)
Cameron and He, 2015 1969-2012 2000 894 (45) 31 (1.6)
Distal Pancreatectomy
Kooby et al, 2008*† 2002-2006 342 334 (98) 1 (0.3)
Kleef et al, 2007 1993-2006 302 105 (35) 6 (2)
Goh et al, 2008 1986-2006 232 107 (46) 7 (3)
Nathan et al, 2009 1984-2006 704 232 (33) 7 (1)
Central Pancreatectomy
Sauvanet et al, 2002† 1990-1998 53 22 (42) 1 (2)
Roggin et al, 2006 1993-2005 10 6 (60) 0 (0)
Crippa et al, 2007† 1990-2005 100 58 (58) 9 (9)
Adham et al, 2008 1987-2005 50 18 (36) 0 (0)
Ocuin et al, 2008 2000-2007 13 12 (92) 1 (8)
Hirono et al, 2009 1999-2008 24 12 (50) 1 (4)
Total Pancreatectomy
Karpoff et al, 2001 1983-1998 35 15 (54) 1 (3)
Billings et al, 2005‡ 1985-2002 99 32 (32) 5 (5)
Müller et al, 2007 2001-2006 100 38 (38) 6 (6)
Reddy et al, 2009 1970-2007 100 69 (69) 8 (8)
Watanabe et al, 2015‡ 1990-2013 44 14 (32) 2 (5)
Epelboym et al, 2013 1994-2011 77 37 (49) 2 (3)
*Matched case-control study.
†
Multiinstitutional study.
‡
Includes completion pancreatectomy patient(s).
systematically reviewed the definitions used for reporting pan- complications after pancreatectomy. Note that the grade of the
creatic fistulae. They generated four consensus definitions rep- complication increases only when a new, more invasiveness or
resentative of those most commonly used in the literature and aggressive treatment is required for management.
applied each to the same control group of pancreatectomies. An example of this in the surgical literature is the develop-
Using these four definitions, the incidence of pancreatic fistulae ment of the Clavien-Dindo classification of surgical com
varied within the same group of patients from 10% to 29%. plications. Clavien and colleagues (1992) recognized the
This lack of consistency is reflected in the literature, where the inconsistency in reporting surgical complications in 1992 and
actual reported incidence of pancreatic fistulae varies similarly proposed a definition and classification system for grading them
from 2% to 29% (Braga et al, 2011; Büchler et al, 2000; in a standardized fashion. A complication, as defined by
Muscari et al, 2006; Reid-Lombardo et al, 2007). Clavien, is any deviation from the normal postoperative course
Regardless of the difficulty inherent in defining complica- and is differentiated from a sequela, which is an “after-effect”
tions, accurate measurement and documentation in a standard- of surgery inherent to the procedure (e.g., inability to walk after
ized manner is vital to improving quality of care by allowing a leg amputation), and a failure to achieve the primary objective
meaningful comparisons between procedures, institutions, and of the surgery, which is a “failure to cure” (e.g., residual tumor
even individual surgeons. With this in mind, several institutions after surgery). The system was updated in 2004 as the Clavien-
have developed classification and grading systems for surgical Dindo classification, which is a graded system of increasing
complications based on the Common Terminology Criteria for severity determined by the presumed long-term consequences
Adverse Events (CTCAE), a system used by the National Insti- of a given complication as well as the invasiveness, level of care,
tutes of Health Cancer Therapy Evaluation Program for clinical and resources required for the intervention needed to correct
trials since 1982 (Clavien et al, 1992, 2009; DeOliveira et al, it (Dindo et al, 2004). The system is made up of five grades,
2006; Grobmyer et al, 2007). This approach supplies a simpli- two of which have subgroups, and a suffix “d” category that
fied, unifying definition for each complication, with grades of can be appended to any grade. Grade I and II complications
increasing severity based upon the clinical impact of the com- are minor and need no specific therapy (I) or pharmacologic
plication and the invasive of the required treatment. Table 27.4 treatment only (II). Complications requiring invasive interven-
demonstrates an example of this approach applied to common tion (endoscopic, radiologic, or surgical) are classified as grade
Chapter 27 Postoperative complications requiring intervention: diagnosis and management 461
Pancreaticoduodenectomy
Büchler et al, 331 127 (38) 7 (2) 4 (1) 54 (16) 12 (4) 13 (4) 13 (4)
2000
Muscari et al, 300 117 (39) 50 (17) 15 (5) — 18 (6) — —
2006
Winter et al, 1175 415 (35) 52 (4) 38 (3) 161 (14) — 91 (8) 35 (3)
2006
Reid- 1507 — 196 (13) 97 (6) 187 (12) 54 (4) — 53 (4)
Lombardo
et al, 2007*
Mezhir et al, 340 147 (43) 20 (6) 23 (7) 29 (9) 12 (4) 46 (14) —
2009†
Braga et al, 700 432 (67) 200 (29) 42 (6) 105 (15) 36 (5) 58 (8) 56 (8)
2011
Cameron and 2000 894 (45) 295 (15) — 410 (21) 32 (2) 222 (11) 69 (3.5)
He, 2015
Distal Pancreatectomy
Kooby et al, 342 170 (50) 99 (29) — — — 36 (11) 6 (2)
2008*†
Kleef et al, 302 105 (35) 35 (12) 14 (5) 14 (5) 10 (3) 8 (3) 26 (9)
2007
Goh et al, 232 107 (46) 72 (31) — — — 17 (7) 11 (5)
2008
Nathan et al, 704 232 (33) 203 (29) 36 (5) — — — 40 (6)
2009
Central Pancreatectomy
Sauvanet et al, 53 22 (42) 16 (30) 3 (6) 1 (2) 2 (4) 2 (4) 3 (6)
2002*
Roggin et al, 10 6 (60) 3 (30) — — 1 (10) — 1 (10)
2006
Crippa et al, 100 58 (58) 44 (44) 15 (15) 2 (2) 1 (1) — 0 (0)
2007*
Adham et al, 50 18 (36) 4 (8) 7 (14) — 3 (6) — 6 (12)
2008
Hirono et al, 24 12 (50) 15 (63) 1 (4) 1 (4) 0 (0) 1 (4) 0 (0)
2009
Total Pancreatectomy
Karpoff et al, 35 15 (54) NA — — — — —
2001
Billings et al, 99 32 (32) NA 6 (6) 8 (8) — 4 (4) 2 (2)
2005‡
Müller et al, 100 38 (38) NA 2 (2) 8 (8) 2 (2) 2 (2) 15 (15)
2007
Reddy et al, 100 69 (69) NA — 11 (11) 14 (14) 18 (18) —
2009
Epelboym 77 37 (49) NA — — — — —
et al, 2013
Watanabe 44 14 (32) NA — 4 (9) — 2 (5) —
et al, 2015‡
*Multiinstitutional study.
†
Matched case-control study.
‡
Includes completion pancreatectomy patient(s).
—, Not available; DGE, delayed gastric emptying; NA, not applicable.
462 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
Gastroparesis
An incomplete paralysis of Mild nausea, early Moderate symptoms; Weight loss refractory to — —
the muscles of the satiety, and able to maintain medical intervention;
stomach wall, resulting bloating; able to nutrition with dietary unable to maintain
in delayed gastric maintain caloric and lifestyle nutrition orally
emptying into the small intake on regular modifications; may
intestine diet need pharmacologic
intervention
Abdominal Infection
An infectious process — — IV antibiotic indicated; Life-threatening Death
involving the abdominal radiologic or operative consequences;
cavity intervention indicated urgent intervention
indicated
Intraabdominal Hemorrhage
Bleeding in the abdominal – Medical intervention or Transfusion, radiologic, Life-threatening Death
cavity minor cauterization endoscopic, or consequences;
indicated elective operative urgent intervention
intervention indicated indicated
Wound Infection
An infectious process — Localized; local IV antibiotic indicated; Life-threatening Death
involving the wound intervention indicated radiologic or operative consequences;
(e.g., topical antibiotic) intervention indicated urgent intervention
indicated
Pancreatic Fistula
An abnormal Asymptomatic; Symptomatic; altered GI Severely altered GI Life-threatening Death
communication between clinical or function function; tube feeding consequences;
the pancreas and diagnostic or TPN or urgent operative
another organ or observations only; hospitalization intervention
anatomic site intervention not indicated; elective indicated
indicated operative intervention
indicated
CTCAE, Common Terminology Criteria for Adverse Events; IV, intravenous; GI, gastrointestinal; TPN, total parenteral nutrition.
Antibiotic intervention includes antifungal and antiviral therapy.
Modified from http://www.ctep.info.nih.gov.
first introduced the idea of exocrine inhibition for the preven- 1995; Montorsi et al, 1995; Pederzoli et al, 1994). Unfortu-
tion of POPF in 1979 when they reported lower complication nately, American trials did not recapitulate these early findings
rates following perioperative continuous somatostatin infusion. and instead showed no reduction in rates of POPF (Lowy et al,
A long-acting synthetic version of somatostatin called octreotide 1997; Yeo et al, 2000). A new somatostatin analogue called
has been studied for use in pancreatic surgery, and several pasireotide, which has a longer half-life and broader binding
European studies initially reported decreased overall complica- profile compared with octreotide, has shown promise recently
tion rates, including POPF (Büchler et al, 1992; Friess et al, in reducing rates of POPF. Allen and colleagues (2014)
464 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
conducted a single-center, randomized, double-blind trial of tion following upper GI tract surgery, particularly after pancre-
perioperative subcutaneous pasireotide in 300 patients under- atic surgery. In many cases, DGE is associated with concurrent
going either PD or distal pancreatectomy and observed a sta- intraabdominal abscesses or POPF and results in significantly
tistically significant decrease in POPF compared with placebo longer hospital stays and increased health care costs (Beane
(9% vs. 21%; P = .006). These results will have to be validated et al, 2014; Yeo et al, 2002). According to the studies included
with additional prospective trials, but there is currently opti- in Table 27.2, incidence of DGE following PD ranges from 9%
mism for a viable new therapy on the horizon. to 21%, although many reports are even higher, depending on
Once POPF develops, by definition, only grades B and the definition used. In 2007, the International Study Group for
C are of any clinical significance warranting specific inter Pancreatic Surgery (ISGPS) proposed a consensus definition
vention. Uncomplicated low-output fistulae can be managed that classified DGE into grades A, B, and C according to clini-
conservatively, which includes adequate drainage of intraab- cal impact determined by nasogastric tube (NGT) require-
dominal collections (see Image-Guided Abdominal Drainage) ment, ability to tolerate oral intake, and need for prokinetic
(see Chapter 30), restriction of oral intake, and nutritional therapy (Tables 27.6A and B) (Wente et al, 2007a). Further-
support (see Chapter 26). Empiric antibiotic therapy may be more, it stipulated that the patient must first undergo an upper
initiated if there is any concern for infection, and all drains GI contrast series or endoscopic evaluation to rule out mechan-
should be kept in place with outputs measured regularly. ical obstruction, such as an early postoperative small bowel
With conservative management, spontaneous fistula closure obstruction or stricture at the anastomosis. Subsequent valida-
will occur in as many as 90% of cases, usually within 4 weeks tion by several studies reported postoperative DGE rates of
(Machado, 2012). 14% to 45%, with grade-specific rates of 6% to 27% (grade A),
A key element of the conservative approach to management 7% to 11% (grade B), and 1% to 12% (grade C) (Akizuki et al,
of POPF is avoidance of oral intake, which prevents food- 2009; Chong et al, 2015; Malleo et al, 2010; Park et al, 2009;
induced stimulation of pancreatic secretions. However, pro- Welsch et al, 2010). The new definition actually increased
longed fasting results in rapid nutritional depletion and impaired reported rates of DGE for some series that previously used
wound healing, so two forms of nutritional support are advo- much more stringent definitions (Akizuki et al, 2009; Malleo
cated for maintaining patients until resolution of their fistulae: et al, 2010).
total parenteral nutrition (TPN) and enteral nutrition (EN) The management of DGE generally consists of supportive
delivered via a distally positioned nasointestinal tube or feeding care, beginning with discontinuation of oral intake and reinser-
jejunostomy (Malleo et al, 2014) (see Chapter 26). tion of an NGT for gastric decompression. Once an upper GI
TPN has traditionally been the mainstay in nutritional series or endoscopy has ruled out mechanical obstruction,
support for POPF because it avoids stimulation of GI secretions patients may be started on a prokinetic agent to improve symp-
and is usually able to meet all necessary nutritional require- toms and shorten time to recovery. If symptoms persist for an
ments. However, long-term complications associated with TPN extended period, the patient may also require some form of
are significant and include sepsis, metabolic derangements, cir- nutritional support and warrants a cross-sectional imaging
rhosis, and atrophy of the GI tract with gut barrier dysfunction evaluation to look for secondary causes of DGE, such as an
(Klek et al, 2011; Malleo et al, 2014). Enteral feeding avoids intraabdominal abscess.
these complications because it does not require a long-term The underlying cause of DGE is unclear and likely multi-
central venous catheter, and it has a trophic effect on the GI factorial, but it may result in part from decreased circulating
tract. Initially, there were concerns that enteral feeding would levels of motilin, a prokinetic peptide hormone located in the
increase exocrine pancreatic secretion and prolong or worsen enterochromaffin cells of the duodenum and proximal small
POPF. In a randomized comparison of TPN and EN in patients intestine (Yeo et al, 1993). Erythromycin, a macrolide antibi-
with grade B POPF, EN was associated with a greater than otic, acts as a motilin agonist and binds its receptors to stimu-
twofold increased probability of fistula closure, with shortened late gastric emptying. Randomized, controlled trials evaluating
times to closure and lower overall cost (Klek et al, 2011) (see erythromycin for use in pancreatic surgery have shown
Chapter 26). decreased incidence of DGE, decreased rates of NGT reinser-
tion, shorter duration of NGT insertion, and shorter time to
Delayed Gastric Emptying oral feeding (Ohwada et al, 2001; Yeo et al, 1993). Based on
Delayed gastric emptying (DGE) is a functional gastroparesis these results, erythromycin is now often used in the treatment
without mechanical obstruction that may occur as a complica- of postoperative DGE.
sources of bleeding, which influences the type of interventions extraluminal source of bleeding may present as intraluminal
available for treatment. This classification system is meant to bleeding should it originate in the setting of an anastamotic
generate groups of increasing clinical impact such that grade A failure, such as a pancreatic dehiscence.
does not result in significant deviation in the normal clinical
course, grade B requires specific therapy and a prolonged hos- POSTPANCREATECTOMY HEMORRHAGE VALIDATION STUDIES
pital stay, and grade C is potentially life threatening and requires Despite the ISGPS authors’ attempt at formulating an explicit
invasive treatment (Wellner et al, 2014). set of guidelines to standardize the definition of PPH, validation
Time of onset may be within 24 hours of surgery (early) or studies to date have reported mixed results. This is partly
anytime thereafter (late). Early hemorrhage is usually indicative because databases used for retrospective analyses often do not
of a technical failure to achieve adequate hemostasis in the capture clinically insignificant mild to moderate bleeding
operating room, whereas late hemorrhage usually occurs in the events. Moreover, the definition relies on nonspecific surrogate
setting of inflammatory intraabdominal processes (pancreatic markers for bleeding, which do not necessarily correlate with
leaks, abscesses, fistulae, and anastomotic ulceration) that actual or surgery-specific bleeding. With this in mind, several
cause vascular erosion or the formation of arterial pseudoaneu- validation studies narrowed the scope of their evaluations by
rysms (Rajarathinam et al, 2008; Wellner et al, 2014; Welsch applying the definition only to severe bleeding, delayed bleeding,
et al, 2011). Late hemorrhages are the most deadly because and/or bleeding from the surgical site (Correa-Gallego et al, 2012;
they can occur unexpectedly days to weeks after surgery— Grützmann et al, 2012; Rajarathinam et al, 2008; Yehuda et al,
between postoperative days 7 and 32 in one study (Choi et al, 2014). These studies report an overall incidence of PPH
2004)—and often present as abrupt, massive bleeding. ranging from 3% to 10.4%, with individual grades ranging from
The severity of hemorrhage is classified as mild or severe 0% (A), 0.6% to 1.7% (B), and 1.2% to 10.4% (C) (Correa-
depending on the degree to which it impacts the postoperative Gallego et al, 2012; Grützmann et al, 2012; Rajarathinam
course. Mild hemorrhage has minimal clinical impact and is et al, 2008; Wellner et al, 2014; Yehuda et al, 2014). Mortality
defined as a drop in hemoglobin concentration of less than among those affected ranges from 3% to 29%, of which the vast
3 g/dL requiring no more than three U of packed red blood majority (71% to 100%) occurs in association with grade C
cells (PRBCs) and no invasive interventions. Alternatively, hemorrhage.
severe hemorrhage is life threatening and characterized by a Two additional studies, one prospective (Ricci et al, 2012)
drop in hemoglobin of greater than or equal to 3 g/dL, with and one retrospective (Welsch et al, 2011), applied the consen-
clinical signs of significant volume loss (tachycardia, hypoten- sus definition strictly as written and reported much higher rates
sion, oliguria) requiring more than three U of PRBCs and/or of PPH, from 27% to 29%. The incidence for each grade was
invasive intervention. 1.8% to 4.8% (A), 15.2% to 20.4% (B), and 5.4% to 9.2%
Location refers to the source of bleeding, which is either intra- (C), with mortality ranging from 7.3% to 19.4%. These studies
luminal (bleeding into the GI tract) or extraluminal (bleeding demonstrate a higher incidence of PPH with a lower associated
into the abdominal cavity). Intraluminal hemorrhage usually mortality, which reflects a broader inclusion of mild to moder-
originates from anastomotic sites, marginal or stress ulcers, and ate bleeding events. In many cases, patients had bleeding,
the cut surface of the pancreas and presents clinically as melena/ transfusions, and mortality unrelated to their surgery that
hematochezia, hematemesis, or blood loss through the NGT. resulted in frequent false positives. For example, patients
Extraluminal bleeding originates from peripancreatic vessels, requiring transfusion for underresuscitation in the operating
pseudoaneurysms, external staple/suture lines, and raw surfaces room, fluid and blood-product management in the setting of
in the operative field. This form of bleeding may be evident sepsis, higher hemoglobin goals due to cardiovascular comor-
from the wound and abdominal drains, or there may be no bidities, or bleeding from unrelated causes or procedures would
external signs of bleeding. It is important to note that an still be considered PPH based on the broad surrogate markers
Chapter 27 Postoperative complications requiring intervention: diagnosis and management 467
used for inclusion (Ricci et al, 2012; Welsch et al, 2011). Hounsfield U) collections. Active arterial bleeding can be seen
Despite these shortcomings, both studies reported that the as extravasation of contrast on arterial-phase contrast-enhanced
definition did effectively segregate patients based on overall CT scans. On delayed-phase images, if obtained, the extrava-
disease severity, clinical impact, and mortality. sated contrast continues to spread if there is active bleeding.
The most important factor in distinguishing types of PPH is On the other hand, a pseudoaneurysm, which can bleed inter-
the time of onset, which correlates with two different mecha- mittently, is an enhancing structure next to an artery that main-
nisms of bleeding and, subsequently, two different mortality tains its shape on delayed CT images (Fig. 27.2).
rates. Current literature shows that early bleeding accounts for Magnetic resonance cholangiopancreatography (MRCP) is
9% to 36% of all PPH and has a better prognosis, regardless a fluid-sensitive magnetic resonance imaging (MRI) sequence
of severity or location, compared with late hemorrhage (Correa- that clearly shows the pancreatic duct, bile ducts, fistulae, and
Gallego et al, 2012; Rajarathinam et al, 2008; Ricci et al, 2012; fluid collections. The MRCP is typically reconstructed into
Wellner et al, 2014; Welsch et al, 2011). In a study of 796 PDs axial and coronal slices, as well as three-dimensional (3D)
by Welsch and colleagues (2011), 35% (81/232) of PPH was images. The site of a pancreatic fistula can be identified in 75%
early with a mortality rate of 1.2%, compared with a mortality of patients on CT, compared with 93% on MRCP (O’Toole
rate of 10.6% among the late hemorrhages (16/151). Older et al, 2007) (see Chapter 19).
studies (and those that do not apply the ISGPS definition
stringently) demonstrate much higher mortality rates of 18%
Interventional Radiology Techniques After
to 64% for delayed hemorrhage (Choi et al, 2004; Rajarathi- Pancreatectomy
nam et al, 2008; Yekebas et al, 2007). This is because early and Many postpancreatectomy complications are managed using
late hemorrhages result from different causes, which have image-guided percutaneous interventions, reducing the need
implications for overall survival. Early bleeding is usually an for reoperation. The most common interventional radiology
isolated issue of inadequate hemostasis due to a technical error. (IR) procedures after PD are: intraabdominal abscess drainage
Late hemorrhage, on the other hand, generally occurs in sicker (72%), percutaneous biliary drainage (PBD) (18%), and angi-
patients with additional underlying complications such as ography with or without embolization (10%) (Baker et al,
POPF, infection/sepsis, and DGE. Each of these additional 2008) (see Chapters 20, 21, and 30).
complications carries its own individual morbidity and mortal-
ity burden, which contributes to the overall mortality observed Image-Guided Abdominal Drainage
in late PPH. To this point, Yekebas and colleagues reported Postoperative abscesses can be drained percutaneously, using
that all 14 PPH-associated deaths in their study were late hem- ultrasound or CT guidance (see Fig. 27.1). Small abscesses
orrhages, 13 (93%) had concomitant POPF, and bleeding was (<3 cm) can usually be treated with antibiotics alone, but larger
the direct cause of death in only 2 (14%) cases (Yekebas et al, collections require both antibiotics and drainage. Complica-
2007). The other 12 patients succumbed to various forms of tions of image-guided drainage of fluid collections are
critical illness, including sepsis, liver failure, and pulmonary infrequent but include bleeding, sepsis, and peritonitis.
complications. Abscesses are typically drained using the Seldinger tech-
nique. A needle is advanced into the collection under ultra-
sound or CT guidance. After aspirating fluid, a stiff guidewire
IMAGING AND IMAGE-GUIDED THERAPY OF is placed through the needle into the collection. The needle is
COMPLICATIONS AFTER PANCREATECTOMY then removed, and a drain is placed over the wire into the
collection. Typically, 8- to 10-Fr drains are placed in thin,
Imaging After Pancreatectomy serous collections, and 10- to 12-Fr drains are placed in thick,
Image-guided interventions to manage postoperative complica- bloody, or purulent collections. Larger drains are available for
tions are common after pancreatic surgery. After PD, 12% very thick collections, up to 20 Fr for locking-loop drains, and
to 22% of patients require percutaneous intervention (Sohn, 36 Fr for straight drains. A retrospective study showed that
2003; Zink et al, 2009) (see Chapter 66). Postoperative imaging 7- and 14-Fr drains worked equally well for abdominal
should be performed if there is suspicion for complications abscesses (Röthlin et al, 1998). Biliary-type drains, which
based on the clinical picture or abnormal laboratory values. have additional side holes, may be helpful for long multilocu-
Computed tomography (CT) is the most common lated collections.
imaging modality for evaluation of the pancreas after surgery. After catheter placement, the abscess is emptied, and speci-
Complications that can be detected on CT include anastomotic mens are sent for gram stain and culture. The fluid can also be
leak, abscess, fistula, and bleeding (Scialpi et al, 2005) (see sent for amylase (to evaluate for pancreatic leak) and bilirubin
Chapter 18). (to evaluate for bile leak). A drain fluid–to–serum bilirubin ratio
Fluid collections such as seromas, abscesses, and pancreatic greater than 5 indicates a bile leak (Darwin et al, 2010), and
pseudocysts can be identified on CT (Fig. 27.1). Rim enhance- drain amylase–to–serum ratio greater than 5 indicates a pan-
ment suggests abscess or pseudocyst. Gas within a collection creatic leak (Shinchi et al, 2006).
suggests infection or enteric leak. Enteric leaks can have a thin
tract containing gas and fluid, extending from an enteric anas- Drain Management
tomosis to an abscess. Oral contrast given prior to the CT can The drain should be flushed with normal saline two to three
leak into the abscess, which is diagnostic of an enteric leak (see times per day to prevent clogging. Drainage from loculated
Chapter 18). collections can be improved by injecting tissue plasminogen
Postoperative bleeding can be evaluated using a CT angio- activator (tPA) into the tube. One report showed an 89%
gram, which should include noncontrast and arterial phases. success rate using tPA to drain abscesses refractory to simple
Hematomas are visible on noncontrast CT as high-density (>20 catheter drainage (Beland et al, 2008). In a postsurgical patient,
468 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
A B
C
FIGURE 27.1 A 77-year-old female patient after distal pancreatectomy for neuroendocrine tumor. A, Postoperative development of a large
rim-enhancing fluid collection in the operative bed, suspicious for abscess or pseudocyst (asterisk). B, Computed tomography (CT)-guided drainage
of the fluid collection with a 10-Fr drainage catheter. Rust-colored fluid was aspirated and sent for analysis, which showed elevated amylase and
negative culture, consistent with a pancreatic leak. The catheter was removed after the output had diminished. C, CT follow-up 10 months after
drain removal showed resolution of the fluid collection (asterisk).
the benefit of tPA should be weighed against the risk of persistent pancreatic leaks is discussed later (see Interventional
bleeding. Management of Pancreaticocutaneous Fistulae).
If the drain output remains high, this suggests an ongoing Minimal output from the drain indicates that the drainage
pancreatic or enteric leak. The drain should be positioned is complete, or that the drain is clogged or malpositioned. Pus
adjacent to the leak for optimal drainage. When output from leaking around a drain suggests that the drain is clogged.
the drain decreases, the locking-loop drain can be exchanged Clogged drains can be exchanged over a guidewire.
for a straight drain, to collapse the abscess cavity adjacent to An abscess drain can typically be removed when the output
the leak. The straight drain can be slowly pulled back during is less than 20 mL/day, the patient has no fever or pericatheter
days or weeks in an attempt to close the fistula. Occasionally, leakage, and the drain flushes easily. An abscessogram or a CT
a persistent fistula is seen on abscessogram, even after the scan can be performed prior to drain removal. An abscessogram
patient is doing well clinically, with no residual abscess cavity shows if the tube is clogged or malpositioned, as well as the size
and no output from the drain. This is called a one-way fistula, of the residual collection and any fistulae. A CT scan shows
and the drain can usually be safely removed. Management of the position of the tube and any undrained collections. On CT,
Chapter 27 Postoperative complications requiring intervention: diagnosis and management 469
A B
C D
FIGURE 27.2 A 63-year-old female patient had clinical evidence of bleeding 3 weeks after pancreaticoduodenectomy for pancreatic
adenocarcinoma. A, Computed tomography angiogram showed a large hematoma (arrowheads) in the subhepatic space, with highly enhancing
components within this hematoma consistent with a pseudoaneurysm (arrows) at the origin of the gastroduodenal artery. B, Catheter angiography
confirmed a pseudoaneurysm (arrow) of the gastroduodenal artery, which was treated by occluding both the proper hepatic (outflow) and common
hepatic arteries (inflow) with stainless steel coils. C, Postembolization angiogram showed coils in the hepatic arteries (arrows) with no enhancement
of the hepatic arteries or the pseudoaneurysm of the gastroduodenal artery. D, A 46-year-old male had gastroduodenal artery stump bleeding after
pancreaticoduodenectomy, which was treated by placement of a covered stent (between arrows) into the hepatic artery. Covered stent placement
preserves hepatic arterial flow.
470 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
a residual collection around an abscess drain indicates a clogged infarction due to collateral arterial supply to the spleen (Yama-
or poorly functioning drain. moto et al, 2008).
The median drainage time is 11 days for sterile fluid collec- Pseudoaneurysms and arterial extravasation can also be
tions, 29 days for abscesses, and 30 days when there is a pan- treated using a covered stent to exclude the pseudoaneurysm
creatic leak (Zink et al, 2009). while preserving distal flow (Heiss et al, 2008; Suzuki et al,
2009). Covered stents are particularly helpful for gastroduode-
Interventional Management of Pancreaticocutaneous Fistulae nal artery stump blowouts (in which coil embolization might
Pancreatic leaks with pancreaticocutaneous fistulae can develop not be technically possible), distal splenic artery pseudoaneu-
after pancreatic surgery. Most fistulae resolve after 1 month of rysms (where embolization has a higher risk of splenic infarc-
conservative therapy, including jejunal feeding, somatostatin tion), common and proper hepatic artery pseudoaneurysms (to
analogue injection, pseudocyst drains, and endoscopic stent preserve arterial flow to the liver), and superior mesenteric
placement in the pancreatic duct (Cabay et al, 1998; Klek et al, artery pseudoaneurysms (to preserve flow to bowel).
2011; Voss & Pappas, 2002). The fistula is likely to persist if Examples of embolization and covered stent placement for
there is complete transection of the pancreatic duct, if there is bleeding after pancreatic surgery are shown in Figure 27.2.
a downstream ductal stricture, or if it is a high-output fistula
(Voss & Pappas, 2002). HEPATECTOMY
Several percutaneous approaches have been described for
reconnecting the pancreas to the GI tract, to divert pancreatic Hepatic resection is widely performed for the treatment of
fluid away from the fistula and allow it to heal. Cystgastrostomy many liver diseases, including malignant and benign tumors,
(surgical, endoscopic, or percutaneous) can be performed if calculi in the intrahepatic ducts, hydatid disease, and abscesses.
there is a pseudocyst associated with the fistula. If the pancre- In the landmark paper by Foster and Berman from 1977,
atic duct is dilated (>4 mm), it can be punctured percutane- overall mortality in a multicenter analysis of 621 hepatic resec-
ously, allowing placement of a drain from the pancreatic duct tions was 13%, and even greater (20%) in patients undergoing
to the stomach or bowel (Cope et al, 2001). However, the major hepatic re section. Mortality for hepatic resections
pancreatic duct is frequently nondilated, as it is decompressed has improved significantly since that time with and currently
into the cutaneous tract. If the pancreatic duct is not dilated, ranges from 0% to 3% at high-volume centers (Table 27.8)
then a snare can be placed into the duct via the cutaneous (Adam et al, 2006; Cescon et al, 2009; Huang et al, 2009;
fistula, providing a target for percutaneous puncture and drain- Hyder et al, 2013; Imamura et al, 2003; Jarnagin et al, 2002;
age of the duct into the stomach (Boas et al, 2015). Koffron et al, 2007; Palavecino et al, 2010; Poon et al, 2004;
Rees et al, 2008). Unfortunately, other outcomes have not
Percutaneous Biliary Drainage improved in parallel with mortality such that overall morbidity
See “Interventional Management of Bilomas and Bile Leaks,” is still reported in the range of 14% to 45% (see Chapter 103).
and “Interventional Management of Biliary Strictures,” later. Since the time of Foster and Berman, the field of hepatobili-
ary surgery has benefited from a better understanding of liver
Angiography, Embolization, and Covered Stent Placement anatomy, advances in cross-sectional imaging technology,
(See Chapters 21 and 30) expanded use of parenchymal-sparing approaches, improved
Hemorrhage is seen in less than 10% of patients after pancre- anesthetic techniques, and better patient selection. These
atectomy but is associated with high mortality (Puppala et al, improvements are reflected in a recent multi-institutional study
2011). Major bleeding is seen on average 19 days after surgery of 2056 patients undergoing hepatic resection between 1990
and is usually preceded by a smaller sentinel bleed (Otah et al, and 2011 (Hyder et al, 2013). In this study by Hyder and col-
2002). Therefore even a small amount of increased bleeding leagues, 90-day mortality was 1.6%, overall morbidity was
from surgical drains or GI bleeding more than 3 days after 19.3%, and liver-specific complications included postoperative
pancreatic surgery should be evaluated immediately. Bleeding ascites (2.5%), biliary leak (3.2%), bleeding (0.9%), abscess
can be due to vessel injury during surgery or due to pancreatic (0.7%), and liver insufficiency/failure (0.5%). Of note, whereas
fluid eroding the vessel wall. bleeding accounts for a minor percentage of overall morbidity
In hemodynamically stable patients, CT angiography can in the current series, 30 years ago it was the primary cause of
identify the bleeding vessel. A CT angiogram is most likely overall mortality following hepatectomy (Foster & Berman,
to be positive if performed when the patient is actively 1977). A list of common complications reported after major
bleeding. Hemodynamically unstable patients should proceed hepatic resections in several large series since 2000 is presented
directly to catheter angiography and intervention, or to the in Table 27.9.
operating room.
Pseudoaneurysms and arterial extravasation after pancreatic Complications Associated With Hepatic Resections
surgery occur in the gastroduodenal artery most commonly, Posthepatectomy Liver Failure
followed by the hepatic artery, superior mesenteric artery, and Posthepatecomy liver failure (PHLF) is one of the most severe
splenic artery (Tien et al, 2008) (see Chapter 124). Selective complications following hepatectomy, and its incidence varies
coil embolization across the pseudoaneurysm is successful in widely in the literature, between 1.2% to 32% (Rahbari et al,
approximately 85% of patients (Tsai et al, 2007). In an other- 2011a) (see Chapter 103). The International Study Group of
wise normal liver, the hepatic arteries on the right or left side Liver Surgery (ISGLS) defined it as postoperatively acquired
can be safely coil embolized, because the embolized lobe of the deterioration in the ability of the liver to maintain its synthetic,
liver will be supplied by the portal vein and intrahepatic arterial excretory, and detoxifying functions, which are characterized
collaterals (Nicholson et al, 1999). The proximal splenic artery by an increased international normalized ratio (INR) and con-
can also be safely coil embolized without complete splenic comitant hyperbilirubinemia on or after postoperative day 5
Chapter 27 Postoperative complications requiring intervention: diagnosis and management 471
TABLE 27.8 Morbidity and Mortality Rates After Hepatic Resection From Large, Single-Institution Series
Primary Hepatic or Major
Years Biliary Tract Metastatic Benign Hepatectomy Morbidity Mortality
Study Inclusive N Cancer N (%) Disease N (%) Disease N (%) N (%)* N (%) N (%)
Jarnagin 1803 817 (45) 880 (49) 99 (6) 110 (6) 47 (3) 97 (5) 344 (19) 154 (9) 94 (5)
et al, 2002
Imamura 1056 208 (20) 230 (22) 1 (.1) 87 (8) 97 (9) NR 274 (26) 194 (18) 43 (4)
et al, 2003
Poon et al, 1222 396 (32) 414 (34) 47 (4) 33 (3) NR NR 164 (13) 63 (5) 115 (9)
2004
Cescon et al, 1500 337 (23) 548 (37) 86 (6) 41 (3) 56 (4) NR NR 97 (7) NR
2009
Hyder et al, 2056 396 (19) NR 9 (.5) 15 (.7) 65 (3) NR 19 (.9) 47 (2) 7 (.3)
2013
NR, Not reported.
(Rahbari et al, 2011a). This may range from a transient decline fail conservative management ultimately require liver transplan-
in liver function requiring no specific intervention (grade A) or tation to survive (Kauffmann & Fong, 2014). In the study
progress to fulminant liver and multisystem organ failure (grade by Hyder and colleagues (2013), only two patients (0.1%)
C) (Kauffmann & Fong, 2014). Mortality for PHLF patients required extracorporeal liver support followed by “rescue” liver
rises dramatically based on grade with rates for A, B, and C transplantation.
reported to be 0%, 12%, and 54%, respectively (Reissfelder
et al, 2011). Risk factors include large-volume blood loss, pro- Bile Leak
longed operative time, and major resection of greater than 50% Bile leakage is a common complication following hepatic resec-
of liver volume (Kauffmann & Fong, 2014; Nonami et al, tions, with an incidence ranging from 3.6% to 12% (Erdogan
1999). PHLF presents with persistent hyperbilirubinemia and et al, 2008). It occurs at the cut surface of the liver remnant,
coagulopathy in the setting of progressive multisystem organ from the closed stumps of hepatic ducts, and from injury to the
failure. Management is largely supportive, and severe cases extrahepatic bile duct. When present, bile leaks may prolong
require transfer to an ICU where intubation, dialysis, pressors, hospital stay, delay drain removal, or even require return to the
and transfusions can be coordinated for multiple failing organ operating room in severe cases. The ISGLS defined a bile leak
systems. Unfortunately, patients who progress to this point and as the drainage of intraabdominal fluid with an increased
472 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
bilirubin concentration (at least three times the serum bilirubin Chapter 24). Multivariate analysis performed by Jarnagin and
concentration) on or after postoperative day 3 (Koch et al, colleagues (2002) identified the number of hepatic segments
2011). This may be determined from the intraabdominal drains resected and operative blood loss as factors predictive of overall
placed at the time of surgery or through invasive interventions morbidity and mortality. Moreover, blood loss, transfusion, and
(i.e., percutaneous drain placement or relaparotomy). Grade A extent of resection have been correlated specifically with
bile leaks are transient with little to no clinical impact, grade B increased rates of postoperative liver failure and bile leaks
leaks require additional diagnostics and potentially percutane- (Brooke-Smith et al, 2015; Kauffmann & Fong, 2014; Nonami
ous drainage, and grade C leaks require relaparotomy for bile et al, 1999). In recognition of these associations, there has been
peritonitis. A prospective, multiinstitutional validation study of great interest in developing techniques aimed at reducing blood
949 hepatic resection demonstrated a 7.3% overall incidence loss and transfusions and limiting resections. One example of
of bile leak, of which 45%, 46%, and 9% were classified as this is the more widespread use of parenchymal-sparing
grades A, B, and C, respectively (Brooke-Smith et al, 2015). approaches, which several studies have reported to have less
Mortality was 7.2% in the setting of bile leak compared with perioperative morbidity without compromising oncologic
1.1% (P < .001) without it. Overall, 16 patients (23%) under- results (de Haas et al, 2008; Gold et al, 2008) (see Chapter
went endoscopic retrograde cholangiopancreatography (ERCP) 108). Another major advance in liver surgery has been the
or percutaneous transhepatic cholangiography, and 30 patients concept of low CVP anesthesia during hepatic resection. Mul-
(43.5%) required additional drainage, either percutaneously or tiple high-quality studies have demonstrated that maintaining
surgically. Interestingly, use of intraoperative drains was identi- a low CVP (<5 mm Hg) reduces blood loss and transfusion
fied as an independent predictor of bile leak but did not affect rates, decreases operative times, decreases renal dysfunction,
the chances of requiring an intervention. Moreover, 100% and and lowers overall morbidity (Li et al, 2014; Melendez et al,
91% of grade A and B leaks, respectively, were detected in cases 1998; Wang et al, 2006) (see Chapter 24).
with intraoperative drains. This suggests that most bile leaks, Techniques and devices intended to improve intraoperative
as defined by the ISGLS, are self-resolving with little to no efficiency and hemostasis during parenchymal transection
clinical impact, and the presence of intraoperatively placed have been studied extensively to determine their effect, if any,
drains simply allows a biochemical diagnosis. on postoperative complications (Pamecha et al, 2009; Poon,
It should be noted that bile leakage rates after complex 2007). Among the numerous techniques studied in random-
resections that also involve biliary reconstruction, for example, ized trials—crush-clamping, stapling systems, vessel sealing
hilar cholangiocarcinoma, are higher than after standard systems (i.e., LigaSure, Covidien, Boulder, CO), and multiple
resections and often involve more complex management (see options for ultrasonic dissection—there does not appear to be
Chapters 51, 52, and 103C). a single “best” option. This may be due to the fact that these
trials are usually performed at high-volume centers where the
Posthepatectomy Hemorrhage skill among experienced liver surgeons could make it difficult
Posthepatectomy hemorrhage (PHH) is defined by the ISGLS to demonstrate small differences among techniques (Arita
as any of the following in the setting of confirmed bleeding et al, 2005; Ikeda et al, 2009; Palavecino et al, 2010;
noted in drains or on imaging: (1) drop in hemoglobin level Patrlj et al, 2010). In a recent Cochrane Review analyzing
of greater than 3 g/dL, (2) any postoperative transfusion of seven randomized controlled trials that compared methods
packed red blood cells (PRBCs) for a falling hemoglobin, or for parenchymal division, the authors concluded that the
(3) the need for invasive intervention (e.g., embolization or crush-clamp technique was the procedure of choice (Pamecha
relaparotomy) (Rahbari et al, 2011b). As with other consensus et al, 2009). Their decision was based on the fact that paren-
definitions, PHH is graded from A to C such that grade A chymal transection devices were slower and significantly more
hemorrhage may require transfusion of up to 2 U of PRBCs, expensive, while offering no advantages in time reduction or
grade B requires more than 2 U of PRBCs, and grade C neces- reduced blood loss compared with crush-clamping (see
sitates invasive intervention. PHH usually occurs within 48 Chapter 103).
hours of surgery as venous bleeding from the raw surfaces of
the liver and diaphragm. This may be exacerbated by altera-
tions in outflow resulting from surgery, elevated central venous IMAGING AND IMAGE-GUIDED THERAPY OF
pressure (CVP), and valsalva maneuvers such as coughing and COMPLICATIONS AFTER HEPATECTOMY
defecating (Kauffmann & Fong, 2014; Lim et al, 2014). It is
also possible, albeit rare, for delayed injury to arterial struc- Imaging After Hepatectomy
tures to manifest postoperatively and for vascular ties or clips Ultrasound, CT, hepatobiliary iminodiacetic acid (HIDA)
to detach from short hepatic vein stumps along the vena cava. scan, and MRI/MRCP are noninvasive diagnostic procedures
Internal validation of the definition for PHH performed on a widely applied to the liver and biliary system. Postoperative
series of 835 hepatic resections demonstrated an incidence of bilomas, hematomas, and abscesses can be detected with these
3%, of which 14% were grade A, 43% grade B, and 43% grade modalities.
C (Rahbari et al, 2011b). The in-hospital mortality for grades The typical appearance of biloma on imaging is that of an
A, B, and C was 0%, 17%, and 50%, respectively. encapsulated fluid collection adjacent to the liver resection
plane. Rim enhancement of a fluid collection suggests infection,
Techniques for Reducing Intraoperative Blood Loss but this is not a specific finding. In some cases, aspiration may
Intraoperative blood loss, transfusion of PRBCs, and extent of be required to distinguish infected and noninfected collections.
hepatic resection have all been reported in numerous studies as A postoperative biloma, hematoma, or seroma might initially
major contributors to mortality and morbidity of all types (Jar- be sterile but can progress to become an abscess. Gas within a
nagin et al, 2002; Rahbari et al, 2011c; Wei et al, 2003) (see collection suggests infection or enteric leak. Topical hemostatic
Chapter 27 Postoperative complications requiring intervention: diagnosis and management 473
agents used during surgery can also contain gas bubbles (see
Interventional Radiology Procedures Posthepatectomy
Chapters 18 and 19).
A HIDA scan, also known as hepatobiliary scintigraphy, is Intrahepatic Abscess Drainage
a nuclear medicine scan that can show biliary leaks (Sandoval Small pyogenic liver abscesses can be successfully treated with
et al, 1997). Although technetium-99m–labeled HIDA has antibiotics alone. Large (>3 cm) unilocular abscesses can be
largely been replaced by other radiotracers (which have treated by percutaneous drainage and antibiotics. Large multi-
improved liver uptake), the term “HIDA scan” remains in loculated abscesses have a lower success rate with percutaneous
common use. A normal HIDA scan initially shows radiotracer drainage, and might require surgery (Hope et al, 2008) (see
uptake in liver, followed by excretion of radiotracer into the bile Chapter 12). Intracavitary tPA can help drain multiloculated
ducts, gallbladder, and small bowel. Pooling of tracer elsewhere collections that are refractory to simple percutaneous drainage
indicates a bile leak. HIDA scans are typically two-dimensional (Beland et al, 2008). When biliary obstruction is present, relief
images acquired with a gamma camera, but fused 3D images of the obstructed biliary tree is mandatory for successful abscess
can also be obtained, using a single-photon emission computed treatment. Abscesses located near the dome of the liver may be
tomography. The 3D images can be helpful for more precise technically more difficult to drain without transgressing the
anatomic localization (see Chapter 17). pleura. Transpleural abscess drains carry a risk of empyema.
MRCP is an MRI protocol optimized for seeing the bile
ducts (see Chapter 19). It can show the anatomy of the biliary Interventional Management of Bilomas and Bile Leaks
tree and any associated bilomas. MRCP can also show a biliary After liver tumor resection, bile can leak from a bile duct injury,
leak, when it is performed using an intravenous contrast agent biliary-enteric anastomosis, or the cut surface of the liver. Bile
that is excreted into the bile ducts, such as gadoxetate (Eovist) leakage can cause bile peritonitis, as well as bilious fluid collec-
(Aduna et al, 2005). (Typically, MRCP is performed without tions that can become infected. These fluid collections can be
intravenous contrast.) MRCP has higher resolution than a drained percutaneously, under CT or ultrasound guidance
HIDA scan and shows the biliary tree more clearly than CT. (Fig. 27.3). When an infected biloma is drained, the fluid can
Acute and subacute hematomas appear as high-density col- initially appear purulent, and then it may turn bilious if there
lections on CT. In addition, active bleeding can be demon- is a continued bile leak after the infection clears. Ideally, the
strated by contrast media extravasation on contrast-enhanced drain should be placed near the bile leak to provide optimal
CT (see Chapter 18). drainage (see Chapter 42).
*
*
A B
FIGURE 27.3 A 46-year-old male patient with hepatitis B infection, status post partial left hepatectomy for hepatocellular carcinoma.
A, Postoperative computed tomography showed a fluid collection at the liver resection margin (asterisk), which was treated with percutaneous
catheter placement. B, Contrast injection into the cavity under fluoroscopy showed a small biloma cavity (asterisk) communicating with the common
hepatic bile duct (arrow), with contrast then flowing into the duodenum (arrowhead). Endoscopic retrograde cholangiopancreatography was per-
formed, and a plastic stent was placed into the common bile duct to decrease the output of the fistula.
474 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
The amount of drain output allows monitoring of the has side holes both above and below the obstruction. An
amount of bile leak over time. Small bile leaks can resolve internal/external biliary drain can be capped if there is no leak,
spontaneously (Viganò et al, 2008). Persistent drainage greater infection, or significant blood in the bile, and should be flushed
than 100 mL/day (at 10 days’ posthepatectomy) may be treated daily with 10 mL normal saline to maintain patency.
with endoscopic or percutaneous biliary drain placement, Biliary drains are typically exchanged every 3 months to
which decompresses the biliary system and diverts bile flow prevent clogging but are exchanged more frequently if cholan-
away from the defect in the bile ducts, allowing the leak to heal gioplasty or other interventions are planned. An over-the-wire
(see Fig. 27.3). Complete transection of a bile duct at the hilum cholangiogram can be performed through a sheath that does
typically requires surgical repair (see Chapter 42). not cross the bile duct injury, to evaluate for persistent leak or
Percutaneous biliary drainage is the preferred treatment for stenosis. If the bile duct injury has resolved on the cholangio-
high bile duct injuries (at or above the bifurcation), and biliary- gram, then an external biliary drain can be placed to maintain
enteric anastomotic leaks, both of which are difficult to access to the bile ducts. This external drain should be capped
access endoscopically. ERCP is less invasive than PBD, and is for 2 weeks without flushing. If the patient passes the capping
the preferred treatment for leaks from the cut surface of trial (no fever, no significant leakage around the tube, no rise
the liver and for accessible common duct leaks (see Chapters in bilirubin), then the drain can be safely removed.
29 and 30). Nonsurgical management of benign biliary strictures are
Percutaneous biliary drainage leads to resolution of 88% to typically managed with endoscopic placement of a plastic biliary
100% of postoperative bile leaks, after an average of 1 to 3 stent, or percutaneous internal/external biliary drainage. Chol-
months of drainage (Cozzi et al, 2006; Ernst et al, 1999). angioplasty can be performed using a high-pressure balloon
Intractable bile leaks can be managed with surgery, portal vein during biliary drain placement or exchange. High pressures and
embolization (Hai et al, 2012), or bile duct embolization with prolonged cholangioplasty (as long as 15 minutes) are typically
N-butyl cyanoacrylate glue (Vu et al, 2006). required to overcome the dense fibrous tissue around biliary
strictures. An 8-mm balloon can be used for intrahepatic stric-
Interventional Management of Biliary Strictures tures and a 10- to 12-mm balloon for common duct strictures.
Postoperative biliary strictures can occur after hepatectomy (see Cholangioplasty can be repeated at 2- to 14-day intervals
Chapter 103), cholecystectomy (see Chapters 38 and 42), cho- (Cantwell et al, 2008; Zajko et al, 1995). For benign biliary
ledochojejunostomy, liver transplant (see Chapter 120), and strictures, cholangioplasty and internal/external biliary drainage
other procedures. These strictures can be caused by direct have a long-term (25 years) primary success rate of 59% and a
biliary injury from surgery, ischemia, or recurrent tumor. secondary success rate of 80% (Cantwell et al, 2008). Failure
Benign and malignant strictures can be difficult to distinguish of these approaches in otherwise healthy patients should prompt
on imaging, and biopsy may be required. Biliary strictures can consideration of operative management (see Chapter 42).
cause jaundice as well as cholangitis. Malignant biliary obstruction can be relieved with a biliary
Low bile duct obstruction (common bile duct or common drainage catheter, to treat cholangitis, pruritus, or to lower bili-
hepatic duct not involving the bifurcation) can be relieved via rubin for chemotherapy. A metal biliary stent can be placed
ERCP and placement of a plastic or metal biliary stent across (percutaneously or endoscopically) for palliation of unresect-
the obstruction (see Chapter 29). High bile duct obstruction able symptomatic biliary obstruction in patients with limited
and biliary-enteric anastomotic strictures, both of which are life expectancy. Metal biliary stents placed for malignant
difficult to access endoscopically, can be treated with percuta- obstruction remain patent for an average of 11 months
neous biliary drain or metal stent placement (see Chapter 30). (Dahlstrand et al, 2009).
Metal stents are typically only used for malignant obstruction,
as they have a limited patency rate—30 months on average Bleeding Complications
when used for benign disease (Tesdal et al, 2005). See “Angiography, Embolization, and Covered Stent Place-
If the biliary stricture cannot be crossed percutaneously, an ment,” earlier.
external biliary drain can be placed. If the biliary stricture can
be crossed, an internal/external biliary drain is placed, which References are available at expertconsult.com.
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CHAPTER 28
Quality of life and hepatobiliary tumors
Julie N. Leal, Piera Marie Cote Robson, and Michael I. D’Angelica
QUALITY OF LIFE AND HEALTH-RELATED associated with improved survival, were severely toxic, and it
QUALITY OF LIFE: WHAT LIES BENEATH THE became apparent that assessing the “quality of survival” was
SURVIVAL CURVE? essential (Izsak & Medalie, 1971). However, most early studies
reporting on HRQoL in oncology simply focused on a single
Quality of life (QoL) is a complex construct that varies during parameter of QoL as assessed by functional indices, such as the
time and across cultures, and cannot be determined by a single Karnofsky Performance Score (KPS) (Karnofsky & Burchnel,
parameter or measurement. In the very broadest of terms, QoL 1948) and the Eastern Cooperative Oncology Group (ECOG)
has been defined as individuals’ perceptions of their position in performance status (Oken et al, 1982).
life in the context of the culture and value systems in which These initial studies lacked multidimensional assessment,
they live, and in relation to their goals, expectations, standards, with no patient-specific interpretation, and by current stan-
and concerns (World Health Organization [WHO], 1993). QoL dards are not true representations of HRQoL.
is multidimensional and influenced by many factors outside the Since these early ventures, the field of qualitative analysis in
realm of health/disease, including financial security, job satis- medicine has advanced significantly. Review of published
faction, personal freedom, and so forth. In the field of medi- HRQoL data from 1990-2004 by Efficace and colleagues
cine, and more specifically surgery, the true interest lies in the (2007) reveal a significant learning curve in the conduct and
aspects of QoL that are influenced by both underlying health/ reporting of HRQoL. Based on a checklist of minimal criteria,
disease status and treatment. Rudimentary to our understand- 39.3% of studies conducted before 2000 were considered
ing of the concept of health-related quality of life (HRQoL) is robust compared with 64.3% of studies published after 2000.
not only comprehension of what QoL is but also an essential It is encouraging that the observed increase in the volume of
appreciation for what “health” is. In the 1946 WHO constitu- published HRQoL studies is paralleled by improved outcome
tion, “health” is defined as a state of complete physical, mental, measurement and reporting.
and social well-being, not merely the absence of disease or These improvements in the study of HRQoL have led to
infirmity (WHO, 1946). Although no globally accepted defini- increasing acceptance of its importance as a valid measureable
tion exists, one can infer from QoL and health definitions that outcome in oncology and surgery. The true magnitude of the
HRQoL refers to the effect of illness and its treatments on value of HRQoL assessment is best highlighted by a policy
functional status, disease-related symptomatology, and psycho- statement from the American Society of Clinical Oncology in
logical and social well-being as perceived by the individual 1996, in which it was said that “QoL as a clinical endpoint is
(Roila & Cortesi, 2001). second in importance only to survival” (Sloan & Dueck, 2004).
Physician concern regarding the subjective impact of disease Nearly two decades since this initial policy statement, the
and its treatment on patients has always been an integral part majority of physicians and surgeons would agree that QoL
of clinical medicine. Since the time of Hippocrates, the simple evaluation is important, and most have a basic understanding
mandate “first, do no harm” has been indoctrinated into the of what is meant by HRQoL outcomes. However, skeptics
medical profession. In the past, the paternalistic nature of med- remain. Critics argue that HRQoL measurement is too subjec-
icine did not ignore patients’ subjective experience of disease, tive, and reported outcomes are esoteric with a lack of clarity
but rather, its interpretation and use in decision making was in terms of the clinical implication/meaning of numeric changes,
thought to be implicit and at the discretion of the doctor. It was limiting any reasonable clinical application (Whalen & Ferrans,
not until the patient-centered model of medical care emerged 2001).
that explicit and standardized measurement of HRQoL moved To address such concerns, Wilson and Cleary (1995) devel-
to the forefront of many clinical research efforts. oped a conceptual framework in which the relationships among
Formal evaluation of HRQoL is rooted in the study of different health outcomes are outlined. This model delineates
chronic diseases (i.e., diabetes, arthritis, claudication, etc.), in these relationships as a continuum from basic biologic pro-
which cure is not the therapeutic goal and patients are often cesses to symptoms to psychological and social implications.
required to adjust and accommodate to long-term functional The model flow is likened to the idea of moving from the cel-
limitations. As is common in any new field of study, initial lular level, to the individual level, to the individual in the
endeavors were fraught with complications, from ambiguity of context of society. In addition, it highlights the fact that indi-
the definition of QoL to the use of an ad hoc questionnaire that vidual patient characteristics and environmental factors will
lacked standardization, validation, and overall generalizability. most certainly contribute to the interpretation of symptoms,
In the field of oncology, early chemotherapeutics, although functional status, and patients’ perception of health. Although
475
476 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
the linkages in this model are simplistic, it provides a basic physical functioning domain have been shown to be an inde-
template to begin evaluating the complex interrelatedness of pendent predictor of survival for multiple different cancers
clinical parameters and HRQoL. It is hoped that characterizing (Gotay et al, 2008; Quinten et al, 2011, 2014).
and elucidating these relationships will improve clinical applica- More specific to hepatobiliary surgery, global QoL, social
tion of HRQoL outcomes. well-being, and physical functioning have all been shown to
Recently, much press has been given to the importance of independently predict survival outcomes in the patient with
“patient-reported outcomes” (PRO). This term is not synony- colorectal liver metastases (CRLMs) and to add to the prog-
mous with HRQoL, but rather encompasses a much wider nostic value of survival models, including standard biomedical
spectrum of outcomes. Basically, PROs include any aspect of data (Earlam et al, 1996; Efficace et al, 2006; Maisey et al,
the patient’s health status reported by the patient without inter- 2002). Similar findings have been observed among patients
pretation by the clinician or anyone else (U.S. Food and Drug with hepatocellular carcinoma (HCC) (Yeo et al, 2006).
Administration, 2006). Furthermore, instruments such as the Whether HRQoL simply reflects a highly sensitive measure of
KPS or the ECOG performance score, although useful and well patients’ overall health status not evaluated elsewhere, or
validated, are not truly HRQoL measurements. They simply whether HRQoL impacts other important areas, such as self-
measure one functional domain without evaluation of impor- care/treatment adherence and thus survival, is unknown. What
tant factors such as disease-related symptoms and psychological is clear is that measurement of HRQoL to aid informed consent
and/or social functioning. Furthermore, the KPS and ECOG and clinical decision making, to facilitate physician-patient rela-
scores are typically reported based on the clinician’s perception tionship and manage expectations, and to help improve prog-
of the patient’s status, which has been shown to differ signifi- nostication is requisite to optimize care of surgical patients.
cantly from patients’ perceptions (Schag et al, 1984). Many As with any outcome measure, it is essential to identify the
symptom scales also exist and have been reported as measure- clinical scenarios in which assessment is appropriate. Conse-
ments of HRQoL; however, they fail to place symptoms in the quently, it is incumbent upon surgeons to define these relevant
context of individual patients. Bona fide HRQoL assessment settings where HRQoL end points will result in clinically
requires multidimensional evaluation with patient input as to meaningful/actionable outcomes. It is suggested that the most
the impact of the disease/illness experience in the context of his pertinent scenarios for surgical patients include evaluation of
or her own life. Only then does it truly represent “what lies palliative interventions or procedures in which survival out-
beneath the survival curve.” comes are thought to be equivocal and/or survival outcomes
similar, but morbidity/side-effect profiles differ significantly
HEALTH-RELATED QUALITY OF LIFE (Blazeby et al, 2006; Bruner et al, 2004; Byrne et al, 2007;
AS AN OUTCOME MEASURE IN SURGERY: Langenhoff et al, 2001; Sajid et al, 2008; Velanovich, 2001).
In fact, the intention of palliative surgery is to mitigate physical
WHY AND WHEN? symptoms in patients with noncurable disease, with the primary
Surgery is unique; it is immediate and, for the most part, irre- goal of improving or maintaining HRQoL (Hofmann et al,
versible. In this high-stakes setting, evaluation of the impact of 2005). Inclusion of HRQoL measurements in studies in which
surgery on HRQoL is essential, and integration of the informa- these specific scenarios are encountered will maximize the clini-
tion gleaned into the informed consent process and clinical cal applicability of the HRQoL outcomes observed.
decision making is the ultimate goal. A recent review of 33
randomized surgical oncology trials, in which HRQoL data SURGEON, PATIENT, OR CAREGIVER: WHO
were collected, indicated that in two-thirds of trials, the HRQoL SHOULD GATHER HRQOL INFORMATION?
information influenced clinical decision making and/or facili-
tated the surgical consent process. Integration of the HRQoL For practical reasons, initial investigations used the external
data was more common among later trials, reflecting the pro- judgment of observers, typically nurses or clinicians, to evaluate
gressively increased value attached to these outcomes by sur- treatment impact on patient QoL. Typically, this included
geons (Blazeby et al, 2006). On a similar note, it has been evaluation of symptoms and overall QoL. This method of
shown that communicating both technical procedural-related obtaining HRQoL data is inherently biased by the observer’s
information and QoL information to the patient and their own internal standards. Multiple studies evaluating the degree
family facilitates an improved physician-patient relationship, of agreement between the proxy ratings of QoL by observers to
reconciles patient expectations, and improves patient satisfac- patient assessments have consistently found very little correla-
tion (Chen et al, 2013; D’Angelica et al, 1998; Detmar et al, tion between the two measures (Choiniere et al, 1990; Kahn
2002; Passik & Kirsh, 2000; Velikova et al, 2004). Further- et al, 1992; Presant, 1984; Slevin et al, 1988; Sprangers &
more, while measurement tools have evolved from generic to Aaronson, 1992; Stephens et al, 1997). Given these findings,
disease/site specific, and subsequently become more sensitive, it is generally accepted that validity of QoL instruments and
focus on HRQoL as a predictive/prognostic variable of out- rigor of results is contingent on patients’ reporting. Unfortu-
comes such as morbidity, mortality, and survival has increased. nately, this requisite self-reporting can become an issue while
Meta-analysis of 30 randomized clinical trials with HRQoL patients are followed during time; disease status and symptoms
data from the European Organization for the Research and worsen, and patients are less likely to fill out instruments,
Treatment of Cancer (EORTC) Quality-of-Life Questionnaire leading to nonrandom missing data, which is a significant chal-
(QLQ)-C30 (core 30 items) revealed that addition of HRQoL lenge in QoL research (Bernhard et al, 1998; Hahn et al,
parameters (physical functioning, pain, anorexia) to sociode- 1998). Feinstein (1987) coined the term “sensibility” of
mographic and clinical variables provides prognostic value and HRQoL instruments to denote the practical issues related to
significantly improves predictive accuracy of models of survival implementation of HRQoL measurements. Many surveys or
(Quinten et al, 2009). Moreover, patient scores within the instruments are impractical and can be overwhelming in length
Chapter 28 Quality of life and hepatobiliary tumors 477
and time required to complete, leading to “questionnaire burn- tools of varying quality exist and can be accessed through the
out” and subsequent patient drop-out. Other issues, such as Patient-Reported Outcome and Quality-of-Life Instruments
literacy and native language, may prohibit patients from com- Database (PROQOLID) (http://www.proqolid.org). The sheer
pleting instruments independently. Recent HRQoL measure- number of measurement tools highlights the expansion of the
ment tools were developed and validated for completion by the HRQoL field; however, it can also make research and interpre-
patient. However, to optimize accrual and retention in HRQoL tation of the literature challenging. The following section briefly
studies, certain situations may dictate that physicians, nurses, outlines general concepts of measurement and instruments,
caregivers, research administrators, or even translators com- whereas specific instruments commonly used in surgical trials
plete questionnaires on the patient’s behalf. are represented in Table 28.1A and Table 28.1B.
For HRQoL results to be respected on the same level as
HRQOL MEASUREMENT TOOLS, other measured clinical variables, the scientific rigor of mea-
INSTRUMENTS, AND INTERPRETATION surement tools is essential and depends upon three primary
concepts: reliability, validity, and responsiveness/sensitivity.
Early in the history of HRQoL assessment in cancer clinical Reliability is the degree to which an instrument is free from
trials, no standard instrument was used, and the default was random error and includes both reproducibility and internal
simply ad hoc trial-specific questionnaires that prohibited com- consistency. Validity is the degree to which an instrument mea-
parison across trials and often even among patients with the sures what it is suppose to measure and consists of content,
same disease (de Haes & van Knippenberg, 1985). These find- criteria,and construct validity. Responsiveness is the ability of
ings prompted a new era in QoL research heralded by the an instrument to detect and measure changes during time and
development of multiple standardized tools/instruments to treatments. A good instrument is stable when nothing has
measure QoL. To date, more than 800 QoL clinical outcome changed and capable of detecting even small changes when they
TABLE 28.1A Generic and Disease Specific Health Related Quality of Life Measurement Instruments—cont’d
HPB-
Author, Year, Type of Description of Quality-of- Specific
Instrument Country Instrument Life Measures Interpretation Modules Comments
EuroQoL EQ EuroQoL Generic EQ-5D-5L (descriptive Each dimension given No Self-administered
5D-5L Group, value/ system): a 1-digit number with minimal
1990, UK preference 5 dimensions, 5 levels expressing the level responder bias
based of severity: Mobility, selected Revision of
self-care, usual Numbers from each EQ-5D-3L,
activities, pain/ dimension are increased levels
discomfort, anxiety/ combined to give of severity from
depression 5-digit number 3-5 to improve
corresponding to a sensitivity and
specific health state; reduce ceiling
preference value is effect
then assigned based
on empirically
derived valuations
(0-1)
Spitzer Spitzer, 1980, Generic EQ-VAS (visual VAS: quantitive No 3 types of data
Quality-of-Life Australia index analogue scale) measure of overall produced:
Index (QLI) 5 items: health perceived by 1. Profile indicating
Activity respondent extent of the
Daily living (self-rated) problems in
Health Higher score = better each domain
Support HRQoL 2. Population-
Outlook weighted health
index
3. Self-rated
assessment of
health status
Quality of Fanshel & Generic 3 scales assessing Each item scored 0-2 No Completed by
Well-being Bush, 1970, value/ daily functioning, 3 and summed to give surgeon, not
Scale (QWB) U.S. preference levels (recall period total score (0-10) patient; newer
*
Multiple based is 6 days): Higher score = better versions modified
adaptations Mobility HRQoL for self-
Physical activity Using empirically administration
Social activity + derived preference Reliable in patients
symptom/problem values: function with definite
complexes levels for each scale physical disease
combined with the Interviewer
most undesirable administered (26
reported symptoms/ symptom/
problems to give a problem
single well-being complexes): long,
score: 0 (death) to 1 complex, difficult
(fully functional) to administer,
Higher score = better and requires
QoL specific training
Self- administered
version (QWB-
SA, 58
symptom/
problem
complexes)
FACT-G Cella, 1993, Disease 27 items, 4 domains: Each item scored 0-4 Yes Comparable across
(Functional U.S. specific: Physical (7) on Likert scale; different cancers
Assessment cancer Social/family (7) items in given Moderate sensitivity
of Cancer Emotional (6) domain are summed to changes over
Treatment– Functional (7) to give overall score time
General) for each domain Published data
Scores for each exists regarding
domain summed to clinically
give overall score important
Higher score = worse changes over
HRQoL time, allowing
improved
interpretation
Chapter 28 Quality of life and hepatobiliary tumors 479
TABLE 28.1A Generic and Disease Specific Health Related Quality of Life Measurement Instruments—cont’d
HPB-
Author, Year, Type of Description of Quality-of- Specific
Instrument Country Instrument Life Measures Interpretation Modules Comments
EORTC Aaronson, Disease 30 items; 9 multiitem Each item in a scale is Yes Comparable across
QLQ-C30 1993, the specific: scales + 6 single scored, and an different cancers
(European Netherlands cancer items: overall scale score Sensitive to
Organization 5 functional scales: from 0-100 is cancer- related
for Research Physical reported changes
and Role Higher-score overtime
Treatment of Social functional/global Published data
Cancer-Core Cognitive scales = better exists regarding
Quality-of-Life Emotional HRQoL clinically
Questionnaire) 1 Global Health/QoL important
Scale changes during
3 symptom scales: time, allowing
Pain improved
Fatigue interpretation
Nausea/vomiting
Functional Living Schipper, Disease 22 items, 5 domains: Higher-score symptom No Single score lacks
Index-Cancer 1984, specific: Physical well-being and scales/single items = sensitivity to
(FLIC) Canada cancer ability worse HRQoL change
Emotional state
Sociability
Family situation
Nausea
Gastrointestinal Eypasch, Disease 36 items, 5 response Scores from all No Assesses QoL
Quality-of-Life 1995, specific: categories (recall questions are pertaining to a
Index (GQLI) Germany any GI over 2 wk): summed and a variety of
and Canada disease Core symptoms items single score is diseases of the
Physical items reported liver, pancreas,
Psychological items Higher score = better and biliary
Social items quality of life system
Disease-specific items Scores from all items Single score lacks
are summed, and a sensitivity to
single score is change
reported
Higher score = better
quality of life
occur. Responsiveness is dependent on the number of items in combining domain scores to give a single value as an indicator
a questionnaire as well as the number of potential responses. of overall HRQoL is not standard, nor is it valid.
From a practical standpoint, the number of items and associ- To date, no “gold-standard” instrument exists for the evalu-
ated responses must be optimized to ensure sufficient respon- ation of HRQoL. Measurement tools are either health-profile
siveness without creating overly cumbersome questionnaires in based—provide a variety of subscores representing each domain
which respondents experience “question fatigue,” leading to of HRQoL—or preference based—provide a single number
increased rates of nonresponse and missing data. A fourth (health index score) from 0 (death) to 1 (perfect health) that is
parameter, “sensibility,” is also essential and refers to the need representative of a patient’s subjective health status at a single
for strategic balance between practicality and the basic neces- time point. Preference values, typically developed from
sity of instruments to be reliable, valid, and sensitive (Feinstein, population-based studies, are applied to the patient-reported
1987). In addition to choosing a reliable, valid, sensitive, and health states to give a single HRQoL score/index. Measurement
practical instrument, a thorough understanding of how a given tools may be further categorized into three clinically relevant
disease progresses and the expected effects of intervention is categories: generic QoL, disease-specific HRQoL, and modular
requisite (Avery & Blazeby 2006). HRQoL tools.
In general, from a content perspective, HRQoL instruments Generic instruments used in many surgical trials include the
typically consist of a variable number of domains containing Medical Outcomes Survey 36-item Short Form (SF-36), the
information focused on a specific area of health/disease (i.e., Nottingham Health Profile (NHP), and the Sickness Impact
physical, social, emotional, role, global functioning). In turn, Profile (SIP). Each of these measurement tools produces a
each domain contains a number of items (questions or state- health profile, with multiple domain-specific subscores, and
ments) for which respondents must provide an answer, either provides a broad overview of the patient’s HRQoL. The generic
categorically (i.e., Likert scale) or in visual analogue form. Each nature of these measures allows comparison across disease
item is individually scored, and scores from all items in a given states and treatment types. However, these surveys can be time
domain are summed to give each domain a specific score consuming to complete and may not provide adequate sensitiv-
(Fraser, 1993). For most multidimensional instruments, ity to identify changes in HRQoL specifically related to different
480 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
TABLE 28.1B Modular Disease Specific Health Related Quality of Life Measurement Instruments
Description of Quality-of-Life
Core Questionnaire Module Author, Year, Country Measurement Comments
Functional Hepatobiliary Heffernan et al, 2002, FACT-G + 18-item subscale, HS can be combined with
Assessment of subscale (HS) U.S. including HPB-specific physical and functional
Cancer Therapy FACT + HS = concerns related to: domain scores of FACT-G
(FACT) FACT-Hep Jaundice to give Trial Outcome
GI obstruction Index (TOI) 7 additional
Fatigue/energy questions (nonscored) at
Each item scored (0-4) and end of HS, addressing
summed to give overall HAIP and biliary drainage
subscale score
FACT Hepatobiliary Yount et al, 2002, 8 key symptoms from Brief index with good
Symptom Index-8 USA 18-item HS scale correlation with scores on
(FHSI-8) including: FACT-G and FACT-Hep
Pain Capacity to discriminate
Nausea patients based on
Fatigue (× 2 items) performance status/
Jaundice treatment; status
Weight loss adequate but not as
Back Pain good as FACT-G
Stomach Pain/discomfort subscales or HS
*Developed in response to Developed primarily based
clinician concern regarding on pancreatic cancer
the time and resources
required to complete and
interpret multidimensional
QoL assessments
European Pancreatic Fitzsimmons et al, 26 -item subscale, including Examples:
Organization for carcinoma 1999, UK items concerning Pain (abdominal, back,
Research and (QLQ-PAN26) pancreas-specific: positional, night)
Treatment of Symptoms Dietary restrictions
Cancer–Quality-of- Treatments GI symptoms
Life Emotional issues Cachexia
Questionnaire– Weight loss
Core 30 (EORTC Jaundice
QLQ-C30) Pruritus
Ascites
Colorectal liver Kavadas et al, 21-item subscale. including Examples:
metastases 2003, UK items concerning Pain (abdominal,back)
(QLQ-LMC21) CRLM-specific: Eating problems (early
Symptoms satiety)
Treatment Fatigue
Emotional issues Lethargy
Jaundice
Taste
Tingling hands and feet
Stress
Loss of enjoyment
Hepatocellular Blazeby et al, 18-item subscale, including Examples:
carcinoma 2004, UK items concerning Fatigue
(QLQ-HCC18) HCC-specific: Body image Jaundice
Symptoms Nutrition
Treatments Pain
Emotional Issues Fevers
Cholangiocarcinoma, Friend et al, 21-item subscale, including Examples:
Gallbladder 2011, UK items concerning CCA/ Eating
Carcinoma GBCA-specific: Satiety
(QLQ-BIL21) Symptoms Jaundice
Treatments Fatigue
Emotional issues Anxiety
Pain
Stress
Worry
CCA, Cholangiocarcinoma; CRLM, colorectal liver metastases; GBCA, gallbladder carcinoma; GI, gastrointestinal; HAIP, hepatic arterial infusion pump; HPB, hepatopancreatobiliary; HRQoL, health-related
quality of life; U.K., United Kingdom; U.S., United States.
Chapter 28 Quality of life and hepatobiliary tumors 481
diseases and/or treatments. Preference-based instruments such HRQoL; however, their practicality makes them attractive
as the Quality of Well-being Scale (QWB) and EuroQoL-5D- alternatives.
3L/5L (EQ-5D-3L) produce a single score/index/utility. These HRQoL is more than the sum of its parts, and it is likely
instruments, which tend to be insensitive to changes, are less that a global assessment in the form of an index is complemen-
frequently used in therapeutic surgical trials focusing on tary to, rather than an alternative to, individual domain evalu-
HRQoL. However, these preference-based methods are essen- ation. It is generally accepted that a single assessment of
tial and often used in the setting of health economics and patients’ perceptions of overall HRQoL is improved over aggre-
policy. When a preference value for given health state is com- gation of individual domain scores, where each domain is
bined with time values (how long a patient spends in a given given equal importance and a “mean” QoL is estimated (Aar-
disease state) the quality-adjusted life-year (QALY) can be gen- onson, 1988; Osoba, 1994). Ideally, optimal HRQoL assess-
erated. This can then be used in conjunction with the cost of ment strategies should include both global- and domain-specific
treatment/procedure to determine the cost per QALY, and deci- measurements.
sions regarding the economically utility of interventions can be The vast array and potential combinations of available mea-
assessed. At present, the cost of health care is exorbitant, and surement tools can be overwhelming and make interpretation/
while we forge ahead toward more and more precision/designer evaluation of HRQoL literature difficult. To critically appraise
medicine, this will only increase, and cost-utility assessment of HRQoL literature, it is essential to understand the tools used
intervention will be essential. to determine HRQoL outcomes so that judgment as to the
Disease-specific tools focus on a single disease state. In the robustness of the results can be made. Table 28.2 outlines
realm of hepatobiliary surgery and cancer, the two most com- HRQoL levels of evidence based on the psychometric proper-
monly used are the Functional Assessment of Cancer Therapy– ties of the measurement tool(s) used. Low level refers to de
General (FACT-G, 27 items) and the EORTC QLQ-C30 facto questionnaires developed for a single study, midlevel to
(Fig. 28.1). These types of instruments focus more on expected questionnaires not developed or validated in study group of
changes specifically related to cancer and its treatment. Con- interest (psychological assessment, depression scales, etc.), and
sequently, they are more sensitive to HRQoL changes and are high level is represented by the aforementioned instruments
good for comparisons across different cancer diagnoses but are that assess QoL in a multidimensional disease-specific manner.
not generalizable to other disease states. The modular approach Two excellent review articles have been published regarding
is specific to patients with cancer. It refers to the use of a core how to interpret/evaluate studies involving HRQoL (Guyatt
cancer questionnaire in conjunction with validated modules et al, 1997; Wu et al, 2014). Both present a standardized
for specific disease sites (i.e., pancreas, liver, biliary modules) approach to critical appraisal and provide a means by which
(Langenhoff et al, 2001). This approach is based on the HRQoL can be integrated into evidence-based medicine.
premise that, although there are similar effects of disease/
treatment across cancers, each primary tumor site is also asso- HEALTH-RELATED QUALITY-OF-LIFE STUDIES
ciated with a unique set of HRQoL concerns. Use of a modular IN HEPATOBILIARY CANCER
approach increases the sensitivity to detect small, yet clinically
relevant, changes in HRQoL. This method has been popular- Measurement and reporting of HRQoL has increased exponen-
ized by the EORTC, in which the core EORTC QLQ-C30 tially during the past decade. The development of reliable, valid,
questionnaire is paired/supplemented with a site- and/or and sensitive measurement tools for use in cancer patients and,
symptom-specific instrument. Site-specific modules validated more specifically, in patients with hepatobiliary malignancy, has
for use among hepatopancreatobiliary (HPB) tumors include led to a vast increase in the number and quality of studies
the following: pancreatic cancer module (PAN26), colorectal assessing HRQoL in patients with HPB-related malignancy.
liver metastases module (LM21), hepatocellular carcinoma The following sections highlight the current status of
module (HCC18), and cholangiocarcinoma/gallbladder carci- HRQoL as it pertains to definitive surgical management as well
noma module (BIL21). A second modular approach, devel- as palliative interventions in patients with advanced HPB
oped and validated in North America, uses the FACT-G as the malignancies. Tables 28.3 to 28.7 summarize the most recent
core questionnaire, which is supplemented with site-/symptom- reports in the literature as well as landmark studies on HRQoL
specific modules, such as the hepatobiliary subscale (FACT- in the setting of HPB malignancy.
Hep; Fig. 28.2). Despite the seeming similarity and potential
overlap of the FACT-G plus supplemented modules with the Pancreatic Resection
EORTC QLQ-C30 plus supplemental models, the two instru- Despite advances in surgical technique and perioperative care
ments have been compared and found to measure different following pancreatic resection, morbidity remains common
aspects of HRQoL (Kemmler et al, 1999). The comprehensive (20% to 30%) (see Chapters 27, 62, and 66). Furthermore, in
nature of these tools provides increased sensitivity; however, the setting of pancreatic cancer, even with complete resection,
practicality, in terms of time and resources required to com- long-term survival is rare. It is therefore not surprising, that
plete, may be prohibitive in some settings. Based on this, with high morbidity and less than optimal survival outcomes,
attempts to develop brief scales that adequately correlate with the impetus for robust HRQoL evaluation among patients
the more extensive evaluations have been attempted. Yount undergoing pancreatic resection has gained significant momen-
and colleagues (2002) developed and tested an eight-item tum. As a consequence of this increased interest, study design
symptom scale from the FACT hepatobiliary subscale that cor- and methodology have improved greatly and appreciably
related well with overall FACT-G scores; however, the ability enhanced the quality of this expanding body of knowledge
to discriminate patients based on performance status/treatment (Table 28.3).
status was limited. Overall, these simplified indices are not as Patients with pancreatic cancer often experience consider-
sensitive or reliable as longer multidimensional evaluations of able symptoms and are at increased risk for impaired HRQoL
482 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
ENGLISH
3. Do you have any trouble taking a short walk outside of the house? 1 2 3 4
6. Were you limited in doing either your work or other daily activities? 1 2 3 4
FIGURE 28.1. European Organization for the Research and Treatment of Cancer Quality-of-life Questionnaire (EORTC QLQ-C30). A user’s agree-
ment is required to use this scale and can be accessed through the website www.eortc.be/home/qol/downloads/index.html.
Chapter 28 Quality of life and hepatobiliary tumors 483
ENGLISH
For the following questions please circle the number between 1 and 7 that best applies to you
29. How would you rate your overall health during the past week?
1 2 3 4 5 6 7
30. How would you rate your overall quality of life during the past week?
1 2 3 4 5 6 7
© Copyright 1995 EORTC Quality of Life Group. All rights reserved. Version 3.0
FACT-Hep (Version 4)
Below is a list of statements that other people with your illness have said are important. Please circle
or mark one number per line to indicate your response as it applies to the past 7 days.
FIGURE 28.2. Functional Assessment of Cancer Treatment–Hepatobiliary Questionnaire (FACT-Hep). (Courtesy Dr. David Cella at www.FACIT.org;
copyright 1987, 1997. Permission for use must be obtained by contacting Dr. David Cella at www.FACIT.org or d-cella@northwestern.edu.)
Chapter 28 Quality of life and hepatobiliary tumors 485
FACT-Hep (Version 4)
Please circle or mark one number per line to indicate your response as it applies to the past 7
days.
compared with population norms (Belyaev et al, 2013; Chan Early postoperative evaluation of HRQoL typically repre-
et al, 2012; Ljungman et al, 2011; Muller-Nordhorn et al, sents a transient state, primarily reflective of a patient’s recovery
2006). Results of HRQoL evaluation following pancreatic from the acute effects of surgery. These findings certainly allow
surgery are divergent and heavily dependent on the cohort surgeons to better inform patients, improve the consent process,
studied and the timing of evaluation relative to surgery. Among and help tailor expectations. However, longer-term follow up
well-selected patients with localized, resectable disease, HRQoL postpancreatectomy is requisite to unveil the true clinical
at 3 months following surgery was reportedly improved (Crippa impact of surgical resection on HRQoL outcomes. In a recent,
et al, 2008; Yeo et al, 2012). Unfortunately, the beneficial find- prospective longitudinal study, HRQoL 12 months after pan-
ings reported in these studies appear to be the exception, with creaticoduodenectomy (PD) for periampullary malignancies
the great majority of investigations reporting stability and/or was evaluated using the SF-36 survey. Despite the heterogene-
decline in HRQoL scores following pancreatic resection ity in cancer subtypes included, and initial decrements, signifi-
(Belyaev et al, 2013; Crippa et al, 2008; Ljungman et al, 2011; cant improvements were observed in the majority of subscales
Mbah et al, 2012; Muller-Nordhorn et al, 2006; Nieveen when measured at 12 months (Chan et al, 2012). Similarly,
van Dijkumet al, 2005; Schniewind et al, 2006). The hetero- significant improvements in HRQoL domains assessed with the
geneity observed in these studies is likely multifactorial and EORTC QLQ-C30 were observed among a group of patients
related, but not limited, to differences in disease stage, HRQoL undergoing partial pancreatectomies for pancreatic adenocar-
instrument used, timing/frequency of measurement, and length cinoma at 6 and 12 months postoperatively. Although baseline
of follow-up. measurements were obtained postoperatively, and absolute
486 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
FACT-Hep (Version 4)
Please circle or mark one number per line to indicate your response as it applies to the past 7
days.
C2 I am losing weight............................................................... 0 1 2 3 4
HRQoL improvement is most certainly overestimated in this jejunostomy (PJ), for a mix of benign and malignant indications
later study, the overall conclusions remain the same (Halloran (Billings et al, 2005; Epelboym et al, 2014; Han et al, 2007;
et al, 2011). Following pancreatectomy, patients tend to expe- Nguyen et al, 2003; Schmidt et al, 2005; Shaw et al, 2005; You
rience surgery-related decline in HRQoL, although the over- et al, 2007). In general, patients undergoing partial pancreatec-
whelming majority of data support a gradual improvement/ tomy for benign disease, regardless of the type (PD, RPD,
return to baseline within the first postoperative year. PPPD, and PSP) had similar long-term global ratings of
To date, several studies have compared HRQoL of patients HRQoL as well as comparable social, functional, and role
undergoing different types of partial pancreatomy—classic scores on the EORTC QLQ-C30. Furthermore, studies of
pancreaticoduodenectomy (PD) versus radical pancreati long-term HRQoL among patients with completely resected
coduodenectomy (RPD) versus pylorus-preserving pancreati- malignant tumors also suggest that HRQoL trends follow the
coduodenectomy (PPPD) versus parenchyma-preservation/ same postoperative trajectory independent of the type of resec-
-sparing pancreatectomy (PSP), with different reconstruction tion and/or reconstruction.
techniques—pancreaticogastrostomy (PG) versus pancreatico- Text continued on p. 494
TABLE 28.3 Studies of Pancreatic Surgery and Health-Related Quality of Life
Study Purpose/ Study Design, N, and
Quality-of-Life End HRQoL Assessment Quality-of-Life
First Author, Journal, Year Population (Patient With) Point Time Points Instrument Quality-of-Life Results Comments
Pancreatic Resection
Nguyen, Journal of Periampullary cancer Primary outcome: Cross-sectional, N = FACT-Hep Assessments were
Gastrointestinal Surgery, randomized to PD or a postoperative 105 (55 PD and completed at mean 2.1 yr
2003 RPD (PD + HRQoL 50 RPD); HRQoL after surgery. No
retroperitoneal lymph assessed at a differences at long-term
node dissection) single, follow-up in HRQoL and
nonstandard GI functional status
postoperative between PD and RPD.
time point RPD patients had a
significantly higher
postoperative complication
rates (43% to 29%, P =
.01)
Van Heek, Annals of Surgery, Unresectable periampullary Primary outcome: Prospective EORTC 2/36 HJ + GJ and 12/29 HJ Completion rates were
2003 cancer randomized to development of randomized trial, QLQ-C30 + patients developed GOO >90% in both groups for
undergo a double GOO N = 65 (36 HJ + PAN26 (P < .01). After an initial the first 4 mo
bypass (HJ + GJ) or a Secondary end GJ, 29 HJ alone) module decline with surgery, postoperatively and 75%
single bypass (HJ) point: HRQoL HRQoL assessed HRQoL returned to in the last 2 mo
preoperatively, at baseline by 4 mo
discharge, and postoperatively and was
q1mo for 6 mo not different between
groups
Billings, J Gastrointestinal Periampullary disease Primary outcome: Cross-sectional SF-36 Health Mean follow-up time: 7.5 yr Only evaluated TP patients
Surgery, 2005 (benign and malignant) longitudinal matched design, Survey, Audit postoperatively. TP cohort alive with no disease at
requiring TP HRQoL N = 27 TP; TP of Diabetes- had lower SF-36 role, and time of survey
cohort age/ Dependant physical and general administration (mean,
gender matched HRQoL (ADD health scores (P < .05). 7.5 yr), “healthy-
1 : 1 with IDDM HRQoL), ADD HRQoL scores were survivor” bias
cohort; HRQoL EORTC decreased but not different
assessed at a Pan26, from IDDM controls
single, nonvalidated
nonstandard, institutional
postoperative survey
time point
Nieveen van Dijkum, British Resectable pancreatic Primary outcome: Prospective Medical After an initial decline,
Journal of Surgery, 2005 tumors (benign and longitudinal longitudinal, N = outcomes HRQoL scores returned to
malignant) undergoing HRQoL 114 (PD = 72, HJ study baseline at 3 mo
PD compared with + GJ = 42); (MSO-24), postoperatively in both
unresectable pancreatic assessed gastrointestinal groups. Rapid decline in
tumors undergoing preoperatively, HRQoL index HRQoL was observed in
double bypass (HJ + postoperatively, (GIQLI) both groups in the 8th wk
GJ) and at 1.5-, 3-, prior to death
6-, 9-, and
12-mo follow-up
Chapter 28 Quality of life and hepatobiliary tumors
Continued
487
TABLE 28.3 Studies of Pancreatic Surgery and Health-Related Quality of Life—cont’d
488
3- and 6-mo
follow-up
Continued
489
TABLE 28.3 Studies of Pancreatic Surgery and Health-Related Quality of Life—cont’d
490
Surgery, 2011 cancer cost utility of cohort, N = 119; Survey and patients compared with only 58 patients (37
curative HRQoL assessed Utility Index controls at all time points early and 27 late); late
treatment for preoperatively, (SF-36-6D (P < .05) data subject to
pancreatic early preference- HRQoL index (0.69) at “healthy-survivor bias”
cancer postoperatively based utility long-term follow-up was
Secondary (<1 yr), or late index, scored not different from index
outcome: postoperatively 0 = death to 1 scores preoperatively
HRQoL (1-5 yr), = perfect (0.65) or early
compared with health) postoperatively (0.63) in
age-matched the treated group
healthy controls
Walter, European Journal of Advanced pancreatic Primary outcome: Prospective EORTC Outside of worse scores on Completion rates: baseline
Surgical Oncology, 2011 cancer undergoing longitudinal longitudinal, N = QLQ-C30 physical functioning 100%, discharge 78/86
palliative resection (PR) HRQoL 86 (61 HJ + GJ, subscales at 6 mo, the HJ (91%), 3 mo 58/86
or double bypass (HJ + between PR 25 PR); HRQoL + GJ group had (67%), 6 mo 41/86
GJ) and HJ + GJ assessed significantly better HRQoL (48%)
preoperatively, at and improved symptoms
discharge, and 3 compared with PR group
and 6 mo
postoperatively
Chan, Journal of Periampullary cancer Primary outcome: Prospective SF-36 Health One mo postprocedure, Completion rates:
Gastrointestinal Surgery, undergoing PD longitudinal longitudinal, N = Survey significant decline in preoperative 100%,
2012 HRQoL 37; HRQoL physical function (P < 1 mo 29/37 (78%),
assessed 0.01) and emotional role 3 mo 26/37 (70%),
preoperatively, 1, (P < .03). At 3 mo, mental 6 mo 28/34 survivors
3, 6, and 12 mo health increased (82%), 12 mo 28/28
postoperatively significantly (P = .02); survivors (100%)
6 mo, physical role (P <
.01), physical pain (P =
.01), social function (P =
.01) improved significantly.
At 12 mo, these changes
were sustained as well as
significant improvement in
vitality (P = .02) and
emotional role (P < .01)
Mbah, Journal of the Pancreatic cancer Primary outcome: Prospective EORTC Following an initial HRQoL data collected as
Pancreas, 2012 undergoing HRQoL longitudinal, N = QLQ-C30 and postoperative decline, part of a prospective
pancreatectomy following 34 HRQoL FACT-Anemia HRQoL returned to trial examining the safety
pancreatectomy assessed baseline at 6 wk. Overall, of intraoperative
in patients with preoperatively complication rate was autotransfusion during
and without and at 2-3 wk, 21%, with no difference in oncologic resections;
complication 6 wk, 3, and HRQoL scores among HRQoL stratified by
6 mo those who did and did not anemia at discharge
postoperatively have complications (P = was also evaluated
.11). At 6 mo, scores on
cognitive functioning
significantly declined (P =
.02).
Belyaev, Langenbecks Pancreatic disease (benign Primary outcome: Retrospective SF-36 Health HRQoL was worse Completion rates:
Archives of Surgery, 2013 and malignant) longitudinal cohort, N = 174 Survey compared with population preoperatively 100%,
undergoing pancreatic HRQoL (105 malignant, norms at all time points, P 3 mo 133/174 (76%),
resection comparison by 69 benign); = .03. Early postoperative 24 mo 83/174 (48%)
procedure and HRQoL assessed HRQoL was best in
diagnosis preoperatively patients undergoing distal
and at 3 and pancreatectomy and worst
24 mo with TP. Patients with
postoperatively, cancer, as opposed to
included benign diagnosis, had
comparison to lower postoperative
age-matched HRQoL and persistent
population norms decline to 24 mo. Patients
with benign tumors/
pancreatitis had initial
drop, followed by slow
trend toward recovery at
24 mo
Chapter 28 Quality of life and hepatobiliary tumors
Continued
491
492
Total pancreatectomy (TP) is a procedure associated with been suggested as an alternative to prophylactic surgical bypass
substantial and irreversible long-term consequences related to (HJ plus GJ), with the potential added benefit of reducing pain
pancreatic insufficiency. Patients undergoing TP are dependent associated with advanced pancreatic malignancy. When directly
on orally administered exogenous pancreatic enzymes to compared, no differences have been shown in terms of opera-
prevent malabsorptive syndromes/chronic diarrhea as well as tive morbidity/mortality and/or overall survival between pallia-
strict insulin administration regimens to balance blood sugars tive resection and bypass. Furthermore, despite the idea that
and mitigate long-term diabetic complications. Not surpris- resection improves pain control, and potentially HRQoL, it has
ingly, TP has the potential to substantially influence many been observed that patients treated with palliative resection
HRQoL domains. In a longitudinal study of 32 patients under- actually experience significantly greater declines in emotional,
going TP for locally advanced central tumors (benign and cognitive, and social-functioning scales as assessed by the
malignant), HRQoL was assessed postoperatively and annually EORTC QLQ-C30 compared with surgical bypass alone
for 4 years thereafter. Interestingly, no difference in the mean (Walter et al, 2011). In combination, these findings suggest
global HRQoL scores between healthy norms and the entire that resection provides no advantage in terms of survival or
TP population was observed; however, physical functioning HRQoL. Consequently, use of resection as a means of pallia-
among the TP group was significantly lower. Compared with tion for advanced pancreatic head tumors should be used
benign counterparts, patients undergoing TP for malignant sparingly.
disease had higher symptom scale scores, suggesting a greater To reiterate, the primary goal of palliative care is symptom
negative impact on HRQoL among this group. The number of management and maintenance of QoL. To this end, pancreatic
patients evaluable at each time point in this study was low, and stenting for the relief of intractable malignant pain has been
longer-term outcomes are subject to the “health survivor” bias evaluated. Wehrmann and colleagues assessed overall QoL
(Hartwig et al, 2015). using the Spitzer Quality-of-life Index (QLI), as well as pain
Recently, Billings and colleagues (2005), compared HRQoL control and opioid analgesic use, at baseline and every 4 weeks
outcomes of 27 long-term survivors (mean, 7.5 years) treated following intervention in patients with unresectable pancreatic
with TP for malignancy with age- and gender-matched con- carcinoma. Stenting was associated with significantly improved
trols. TP patients experienced a negative impact on their QoL pain control at 4 weeks, which persisted out to 12 weeks. QLI
and health status compared with the general population; scores paralleled pain scores and were improved versus baseline
however, compared with patients with insulin-dependent dia- at the 4-week time point, with return to baseline levels at 12
betes mellitus (IDDM) from other causes, the differences were weeks (Wehrmann et al, 2005). Stenting of the pancreatic duct
no longer observed. Similarly, Epelboym and colleagues (2014) in select patients with advanced pancreatic malignancy and
compared HRQoL between patients treated with TP versus PD significant pain transiently improves pain control and HRQoL
with IDDM. Patients in the TP group had a slightly higher and is most certainly a reasonable option for palliation of these
number of hypoglycemic events, but no significant differences patients (see Chapter 69).
were observed in global HRQoL scores. A subsequent study
matched TP patients to IDDM patients and compared global Hepatic Resection
HRQoL scores using the EORTC-QLQ-C30 plus the PAN26 In the early eras of hepatic surgery, mortality ranged from 30%
module and diabetes-specific QoL scores. Overall, TP patients to 60%, and elective intervention was rare. However, similar to
reported worse global HRQoL compared with matched IDDM pancreatic resection, improvement in surgical technique, peri-
patients; however, when using the diabetes-specific measure- operative care, and multidisciplinary team management has led
ment tool, there were no significant differences (Roberts et al, to significant decreases in morbidity and mortality (from >50%
2014). These findings suggest that although TP impacts down to 2-3%) associated with hepatic resection (Jarnagin et al,
HRQoL, the changes observed are comparable to those seen in 2002) (see Chapter 103). As a consequence, hepatic resection
patients with IDDM alone and/or other types of pancreatic has become the standard of care for definitive management of
resection. This suggests that if TP is indicated, concerns regard- many hepatic tumors. The increased use of hepatectomy for
ing the impact of pancreatic insufficiency on HRQoL should both primary and metastatic hepatic cancers has undoubtedly
not obviate intervention in well-selected patients. improved survival outcomes; however, questions regarding the
Many patients with pancreatic cancer are seen late with impact of hepatic resection on HRQoL remain. At present, our
disease that is not amenable to curative resection. Although less increasing ability to measure HRQoL in a psychometrically
common in the era of percutaneous and endoscopic interven- valid and clinically applicable fashion has resulted in a vast
tions, some patients may require or may be best served with increase in the number and quality of studies addressing
surgical palliation of gastric and/or biliary obstructions (see HRQoL as it pertains to hepatic resection and treatment of
Chapter 69). In a randomized study, Van Heek and colleagues hepatic tumors (Table 28.4).
compared HRQoL following prophylactic double bypass with HRQoL in the early postoperative period primarily reflects
hepaticojejunostomy (HJ) plus gastrojejunostomy (GJ) to single procedure-related factors (i.e., incisional pain, mobility limita-
biliary bypass (HJ) alone. In terms of HRQoL measures, no tions, complications, etc.). To date, multiple studies have eval-
differences were observed between groups. However, an 18% uated the short-term impact of hepatic resection on HRQoL
reduction in the risk of gastric outlet obstruction and need for (Chen et al, 2004; Eid et al, 2006; Langenhoff et al, 2006;
repeat intervention was observed in the HJ-plus-GJ group. Martin et al, 2007; Miller et al, 2013; Wiering et al, 2011).
HRQoL was not reassessed or compared among those who did Among patients undergoing hepatectomy for primary hepatic
and did not develop obstructive symptoms requiring secondary cancer (HCC/intrahepatic cholangiocarcinoma [ICC]), a sig-
intervention. This is unfortunate because this may have influ- nificant decline in mean scores on the Gastrointestinal Quality-
enced longer-term HRQoL (Van Heek et al, 2003). Palliative of-life Index (GQLI) was observed 2 to 10 weeks postoperatively
resection for advanced carcinoma of the pancreatic head has (Chen et al, 2004). The initial decline was followed by a
TABLE 28.4 Studies of Hepatic Resection and Health-Related Quality of Life
Study Purpose/
First Author, Journal, Population (Patient Quality-of-Life End Study Design, N, and Quality-of-Life
Year With:) Point Assessment Time Points Instrument Quality-of-Life Results Comments
Hepatic Resection
Poon, Archives of HCC Primary outcome: Prospective longitudinal FACT-G, translated At 3 mo, global HRQoL, PWB, EWB, and Disease recurrence
Surgery, 2001 undergoing longitudinal N = 76 (66 HR, 10 into Chinese SWB significantly improved over was treated with
HR HRQoL controls—unresectable baseline and were maintained out to TACE, systemic
HCC treated with 2 yr among the HR group; no changes chemotherapy,
TACE); HRQoL were observed in HRQoL measures and/or BSC
assessed q3mo for among unresected controls at 3 mo,
2 yr and decline was observed starting at
9 mo. Disease recurrence was
associated with a significant decline in
mean HRQoL (P < .001)
Chen, Hepatobiliary Primary hepatic Primary outcome: Prospective longitudinal, Gastrointestinal QoL Mean GQLI was decreased at 2-10 wk 47% (17/36) patients
and Pancreatic cancer short-term and N = 36; HRQoL Index (GQLI) postoperatively, followed by a gradual died by 9-mo
Disease undergoing longitudinal assessed return to baseline by 4 mo, and at follow-up
International, 2004 HR HRQoL preoperatively; at 2, 5, 9 mo. Mean GQLI scores were
and 10 wk; 4, 6, and increased above baseline measures.
9 mo; and 1, 1.5, and Disease recurrence was associated with
2 yr postoperatively a steady decline in HRQoL
Langenhoff, British Hepatic Primary outcome: Prospective cohort, N = EORTC QLQ-C30 and Group 1: decrease in global and functional
Journal of Surgery, malignancy short-term and 97 (group 1 = HR [n = EQ-5D-3L + HRQoL domains; decrease in EQ-VAS
2006 undergoing longitudinal 60], group 2 = EQ-VAS and symptoms at 2 wk, with return to
HR (CRLM, HRQoL unresectable at baseline at 3 mo; stable or improved
CCA, HCC, laparotomy [n = 19], out to 12 mo
and other group 3 = Group 2: decrease in global and functional
hepatic unresectable at HRQoL domains; decrease in EQ-VAS
metastases) presentation [n = 20]); and increased symptoms at 2 wk, with
HRQoL assessed at continued decline and ongoing
baseline and 0.5-, 3-, symptoms
6-, and 12-mo Group 3: no change in global, functional,
follow-up or symptoms, HRQoL domains, or
EQ-VAS at 2 wk or 3 mo, decrease in
global and functional domain-specific
QoL at 6 mo
Eid, Cancer, 2006 Hepatic Primary outcome: Prospective longitudinal, FACT-Hep, FHSI-8, Major hepatectomy associated with
malignancy comparison of N = 40 (24 major POMS, EORTC decrease in physical and functional
undergoing HRQoL based hepatectomy, 8 minor QLQ-C30 + PAN26 domain scores on FACT-Hep at 6 wk
HR or on type of hepatectomy, 8 module; global compared with minor resection or RFA.
surgical RFA surgical surgical RFA); HRQoL rating of change No differences in HRQoL measures at 3
(CRLM, CCA, intervention assessed at baseline, scales (6 domains, and 6 mo were observed between
HCC, other discharge, first scales −7 to +7) interventions. A similar trend was
metastases) postoperative visit, observed for all HRQoL measures
6 wk, 3 mo, and 6 mo (POMS, EORTC QLQ-C30/PAN36,
FHSI-8, global rating scales)
Continued
Chapter 28 Quality of life and hepatobiliary tumors
495
TABLE 28.4 Studies of Hepatic Resection and Health-Related Quality of Life—cont’d
496
Study Purpose/
First Author, Journal, Population (Patient Quality-of-Life End Study Design, N, and Quality-of-Life
Year With:) Point Assessment Time Points Instrument Quality-of-Life Results Comments
Lee, Journal of HCC Primary outcome: Cross-sectional cohort, N WHOQoL-BREF and Compared with population norms, HCC 70% Hepatitis B
Surgical Oncology, HRQoL in HCC = 161 (121 HR, 31 EORTC QLQ-C30 was associated with decrease in social
2007 compared with TACE, 8 PEI, 1 BSC) (Taiwanese and psychological domains and
population HRQoL assessed at translation) improved environment domains; HR
norms and single time point was associated with improved HRQoL
between compared with TACE/PEI/BSC
treatment type
Martin, Surgery, 2007 CRLM, CCA, or Primary outcome: Prospective longitudinal FACT-HEP, FHSI-8, Major hepatectomy associated with Major hepatectomy
HCC time to return to N = 32 (24 major EORTC QLQ-C30 + decline in all measures of HRQoL = ≥3 Couinaud
undergoing baseline HRQoL hepatectomy, 8 minor PAN26 module, postoperatively; HRQoL nadir scores segments
HR hepatectomy); HRQoL POMS; global observed at 6 wk, with return to
assessed at consent, rating scale (6 baseline values by 3 mo. Minor
discharge, first domains, scales −7 resection was associated with
postoperative visit, to +7) decrements in all measures at
6 wk, then 3, 6, and discharge; nadir HRQoL scores
12 mo observed at initial postoperative visit
and returned to baseline by 6 wk
postoperatively
Dasgupta, British Hepatic Primary outcome: Prospective longitudinal, EORTC QLQ-C30 Decrease from baseline to 6 mo in 44/103 (43%) alive
Journal of Surgery, malignancy longitudinal N = 103 (74 CRLM, 9 physical functioning domain and at last follow-up
2008 undergoing HRQoL CCA, 8 HCC, 12 increase in dyspnea/fatigue. At 12 mo,
HR (CRLM, other); HRQoL physical function and fatigue return to
CCA, HCC, assessed at baseline, baseline but dyspnea persistent.
other 6, 12, and 36-48 mo Survivors with no recurrence at
metastases) 36-48 mo had improved global HRQoL
PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
chemoembolization; VAS, visual analogue scale; WHOQoL-BREF, World Health Organization Quality-of-Life–BREF (abbreviated) assessment.
497
498 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
gradual return to baseline by 4 months, and in patients without CRLMs. However, in a recent study by Rees and colleagues
recurrence, mean GQLI was greater than baseline assessment (2012, using the EORTC QLQ-C30 in conjunction with the
by 9 months. This postoperative trend in HRQoL following liver-specific module, found that as many as 10% of patients
hepatic resection has been observed in multiple studies (Eid had persistent severe symptoms of pain and decrements in
et al, 2006; Langenhoff et al, 2006; Martin et al, 2007; Miller sexual function at 1 year following resection of CRLMs.
et al, 2013; Wiering et al, 2011) and appears similar regardless Longer-term follow-up of this study cohort suggests that, even
of underlying tumor type (primary/metastatic) or HRQoL mea- at a median of 8 years follow-up, 5% of patients still have sig-
surement tool used (EORTC QLQ-C30, FACT-G, FACT- nificant symptoms (Rees et al, 2014). This study did not
Hep, GQLI, etc.). Although the extent of resection may alter account for the use of preoperative or postoperative chemo-
the degree/duration of HRQoL decline postoperatively, in the therapy or further treatments. Consequently, it is difficult to
absence of disease recurrence, the overall trend remains the discern if the reported persistent symptoms are related to
same (Chen et al, 2004; Eid et al, 2006; Martin et al, 2007). CRLMs, hepatic resection, previous surgery for primary tumor,
In direct contrast to patients undergoing curative resection, or ongoing oncologic therapy.
patients found to have unresectable disease at the time of lapa- Overall survival is increased among patients with resectable
rotomy experience a steady decline in global HRQoL and all CRLMs. Unfortunately, disease recurrence requiring further
functional subscales, with persistence of symptoms throughout oncologic therapy is the norm and may influence HRQoL. In
follow-up (Langenhoff et al, 2006; Wiering et al, 2011). Lapa- a well-designed prospective study by Wiering and colleagues
rotomy for hepatic malignancy, without resection of disease (2011), patients undergoing hepatic resection and having less
negatively impacts both early and longer-term HRQoL out- than or equal to four CRLMs were followed for 3 years and
comes. As such, meticulous preoperative evaluation is essential HRQoL assessed at predefined time points. Overall, disease
to avoid subjecting patients to futile intervention. recurrence was associated with a decline in HRQoL as mea-
Compared with short-term postoperative HRQoL, longitu- sured by the EQ-5D-3L plus EQ-VAS (visual analogue scale).
dinal evaluation (≥3 to 6 months) following hepatic resection However, this decline in HRQoL was mitigated by the ability
is less reflective of the technical procedure and more likely to undergo repeat curative resection of recurrent disease.
related to patient- and disease-specific factors (Banz et al, HRQoL scores of patients who underwent complete re-resection
2009; Bruns et al, 2010). Overall, patients with HCC have were similar to those of patients who never experienced a recur-
worse psychological and social functioning compared with rence. Dasgupta and colleagues (2008) also report a decrement
population norms (Lee et al, 2007), and not surprisingly, in global HRQoL on the EORTC QLQ-C30 in the setting of
patients amenable to complete resection have improved recurrence. Similar decrements in HRQoL have been observed
HRQoL compared with HCC treated with transarterial che- following recurrence of HCC (Chen et al, 2004; Poon et al,
moembolization (TACE), percutaneous ethanol injection, and/ 2001), and following repeat resection of recurrent HCC,
or best supportive care (Toro et al, 2012) (see Chapters 91, 96, HRQoL trends parallel to what is seen with CRLMs (Tanabe
and 98). In a long-term evaluation of hepatic resection for et al, 2001). At present, it is reasonable to suggest that recur-
HCC in patients with persevered hepatic function, significant rence of disease following hepatic resection for malignancy
improvements in mean HRQoL and subscale scores were portends worse HRQoL; however, this decrement may be tran-
observed at 3 months and persisted out to 2 years follow-up sient if complete surgical reexcision can be achieved.
(Poon et al, 2001). Similar improvement was not observed in
a control group with HCC undergoing TACE. Chen and col- Locoregional Treatment of Hepatic Tumors
leagues (2004) also observed similar long-term trends in Locoregional therapy (LRT), including hepatic arterial embo-
patients undergoing hepatic resection for HCC. However, find- lization and ablation, may be used with curative and/or pallia-
ings from these studies contrast with those of Mise and col- tive intent for both primary and metastatic tumors of the liver
leagues (2014), in which no change in the physical component (see Chapters 96 to 98). These therapies treat disease/symptoms
scale on SF-36 and minimal change on the mental component using percutaneous methods, thereby avoiding the morbidity of
scale were observed following hepatectomy for HCC. The an open or laparoscopic surgical procedure. In addition to
measurement tools used in these studies differed (disease- bland embolization (hepatic artery embolization), chemother-
specific FACT-G vs. generic SF-36) in terms of sensitivity to apy and radiotherapy may be delivered to the liver locally via
change and may account for the observed differences. It is TACE and yttrium-90 (90Y) microsphere radioembolization
likely that longer-term HRQoL assessment in patients with (see Chapter 96). Ablative therapies vary by the agent/energy
HCC is heavily dependent on the type and severity of underly- source used to induce cell damage/death and include thermal
ing hepatic disease as well as other associated comorbidities. (radiofrequency, microwave, or cryotherapy) (see Chapters 98B
Future studies stratifying for these potential confounders are and 98C), electrical (irreversible electroporation) (see Chapter
necessary. 98C), and chemical (alcohol injection) (see Chapter 98D) tech-
CRLMs are the most common indication for hepatic resec- niques. The use of LRT to treat hepatic tumors has increased
tion, and multiple studies have assessed longer-term HRQoL substantially, and the impact on morbidity/mortality and sur-
outcomes among these patients (Banz et al, 2009; Bruns et al, vival has been well documented. In general, these types of
2010; Diouf et al, 2014; Earlam et al, 1996; Langenhoff et al, “hard” clinical outcomes are similar across locoregional thera-
2006; Rees et al, 2014) (see Chapter 92). Based on the litera- pies; as such, studies evaluating HRQoL and LRT for primary
ture, there is general consensus that following an initial post- and metastatic hepatic tumors are rapidly emerging (Table
operative decline, global HRQoL tends to return to baseline 28.5).
and at times exceeds baseline scores during longer-term HCC is the most common primary hepatic tumor (see
follow-up. Likewise, disease-specific symptoms and symptom Chapter 91). Because HCC typically arises in the setting of
scales tend to follow a similar trajectory after hepatectomy for underlying cirrhosis, treatment decisions are dependent on
TABLE 28.5 Studies of Locoregional Therapy for Hepatic Tumors and Health-Related Ouality of Life
Study Design, N, and
First Author, Journal, Population (Patient Study Purpose/Quality-of-Life HRQoL Assessment Time Quality-of-Life
Year With) End Point Points Instrument Quality-of-Life Results Comments
Locoregional Treatments
Steel, HCC treated with Primary outcome: HRQoL Prospective cohort, N = FACT-Hep Overall, HRQoL and scores on all Overall, survival at 6 mo
Psychooncology, TACE (cisplatin) and survival 28; HRQoL assessed subscales declined from baseline not different between
2004 or 90Y preprocedure and 3, to 6 mo for both groups. At 3 mo, groups; only 14
radioembolization 6, and 12 mo FWB and overall HRQoL scores patients evaluable at
postprocedure were higher in 90Y group (P < .01). 6 mo
At 6 mo, FWB remained
significantly improved over TACE,
but overall HRQoL was not
different
Ruers, Annals of Nonresectable Primary outcome: Prospective EuroQoL-5D-3L Baseline HRQoL similar between All patients underwent
Surgical Oncology, CRLM treated comparison of longitudinal, N = 201 and EORTC groups. All groups experienced an initial laparotomy; no
2006 with surgical longitudinal HRQoL (117 HR, 45 surgical QLQ-C30 initial decline in HRQoL and difference in median
ablation ± and survival ablation, 39 CTX) physical function at 3 wk OS between ablation
resection vs. survival data; HRQoL postprocedure. Ablation and HR and CTX groups (31
systemic assessed groups return to baseline at 3 mo, and 26 mo,
chemotherapy preprocedure and at whereas CTX did not. HR was respectively)
(CTX) 3, 6, 9, and 12 mo associated with higher HRQoL
for randomly than both ablation and CTX;
selected members of however, HRQoL in ablation group
the cohort; N = 109 was significantly higher than CTX
(53 HR, 29 surgical group from 3-12 mo
ablation, 27 CTX)
Wang, Quality of Life HCC treated with Primary outcome: Prospective FACT-G (Chinese TACE + RFA group higher overall
Research, 2007 TACE or TACE+ short-term longitudinal, N = 83 translation) FACT-G, SWB, and FWB scores
percutaneous postprocedure HRQoL (43 TACE, 40 TACE at 3 mo postprocedure (P < .01).
RFA + RFA); HRQoL Predictors of HRQoL were
assessed Child-Pugh class and tumor
preprocedure and recurrence
3 mo postprocedure
Bonnetain, Quality of Advanced HCC Primary outcome: Retrospective Spitzer QLI Higher Spitzer QLI at baseline Combined HRQoL data
Life Research, treated with determine the value of evaluation of 2 associated with increased median from 2 RCTs of
2008 tamoxifen, TACE, baseline HRQoL scores randomized clinical OS (P < .01). In addition to palliative treatment
or BSC in the in predicting overall trials, N = 489; common variables used in for HCC: (1)
palliative setting survival HRQoL assessed at classification systems (Okuda/ tamoxifen to best
(primarily baseline only CLIP/BCLC), HRQoL was the supportive care (N =
alcohol-related single best prognostic factor for 416), (2) TACE to
cirrhosis) survival tamoxifen only (N =
122)
Kalinowski, Unresectable liver; Primary outcome: safety Prospective EORTC Overall, an initial decrease in mean Late decline in HRQoL
Digestion, 2009 only and efficacy of 90Y longitudinal, N = 9; QLQ-C30 + HRQoL scores occurred following was associated with
90
neuroendocrine Secondary outcome: HRQoL assessed LMC21 Y. At 6 mo, the majority of tumor recurrence/
tumor longitudinal HRQoL preprocedure, and 3, module patients had improvement in disease progression
metastases 6, 9, 12 mo HRQoL scores, followed by a
Chapter 28 Quality of life and hepatobiliary tumors
AFP, α-Fetoprotein; BCAA, branched-chain amino acids; BCLC, Barcelona Clinic Liver Cancer Classification; BSC, best supportive care; CLIP, Cancer of the Liver Italian Program HCC (heptocellular carcinoma) Classification system; CRLM, colorectal liver metastases;
CTX, systemic chemotherapy; DFS, disease-free survival; EORTC QLQ-C30, European Organization for the Research and Treatment of Cancer Quality-of-Life Questionnaire–Core 30; EWB, emotional well-being; FACT, Functional Assessment of Cancer Therapy; FWB,
functional well-being; HAE, hepatic artery embolization; HCC, hepatocellular carcinoma; HCV, hepatitis C virus; Hep, hepatobiliary; HR, hepatic resection; HRQoL, health-related quality of life; ICC, intrahepatic cholangiocarcinoma; NT, no treatment; Okuda, Okuda
Prognostic Classification; OS, overall survival; PWB, physical well-being (FACT); QLI, Quality-of-Life Index; RCTs, randomized controlled trials; RFA, radiofrequency ablation; SF-36, 36-item Short Form; SIRT, selective internal radiotherapy; SWB, social well-being (FACT);
501
TACE, transarterial chemoembolization; TOI, Trial Outcome Index; WHOQoL-BREF, World Health Organization Quality-of-Life project (short form of WHOQoL-100); 90Y, yttrium-90 radioembolization.
502 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
tumor characteristics/disease burden, hepatic function, and actually one of the strongest predictors of overall survival
performance status. Transplant and hepatic resection are the (Bonnetain et al, 2008).
primary curative therapies; however, these are limited to a To date, no single LRT modality has consistently been
minority of patients (see Chapters 103 and 115). As a conse- shown to be superior to others in terms of HRQoL outcomes.
quence, LRT has emerged as the mainstay of treatment for All of the studies, excluding a very small (n = 18) pilot study,
many patients with HCC. Although some patients may be are nonrandomized and thus subject to inherent disease- and
rendered disease free, LRT in the setting of HCC is typically patient-related selection bias. Review of the literature suggests
noncurative and offered to provide local disease control and that in general, 90Y radioembolization and RFA are associated
ameliorate symptoms. As a consequence, interest in HRQoL with better HRQoL compared with TACE (Hamdy et al, 2013;
associated with LRT has focused primarily on this population Salem et al, 2013; Steel et al, 2004; Toro et al, 2012), and
of patients. Although, LRT is used in the treatment of hepatic TACE in combination with RFA is yields better outcomes than
metastases from neuroendocrine tumors (NET) and CRLMs, TACE alone (Wang et al, 2007). TACE and 90Y radioemboliza-
limited data are available regarding the impact of LRT on tion are typically used to treat multifocal unilobar/segmental
HRQoL in these populations (Kalinowski et al, 2009; Ruers disease, whereas RFA is indicated for small solitary lesions or
et al, 2006). low-volume multifocal disease; as such, comparison between
Compared with published population norms, patients with treatments without randomization or matching for extent of
HCC have lower overall HRQoL (Hamdy et al, 2013). Mul- disease/hepatic function is limited. A single, small, randomized
tiple studies have evaluated short-term (0 to 3 months) post- pilot study of TACE versus selective internal radiotherapy was
procedural HRQoL among patients with HCC treated with recently completed. HRQoL was a secondary end point of the
LRT (Hamdy et al, 2013; Kolligs et al, 2015; Salem et al, trial, and when using the FACT-Hep scale, no significant dif-
2013; Shun et al, 2012; Wang et al, 2007). In general, regard- ferences were observed between the treatments arms at 6 or 12
less of modality (TACE/90Y radioembolization/radiofrequency weeks of follow-up.
ablation [RFA]) and/or HRQoL instrument used, most patients Despite the limitations of the available literature, small
experience a transient decrement in overall HRQoL very early sample sizes, heterogenous patient populations, and lack of
(1 to 3 weeks) after intervention. This is typically followed by randomization, it is reasonable to conclude that HRQoL follow-
an improvement in most subscales/domains (physical, emo- ing LRT for HCC is improved in the short term, whereas
tional, social, mental/psychological), global HRQoL, and longer-term outcomes vary and are likely strongly influenced by
symptoms from 4 to 12 weeks. patient- and disease-specific variables. Furthermore, the clinical
The impact of LRT on longer-term HRQoL has also been indications and patient populations amenable to TACE versus
extensively evaluated (Eltawil et al, 2012; Huang et al, 2014; RFA versus 90Y radioembolization are inherently different. At
Kuroda et al, 2010; Steel et al, 2004; Toro et al, 2012; Wible present, no one form of LRT has consistently been associated
et al, 2010). Similar to short-term evaluations most longitudi- with superior HRQoL. Overall, in patients with unresectable,
nal studies report an initial early decline in HRQoL regardless nontransplantable liver, only HCC treatment with LRT pro-
of LRT modality. However, because the natural history of vides local disease control and likely improves patients overall
HCC differs based on the etiology of underlying hepatic HRQoL during the first 6 to 12 months following intervention.
disease (i.e., hepatitis C virus cirrhosis vs. hepatitis B virus cir-
rhosis), it is not surprising that reported longitudinal HRQoL Palliative Treatments
outcomes with LRT treatment of HCC vary (see Chapters 70 Surgery for tumors of the pancreas, liver, and bile ducts has
and 76). Steel and colleagues (2004) found a persistent improved over time; however, as many as 85% of patients with
decrease in global HRQoL and all subscales from baseline to 6 HPB malignancies are seen late with advanced-stage disease
months following TACE (cisplatin) or 90Y radioembolization. that is not amenable to surgical intervention. In this setting,
Interestingly, in this study, despite having greater disease significant complications related to the precarious location of
burden and lower reported HRQoL at treatment initiation, these tumors are common and often require intervention to
patients undergoing 90Y radioembolization had better func- ameliorate associated symptoms. The goal of treatment in this
tional well-being at 3 and 6 month follow-up when compared setting is palliative. It is therefore critical that interventions
with those treated with TACE. Other studies of TACE (Eltawil minimize morbidity and improve symptoms to maintain or
et al, 2012; Wible et al, 2010) as well as RFA (Kuroda et al, improve HRQoL.
2010) for unresectable HCC have reported no significant
changes in HRQoL parameters during longer-term follow-up. Gastric Outlet Obstruction
Toro and colleagues (2012) evaluated longitudinal HRQoL Malignant gastric outlet obstruction (GOO) occurs when the
among patients undergoing hepatic resection, RFA, TACE, or pyloric channel or duodenum is externally compressed by
no treatment (NT). With the exception of the NT group, all tumor and/or internally obstructed because of local tumor inva-
patients (resection, RFA, TACE) reported persistent improve- sion (see Chapter 69). It is a debilitating complication of
ments in HRQoL from 3 to 24 months. In this study, com- advanced malignancies, occurring in 20% to 30% of periampul-
pared with TACE and NT groups, patients treated with RFA lary cancers. The predominant symptoms associated with GOO
had significantly better physical and emotional well-being. include early satiety, bloating, nausea, vomiting, reflux, and
Improved longer-term HRQoL following LRT was also abdominal pain, often leading to anorexia, weight loss, and
observed in a recent study comparing hepatic resection with cachexia. Treatment of GOO is not only essential to improve
RFA in patients with small (<3 cm) HCC (Huang et al, 2014). symptoms but also to allow suitable candidates to return to or
HRQoL is not only important as a clinical outcome, but cor- initiate other oncologic therapy. Before the development
relational studies have shown that among patients undergoing of endoscopic and minimally invasive techniques, treatment
transarterial embolic therapy for HCC, baseline HRQoL is of GOO required laparotomy and open surgical bypass
Chapter 28 Quality of life and hepatobiliary tumors 503
(gastrojejunostomy [GJ]). More recently, advancements in postprocedure time point); as such, the conclusions regarding
both laparoscopic and endoscopic techniques has led to the HRQoL outcomes are difficult to interpret.
development of less invasive means of treating GOO, including Overall, studies reporting on HRQoL following palliative
laproscopic gastrojejunostomy (LGJ), percutaneous endoscopic procedures for GOO are limited in size, follow-up, and most
gastrostomy/jejunostomy (PEG/PEJ), or endoscopic/radiologic importantly, response rates. Reported median overall survival
duodenal stenting (DS). At present, determining which inter- of patients with advanced/end-stage malignancy and GOO
vention to use requires a balanced assessment of life expec- ranges from 7 to 20 weeks; therefore even short-term follow-up
tancy, risks and benefits of each intervention, the potential need can be difficult, and results are inherently biased in that patients
for repeat intervention, and the overall impact on HRQoL. In returning questionnaires/surveys represent a “healthy survivor”
the context of palliative interventions for GOO, HRQoL has subgroup. Furthermore, HRQoL is most commonly reported
only been assessed as the primary outcome in one study; as a secondary outcome of safety and efficacy trials; as such,
however, it has been assessed extensively as a secondary minimal HRQoL data is reported (i.e., single global measures
outcome (Table 28.6). It should be noted that many studies of reported as means, little evaluation of subscales, etc.), and the
HRQoL related to treatment of GOO have used a tool designed robustness of analysis and methodology is suboptimal. Despite
specifically for this patient population, called the Gastric Outlet this, available literature would suggest that relief of obstruction
Obstruction Scoring Scale (GOO-SS) (Dolz et al, 2011; van obviates the main symptoms associated with GOO, leading to
den Berg et al, 2013; van Hooft et al, 2009). Although the scale a stabilization of HRQoL. The palliative nature of intervention
only evaluates a single domain (physical), it is often reported for GOO demands assessment of HRQoL. At present, addi-
as a surrogate for HRQoL. tional prospective studies with HRQoL as a primary outcome
To date, a single randomized trial of 27 patients with malig- measure are necessary to define the true relationship between
nant GOO (56% pancreatic cancer) treated with DS (n = 13) treatment of malignant GOO and HRQoL.
versus LGJ (n = 14) has been completed (Mehta et al, 2006).
The underlying fragility of this group of patients is highlighted Malignant Biliary Obstruction
by the high rate of hospital mortality (DS at 17% and LGJ Malignant biliary obstruction (MBO) is common in the setting
at 23%). Not surprisingly, LGJ was associated with longer of pancreaticobiliary cancers (see Chapters 49, 51, and 65). In
hospital stay (LOS) and greater postprocedural complications fact, jaundice is often the initial clinical presentation of these
compared with DS. However, the procedural success rate in tumors. Hyperbilirubinemia is associated with increased periop-
the DS group (77%) was lower than in the LGJ group (100%). erative risk in certain situations and is a contraindication to many
Physical and mental HRQoL scores on the SF-36 at baseline chemotherapy regimens. Furthermore, biliary obstruction may
were similar between groups. Among evaluable patients at be associated with symptoms of anorexia, weight loss, pruritus,
1 month follow-up (n = 13, 6 LGJ and 7 DS), patients treated and malabsorption, leading to significant functional impair-
with DS had improved physical HRQoL scores, whereas no ment. As such, intervention to alleviate MBO is undertaken for
changes in HRQoL were observed in the LGJ group. The two primary reasons: to allow initiation of definitive oncologic
authors concluded that DS provided improved palliation versus therapy (surgery and/or chemotherapy) and/or to obviate associ-
LGJ based on decreased LOS, morbidity, and increased physi- ated symptoms. In the past, surgical bypass with hepaticojeju-
cal HRQoL at 1 month; however, this must be viewed in light nostomy (HJ) was the mainstay of treatment for MBO. However,
of the decreased procedural success rates of DS and need for in the current era, ES and radiologically guided percutaneous
potential repeat intervention. Similarly, Schmidt and colleagues biliary drainage (PBD) are the most common procedures used
(2009) observed improvements in global HRQoL, physical to relieve jaundice (Artifon et al, 2006; Mihalache et al, 2010)
and role functioning, and a decrease in symptoms following (see Chapters 29 and 30). Most recently, intraluminal brachy-
palliative intervention (endoscopic stenting [ES] and surgical therapy (ILBT) has also been proposed as a mechanism to treat
bypass) among 50 patients with malignant GOO at 3 months MBO. Initial reports regarding ILBT for MBO suggest improve-
postprocedure. ment in HRQoL and are encouraging. (Aggarwal et al, 2013).
DS is the most recent addition to the armamentarium of Decisions regarding the type of intervention for MBO are
procedures available to palliate GOO, and prospective trials complex and must take into account not only anatomic location
evaluating safety and efficacy have also included an evaluation but also life expectancy, intended future oncologic therapy,
of HRQoL outcomes and/or symptom relief (Dolz et al, 2011; safety/efficacy, and HRQoL. To date, multiple studies have
van den Berg et al, 2013; van Hooft et al, 2009 ). In terms of evaluated management strategies for MBO, many of which have
symptom relief, evaluated with GOO-SS, placement of ES was included analysis of HRQoL outcomes (Table 28.7).
consistently associated with symptom improvement and Several studies have assessed different methods of biliary
increased oral intake across studies. In two of three studies drainage and compared subsequent impact on HRQoL. Surgi-
reporting HRQoL outcomes, no changes in global measures of cal bypass for MBO is uncommon in developed countries and
HRQoL were observed at 1 month follow-up (Dolz et al, 2011; data pertaining to its impact on HRQoL are limited. In a study
van Hooft et al, 2009). Although no untreated GOO control from Brazil, where surgical bypass remains common, a com-
group was included, and the HRQoL in this population was not parison was made between ES and surgical bypass (choledo-
documented, it is likely that HRQoL would decline with chojejunostomy or cholecystojejunostomy) in patients with
progressive/untreated GOO and that stability of global measures metastatic pancreatic cancer. Regardless of treatment type,
represents a positive HRQoL outcome. Conversely, the most global HRQoL improved from baseline at 30- and 60-
recent study by van den Berg and colleagues (2013) reported days follow-up, respectively, but returned to preprocedure
significant improvements in global HRQoL following ES. This values by 120 days. However, global HRQoL scores in patient
study compared preprocedural HRQoL measure with the mean treated with ES were significantly higher at all time points,
HRQoL for the entire follow-up period (not standardized compared with the surgery group. No differences in procedural
504
TABLE 28.6 Studies of Palliative Intervention for Malignant Gastric Outlet Obstruction (GOO) and Health-Related Quality of Life
Study Design, N, and
First Author, Journal, Population (Patient Study Purpose/ HRQoL Assessment Time Quality-of-Life
Year With) Quality-of-Life End Point Points Instrument Quality-of-Life Results Comments
(choledochojejunostomy short-term HRQoL was associated with significantly higher groups; overall cost of
or HRQoL assessed HRQoL than surgery at 30 days (P = care from treatment to
cholecystojejunostomy) preprocedure .04) and 60 days (P = .05) death was significantly
or ES and 30, 60, and reduced with ES
120 days ($4270 USD) vs. HJ
postprocedure ($8320 USD)
Saluja, Clinical Unresectable gallbladder Primary outcome: Prospective WHOQoL– At 1 mo postprocedure, no change was Median OS was not
Gastroenterology carcinoma with hilar short-term randomized trial, BREF-26 observed in global HRQoL for either different between
and Hepatology, obstruction undergoing HRQoL and N = 54 (27 ES, and group; however, symptom scale scores groups. Clinical
2008 ES or PBD with plastic clinical 27 PBD); EORTC were improved in both PBD and ES. At procedural success
stent effectiveness of HRQoL QLQ-C30 3 mo, both groups showed a trend was higher in the PBD
biliary drainage assessed toward improvement in all domains of group (89%) vs. ES
preprocedure HRQoL assessed. PBD was associated (41%), and cholangitis
and 1 and 3 mo with improved physical and was less common with
postprocedure psychological scores compared with ES PBD (11%) compared
(P = .02) as well as greater improvement with ES (48%)
in symptom scores at 3 mo
Robson, Annals of MBO undergoing PBD Primary outcome: Prospective cohort, FACT-Hep VASP scores (pruritus symptoms) Median OS = 4.7 mo,
Surgical short-term N = 109; HRQoL and VASP significantly improved during time; mortality 10% at 1 wk,
Oncology, 2010 HRQoL, assessed however, overall HRQoL as measured 28% by 8 wk; 100%
symptom control, preprocedure by mean FACT-Hep scores were technical procedural
morbidity/ and 1 and 4 wk significantly decreased at 1 and 4 wk success but 50% major
mortality and postprocedure postprocedure complications
procedural
efficacy
Larssen, Surgical Malignant GI obstruction Primary outcome: Prospective cohort, EORTC Global HRQoL as well as nausea/vomiting, In addition to biliary
Endoscopy, 2011 undergoing ES SEMS short-term N = 162 (40 QLQ-C30 and appetite loss, and pruritus obstruction, study
HRQoL [25%] biliary); ± STO22 ± symptoms were significantly improved in cohort included
Secondary HRQoL PAN26 patients with biliary obstruction treated patients undergoing
outcome: assessed with SEMS. Both patients and esophageal, duodenal,
comparison of preprocedure physicians reported symptom and colonic SEMS
physician- and and 2 wk improvement; however, degree of
patient-rated postprocedure improvement reported by physicians
treatment effect was higher than that of patients
Artifon, Journal of MBO with history of a Primary outcome: Prospective SF-36 Health No difference in HRQoL measured at 7 or One hundred percent
Clinical failed ERCP undergoing clinical and randomized trial, Survey 30 days postprocedure for either group clinical and technical
Gastroenterology, PBD or EUS-CD technical N = 25 (13 success in both
2012 procedural EUS-CD, 12 groups; complication
success PBD); HRQoL rates and procedural
Secondary assessed costs not different
outcome: cost, preprocedure between groups
morbidity, and and 7 and 30
HRQoL days
postprocedure
Aggarwal, MBO undergoing palliative Primary outcome: Prospective EORTC Significant improvement in overall HRQoL Median OS = 8.7 mo
Brachytherapy, ILBT with access via symptom control, longitudinal, N = QLQ-C30 post-PBD, post-ILBT, and at last
2013 PBD HRQoL, and 18; HRQoL follow-up. Physical and social
survival assessed functioning scores were improved at all
pre-PBD, time points, as was insomnia symptom
post-PBD, scale. The percentage of patients who
pre-ILBT, reported pruritus and icterus declined at
post-ILBT, and each time point
follow-up
Barkay, Journal of MBO undergoing ES Primary outcome: Prospective FACT-G Significant improvement in global HRQoL
Clinical longitudinal longitudinal, N = and PWB, EWB, and FWB subscales at
Gastroenterology, HRQoL 164; HRQoL 30 and 180 days. Weight loss, appetite,
2013 assessed pruritus, and pain improved significantly
preprocedure, at at both time points
30 and 180
days
postprocedure
Moses, World Infrahilar MBO undergoing Primary outcome: Multicentered SF-36 Health At baseline, SEMS group had significantly Time to stent failure
Journal of ES randomly assigned time to stent prospective Survey worse physical functioning scores; no significantly longer
Gastroenterology, to pcSEMS or PS failure randomized trial, differences were observed between among the pcSEMS
2013 Secondary N = 85 enrolled: groups thereafter. At 1 mo, vitality was group, and cholangitis
outcome: 74 with HRQoL improved, and at 6 mo physical was less common; no
morbidity, data (36 PS, 38 functioning was improved in the difference in OS
mortality, KPS, pcSEMS); pcSEMS group. PS was associated
HRQoL HRQoL with significant improvement in
assessed subscales of bodily pain, social
preprocedure at functioning, and mental health at 1 mo
baseline and 1,
3, 6, 9, 12, and
15 mo
CBD, Common bile duct; EWB, emotional well-being; EORTC QLQ-C30, European Organization for the Research and Treatment of Cancer Quality-of-Life Questionnaire–Core 30; ERCP, endoscopic retrograde cholangiopancreatography; ES, endoscopic stenting; EUS-CD,
endoscopic ultrasound-guided cyst drainage; FACT, Functional Assessment of Cancer Therapy; FWB, functional well-being; GI, gastrointestinal; HRQoL, health-related quality of life; LBT, intraluminal brachytherapy; KPS, Karnosfsky Performance Score; MBO, malignant
Chapter 28 Quality of life and hepatobiliary tumors
biliary obstruction; OS, overall survival; pcSEMS, partially covered self-expanding metallic stent; PAN26, pancreatic cancer module-26; PBD, percutaneous biliary drainage; PS, performance score; PWB, physical well-being; SEMS, self-expanding metallic stent; SF-36,
36-item Short Form; STO22, EORTC gastric specific QoL Module; T-bili, total bilirubin; WHOQoL–BREF-22, World Health Organization Quality-of-Life assessment (abbreviated version, 22 items); VASP, visual analogue scale for pruritus assessment.
507
508 PART 3 ANESTHETIC MANAGEMENT: PREOPERATIVE AND POSTOPERATIVE CARE
complications or survival were observed between groups. The either PBD or ES. At 1 month follow-up, no significant change
equivalence in morbidity and mortality between procedures in overall HRQoL was observed between the groups; however,
with improved HRQoL suggests ES may be superior to surgical at 3 months a trend toward improvement was noted in both.
bypass in select patients. Compared with ES, PBD was associated with significantly
Techniques of ES and PBD for MBO have undergone greater improvement in physical and psychological domains.
significant evolution and advancement during the past decade. Both groups experienced improvement in symptoms, but PBD
Similarly, studies evaluating not only safety/efficacy of these was associated with significantly greater improvements in
interventions, but also HRQoL, have increased substantially. fatigue compared with ES. Conversely, evaluation of patients
ES for MBO is associated with reasonable clinical and technical randomly assigned to PBD or endoscopic ultrasound-guided
success. Reduction in total bilirubin levels by at least one-third choledochoduodenostomy (EUS-CD) revealed no significant
of preprocedural values with ES has been associated with change in HRQoL in the 30 days following intervention (Artifon
improved social and mental functioning as measured by SF-36; et al, 2012). Furthermore, there were no significant differences
however, these HRQoL improvements appear to be mitigated between the PBD and EUS-CD groups. It appears that, regard-
by the absolute preprocedure bilirubin (preprocedure total bili- less of procedure performed, relief of obstruction per se pro-
rubin ≥ 14 mg/dL; no change in HRQoL parameters) (Abraham vides symptom relief and at best stabilizes HRQoL, which
et al, 2002). Furthermore, in an assessment of 40 patients among this fragile cohort likely represents a positive outcome.
undergoing ES with self-expanding metal stents (SEMS),
global HRQoL on the EORTC QLQ-C30 was improved, as CHALLENGES IN HEALTH-RELATED QUALITY-
were symptoms of nausea/vomiting, appetite, and pruritus at 2 OF-LIFE RESEARCH AND FUTURE DIRECTIONS
weeks postprocedure (Larssen et al, 2011). Using the FACT-G
questionnaire, Barkay and colleagues (2013) also evaluated ES Despite the widespread implementation of HRQoL assessment,
for MBO and found improvement in global HRQoL and physi- interpretation of findings and implementation at the clinical
cal, emotional, and functional well-being at both 1 and 6 practice level is a significant challenge. Merely stating a “P”
months of follow-up. Likewise, a recent study comparing par- value, indicating a statistical difference, is the standard; however,
tially covered self-expandable metal stents with plastic stents, determining how this is to be interpreted clinically is a challenge
revealed no difference between treatments in terms of HRQoL and is one of the major criticisms of HRQoL research. To date,
but a general trend in both arms toward an improvement in this has significantly limited the clinical applicability of HRQoL
global HRQoL and subscales (Moses et al, 2013). Taken in research outcomes. As of 2005, only 25% of HRQoL studies
concert, these findings suggest that ES for MBO improves reported on the clinical significance, and thus applicability, of
short-term HRQoL and symptoms; however, conclusions their findings (Efficace et al, 2007). Several methods have been
regarding longer-term HRQoL outcomes are limited by the suggested to rectify this issue, including establishment of a
substantial decrements in survey completion with prolonged minimal important difference (MID)—the smallest difference
follow-up. in a score in the domain of interest that a patient perceived as
In a prospective evaluation of 109 patients with MBO pre- beneficial and that would mandate a change in patient manage-
senting for PBD, significant improvements in pruritus symp- ment (Jaeschke et al, 1989). Two primary methods for deter-
toms were observed, but overall HRQoL, as assessed by mining a MID for HRQoL outcomes exist: distribution based
FACT-Hep, significantly declined during the 4 week period (estimate based on observed scores in a sample) and anchor
following PBD. The mortality rate was extremely high—28% based (compare, or anchor, HRQoL differences/changes to
at 8 weeks post-PBD, highlighting the degree of illness and other clinical variables or patient’s subjective assessment).
frailty among this patient population (Robson et al, 2010). Although imperfect, a MID provides a means by which to place
PBD followed by ILBT has recently been touted to reduce HRQoL into a clinical context. Proponents for both forms of
localized tumor burden and result in improved biliary drainage measurement of MID exist; however, a combination of both
and symptom relief. In a study of high-dose ILBT 18 patients methods, where feasible, likely yields the most clinically useful
with advanced pancreaticobiliary or metastatic cancer under- and accurate information (Revicki et al, 2008).
went PBD, followed by two ILBT sessions 1 week apart. In Longitudinal studies of HRQoL are essential in the current
conjunction with significant improvement in symptoms (100% era, where disease treatments are becoming more and more
resolution of pruritus), global HRQoL as well as physical and complex and survival “with” disease is common. However, this
social functional scores were improved at all assessment points. assessment is subject to several biases, including “response
It appears that PBD alone significantly improves biliary obstruc- shift,” whereby patients recalibrate their internal standards
tive symptoms; however, in the absence of further treatments, regarding HRQoL during the course of treatment/follow-up
HRQoL seems to decline in a fashion expected of end-stage and “healthy survivor”; while time passes, sicker patients are less
pancreaticobiliary cancers. likely to complete surveys, and therefore longer-term results are
ES was initially preferred to PBD because drainage was heavily biased toward patients who are fairing the best. Although
internal and thought to be more readily achievable. However, methods exist in to attempt combating these issues, their use
advances in interventional radiology and the development of is rare and the approaches lack validation. Furthermore, long-
internal stents for percutaneous delivery suggest that safe can- term studies are often limited by the logistics of survey admin-
nulation of the biliary tree and adequate internal drainage can istration and practicality.
be achieved with both PBD and ES. The growing number of Missing data is a common and critical concern when inter-
techniques and methods for ES and PBD has led to multiple preting HRQoL data. The consequences of missing HRQoL
comparative evaluations of the two procedures. Recently, Saluja information depends on both the amount and the cause of
and colleagues (2008) randomly assigned patients with unre- missing data. It is to be expected that some information will be
sectable gallbladder carcinoma and hilar obstruction to undergo missing at random; the real concern comes when “missingness”
Chapter 28 Quality of life and hepatobiliary tumors 509
is not a random event. There are multiple mechanisms by personalized medicine, HRQoL researchers have developed
which to assess the importance of missing data, including com- GENEQoL, an initiative assessing potential links between
parison of statistical means from patients with complete HRQoL outcomes and genetics. Given that HRQoL may be
follow-up to those with incomplete follow-up, to see if there is predictive of clinical outcomes, the ultimate goal of such inves-
a difference between groups in HRQoL indices. If this is indeed tigations would be the development of a HRQoL genetic sig-
the fact, data are nonignorable missing data and must be nature to be used as a predictor of patient outcomes (Sloan &
accounted for or explained. Given the significant impact of Zhao, 2006; Sprangers et al, 2009).
missing data in HRQoL assessment, especially in studies during HRQoL research in surgery is in its infancy and, as such,
time, the best method to deal with it is in fact preventive. Trials faces many challenges, from study design and implementation
assessing HRQoL should be designed in a fashion such that to clinical application. However, it is encouraging that enthu-
implementation strategies and rigorous follow-up are in place siasm surrounding development of this field continues to rise
at the outset. among surgeons and institutions alike. In the future, collabora-
Future directions in HRQoL are based on item response tion between surgeons, statisticians, qualitative researchers, and
theory and include computerized adaptive testing in which most importantly, patients will be essential to further the devel-
patients’ responses to a given question will prompt the subse- opment and clinical application of HRQoL outcomes in surgery.
quent line of questions, thus individualizing surveys. Further- Furthermore, as the landscape of medicine continues to evolve,
more, the use of electronic surveys is increasingly become become more complex, and offer more life-saving/prolonging
part of standard clinical care such that questionnaires are treatments, there is no doubt that HRQoL measurement and
completed prior to each clinic visit, immediate feedback understanding will become increasingly valuable and essential
is generated for the patient and treating physician, and impor- for optimal patient care.
tant patient-centered concerns may be addressed and decisions
made. Likewise, in response to increasing fervor surrounding References are available at expertconsult.com.
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CHAPTER 29
Interventional endoscopy: technical aspects
Dennis Yang and Christopher John DiMaio
OVERVIEW
itself into the papilla. Alternatively, the cannula or sphinctero
The field of diagnostic and therapeutic biliary endoscopy has tome can engage the ampullary orifice first before using the
evolved rapidly since the first reports of endoscopic sphincter guidewire to effectively seek out the path to the desired duct
otomy in 1974. A variety of interventional endoscopic pro via fluoroscopy.
cedures have gained widespread acceptance as therapeutic
alternatives to operative management for a spectrum of biliary Endoscopic Retrograde Cholangopancreatography
disorders. Although endoscopic retrograde cholangopancrea
tography (ERCP) remains a common endoscopic technique
Pancreatic Duct Wire or Stent Placement to Facilitate
for the evaluation and management of biliary diseases, there Biliary Access
has been a trend toward alternative modalities, including There are various alternative endoscopic techniques that can
an expanding role for endoscopic ultrasound (EUS)-guided be used when attempts at biliary cannulation result in repeated
therapy (see Chapter 16). This chapter focuses on the current pancreatic duct entry. In the “double-wire technique,” a guide
technical aspects of endoscopic biliary intervention. wire is purposely placed in the pancreatic duct while the biliary
cannulation device is preloaded with a second guidewire to
reattempt biliary cannulation. Theoretically, the pancreatic
TECHNIQUES FOR BILIARY ACCESS guidewire assists by straightening the common channel and
common bile duct (CBD), thus facilitating biliary cannulation.
Endoscopic Retrograde Cholangopancreatography Furthermore, the direction of the pancreatic wire exiting the
Standard Cannulation Technique papilla on endoscopy may provide anatomic cues regarding the
Selective cannulation is a prerequisite for biliary endoscopic optimal axis for biliary cannulation. Although this technique
intervention. There are multiple devices that can be used for has been associated with high rates of cannulation in difficult
successful cannulation during ERCP, including standard can situations, it has not been conclusively shown to be superior to
nulation catheters and sphincterotomes. Standard biliary can standard cannulation (Herreros de Tejada et al, 2009; Maeda
nulation catheters can have one or more lumens, allowing the et al, 2003). Alternatively, instead of a wire, a pancreatic duct
injection of contrast material and passage of a guidewire to stent can also be placed during difficult biliary cannulation. The
achieve cannulation. In contrast to the standard catheter, a pancreatic duct stent may reduce the risk of PEP by ensuring
sphincterotome also has an electrosurgical cutting wire at the pancreatic duct drainage and by minimizing further inadvertent
distal end of the catheter that enables immediate sphincterot entry into the pancreatic duct on repeated attempts at biliary
omy following cannulation when indicated. Furthermore, pro cannulation (Ito et al, 2010; Lee et al, 2012).
viding tension on the cutting wire permits upward bowing of
the sphincterotome, which can facilitate alignment of the tip in Access “Precut” Sphincterotomy for Biliary Access
the proper axis for biliary cannulation. Access “precut” sphincterotomy refers to the technique of
There are various techniques that can be used to gain access incising the papilla prior to obtaining biliary access. Precutting
to the biliary system. The traditional approach entails the use can be a useful technique to achieve selective bile duct cannula
of a catheter to engage the papillary orifice, followed by injec tion when free or wire-guided approaches fail. The needle-knife
tion of contrast to delineate the trajectory and pathway of the (NK) catheter is typically used for this procedure. The NK
bile duct. Following this, the catheter and/or a guidewire can catheters have a retractable bare electrosurgical cutting wire
be inserted directly into the bile duct. Over the past decade, that extends from the tip of the catheter. The exposed needle
guidewire-assisted cannulation has become the favored can then be inserted into the papillary orifice, and the cut is
approach over a contrast-assisted free cannulation technique directed upward in the axis of the bile duct, generally in the 11
because it increases the primary cannulation success rate and to 12 o’clock position. Another variation of this technique
has been associated with lower rates of post-ERCP pancreatitis involves using the NK to begin an incision above the ampullary
(PEP), as it virtually eliminates the possibility of inadvertent orifice to directly access the CBD by creating a biliary fistula
contrast injection of the pancreatic duct (Cheung et al, 2009; (“fistulotomy”).
Lee et al, 2009; Tse et al, 2013). The small-diameter guidewire Precut sphincterotomy has been associated with biliary
with a hydrophilic tip can be advantageous for bile duct can cannulation rates exceeding 90% (Navaneethan et al, 2014).
nulation over the larger-diameter cannula or sphincterotome by However, precutting is not without risk, as the incision is per
minimizing trauma at the papilla. Wire-assisted cannulation can formed without the guidance of a wire within the duct. Previous
be performed by directly probing and advancing the guidewire large multicenter studies have identified precutting as a risk
511
512 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
factor for adverse events, such as acute pancreatitis, hemor The incision is made by upward lifting of the sphincterotome
rhage, and perforation, independent of the endoscopist’s expe with pressure against the papillary roof, but not excessively, to
rience (Freeman et al, 2001; Masci et al, 2001). More recently, avoid a rapid large incision (“zipper”) (Fig. 29.1B). The com
several studies have suggested that precut sphincterotomy may bination of a high cutting current blended with a low coagula
be a surrogate marker of difficult cannulation and not an inde tion current is frequently used, as this is felt to decrease the risk
pendent predictor of PEP (Bailey et al, 2010; Manes et al, of thermal transmission to the adjacent pancreatic tissue and
2009). Indeed, subsequent studies, including multiple meta- hence minimize the risk of pancreatitis. The size of the sphinc
analyses of both randomized and nonrandomized trials indicate terotomy varies on a case-by-case basis and can be limited by
that early precut implementation may be associated with a the length of the intraduodenal portion of the CBD. In general,
lower risk of PEP compared with persistent attempts at the sphincterotomy should be of adequate size to allow the
regular cannulation followed by precutting (Cennamo et al, passage of the stone in the CBD. The size of sphincterotomy
2010; Choudhary et al, 2014). Furthermore, overall complica can be gauged by the ability to move the bowed sphincterotome
tion rates are similar between an early precut sphincterotomy across the opening, by passing an inflated balloon catheter
approach versus persistent attempts at biliary cannulation through the site, and/or by elimination of the tapering or
(Navaneethan et al, 2014). Overall, it is important to empha “pinch” of the intraampullary bile duct seen on fluoroscopy.
size that precut sphincterotomy should be reserved for patients
with a strong indication for biliary access in whom standard Biliary Sphincteroplasty
techniques have failed. This approach should be performed by Endoscopic balloon dilation (sphincteroplasty) of the biliary
an experienced biliary endoscopist familiar with the nuances sphincter muscle was initially proposed as an alternative to
and technical aspects of this approach. endoscopic sphincterotomy. In this procedure, following selec
tive biliary cannulation and placement of a wire in the bile duct,
Transpancreatic Precut Sphincterotomy a balloon-tipped catheter (i.e., CRE balloon or Hurricane RX
(Goff Technique) dilation balloon; Boston Scientific, MA) is advanced over the
Transpancreatic precut (transeptal) sphincterotomy for biliary guidewire. The deflated balloon is positioned across the papilla
access was first described by Goff et al (1995). In this technique, and inflated with radiopaque contrast medium under both endo
following selective cannulation of the pancreatic duct, precut scopic and fluoroscopic visualization (Fig. 29.1C). The inflated
sphincterotomy is performed by cutting the septum between balloon is maintained until the “waist” corresponding with the
the pancreatic and bile duct with the standard sphincterotome biliary sphincter disappears, usually for 15 to 30 seconds. The
directed cephalad toward the bile duct. Since its introduction, optimal balloon size for sphincterotomy has not been estab
several studies have demonstrated high rates of bile duct can lished; however, one should generally avoid inflating the balloon
nulation (82% to 100%) without increased complication rates to a size larger than the diameter of the distal CBD to avoid bile
compared with standard NK precut sphincterotomy (Catalano duct injury (Binmoeller & Schafer, 2001). The main advantage
et al, 2004; Kapetanos et al, 2007). Additional advanced tech of sphincteroplasty is that it results in transient widening of the
niques for biliary access, including those in patients with surgi biliary sphincter such that the biliary sphincter will remain intact
cally altered anatomy, will be covered later in this chapter. and functional postprocedure. This may be advantageous in
children, as an intact biliary sphincter will presumably decrease
TECHNIQUES FOR THE MANAGEMENT the risk of recurrent choledocholithiasis. Furthermore, because
OF CHOLEDOCHOLITHIASIS there is no cutting involved with sphincteroplasty, there is a
lower risk of procedure-related bleeding. Thus use of this tech
Gallstone disease is an endemic condition in developed coun nique may be preferred to sphincterotomy in patients who are
tries, representing a major health burden with annual costs at increased risk of bleeding, such as those on antiplatelet or
of $6.5 billion in the United States (Shaffer et al, 2006). anticoagulation therapy that cannot be held for the procedure.
Choledocholithiasis is concomitantly present in up to 20% Primary biliary sphincteroplasty can also be helpful in facilitating
of patients with cholelithiasis at the time of cholecystectomy biliary cannulation in patients with surgically altered anatomy
(Menezes et al, 2000). Currently, ERCP with biliary sphincter in whom standard sphincterotomy cannot be performed safely
otomy and stone extraction is considered the first-line manage or is technically difficult. The main drawback of performing
ment for choledocholithiasis (Fig. 29.1A) (see Chapters 36 sphincteroplasty alone is its association with a higher risk
and 37). of pancreatitis and lower rates of stone clearance compared
with sphincterotomy (Baron & Harewood, 2004; DiSario et al,
Biliary Sphincterotomy 2004). However, when performed in conjunction with sphinc
Endoscopic sphincterotomy aims at opening the terminal part terotomy, sphincteroplasty has been shown to reduce the need
of the CBD by cutting the papilla and sphincter muscles. The for additional interventions for CBD stone clearance, particu
basic technique of sphincterotomy has not changed significantly larly in the setting of large biliary calculi (≥15 mm) (Madhoun
since its initial description. The standard sphincterotome, the et al, 2014; Teoh et al, 2013). Furthermore, balloon sphinctero
Erlangen “pull-type” model, consists of a catheter containing plasty following sphincterotomy has been shown to be safe, with
an electrosurgical cutting wire exposed 20 to 25 mm near the comparable complication rates compared with sphincterotomy
tip of the sphincterotome. The leading tip distal to the wire, alone (Maydeo & Bhandari, 2007; Weinberg et al, 2006).
the “nose,” is 5 to 10 mm in diameter. Once deep biliary can
nulation has been achieved, the sphincterotome is retracted Stone Extraction
slowly, until one fourth to one half of the wire length is exposed Several series have shown that 82% to 100% of bile duct stones
outside the papilla. The sphincterotome is slightly bowed so can be removed effectively following endoscopic sphincterot
that the cutting wire is in contact with the roof of the papilla. omy with a combination of balloon catheters or wire baskets
Chapter 29 Interventional endoscopy: technical aspects 513
A B
C D
FIGURE 29.1. Endoscopic management of choledocholithiasis. A, Cholangiogram showing diffusely dilated biliary system with stone in the
common bile duct (arrow). Biliary sphincterotomy (B), followed by sphincteroplasty (C). D, Extraction of large stone.
(Bergman et al, 1997; Cotton et al, 1980; Natsui et al, 2013) Lithotripsy
(Fig. 29.1D). Standard stone extraction techniques may fail when a stone
Extraction balloon catheters are available in different sizes is large, impacted, proximal to a stricture, or when stones
(8.5to 20 mm) and in most centers are the standard first-line are multiple. A variety of modalities are currently available to
approach for stone extraction, given their ease of use and lack fragment these difficult stones before extraction, including
of risk of becoming entrapped within the duct. The extraction mechanical lithotripsy, endoscopic intraductal lithotripsy, and
balloon is inflated (to the diameter of the bile duct) above the extracorporeal shock-wave lithotripsy.
stone and pulled back gently to the level of the papilla. In the
setting of multiple stones, it is important to remove the stones Mechanical Lithotripsy
individually starting with the most distal one, to avoid stone Mechanical lithotripsy has been the most frequently used litho
impaction. tripsy approach, given its ease of use and availability, with
Similarly, there are also a variety of wire baskets in different success rates of 90% and higher (Chang et al, 2005; Stefanidis
sizes and configurations. The stone is entrapped between the et al, 2011). There are two variations to the technique of
wires when the basket is closed, and subsequent removal is mechanical lithotripsy: an external-type lithotriptor method
achieved by traction removal of the basket in the axis of the bile and an integrated through-the-endoscope method. Using
duct. The effective traction of the wire basket often allows effec the external-type lithotriptor, the stone is captured within a
tive removal of medium- to large-size stones within the CBD standard Dormia basket, the basket handle is cut off, and
or stones that are “floating” within a dilated bile duct and thus the endoscope is removed. A coiled metal sheath is inserted
easily slip around a balloon. Conversely, the extraction balloon over the wire until its tip is in contact with the stone, and
may be more suitable for the removal of small stones/fragments mechanical lithotripsy is performed by turning the crank handle,
that are difficult to entrap between the wires or when opening crushing the stone between the basket wires and the metal tip
of the basket is constrained by duct caliber. of the sheath. In the integrated through-the-endoscope system,
514 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
a special lithotripsy basket contained within a metal sheath is TECHNIQUES FOR THE MANAGEMENT OF
inserted through the accessory channel of the endoscope. Once BILIARY STRICTURES
the stone is captured within the basket, forceful traction on the
wires against the metal sheath results in stone fragmentation. ERCP with stenting is a well-standardized technique com
The most common reasons for failure include large stones monly used to relieve biliary obstruction secondary to both
exceeding 2 cm in size and stone impaction. Basket impaction benign and malignant disease (see Chapters 42, 51, and 52).
within the duct or rupture of the traction wires has been The goal is to relieve the biliary obstruction that can potentially
reported in up to 4% of the cases, which may require external lead to complications, such as jaundice, pruritus, cholangitis,
salvage lithotriptor or surgical retrieval of the retained basket chronic liver disease, and liver failure.
and stone (Garg et al, 2004). Biliary stricture characterization can be a diagnostic chal
lenge that requires a multidisciplinary approach with the inte
Endoscopic Intraductal Lithotripsy gration of laboratory testing, noninvasive and invasive imaging,
Failure of mechanical lithotripsy may be secondary to the and tissue sampling methods. This section focuses on the tech
inability to ensnare the stone within the wires of the basket, nical aspects and outcomes associated with endoscopic man
which can be due to the presence of a stone occupying the agement of benign and malignant biliary strictures. Advances
entire diameter of the duct lumen. This effectively prohibits in endoscopic imaging and tissue sampling for the diagnosis of
adequate opening and manipulation of the basket. Further biliary strictures will be covered later in this chapter.
more, stones located above a stricture, or stones larger than the
biliary sphincterotomy and/or sphincteroplasty may not be Types of Biliary Stents
amenable to standard extraction if the bile duct exit path is Plastic Stents
narrower than the stone. In such instances, it is often necessary Plastic biliary stents are composed of polyethylene, polyure
to fragment the stones using alternative means. thane, or Teflon. Stent diameter and length range from 5 Fr to
Intraductal shock-wave lithotripsy under direct visualization 12 Fr and 5 to 18 cm, respectively (Pfau et al, 2013). Plastic
through a cholangioscope is an alternative modality for the stents are available in a variety of configurations: straight,
fragmentation of these refractory calculi. In electrohydraulic angled, curved, with flaps (flanged), or coiled at one or both
lithotripsy (EHL), the creation of a spark within fluid medium ends (single or double pigtail) for anchorage. All plastic stents
results in the generation of a propagating shock wave capable are radiopaque, some with additional markers at the proximal
of fragmenting intraductal stones. Laser lithotripsy (LL) is and distal end of the stents to facilitate visualization under fluo
based on the principle of transforming optical energy into roscopy. Insertion is via a push catheter over a guidewire.
mechanical energy. In LL, focusing the high-power density Duration of stent patency is largely dependent on the size of
laser light on the surface of the calculi results in the transforma the inner diameter, with 10-Fr and larger stents remaining
tion of matter into a plasma state, a gaseous collection of ions patent, on average, for approximately 3 months, and stent
and free electrons. Subsequently, the plasma expands, inducing occlusion developing secondary to bacterial colonization,
an oscillation wave with tensile/compressive forces directed at sludge, or tissue debris (Donelli et al, 2007).
the stone, leading to fragmentation (DiSario et al, 2007). Once
the stone is fragmented, then standard extraction techniques Self-Expandable Metal Stents
with balloons and baskets can be used. The effectiveness of Self-expandable metal stents (SEMSs) are composed of stain
EHL and LL for stone removal is similar, with clearance rates less steel or a variety of metal alloys, such as nitinol (nickel
ranging from 75% to 98% (Arya et al 2004; Swahn et al, 2010). and titanium combination) or platinol (platinum core with
Adverse events with EHL and LL have been reported in 3% to nitinol encasement). This material is malleable, which allows
14% of cases, with the most common being cholangitis and the SEMSs to adapt to many configurations without compro
bleeding, and rarely, bile duct injury. Prophylactic antibiotics mising radial expansile force. SEMSs are configured into a
are recommended for patients undergoing cholangioscopy cylinder by interwoven wires and are deployed from a con
given the increased risk of cholangitis/sepsis (Piraka et al, strained position within a delivery catheter. Stent diameter and
2007). length vary from 6 mm to 10 mm and 4 to 12 cm, respectively.
The larger stent diameter compared with plastic stents results
Extracorporeal Shock-Wave Lithotripsy in increased duration of stent patency (on average, 6 to 12
Extracorporeal shock-wave lithotripsy (ESWL) is an adjunctive months). SEMSs can be covered, partially covered, or uncov
safe and effective method of delivering shock waves. The tech ered. The covering consists of a silicone, polycaprolactone,
nique can be used for stone fragmentation under ultrasound or polyether polyurethane, polyurethane, or expanded polytetra
fluoroscopic guidance, after contrast is instilled via a nasobiliary fluoroethylene fluorinated ethylene propylene lining (Webb
catheter to aid in stone visualization (Tandan et al, 2009). et al, 2013). Covering reduces tumor or hyperplastic tissue
Multiple ESWL sessions are generally required. Adverse events, ingrowth but is associated with higher migration rate compared
including hemobilia, cholangitis, pancreatitis, and cardiac with uncovered metal stents (Lee et al, 2013). Partial or fully
arrhythmias, have been reported in 10% to 35% of cases covered SEMSs can typically be removed, whereas uncovered
(Muratori et al, 2010). The need for ESWL has decreased as stents are considered permanent.
the effectiveness of intraductal lithotripsy has improved, with
several randomized studies suggesting superior ductal clearance Endoscopic Management of Benign Biliary Strictures
and fewer treatment sessions with LL compared with ESWL Most cases of benign biliary strictures are secondary to post
(Jakobs et al, 1997; Nehaus et al, 1998). Thus ESWL is not operative iatrogenic injury, following cholecystectomy or at
routinely considered the first-line treatment of refractory bile the site of a biliary anastomosis after biliary surgery or liver
duct calculi. transplantation (Fig. 29.2A) (see Chapter 42). Benign biliary
Chapter 29 Interventional endoscopy: technical aspects 515
A B C
FIGURE 29.2. A, Cholangiogram showing a benign biliary anastomotic stricture (arrow) after orthotopic liver transplantation. Balloon dilation across
the stricture (B), followed by placement of three plastic biliary stents (C).
strictures may also result from ischemic injury and/or inflam Efficacy and Outcomes of Endoscopic Stenting of Benign
matory processes (Table 29.1). Comprehensive evaluation of a Biliary Strictures
biliary stricture and its etiology should always be sought prior Balloon dilation and plastic stenting has traditionally been the
to any therapeutic endoscopic intervention. Magnetic reso mainstay of endoscopic therapy for benign biliary strictures
nance cholangiopancreatography (MRCP) is a noninvasive (Van Boeckel et al, 2009). The long-term results of endoscopic
imaging modality that can accurately delineate the biliary therapy are dependent on the underlying etiology, with postop
anatomy, site, and length of the biliary stricture and thus erative benign biliary strictures (i.e., postcholecystectomy,
provide useful information for ERCP planning (Costamagna & biliary anastomotic strictures following liver transplantation)
Boskoski, 2013). more responsive to treatment compared with biliary strictures
associated with chronic pancreatitis. In postoperative benign
Endoscopic Technique biliary strictures, Bergman and colleagues (2001) reported
ERCP is performed following detailed assessment of the type restenosis rate of 20% after a median follow-up of 9.1 years in
and site of the biliary stricture. The key technical step is to patients who had two 10-Fr stents exchanged every 3 months
negotiate the stricture and achieve biliary access with the use for a total of 12 months. In a separate study of 45 patients with
of a guidewire. This process can be challenging, and the use of postoperative biliary strictures, Costamagna and colleagues
different sizes and types of hydrophilic guidewires in addition (2001) inserted the maximum number of plastic biliary stents
to guidewire manipulation with steerable catheters or sphinc possible (mean, 3.2; range, 1 to 6) per ERCP session, with stent
terotomes is often necessary. Although not required in all cases, exchange performed every 3 months (mean duration of treat
biliary sphincterotomy may need to be performed to facilitate ment, 12 months). This more aggressive biliary stent approach
subsequent therapy, including stricture dilation and stent was associated with no recurrence of symptoms due to biliary
placement. stricture at a mean follow-up of 49 months (range, 2 to 11
Stricture dilation can be performed using push-type dilation years). In contrast, long-term outcomes of endoscopic therapy
catheters (bougies) or hydrostatic balloons (range, 4 to 10 mm for bile duct strictures in the setting of chronic pancreatitis are
516 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
significantly less favorable, with one study reporting successful surgical resection, and in those with borderline resectable
endoscopic treatment in only 38% of the cases and persistence disease who may benefit from neoadjuvant chemotherapy. In
of strictures even when endoscopic stenting was performed patients with unknown resectability, placement of the shortest-
beyond a 12-month period (Cahen et al, 2005). length SEMS to bridge a distal stricture should not interfere
Fully-covered SEMSs (FCSEMSs) have been proposed as with subsequent pancreaticoduodenectomy if indicated (Cavell
an alternative to plastic stents for the management of benign et al, 2013). Conversely, if the biliary stricture is proximal and
biliary strictures (Kaffes et al, 2013). Multiple studies have definitive diagnosis and/or staging is not certain, plastic biliary
shown high success rates, with a large prospective multicenter stents can be placed for biliary decompression while workup is
study reporting an overall stricture resolution rate of 90% completed.
(Costamagna et al, 2001). However, similar to prior studies
with plastic stents, long-term stricture resolution rates with Palliative Biliary Drainage of Distal Bile Duct Obstruction
FCSEMs are significantly lower (46% to 75%) for patients with Distal malignant biliary obstructions are typically defined as
chronic pancreatitis (Poley et al, 2012; Tarantino I et al, 2012), those distal to the cystic duct insertion, although this definition
reiterating the refractory nature of this type of strictures to is suboptimal, given the substantial anatomic variability. Thera
endoscopic therapy. peutic options include surgical bypass, percutaneous decom
Overall, the clinical success rates between plastic stents and pression, and endoscopic stenting. A large meta-analysis of
FCSEMSs are comparable, albeit the latter have been associ 2436 patients demonstrated that endoscopic stenting was asso
ated with less endoscopic sessions for stricture resolution ciated with a lower risk of procedural complications than tra
(Kaffes et al, 2012). Further prospective, randomized studies ditional surgical bypass. Overall, SEMSs were not superior to
are needed to compare the long-term efficacy, safety, and cost- plastic stents in terms of technical success, therapeutic success,
effectiveness between metal and plastic stents for the manage or complications but were associated with improved patency
ment of benign biliary strictures. To date, the ideal number of rates (Moss et al, 2007). The shorter patency rate of plastic
stents, the type of stent, and the duration of stent placement stents has been associated with increased repeat endoscopic
for benign stricture resolution remain highly debated and often interventions to reestablish biliary drainage and more hospital
vary from case-by-case basis. ization days compared with SEMSs (Kaassis et al, 2003).
Several studies have not demonstrated differences in stent
Endoscopic Management of Malignant Biliary Strictures patency rates between covered and uncovered SEMSs for distal
Malignant biliary obstruction is most frequently seen in the malignant biliary obstruction, albeit a subsequent meta-analysis
setting of pancreaticobiliary malignancy, but it can also be due suggested possible prolonged patency with covered SEMSs but
to many other etiologies (see Table 29.1). When indicated, a trend toward increased stent migration and tumor overgrowth
endoscopic therapy is considered the mainstay therapy for (Park do H et al, 2006; Saleem et al, 2011; Yoon et al, 2006).
biliary decompression. A careful multidisciplinary review of the Ultimately, the optimal stent choice depends on various factors,
indication and appropriateness of any endoscopic intervention including establishment of diagnosis, need for reinterventions,
should be sought prior to any procedure. operator’s expertise, cost analysis, and the patient’s life
expectancy.
Preoperative Biliary Drainage
The routine need for preoperative biliary decompression in Palliative Biliary Drainage of Proximal Bile Duct
patients with resectable pancreaticobiliary disease remains con Obstruction (Hilar)
troversial. From a technical standpoint, the placement of a Malignant biliary obstructions at the biliary confluence can be
short plastic or metal biliary stent does not appear to interfere technically challenging (see Chapter 51). The extent of the
with subsequent pancreaticoduodenectomy. However, routine biliary obstruction is commonly classified based on the modi
preoperative biliary drainage may be associated with increased fied Bismuth-Corlette classification and can be summarized as
complications and not necessarily with improved postoperative follows: Bismuth type I strictures involve the proximal common
outcomes compared with patients who proceed directly to hepatic duct but not the confluence of the left and right ductal
surgery. In a multicenter randomized, controlled trial of 202 systems, type II involves the confluence but spares the segmen
patients with resectable pancreatic cancer, the rates of compli tal hepatic ducts, type IIIa and IIIb involve either the right or
cations were significantly higher in patients who underwent left segmental hepatic ducts, respectively, whereas both seg
preoperative biliary drainage (74%) compared with those who mental hepatic ducts are involved in type IV (Larghi et al,
underwent surgery alone within 1 week of diagnosis (39%) 2008). Biliary drainage with stent placement can be particularly
(Van der Gaag et al, 2010). Limitations of this study include a difficult in those with advanced complex strictures (Bismuth
25% ERCP failure rate and the use of plastic stents. In a sepa type II and above). Evaluation with noninvasive imaging (i.e.,
rate study, Aadam and colleagues (2012) reported SEMS MRCP) to delineate the anatomy is mandatory for preproce
patency rate of 88% in 55 patients who underwent neoadjuvant dural planning and helps limits contrast injection during the
therapy for a median time of 104 days. A multicenter study of ERCP and the risk of contaminating undrainable segments.
241 patients with resectable and borderline-resectable carci Furthermore, evaluation of the side of the liver (i.e., lack of
noma of the head of the pancreas demonstrated successful atrophy, patent portal vein branch, and lack of extensive seg
placement of SEMSs in all patients as they underwent neoad mental biliary involvement) that will provide the best biliary
juvant therapy with a stent occlusion rate of 5.8% at a mean drainage is critical. It is of utmost importance that the best
time of 6.6 months (Siddiqui et al, 2013). Thus, although approach (including percutaneous approaches) be evaluated in
routine endoscopic intervention prior to curative surgery may a multidisciplinary review.
not be necessary in all patients, there is evidence to suggest a In patients with strictures that do not involve the confluence
role for preoperative biliary drainage in the case of delayed of the right and left hepatic ducts (Bismuth type I), adequate
Chapter 29 Interventional endoscopy: technical aspects 517
A B C
FIGURE 29.3. A, Cholangiogram showing a type IIIb malignant hilar obstruction with upstream dilation of the right and left hepatic ducts. Balloon
dilation across the stricture (B) and placement of bilateral uncovered metal biliary stents to drain both lobes of the liver (C).
biliary drainage is often achieved by the placement of a single obstruct drainage of adjacent ducts. For stent implantation, a
biliary stent. Controversy exists as to whether both lobes of the guidewire is advanced across the malignant stricture into the
liver need to be drained when a bifurcation lesion obstructs duct preselected for drainage (Fig. 29.3A). After wire place
both lobes. The main determining factor associated with effec ment, if necessary, dilation of a tight stricture can be performed
tive drainage is the liver volume to be drained. In principle, with a balloon catheter or bougie (Fig. 29.3B). A sphincterot
jaundice can often be relieved when approximately 25% to 30% omy is not necessary when the distal ends of the stents are
of the liver is adequately drained (Dowsett et al, 1989). In a positioned within the duct, which may reduce the risk of post
more recent study, the volume of liver drained (>50%) as stenting cholangitis. On the other hand, stent revision is techni
assessed by computed tomography (CT) imaging was the main cally less demanding and more accessible when the distal end
predictive factor of effective drainage following endoscopic of the stents protrude out of the papilla (Fig. 29.3C). Regard
stenting for malignant hilar biliary strictures. Indeed, drainage less of stent positioning, all patients who undergo endoscopic
of greater than 50% was also associated with a longer median therapy for these complex strictures should receive prophylactic
survival (Vienne et al, 2010). Thus the goal of endoscopic antibiotics.
therapy should be directed at achieving drainage volume greater In summary, endoscopic stenting of proximal biliary obstruc
than 50%, irrespective of whether unilateral or multisegmental tion is challenging. Preprocedural cross-sectional imaging and
stenting is performed. multidisciplinary review is essential in the selection of the target
Several studies have suggested that unilateral stent place parenchyma for drainage and the optimal approach (percutane
ment and drainage is adequate in most patients with nonresect ous vs. endoscopic). If endoscopic approaches are favored, this
able malignant hilar lesions. From a technical standpoint, planning will in turn help maximize biliary drainage by target
unilateral stents have been shown to be associated with a higher ing the dominant biliary systems, limit the use of contrast
rate of successful endoscopic placement and lower rate of com during the procedure, and avoid intubating atrophic segments
plications compared with bilateral stents (De Palma et al, 2001; or areas that cannot be effectively drained.
Mukai et al, 2013). Iwano and colleagues (2011) reported that
unilateral drainage was associated with lower incidence of liver Photodynamic Therapy
abscess compared with bilateral drainage. Nonetheless, endo Photodynamic therapy (PDT) is based on the ability of photo
scopic insertion of multiple stents may be required when effec sensitizers to generate cytotoxic oxygen species in the target
tive drainage of greater than 50% of the liver volume involves tissue upon exposure to light of an appropriate wavelength.
several hepatic segments or to ensure drainage of all opacified Photosensitizing agents (sodium porfimer or aminolaevulinic
ducts. Chang and colleagues (1998) reported a higher survival acid) are injected intravenously preprocedurally, and ERCP is
rate in patients with bilateral drainage compared with those subsequently performed 2 to 4 days thereafter. A catheter with
with persistent duct opacification following unilateral drainage. a quartz fiber coupled with a diode laser emitting a wavelength
Despite the increased technical difficulty and higher costs, of 630 nm is inserted into the bile duct through the accessory
several recent studies have also reported higher stent patency channel of the endoscope. The catheter is directed against the
and decreased reintervention for stent occlusion with bilateral photosensitized malignant cells, causing tumor cell death by the
compared with unilateral stent placement (Liberato & Canena, generation of oxygen free radicals.
2012; Naitoh et al, 2009). In a randomized controlled trial, Ortner and colleagues
Several studies have suggested that SEMSs are preferable to (2003) compared PDT with stenting versus stenting alone in
plastic stents based on higher rates of successful drainage, pro patients with nonresectable cholangiocarcinoma. The authors
longed patency, prolonged survival, and lower rates of compli demonstrated that PDT resulted in prolongation of survival
cations (Naitoh et al, 2009; Vienne et al, 2010). The use of (493 days with PDT plus stenting compared with 98 days in
uncovered SEMSs is preferred for proximal malignant biliary stent-alone group) and improved biliary drainage and quality of
strictures as placement of a covered stent can potentially life. Subsequent nonrandomized studies have also demonstrated
518 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
A B
FIGURE 29.4. A, Cholangiogram showing contrast extravasation (arrow) at the biliary anastomosis in a patient after liver transplantation, consistent
with bile leak. B, Bile leak treated by placing a plastic stent across the biliary anastomosis.
reduction in serum bilirubin and increased survival with PDT intraductal filling has occurred (Fig. 29.4A). The aim of endo
(Kahaleh et al, 2008; Prasad et al, 2007). Main limitations of scopic therapy is to decrease the transpapillary pressure gradi
PDT include limited availability, high costs, risk of infection ent, thus favoring transpapillary bile flow rather than
(i.e., cholangitis, liver abscess), and risk of photosensitivity extravasation at the site of the leak (Sandha et al, 2004). This
reaction. can be achieved by performing a biliary sphincterotomy, place
ment of a transpapillary biliary stent, or both. In most instances,
Radiofrequency Ablation placement of a plastic biliary stent (7 Fr or 10 Fr) is sufficient
Radiofrequency ablation (RFA) relies on the generation of without the need of a sphincterotomy and its potential associ
high-frequency alternating electromagnetic energy resulting in ated risks (Katsinelos et al, 2008) (Fig. 29.4B). It is not neces
thermal injury to the target tissue (see Chapter 98B). Intra sary to place the proximal end of the stent beyond the site of
ductal RFA for malignant strictures has become feasible with the leak as reduction of the pressure inside the duct alone
the introduction of a novel RFA probe. The Habib Endo HBP is generally sufficient. Typically, the stent is left in place for
probe (EMcision, London, England) is a bipolar 8-Fr catheter approximately 4 to 6 weeks. Various studies have reported
with two stainless steel electrodes, 8 mm apart, located at the endoscopic success rates for the management of bile leaks
distal tip. The probe can be inserted into the working channel between 90% to 100% (Kaffes et al, 2005; Kim et al, 2014;
of the duodenoscope and advanced into the bile duct over a Ryan et al, 1998). In the minority of cases in which the bile
guidewire. The probe is subsequently activated at 10 W of leak is refractory to endoscopic therapy with plastic stent place
energy for 90 seconds at a time, resulting in local coagulation ment and/or sphincterotomy, upsizing the stent or placing mul
necrosis (Webb & Saunders, 2013). tiple plastic stents can be performed in subsequent sessions
Recent studies have confirmed the safety and efficacy of until resolution is documented. A small pilot study suggested
RFA as an adjunct to SEMSs in patients with a malignant a potential role for FCSEMSs in patients with bile leak refrac
biliary stricture. Figueroa-Barojas and colleagues (2013) dem tory to plastic stent placement; however, these preliminary find
onstrated improvement in stricture diameter following RFA as ings have not been corroborated by larger, multicenter studies
well as 30-day stent patency. The same group subsequently (Kahaleh et al, 2007).
compared metal stenting with RFA versus stenting alone. In It should be noted that, in the presence of a perihepatic bile
their retrospective study, RFA was an independent predictor of collection, endoscopic stenting alone does not result in the
survival, with comparable stent patency rates between both reabsorption of the established biloma. Thus symptomatic
groups (Sharaiha et al, 2014). Further studies including ran bilomas will need to be drained percutaneously (see Chapters
domized controlled trials over a longer period are needed to 27 and 30). An output of less than 10 mL per day through a
validate these preliminary findings. percutaneous drain is associated with bile leak resolution and
can be used as a surrogate indicator for stent removal.
TECHNIQUES FOR THE MANAGEMENT
OF BILE LEAK ENDOSCOPIC MANAGEMENT OF
AMPULLARY ADENOMAS
Bile leak is a well-known complication from injury to the biliary
tree, either secondary to trauma (see Chapter 122) or iatro Ampullary adenomas are dysplastic glandular lesions that arise
genic following laparoscopic cholecystectomy (see Chapters 35 from either the major or minor duodenal papilla. These lesions
and 38), liver resection (see Chapter 103), or transplantation can occur sporadically or arise in the context of genetic syn
(see Chapter 120). Bile leaks can be classified as either high dromes, such as familial adenomatous polyposis. If not removed,
grade or low grade. High-grade leaks demonstrate rapid extrav ampullary adenomas can undergo malignant transformation to
asation of contrast during cholangiogram, whereas low-grade ampullary cancer, with a reported incidence from 25% to 85%
leaks exhibit contrast extravasation only after near-complete (Hirota et al, 2006; Seifert et al, 1991; Takashima et al, 2000).
Chapter 29 Interventional endoscopy: technical aspects 519
With advances in therapeutic endoscopy, endoscopic ampul lesion is generally tethered down by the bile and pancreatic
lectomy has become an acceptable alternative therapy to surgery duct. Thus submucosal injection may actually raise the sur
for ampullary adenomas (see Chapter 59). rounding mucosa, create a depressed center (“valley effect”),
and interfere with en bloc excision and subsequent attempts at
Diagnosis and Local Staging bile and pancreatic duct access (Harewood et al, 2005; Irani
Prior to endoscopic ampullectomy, preoperative assessment et al, 2009).
with both a forward- and side-viewing endoscope is routinely For most ampullary lesions, the tip of the snare is positioned
performed to further characterize the lesion. Endoscopic find against the wall of the duodenum at the superior aspect of
ings, including spontaneous bleeding, friability, ulceration, the mass. The snare is then slowly opened and the snare cath
and induration, are often associated with malignant lesions. eter advanced slowly to allow the open snare to encircle the
Biopsies obtained during endoscopy can assess for dysplasia or lesion. Once achieved, the snare is slowly closed while simul
unsuspected carcinoma, although malignancy may be missed taneously advancing the snare catheter toward the base of
in up to 30% of tumors when forceps biopsy specimens are the lesion, followed by polypectomy. Thermal therapy (i.e.,
obtained (Elek et al, 2003). Hence other advanced imaging argon plasma coagulation, monopolar and bipolar coagulation,
modalities, including magnifying endoscopy and narrow-band neodymium:yttrium-aluminum-garnet laser) can be used to
imaging, have been proposed as complementary techniques to fulgurate any residual tissue following piecemeal or incomplete
help predict histologic characteristics of ampullary lesions resection, with caution to avoid excessive tissue destruction
(Uchiyama et al, 2006). around the biliary and pancreatic duct orifices.
EUS has been shown to be superior to CT, angiography, Numerous studies have demonstrated decreased com
and magnetic resonance imaging for local tumor staging, plications with ampullectomy when prophylactic pancreatic
including assessment of the size of lesion and involvement/ stenting is performed (Martin et al, 2003; Yamao et al, 2010).
infiltration of the periampullary wall layers, the CBD, and the Indeed, placement of a prophylactic pancreatic stent is strongly
pancreatic duct (Chen et al, 2009; Manta et al, 2010) (see recommended as it decreases the risk of post-ERCP pancreati
Chapter 16). Many experts agree that smaller lesions (<1 cm) tis following ampullectomy (Harewood et al, 2005; Singh
without suspicious signs of malignancy (ulceration, spontane et al, 2004). Whether ERCP with pancreatic and biliary
ous bleeding, biopsies positive for high-grade dysplasia or car sphincterotomy/stent placement is performed pre-resection or
cinoma) may not require EUS evaluation prior to endoscopic postresection is often dependent upon the endoscopist’s prefer
resection (Baillie, 2005). When performed, EUS can help strat ence (Fig. 29.5C). Because identification of the pancreatic
ify which lesions are amenable to endoscopic ampullectomy. orifice following ampullectomy can be challenging, some
ERCP and intraductal ultrasound (IDUS) can also aid in the authors favor performing pancreatography with iodinated con
detection of tumor extension into either ductal system (De trast diluted with methylene blue or indigo carmine prior to
Palma et al, 2014). resection. The blue-stained pancreatic orifice can theoretically
be more readily identified adjacent to the bile-stained biliary
Endoscopic Therapy orifice and thus facilitate postresection cannulation (El Hajj
Endoscopic ampullectomy (papillectomy) can be considered et al, 2013). Prophylactic biliary sphincterotomy and/or stent
once malignancy has been reasonably excluded. This procedure ing is not widely performed nor uniformly recommended unless
is performed with the standard monopolar diathermic snare there is concern for inadequate biliary drainage following
used for colon polypectomy. The aim of endoscopic excision is ampullectomy (Adler et al, 2006).
to obtain complete removal of the ampullary lesion, preferably Patients who have undergone endoscopic ampullectomy
en bloc (Fig. 29.5A and B). When performing this technique, should undergo routine surveillance. A systematic review esti
it is common for the intraampullary portions of the CBD and mated recurrence rates of 0% to 33% with larger size and
pancreatic duct to be removed as well. Submucosal injection is intraductal extension as recognized risk factors (Han et al,
not routinely recommended, as the center of the ampullary 2006). Endoscopic surveillance should be performed with a
A B C
FIGURE 29.5. Endoscopic ampullectomy. A, Ampullary adenoma. Ampullectomy with en bloc resection (B), followed by biliary and pancreatic
duct stenting (C).
520 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
side-viewing duodenoscope; the timing interval is dependent In addition to the potential risks associated with conven
on several factors, including histology and margin status of tional ERCP, Bilroth II anatomy increases the risk of adverse
resected specimen, history of familial adenomatous polyposis, events, including perforations at the gastrojejunal anastomosis
and the patient’s age and comorbidities. Furthermore, any or within the afferent limb itself (Faylona et al, 1999; Kato
specimen with unexpected malignancy should be referred for et al, 2014). Thus the endoscopist should be familiar with
surgical consultation. multiple techniques and be prepared to change strategies on a
case-by-case basis depending on the intraprocedural findings.
limbs that must be traversed. Hence alternative access routes the duodenum (Gupta et al, 2014). Bile is aspirated, and con
through the remnant stomach directly to the native papilla trast is injected to confirm position inside the bile system. A
have been explored. Previous studies have reported successful hydrophilic guidewire is then advanced antegrade through the
ERCP through a surgical or percutaneous gastrostomy, with EUS needle and into the bile duct and manipulated across the
the main limitation being the need for a 2-week period for tract papilla. The echoendoscope and needle are carefully removed
maturation, and thus this technique is not applicable in cases while maintaining the guidewire in place. The duodenoscope
requiring urgent ERCP (Gutierrez et al, 2009; Tekola et al, is then inserted and advanced to the duodenum with visualiza
2011). Conversely, to obviate the need for a two-step process, tion of the wire traversing the papilla. The distal end of the
laparoscopy has been used to create a point of access to the indwelling guidewire can be grasped with forceps or snare,
remnant stomach, allowing immediate ERCP by inserting the withdrawn through the accessory channel, and a cannulation
duodenoscope through the trocar. In a retrospective study com catheter back-loaded over the guidewire and readvanced to the
paring laparoscopic-assisted ERCP (LA-ERCP) to balloon- papilla. Alternatively, biliary cannulation can be accomplished
enteroscopy–assisted ERCP (BEA-ERCP), LA-ERCP was in the standard retrograde fashion adjacent to the indwelling
significantly superior to BEA-ERCP in both cannulation rate wire. Overall success and complication rates of the EUS-guided
and therapeutic success (100% vs. 59%, P < .001) (Schreiner rendezvous technique are 81% and 10%, respectively (Iwashita
et al, 2012). More recently, a technique using percutaneous- et al, 2014).
assisted transprosthetic endoscopic therapy has been described
(Law et al, 2013). In this technique, an enteroscope is advanced Endoscopic Ultrasound—Guided Antegrade Biliary Drainage
transorally into the excluded stomach, followed by the creation Antegrade placement of a biliary stent can be accomplished in
of a percutaneous endoscopic gastrostomy. The gastrostomy cases when ERCP cannot be performed due to luminal obstruc
tract is then dilated to allow the placement of a FCSEMS. A tion proximal to the papilla or in cases where the papilla cannot
duodenoscope can then be advanced through the stent to be reached (i.e., RYGB). After obtaining biliary access under
perform antegrade ERCP. Other techniques using EUS to gain EUS guidance, the transmural tract is dilated with either a
gastrostomy access have also been reported. Following identi balloon catheter or bougie to allow advancement of the stent
fication of the excluded stomach under EUS, access can be into the bile system with subsequent deployment across the
obtained by using a lumen-apposing metal stent to create a obstruction. In aggregate, success and complication rates
gastrogastric fistula through which a duodenoscope is inserted reported from small case series are 77% and 5%, respectively
to perform ERCP at the same session (Kedia et al 2014). The (Iwashita et al, 2014).
main concerns with this technique include risk of weight regain
with a patent gastrogastric fistula and stent migration. Further Endoscopic Ultrasound—Guided Transluminal
larger prospective studies are needed before these innovative Biliary Drainage
techniques can be endorsed. EUS-guided transluminal drainage can be considered after
In summary, selection of the appropriate technique for failed ERCP (i.e., luminal obstruction, surgically altered
biliary access in patients with surgically altered anatomy should anatomy, unsuccessful biliary cannulation) and as an alternative
be individualized and would likely involve a combination of to percutaneous transhepatic biliary drainage or surgery. A
methods and endoscopic tools based on patient factors and EUS-guided transluminal approach also permits biliary decom
operator’s expertise. pression in cases when EUS-guided antegrade biliary access is
not feasible because the wire cannot be advanced across the
Endoscopic Ultrasound—Guided Biliary Drainage papilla (i.e., impacted biliary calculi, papillary stenosis, and
ERCP success rates for biliary and pancreatic duct decompres tumor infiltration). Biliary access can be obtained either via an
sion are reported to be around 90% to 95% of the cases in the intrahepatic (hepaticogastrostomy) or extrahepatic choledocho
hands of experienced endoscopists (Kedia et al, 2013). Follow duodenostomy) approach, with studies demonstrating similar
ing initial failed ERCP, the recommended next step is to reat success rates (91% to 96%) between both routes (Artifon et al,
tempt the ERCP. If repeat ERCP is unsuccessful, alternative 2015) (Fig. 29.6A). With either approach, bile duct access is
methods of biliary decompression have traditionally included obtained under EUS and fluoroscopic guidance, followed by
percutaneous transhepatic drainage or surgery. With the dilation of the fistula and stent placement (Fig. 29.6B and D).
advancement of curvilinear-array echoendoscopes and periph The use of both plastic (straight or pigtail) and SEMSs have
eral devices, EUS-guided biliary drainage has become increas been reported, with overall success rates ranging from 72% to
ingly reported (Kahaleh et al, 2006). 100% (Tarantino et al, 2012). There are no comparative studies
between plastic and SEMSs, and the optimal stent has not been
Endoscopic Ultrasound Rendezvous Technique clearly established. In general, plastic stents are less expensive
EUS-guided wire placement into the bile duct in an antegrade but have a shorter patency rate compared with SEMSs. Among
fashion has been used to facilitate subsequent retrograde biliary the types of SEMSs, uncovered SEMSs may have a lower risk
cannulation when standard ERCP has failed. The point of of displacement compared with the partially or fully covered
biliary duct entry (intrahepatic vs. extrahepatic) depends on SEMSs but may be associated with a higher risk of bile leak and
accessibility and which route facilitates wire manipulation. peritonitis if they become displaced (Itoi et al, 2011). More
Whether it is through an intrahepatic or extrahepatic approach, recently, there have been reports on EUS-guided choledocho
a therapeutic linear echoendoscope is used to visualize the bile duodenostomy with a novel lumen-apposing fully covered metal
duct from the stomach or small intestine. Once an avascular stent (AXIOS stent; Xlumena, Mountain View, CA) for malig
plane has been identified using Doppler ultrasonography, a nant biliary obstruction (Glessing et al, 2015; Itoi et al, 2013).
EUS needle is advanced into the bile duct. Effort should be This novel fully covered, wide-lumen, low-profile stent allows
placed in directing the needle angle caudally in the direction of close apposition of the walls of the gastrointestinal lumen and
522 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
A B
C D
FIGURE 29.6. Endoscopic ultrasound (EUS)-guided biliary drainage. A, Cholangiogram showing complete distal bile duct obstruction with
diffuse upstream dilation. B, The common bile duct is accessed by using an EUS needle. C, A guidewire is left across the choledochoduodenostomy.
D, After dilating the tract, a stent is successfully deployed.
bile duct, theoretically minimizing the risk of migration or yield (Barkun et al, 2006). Once completed, the brush is
leakage. Further studies are needed to evaluate outcomes associ resheathed and the catheter withdrawn.
ated with these stents and their role in EUS-guided biliary The diagnostic yield of brush cytology for biliary strictures
drainage. is low, with most studies reporting poor sensitivity of 27% to
56% (Victor et al, 2012). Neither longer cytology brush designs
ENDOSCOPIC BILIARY TISSUE ACQUISITION nor prebrushing stricture dilation have conclusively shown
AND ADVANCED IMAGING TECHNIQUES improvement in sensitivity (de Bellis et al, 2003; Fogel et al,
2006). The poor sensitivity of brush cytology has often been
The role of ERCP as a diagnostic tool has diminished with the attributed to sampling error and low cellular yield due to
advent of multiple noninvasive imaging tests of the biliary the scirrous nature of cholangiocarcinoma, and due to the fact
system, including high-resolution CT and MRCP. One notable that pancreatic adenocarcinomas frequently cause only extrin
exception to this trend is the need for ERCP with tissue sam sic compression of the distal bile duct, rather than frank
pling in suspected malignant biliary obstruction. invasion.
detection of malignancy (de Bellis et al, 2003), a recent meta- increased the sensitivity from 47% to 84% without a change in
analysis indicates that both brushings and biopsy are compa specificity.
rable (pooled sensitivity of 45% and 48%, respectively) Overall, ERCP with brush cytology and/or intraductal biop
(Navaneethan et al, 2015). ERCP with combined tissue pro sies should be performed in the initial evaluation of indetermi
curement with brush cytology and intraductal biopsies have nate biliary strictures. Advanced cytologic methods, such as
demonstrated a mild improvement, with sensitivity ranging DIA and FISH, can potentially improve sensitivity, especially
from 60% to 75% (Kitajima et al, 2007; Rösch et al, 2004) (see in the setting of negative cytology and histology. It should be
Chapter 30). stressed that a multidisciplinary review of the indication for
intrabiliary tissue sampling is of critical importance. Some stric
Molecular Analysis of Tissue Samples tures do not require biopsy if surgery is indicated on clinical
Chromosomal abnormalities are typically seen in malignant and radiologic grounds, and other biopsy approaches may be
biliary strictures (see Chapter 9C). Flow cytometry has been more appropriate.
commonly used to identify aneuploidy in tissue specimens.
Several studies have shown that flow cytometry for DNA Advanced Endoscopic Biliary Imaging
evaluation yields improved sensitivity (42%) but at the expense Peroral Cholangioscopy
of lower specificity of 70% to 77% (Ryan et al, 1994) for Peroral cholangioscopy is a technique that permits direct endo
the diagnosis of malignant biliary strictures. Furthermore, scopic visualization of the bile ducts by using miniature endo
flow cytometric analysis requires large cellular samples, which scopes and catheters inserted through the accessory port of a
can be challenging with current endoscopic tissue sampling duodenoscope. In the endoscope-based (“mother-daughter”)
techniques. system, a small, thin endoscope (daughter) is inserted through
New ancillary cytologic techniques, including digital image the accessory channel of the duodenoscope (mother). The main
analysis (DIA) and fluorescent in-situ hybridization (FISH) limitation of this system is the requirement of two separate
have been introduced to increase the diagnostic yield of routine endoscopists to operate each scope during the procedure.
cytology. DIA uses a computer assessment to quantify DNA Conversely, the catheter-based system requires only a single
content, chromatin distribution, and nuclear morphology to endoscopist. In this system, an independent instrument with a
assess for aneuploidy. In a single-center prospective study, DIA four-lumen catheter and an operator interface that allows four-
had a higher sensitivity (39%) compared with routine cytology way tip deflection is attached at the shaft of the duodenoscope.
(18%), albeit with a significantly lower specificity (77% vs. A 0.77-mm fiber optic probe can then be inserted through the
98%, respectively) (Baron et al, 2004). FISH is a cytogenetic flexible 10-Fr catheter, which is then advanced into the biliary
technique that uses fluorescent probes that selectively bind to tract through the accessory channel of the duodenoscope. A
specific portions of selected chromosomes, allowing assessment biliary sphincterotomy is often required to allow passage of the
of polysomy via fluoroscopic microscopy. A potential advantage catheter into the duct. In addition to the channel for the optical
of FISH is that it requires fewer cells for analysis compared probe, the catheter includes a 1.2-mm accessory channel and
with routine cytology or flow cytometry. Although the addition two 0.6-mm irrigation channels (Chen et al, 2007).
of FISH has been shown to improve sensitivity (14% to 24%) Peroral cholangioscopy has been primarily used for the man
when cytology is negative for malignancy, and abnormal FISH agement of refractory choledocholithiasis (discussed earlier
results are more likely in the presence of carcinoma, the overall in this chapter) and for the evaluation of indeterminate biliary
accuracy rates are still suboptimal (Fritcher et al, 2009; Levy strictures. Cholangioscopy allows direct visualization and
et al, 2008). More recently, Gonda and colleagues (2012) dem inspection of mucosal abnormalities of the biliary epithelium
onstrated that including the deletion of the 9p21 locus (p16) (Fig. 29.7). Findings of irregularly tortuous and dilated blood
in the diagnostic criteria of FISH for malignant biliary strictures vessels, intraductal lesions, ulcerations, or papillary mucosal
A B C
FIGURE 29.7. Evaluation of a dominant common bile duct stricture (CBD) in primary sclerosing cholangitis (PSC). A, Magnetic resonance
cholangiopancreatography revealing a long-segment distal CBD stricture (arrow) with upstream biliary dilation. B, Cholangiogram showing long CBD
stricture, upstream extrahepatic dilation, and intrahepatic ducts with beading consistent with PSC. C, Direct visualization of the bile duct with peroral
cholangioscopy reveals a smooth, scarred stricture.
524 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
projections on cholangioscopy are highly associated with under et al, 2001). Conversely, the restricted depth of penetration
lying malignancy (Kim et al, 2000). In a prospective multi with IDUS and the inability to perform fine needle aspiration
center study, cholangioscopy was able to distinguish malignant significantly limits its utility for assessing advanced tumor
from benign biliary lesions in 92% of cases by visualization extension and nodal and metastatic staging.
alone (Osanai et al, 2013). Furthermore, direct visualization IDUS is a promising advanced endoscopic imaging modality
during cholangioscopy also permits selective targeted tissue that permits high-resolution images of the bile system. This
sampling, with studies showing adequate biopsies in 72% to advantage is hindered by the limited depth of penetration
97% of cases (Chen et al, 2011; Draganov et al, 2011) and and ability to examine more distal sites. Further studies are
an accuracy for malignant lesions as high as 87% (Kalaitzakis needed to validate its place as an adjunct imaging tool to ERCP
et al, 2012). Peroral cholangioscopy has also been used for the and EUS.
diagnosis of malignancy in primary sclerosing cholangitis
(Tischendorf et al, 2006) and evaluation of biliary complica Confocal Laser Endomicroscopy
tions following liver transplantation (Balderramo et al, 2013). Confocal endomicroscopy (CLE) allows real-time high-
Overall, cholangioscopy represents an evolving novel technol resolution evaluation of gastrointestinal mucosal histology in
ogy for the evaluation of undifferentiated biliary strictures, vivo. Imaging is achieved by the projection of a low-power laser
exclusion of occult malignancy, and management of biliary light passed through a confocal aperture. The focused beam
stones. The introduction of a new high-definition cholangio targeted on a specific layer of tissue is then captured by a pho
scope may potentially facilitate improved bile duct examination todetection device and transformed into electrical signals pro
and define its adjunctive role to conventional ERCP within the cessed into grayscale images (Nakai et al, 2014). Because CLE
spectrum of biliary diseases (Parsi et al, 2014). relies upon tissue fluorescence, intravenous fluorescein dye (5
to 10 mL of 10% fluorescein) is administered to highlight tissue
Endoscopic Intraductal Ultrasound structures (individual cell structures, vasculature) prior to
The evolution of EUS has led to the development of small- imaging. The lack of contrast uptake by neoplastic tissue results
caliber ultrasound probes (2.9 mm or less in diameter) for in a contrasted dark appearance compared with adjacent normal
biliary endosonography. These IDUS miniprobes are intro structures.
duced through the accessory channel of the duodenoscope over There are two currently available CLE systems: endoscope-
a guidewire and advanced into the bile duct. IDUS operates at based CLE and probe-based CLE (pCLE). The former is too
higher frequencies (12 to 30 Mhz), with penetration of 2 cm large, as the CLE is integrated in the tip of the endoscope, and
at higher image resolution (0.07 to 0.18 mm) compared with thus biliary examination is generally performed with CLE
standard EUS (Gabbert et al, 2013). The bile duct appears as probes that can be inserted through the accessory channel of
three layers on IDUS. The innermost hyperechoic layer cor the duodenoscope. The laser (488 nm, blue light) is transmit
responds to the mucosa and bile interface. The middle ted through thousands of optimal fibers within the probe
hypoechoic layer corresponds to the discontinuous fibromus (cholangioflex-probe is 9 mm in diameter), and subsequent
cular layer, whereas the outermost hyperechoic layer represents confocal image data are collected at a frame rate of 12 frames/
the subserosal fat plane (Tantau et al, 2008). second with a limited field of vision of 325 µm. pCLE can be
IDUS has been used for the evaluation of suspected cho challenging, as optimal imaging requires significant probe and
ledocholithiasis. Several studies have reported increased patient stability.
sensitivity of IDUS (97% to 100%) over both ERCP and trans The indications for pCLE in biliary disease have not been
abdominal ultrasonography (81% and 45%) for the detection established, but studies have suggested a potential role in the
of bile duct stones in patients with normal cholangiography evaluation of biliary strictures suspicious for malignancy. In a
(Das et al, 2001; Ueno et al, 1997). However, with the high large prospective multicenter study of pCLE during ERCP for
diagnostic accuracy of EUS (sensitivity of 89% and specificity pancreatobiliary strictures, pCLE was associated with an accu
of 94%) for detecting choledocholithiasis in patients with sus racy rate of 81%, sensitivity of 98%, and specificity of 67% in
pected choledocholithiasis, the role of IDUS in the diagnostic the detection of malignancy. pCLE increased accuracy to 90%
algorithm of biliary stone disease remains to be determined compared with 73% by ERCP with tissue sampling alone
(Garrow et al, 2007; Petrov et al, 2009). (Meining et al, 2011). Despite these promising preliminary
Several studies have reported IDUS findings concerning for results, subsequent studies have suggested a wide discrepancy
biliary malignancy. These criteria include the presence of a in the interpretation of pCLE findings between endoscopists
hypoechoic mass, disruption of the normal bile duct structure, for both benign and malignant pancreaticobiliary lesions
abnormal stricture borders (asymmetry, notching), or the pres (Bakhru et al, 2013; Talreja et al, 2014). The inconsistent
ence of suspicious lymph nodes (>1 cm, hypoechoic, round interpretation among practitioners emphasizes the need for
with smooth borders). In a prospective study, ERCP/IDUS was both formal structured training in pCLE (Dunbar et al, 2007)
associated with a correct diagnosis for malignancy in 88% and validation of the currently established diagnostic criteria
patients compared with 76% with ERCP alone (Domagk et al, (Meining et al, 2012).
2004). Furthermore, IDUS has been shown to improve local
tumor staging for cholangiocarcinomas in various studies, even References are available at expertconsult.com.
compared with standard EUS (Menzel et al, 1999; Tamada,
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1997.
CHAPTER 30
Radiologic hepatobiliary interventions
Karen T. Brown and Anne M. Covey
RADIOLOGIC HEPATOBILIARY INTERVENTIONS In patients with hepatic encephalopathy and portal hyper-
tension, or patients with “left-sided portal hypertension”
Minimally invasive hepatic intervention is indicated in a wide (gastric varices due to splenic vein occlusion), balloon-occluded
range of pathologic conditions and can be generally divided into retrograde transvenous obliteration (BRTO) or balloon-
vascular, biliary, and hepatic parenchymal procedures. The occluded antegrade transvenous obliteration (BATO) may be
objective of this chapter is to provide a broad overview of the preferable to TIPSS. BRTO and BATO refer to procedures in
spectrum of interventions that can be performed in a percuta- which a high-risk or bleeding gastric varix is catheterized
neous fashion by using imaging guidance. Greater detail will be and sclerosed typically with a mixture of Ethiodol, Sotradechol,
found in individual chapters devoted to each topic. and air agitated through a three-way stopcock (Saad et al,
2012).
Vascular Procedures In some cases, portal vein narrowing or occlusion due to
The liver is an extremely vascular organ with nutrient supply extrinsic compression by tumor may cause symptoms similar
from both the portal vein and hepatic artery and drainage via to those seen in cirrhotic portal hypertension. In such cases,
the hepatic veins. These vessels are common targets for the placement of a self-expanding stent can relieve varices and
interventional radiologist. ascites. This is most commonly seen in patients with locally
advanced pancreaticobiliary cancer where portal vein stenting
Portal Vein may also improve thrombocytopenia, broadening chemother-
The majority of the nutrient blood flow to the liver is via the apy options (Fig. 30.1).
portal vein, which drains the splanchnic circulation and spleen. Another procedure that has become relatively common is
The most common abnormality involving the portal vein is portal vein embolization (PVE), as an adjunctive procedure
portal hypertension, typically as a sequela of cirrhosis (see prior to hepatic resection. In patients with a suboptimal future
Chapters 76, 81, 83, and 87). Clinical manifestations of portal liver remnant (FLR) volume, which can be assessed volumetri-
hypertension include splenomegaly, thrombocytopenia, varices, cally (i.e., with computed tomography [CT] or magnetic reso-
ascites, and liver failure. In 1969, Rosch and colleagues reported nance imaging [MRI]) or functionally (e.g., indocyanine green
the first case of transjugular intrahepatic portosystemic shunt clearance), contralateral PVE can be performed to induce pre-
(TIPSS) in dogs. Thirteen year later, Colapinto and colleagues operative hypertrophy of the FLR (May et al, 2013) (see
(1982) reported the first human application of TIPSS. In this Chapter 108C). In patients with cirrhosis, most surgeons
procedure, a path is created from the hepatic vein to the portal believe that a FLR of greater than 40% of the total liver volume
vein through the liver parenchyma, thereby decreasing portal (TLV) is optimal. In patients without underlying liver disease,
pressure and relieving patients from intractable ascites or acute a FLR of greater than 25% may be acceptable. Other risk
variceal bleeding. Initially the tract was formed with serial dila- factors for impaired liver function include diabetes, prior che-
tors or balloon dilation with limited success. When the Palmaz motherapy, and steatosis, and so the desired volume of the FLR
metallic balloon expandable stents became available in the mid- is estimated on a case-by-case basis.
1980s (Palmaz et al, 1986), procedural success improved, and PVE to improve the safety of hepatic resection was first
the technique gained widespread acceptance. Further refine- proposed by Makuuchi and colleagues in 1989. Initially, this
ment to the use of covered self-expanding stents has improved procedure was performed via a transileocolic approach that
long-term patency, making this a viable option for not only required laparotomy and general anesthesia. Although ligation
patients with life-threatening hemorrhage but also as a means of a portal vein branch can be carried out during a laparotomy,
to control intractable ascites (Boyer & Haskal, 2005; Saad, today this procedure is most commonly performed percutane-
2014). ously, typically as an outpatient. Access to the ipsilateral portal
The most significant complication of TIPSS is hepatic vein is made with a 21-gauge needle, and typical angiographic
encephalopathy due to the volume of blood shunted past the catheters are used to perform venography and embolization. A
liver parenchyma. As a result, the presence of hepatic encepha- wide range of agents have been used to perform the procedure,
lopathy is a relative contraindication to the procedure. Other including ethanol, Gelfoam, thrombin, polyvinyl alcohol, glue,
contraindications include right heart failure, hepatic vein occlu- spheric embolic agents, coils, and sclerosing agents. No agent
sion, and sepsis. has proven superior; each is expected to increase the absolute
525
526 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
A B
C D
FIGURE 30.1 A, Transhepatic portal venogram in a patient with cholangiocarcinoma shows irregular narrowing of the portal vein. Varices are seen
as a manifestation of portal hypertension. B, After placement of a self-expanding metallic stent across the stenosis, there is good flow across the
stent. The varices are no longer evident. Coronal computed tomography image before (C) and after (D) portal vein stent shows decrease in spleno-
megaly. The platelet count rose from 70 to 180 K/mcL within days of stent placement.
FLR/TLV in the range of 8% to 10%. Complications are Subsequently, transarterial treatments have been applied to a
uncommon, the most significant being nontarget embolization wide variety of hypervascular tumors, including sarcoma
to the main portal vein or portal vein supplying the FLR, which and breast cancers, as well some tumors that are not particu-
could preclude operation. This occurs in less than 1% of larly hypervascular by imaging, such as colon cancer or
patients (van Lienden et al, 2013). cholangiocarcinoma.
Different forms of treatment have been administered via
Hepatic Artery the hepatic artery to treat such tumors, including chemother-
Unlike portal vein interventions, which are most commonly apy infusion, bland (particle) embolization (transcatheter arte-
undertaken to treat the sequela of portal hypertension or, in the rial embolization [TAE]), transarterial chemoembolization
case of PVE, as adjunct to hepatic resection, most transarterial (TACE), embolization with drug-eluting beads (DEB-TACE),
interventions in the liver are done to effect treatment of unre- and radioembolization (RAE) (see Chapter 96). Two random-
sectable malignancy or for control of bleeding in the setting of ized trials have demonstrated improvement in overall survival
trauma (see Chapters 21, 96, 122, 124, and 125). in patients with HCC treated with TACE compared with
Both primary and metastatic liver tumors derive most of patients who received best supportive care (Llovet et al, 2002;
their blood supply from the hepatic artery, unlike the non– Lo et al, 2002). To date, there has been no study conclusively
tumor-bearing parenchyma, which receives the majority of demonstrating a significant difference in overall survival
nutrient flow from the portal vein. Therefore administering a among any method of TACE, TAE, or RAE (Brown et al,
treatment to the artery can effect tumor regression without 2012).
causing collateral damage to the underlying parenchyma. Indications for arterially directed therapy include control of
In the mid-1970s, it was recognized that the unusual dual symptoms (pain or hormonal-related symptoms due to neuro-
vascular supply to the liver might allow effective transarterial endocrine liver metastases), progression of disease on systemic
treatment for hypervascular metastases from neuroendocrine treatment, prolongation of survival, and local tumor control to
tumors, as well as primary hepatocellular carcinoma (HCC). maintain eligibility for liver transplant (in the case of selected
Chapter 30 Radiologic hepatobiliary interventions 527
patients with HCC). Transarterial therapies are rarely, if ever, Early posttransplant screening Doppler ultrasound (US) can
curative and instead are intended to be repeated upon disease be used to detect abnormal flow in the hepatic artery. If this
progression. In cases of minimal disease burden, ablation may test is abnormal, a contrast study (US, CT, or angiography)
be performed in conjunction with embolization as a potentially should be considered. To salvage the organ, a precious resource,
curative therapy (see Chapter 98). In this instance, performing revascularization is often attempted after documentation of
the embolization immediately prior to ablation has the advan- abnormal flow, even in asymptomatic patients (Pareja et al,
tage of depositing contrast-laden particles within the tumor to 2010).
assist in targeting with the ablation device. In addition, occlud- Hepatic artery complications after transplant include occlu-
ing arterial blood flow may increase the zone of ablation sion, stenosis, and pseudoaneurysm. In the case of stenosis or
(Tanaka et al, 2013). In some cases, the angiogram may iden- occlusion, revascularization with catheter-directed thromboly-
tify additional sites of disease undetected on preprocedure sis, angioplasty, and/or stent placement has been effective in the
imaging, changing the treatment plan. majority of cases. Pseudoaneurysm is a rare, but potentially
Selection criteria differ slightly with each treatment option. fatal, complication that may be treated with a covered stent
Broadly speaking, patients with unresectable disease involving graft (see Chapters 120 and 124).
less than 50% of the liver without underlying liver disease or Following blunt trauma, the liver is the second most com-
with well-compensated (Childs-Pugh score A or B7) cirrhosis monly injured abdominal organ (the spleen is first) (see Chapter
may be candidates. In the past, portal vein occlusion was con- 122). The American Association for the Surgery of Trauma
sidered an absolute contraindication because of the reported Injury Scoring Scale was developed to help guide management
higher complication rate and risk of death. More recently, series of these patients (Tinkoff et al, 2008). Injuries to the hepatic
of patients with portal vein occlusion treated with TAE, TACE, artery include pseudoaneurysms, which can be unifocal or mul-
and RAE have shown efficacy without a significant increase in tiple resulting in a “starry sky” appearance of multiple sites of
complications, thus supporting its use in this group of patients extravasation/injury on angiography. Focal extravasation or
with limited treatment options (Kim et al, 2009; Lau et al, pseudoaneurysm is usually treated with coil embolization of the
2013; Maluccio et al, 2008). affected vessel just distal and proximal to the injury, or with a
The complication profiles differ slightly between the various covered stent. In the case of multifocal injury, particle emboli-
transarterial therapies. TACE is infrequently associated with zation of the hepatic artery may be performed. Because of the
bone marrow suppression and alopecia. Radiation-induced dual blood supply to the liver discussed earlier, embolization of
liver failure occurs in 1% to 2% of patients who undergo RAE. the hepatic artery in the presence of a patent portal vein is rarely
With varying frequency, each intraarterial therapy is associated of clinical consequence to the patient. Hepatic artery injury
with arterial sclerosis and arterial occlusion, which can make may occur following iatrogenic hepatic interventions, either
future intervention more difficult (Miyayama et al, 2006). This surgical or percutaneous, such as biliary drainage or TIPSS,
is more commonly seen with TACE and drug-eluting beads and is treated similarly with coil embolization or covered stent
than with TAE (Erinjeri et al, 2010; Geschwind et al, 2003) placement.
but may be seen with any modality. The clinical relevance of
this angiographic finding is that over time tumors can derive Hepatic Vein
arterial supply from nonhepatic collateral vessels, making The least common vascular target of endovascular intervention
treatment more challenging and creating a higher risk of in the liver is the hepatic vein. Budd-Chiari is a potentially life-
nontarget embolization. Branches that commonly give rise to threatening disease of heterogeneous etiology resulting in
extrahepatic tumor supply include the right phrenic, internal obstruction of hepatic venous outflow, which occurs in less than
mammary, gastroduodenal, intercostal, and renal capsular 1 per million persons (see Chapter 88). Acutely, patients are
arteries. symptomatic with abdominal pain and ascites, and over time,
Complications include nontarget embolization, liver failure, centrilobular fibrosis and cirrhosis may develop. Initial therapy
vessel injury, and postembolization syndrome. Postemboliza- includes systemic anticoagulation, but the benefit of anticoagu-
tion syndrome occurs in the majority of patients and consists lation alone is debatable. Patients with ongoing symptoms
of some degree of pain, fever, and/or nausea. This can last for may benefit from thrombolysis, venoplasty, and/or stent place-
several days. Prolonged pain may suggest nontarget emboliza- ment and, in some cases, TIPSS (Copelan et al, 2015) (see
tion to the pancreas, resulting in pancreatitis, or to the gallblad- Chapter 87).
der or upper gastrointestinal (GI) tract, resulting in cholecystitis, Stenosis of the intrahepatic or suprahepatic inferior vena
or gastric or duodenal ulceration. cava may occur as a complication following orthotopic liver
The hepatic artery is also a vessel that may require interven- transplantation, and symptomatology mimicking Budd-Chiari
tion after liver transplant. Following primary graft malfunction, may ensue. Elevated velocities by Doppler US suggest the diag-
hepatic artery thrombosis is the second leading cause of graft nosis, and a pressure gradient of greater than 6 mm Hg across
failure after liver transplant and is a major cause of transplant- the stenosis at venography is diagnostic (Kubo et al, 2006).
related mortality. This complication can result from technical Venoplasty or, in select cases, stent placement can alleviate
issues with the anastomosis, including disparate diameters of symptoms and preserve graft function.
donor and recipient vessels, and tension on, or kinking of, the
anastomosis. In most cases, HAT occurs within the first 100 Biliary Intervention
days and manifests as fulminant hepatic necrosis and/or biliary Noninvasive imaging of the biliary tree with contrast-enhanced
tract ischemia and necrosis, resulting in sepsis. Because these CT and MRI have virtually eliminated the need for invasive
patients are immunosuppressed to prevent graft rejection, the percutaneous transhepatic cholangiography to diagnose biliary
gram-negative sepsis resulting from biliary necrosis can be very tract disorders (see Chapter 20). Therefore percutaneous tran-
difficult to treat (see Chapter 120). shepatic cholangiography is rarely performed for diagnostic
528 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
A B C
FIGURE 30.2 A, Cholangiogram in a patient with metastatic colon cancer shows a short-segment occlusion of the central right hepatic duct. After
stent placmeent extending from the right posterior hepatic duct to the common hepatic duct (B), there is good flow into the duodenum across the
preserved sphincter of Oddi (C).
purposes alone, but rather at the time of planned biliary inter- a longer median patency (3 to 9.1 months vs. 1.8 to 5.5
vention. Percutaneous transhepatic biliary drainage or stent months), but there is no difference in overall patient survival
placement can be performed to relive symptoms caused by (Levy et al, 2004). When feasible, primary stent placement is
obstructive jaundice, including pruritus, anorexia, and cholan- preferred because it does not require an exteriorized device.
gitis. Bliiary drainage can also be performed to lower the bili- Additionally, if there are incompletely drained ducts, having a
rubin preoperatively or to allow for chemotherapy or, in the catheter may put patients at risk for developing cholangitis
setting of bile leak, to divert bile (Migita et al, 2009). Less because bile colonization occurs within 48 hours, and when a
common indications include access to treat biliary stone disease primary stent is placed, there is less opportunity for contami-
or to facilitate intraductal therapies, such as brachytherapy. nating incompletely drained ducts. Finally, in high bile duct
In general, bile duct obstruction below the common hepatic obstruction, stents can often be placed above the papilla.
duct (i.e., “low” bile duct obstruction) (Bismuth et al, 1992) is Without reflux of bowel contents or an exteriorized device, the
best treated endoscopically because placement of a plastic or sterility of the biliary tree is maintained so that if or when
self-expanding metal stent (SEMS) can drain the entire biliary patients present with occluded stents the likelihood of present-
tree through the normal orifice of the sphincter of Oddi. In ing with cholangitis is greatly diminished (Fig. 30.2).
cases of high bile duct obstruction, (at or above the cystic duct Metal stents also may be covered with polyurethane, with
insertion) percutaneous drainage is preferred because this the goal of preventing tumor ingrowth, resulting in improved
allows a specific duct to be targeted for drainage without con- patency. Unfortunately, this has not been shown to be the case,
tamination of nontarget ducts. and increased complications of acute cholecystitis (Isayama
Ideally, the need for drainage and optimal plan for a given et al, 2004) and stent migration have been seen (Yoon et al,
patient is made by multidisciplinary consensus involving hepa- 2006). Covered stents are not generally indicated in high bile
tobiliary surgeons, gastroenterologists, and interventional radi- duct obstruction because of the risk of occluding segmental bile
ologists. Preprocedure planning must include high-quality ducts. Further studies are needed to establish the indications
imaging of the liver and biliary tree. Contrast-enhanced CT for covered versus bare metal stents.
and MRI are extremely useful to show biliary anatomy and
pathology (see Chapters 18 and 19). In some cases, US may Bile Duct Biopsy
add additional information about the level of obstruction and In some cases, the etiology of biliary obstruction may not be
patency of portal vein branches, but US alone is not sufficient evident at the time of drainage. Bile obtained at the time of
for preprocedure planning (see Chapter 15). A dose of prophy- drainage may be sent for cytology but diagnostic sensitivity is
lactic broad-spectrum antibiotic to cover enterococci, strepto- relatively low. Bile duct biopsy may be helpful in establishing
cocci, and aerobic and anaerobic gram-negative bacilli is a diagnosis of intraductal pathology (e.g., cholangiocarcinoma)
recommended prior to biliary intervention. This is particularly and in differentiating recurrent tumor from ischemic/
important when there has been bile duct reconstruction or postoperative stricture (see Chapters 22 and 51). At the time
biliary instrumentation because, in this setting, the incidence of biliary drainage, endoluminal brush or forceps biopsy of the
of colonized bile is high. stricture depicted by cholangiography can be used to obtain a
With malignant biliary obstruction in the absence of signs sample. These techniques are most useful for intraductal
or symptoms of cholangitis, placement of a primary SEMS may pathology (e.g., cholangiocarcinoma) in contradistinction to
be performed. Compared with plastic stents, metal stents have extrinsic masses that may cause biliary obstruction (e.g., hilar
Chapter 30 Radiologic hepatobiliary interventions 529
A C
B
FIGURE 30.3 A, Ultrasound demonstrates multiple echogenic stones (arrow) with posterior acoustic shadowing. B, Coronal computed tomography
demonstrates gallbladder wall thickening and small amount of pericholecystic fluid, as well as endoscopic stent placed the day before that extends
to common hepatic duct, covering cystic duct origin. C, Image obtained after placement of cholecystostomy catheter demonstrates multiple stones
in the gallbladder with no opacification of the cystic duct or contrast entering the stent.
adenopathy or parenchymal liver mass.) In cases in which gallbladder or biliary tree for stone removal or to provide biliary
establishing a diagnosis is difficult, the biliary tree can be opaci- drainage in patients with common bile duct obstruction distal
fied through an indwelling drainage catheter and the stricture to the insertion of the cystic duct. When performed in the
targeted with a percutaneous fine needle. Cholangiographic setting of gallstones, it is often used as a temporizing measure,
guided-needle biopsy can be used to diagnose both intraductal to allow the resolution of sepsis and optimization of the patient’s
and extraductal causes of obstruction. medical conditions for subsequent cholecystectomy.
In cancer patients with bile duct obstruction, it is not
Percutaneous Cholecystostomy uncommon to see cholecystitis complicating SEMS placement
Percutaneous cholecystostomy is most commonly indicated for when gallstones are present and the stent covers the cystic duct
the treatment of acute acalculous cholecystitis in severely ill orifice, particularly when contrast is seen within the cystic duct
hospitalized patients but may also be used to treat calculous or gallbladder (Fig. 30.3). Some of these patients undergo
cholecystitis in patients who are too sick for, or in whom comor- subsequent cholecystectomy, but in palliative situations, the
bidities preclude, definitive cholecystectomy (see Chapters 33 patients may live with a cholecystostomy catheter. Cholecystos-
and 34). It may also be performed to provide access to the tomy has been reported effective as definitive therapy in
530 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
very-high-risk patients with calculous cholecystitis who have not seen when the patient returns for a repeat study after their
remained asymptomatic after catheter placement (Nasim et al, first dilation, the stricture can be dilated with a larger balloon.
2011). After cholecystostomy, clinical resolution of infection Particularly resistant strictures dilated have been treated by
occurs within 24 to 48 hours in the vast majority of cases. When some operators using cutting balloons with good, durable
performed for acalculous cholecystitis, the catheter can be results (Murkund et al, 2015).
capped once it begins to drain bile, a clear sign that the cystic
duct is patent, but the catheter should not be removed until Hepatic Cysts
tract maturation has occurred. In general, this occurs within 2 Liver cysts occur in up to 5% of the population and are inci-
to 3 weeks (Hatjidakis et al, 1998). Tract maturation may dentally seen on cross-sectional imaging (see Chapters 75 and
happen earlier when a transhepatic rather than transperitoneal 90B). They can slowly enlarge and rarely become symptomatic,
route to the gallbladder has been employed. If stone removal although symptoms from mass effect may develop if they
from the gallbladder is to be undertaken this should also be impinge on adjacent structures. In addition, bleeding may occur
performed after tract maturation. into the cyst, causing pain. A simple liver cyst should be dif-
ferentiated from a cystic tumor. The most common mimic of
Biliary Stone Disease the simple cyst is a cystadenoma that has the potential to
Stones can be removed from the gallbladder or biliary tree using become a cystadenocarcinoma. Unfortunately, cross-sectional
a variety of approaches and methods (see Chapters 36 and 37). imaging studies do not reliably distinguish between these
When there is a retained common bile duct stone after chole- two entities. Metastases that become necrotic can appear
cystectomy and a T-tube has been left in place, this is accom- cystic, particularly treated metastases from GI stromal tumor;
plished via the T-tube tract following tract maturation. When however, history and previous imaging will usually make the
choledocholithiasis occurs in a patient with remote cholecys- distinction.
tectomy, it is performed through a transhepatic approach. Cho- Treatment of simple liver cysts is not warranted unless the
ledocholithiasis may present with cholangitis or be asymptomatic. patient is symptomatic and the symptoms are clearly related to
The first step in percutaneous stone removal is placement of a the cyst. Simple aspiration can provide temporary relief, and,
percutaneous biliary drainage catheter. After a period of 2 to 3 when the symptoms are relieved, serves as proof of association,
weeks of drainage, during which a mature tract forms, the but recurrence after aspiration is 100%. Drainage and sclerosis
biliary catheter is exchanged for a large diameter sheath. The has been reported but has generally been replaced by laparo-
first order of business then is balloon sphincterotomy, followed scopic unroofing of the cyst, which is typically well tolerated by
by pushing smaller calculi into the duodenum using a balloon. the patient and avoids problems associated with an indwelling
If the stones are too large to pass through the dilated ampulla, catheter (see Chapter 75). Cystadenomas, because of the risk
they can be broken up using baskets, snares, or even lithotripsy. of malignancy, require surgical resection.
Once the duct is thought to be clear, the internal external drain-
age catheter is replaced. The patient returns in 1 to 2 weeks, Hepatic Abscess
and sheath cholangiography is performed to look for retained Most liver abscesses in the United States are pyogenic, caused
stones. If the ducts are clear, the internal external catheter is by bacteria (see Chapter 72). Amebic abscesses caused by Ent-
replaced with an external drain above the ampulla and then amoeba histolytica and fungal abscesses each account for about
capped. If the patient does well with the catheter capped, it can 10% of liver abscesses (see Chapter 73). Pyogenic liver abscesses
be removed without further imaging. are usually polymicrobial, and an etiology can often be discov-
ered. Ascending hematogenous infection from the GI tract is a
Bile Duct Injury common etiology, and patients with diverticulitis or appendicitis
The bile duct can be injured from blunt or penetrating trauma may present with a liver abscess. Cross-sectional imaging studies
but is probably most commonly injured at the time of surgery are fairly typical, demonstrating a complex collection that
(see Chapters 42 and 122). There was a fairly high rate of bile appears to have many septa (Fig. 30.5), resembling a cauli-
duct injury when laparoscopic cholecystectomy was initially flower. Despite this appearance, these can be successfully treated
introduced, at least in part related to lack of operator experi- percutaneously in combination with antibiotics, although cath-
ence, but now mostly related to unrecognized bile duct anoma- eter drainage may be prolonged (Mezhir et al, 2010). Imaging
lies (see Chapters 35 and 38). When the bile duct is clipped or should include the pelvis, with careful evaluation for a potential
transected, there is little that can be done percutaneously other source. Patients who develop bile duct obstruction, particularly
than draining the obstructed duct or diverting the transected in the setting of bactibilia related to previous biliary-enteric
one. When postoperative strictures occur, patients may present bypass, transampullary stent placement, or a preexisting percu-
with cholangitis, pruritus, jaundice, or any combination. Some- taneous drain, also may present with a liver abscess, although,
times, the biliary tree does not appear dilated or is only mini- in this situation it is better classified as an infected biloma (Fig.
mally dilated. Percutaneous access to the biliary tree is 30.6) and appears less complex than a true pyogenic liver
established first, and then the stricture is crossed (Fig. 30.4). abscess. Causes of infected biloma include stent obstruction,
An internal external catheter is left across the stricture for a recurrent tumor, or anastamotic stricture, and a catheter placed
couple of weeks as tract maturation occurs. The patient returns, for biloma drainage will continue to drain bile unless the cause
and the stricture is dilated with a balloon (Lee et al, 2012). of obstruction is eliminated. Liver abscess can also occur as a
When applied to bilioenteric anastomoses, success is likely in complication following embolization of liver tumors in the same
the majority of patients, with stricture recurrence in as few as patient group with compromised sphincter of Oddi and bactibilia
5% of patients on long-term follow-up (Janssen et al, 2014). (Mezhir et al, 2011) (see Chapter 96). This should always
Dilation of the common bile duct is not likely to be successful be considered in the preprocedure evaluation of patients under-
using a balloon of less than 10 mm. If an acceptable result is going hepatic artery embolization that have had a previous
Chapter 30 Radiologic hepatobiliary interventions 531
A B
C D
FIGURE 30.4 A, Coronal computed tomography demonstrating bile duct dilatation to level of bilioenteric anastomosis. B, Stricture at anastomosis
shown on cholangiogram at time of initial drainage. Filling defects are air bubbles. C, Stricture is dilated with a 10-mm balloon. D, Cholangiogram
obtained 3 weeks after dilation with widely patent bilioenteric anastomosis.
pancreatoduodenectomy (Fig. 30.7) or colonized bile for any fever and abdominal pain. Hepatomegaly occurs often, par-
reason. True liver abscesses should be distinguished from “peri- ticularly with large cysts. When cysts are small, aspiration may
hepatic” collections that occur postoperatively, are not in the be necessary to differentiate amebic from pyogenic abscess
parenchyma of the liver, and are usually much easier to treat because amebic antibodies may not be detected at presenta-
(Fig. 30.8) (see Chapters 27 and 103). tion, although they typically appear later. Symptoms resolve
quickly with administration of metronidazole, and interven-
Amebic Abscess tion beyond that is rarely needed unless there has been
Unlike pyogenic hepatic abscess, amebic abscesses are typi- rupture. A recent randomized trial of 57 patients with
cally associated with travel history to an endemic region (see abscesses 5 to 10 cm in size found that although fever and
Chapter 73). At presentation, patients almost universally have pain resolved sooner in the group treated with aspiration and
532 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
A B
FIGURE 30.5 A, Ultrasound of abscess demonstrating complex echotexture with multiple septa and enhanced through-transmission. B, Coronal
computed tomography scan image demonstrating typical “cauliflower” appearance of pyogenic liver abscess with multiple septa.
metronidazole, compared with metronidazole alone, the dif- cancer will develop liver metastases during the course of their
ference was not statistically significant, and there was no dif- disease (see Chapter 92). In almost half of these patients,
ference in morbidity, mortality, treatment failure, days to disease is limited to the liver, and up to 25% of these patients
normalization of leukocytosis, or duration of hospital stay have resectable disease. More effective systemic chemotherapy
between the two groups (Bammigatti et al, 2013). (see Chapters 99 and 100) and advances in techniques
of hepatic resection (see Chapter 103) have combined to
Echinococcal Cysts improve survival and increase rates of hepatic resection. Con-
Hydatid cystic disease is a parasitic disease cause by Echinococ- comitantly, there have been advances in interventional radio-
cus granulosa (see Chapter 74). The larvae of this parasite cause logic techniques of percutaneous thermal ablation, including
the disease, which is endemic in Mediterranean, Middle radiofrequency, microwave, laser, and cryoablation, as well as
Eastern, and South American countries and in New Zealand irreversible electroporation (see Chapter 908). All of these tech-
and Turkey, where people are in close contact with sheep and niques are less costly, safer, and result in shorter hospital stays
dogs. The most common site of disease is in the liver (50% to than hepatic resection and could be applied in place of surgical
80%), followed by the lung (5% to 30%). Surgery is the primary resection in well-selected cases, although the risk of local recur-
method of treatment; however, percutaneous approaches have rence is higher. With increased screening of patients with hepa-
been investigated in recent years. In a study from 2005, Paksoy titis C and earlier detection of smaller HCCs, percutaneous
and colleagues reported on 59 patients with 109 hydatid cysts ablative techniques also have application in patients with HCC
that were treated percutaneously, injecting either hypertonic and underlying cirrhosis who may not be candidates for resec-
saline or albendazole sodium as the scolicidal agent. All patients tion because of their underlying liver disease, or as an adjunc-
were given 10 mg/kg/day of albendazole beginning 48 hours tive method of maintaining them on a transplant list. There
before their procedure, and this was continued for 2 months are other tumors that might be treated with ablation, assuming
postprocedure. Directly before the procedure, they received they meet number, size, and location criteria for successful
diphenhydramine and hydrocortisone to prevent anaphylactic treatment.
reactions. Treatment was safe and effective in both groups, with
only one recurrence in the group treated with hypertonic saline. Criteria for Treatment
This compares well with a reported 4% incidence of recurrence Even the most advanced ablative techniques are limited with
following surgery. Although all cysts returned to their initial size regard to the tumor size that can be successfully treated. It has
directly following aspiration and injection, successful treatment recently been shown that an ablative “margin” is critical to a
was associated with decrease in size over time. successful ablation, with a margin of at least 5 mm on CT 4 to
8 weeks following ablation associated with the best local tumor
Hepatic Ablation control (Wang et al, 2013). Most commercially available abla-
Tumors tion systems result in an elliptic volume of coagulative necrosis,
Colorectal cancer is the third most common malignancy in the with a maximum long axis of 4 cm, limited by properties of the
United States, and most disease-related deaths are secondary local tumor/tissue environment. For this reason, successful abla-
to metastatic disease. Up to 50% of patients with colorectal tion, with a low rate of local tumor recurrence is seen most often
Chapter 30 Radiologic hepatobiliary interventions 533
A B
C
FIGURE 30.6 A, Computed tomography (CT) of a patient with pancreatic cancer and distal bile duct obstruction who has had a metallic stent
placed; note gas in bile ducts. B, Three months later, the patient presents with fever and elevated white blood cells, and CT at the same level now
demonstrates a gas/fluid collection in right liver (arrow). C, Catheter study 1 week later outlines communication to biliary tree with an obstructing
filling defect at the confluence of the bile ducts (arrow).
in tumors less than 3 cm in size, and the best results are obtained Subcapsular tumors can be difficult to treat effectively. Struc-
in tumors 2.5 cm or less. Larger tumors, or those with complex tures that may be injured by heat or cold, such as bile ducts and
geometry, are unlikely to be effectively treated by attempting to other adjacent organs, might preclude safe treatment, although
extend the thermal effect by using multiple overlapping applica- irreversible electroporation has been developed, in part, to deal
tions. The location of the tumor may also limit effectiveness of with that issue. It is fair to say that ideal patients for percutane-
ablation or ability to use the technique safely. Tumors that are ous ablation should have oligometastatic disease with three or
adjacent to high-flow blood vessels (portal vein, hepatic vein, fewer tumors, all less than 3 cm in size, that are not adjacent to
inferior vena cava) will be cooled where they are in contact a major bile duct or bile duct branch or in contact with any
with the blood vessel so that the application of heat will be less high-flow vessel, especially one greater than 5 mm in size. Local
effective at that margin and the risk of recurrence higher. tumor recurrence and survival rates are both related to the
534 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
A B
FIGURE 30.7 A, Patient with neuroendocrine tumor metastatic to liver, with several lesions evident in right liver. B, Computed tomography 3 weeks
postembolization when patient presented with fever and elevated white blood cells, demonstrating thick-walled abscess at location of treated tumor.
A B
FIGURE 30.8 Axial (A) and coronal (B) images from a patient with perihepatic postoperative fluid collection. Note how it “pushes” on hepatic
parenchyma.
number of tumors treated, and the best outcome is found in the 1- to 2-cm range because they retain dense contrast. Finally,
patients with a solitary tumor. it is possible to target areas of the tumor that may show less
Size criteria can probably be extended in HCC or other deposition of embolic material and in which recurrence is likely
vascular tumors that can be embolized first (Fig. 30.9). In this (Wang et al, 2013).
instance, addition of ablation to embolization provides several
theoretical advantages. In the first instance, it provides a Results
method of “double kill,” whereby the tumor is exposed to two Unfortunately, existing evidence for ablation of hepatic colorec-
tumoricidal events: ischemia and lethal temperature (Elnekave tal metastases is primarily from single-arm retrospective and
et al, 2013). Because embolization results in cessation of prospective studies with no published randomized trial (Wong
flowing arterial blood, the primary blood supply to hepatic et al, 2010). Overall survival, ranging from 14% to 55%, and
tumors, heat resulting from ablation does not need to overcome local recurrence rates of 4% to 60% are reported following
the cooling effects of flowing blood in the tumor or immediate treatment of colorectal metastases. Optimal conditions—small
environment, theoretically increasing efficiency of the process, tumors limited to the liver, not adjacent to blood vessels, and
resulting in more effective heating of the tissue. Second, when in the hands of experienced interventionalists—should result in
ablation is performed directly following embolization, it local control in 98% of lesions (Gervais et al, 2009). For small
becomes much easier to radiologically target small tumors in HCC, three randomized trials do exist that compare surgical
Chapter 30 Radiologic hepatobiliary interventions 535
A B
C D
E
FIGURE 30.9 Arterial (A) and (B) venous phase computed tomography (CT) in a patient with 5-cm solitary hepatocellular carcinoma in a background
of nonalcoholic steatohepatitis. Immediately following embolization (C) there is retained contrast in the embolized tumor, and ablation is performed
with a single-needle radiofrequency electrode. After ablation, the track of the needle electrode can be seen with tiny “gas bubbles” at the periphery
of the tumor (D). Complete radiologic response by imaging on follow-up CT 6 weeks after treatment (E).
536 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
resection to radiofrequency ablation (Chen et al, 2006; Feng 2013), this may have been due to a difference in tumor size. In
et al, 2012; Huang et al, 2010 ); two of these reported equiva- the resection group, 98% of solitary lesions were less than 3 cm
lence with 3-year survivals of about 70% and recurrence-free in size; in the ablation group, only 47% of solitary tumors were
survival of 50% to 60%. Only the study by Huang demon- less than 3 cm. It is likely that, with careful selection, small
strated a difference with surgical resection being superior to solitary HCC can be treated as effectively with ablation as with
ablation, providing both a 5-year survival (75.7% vs. 54.8%) surgical resection.
and recurrence-free survival (51.3 vs. 28.7%) advantage. As
was alluded to in a review article from 2013 (Cucchetti et al, References are available at expertconsult.com.
Chapter 30 Radiologic hepatobiliary interventions 536.e1
OVERVIEW of patients (Babel et al, 2009) (see Chapter 2). There are a
number of ductal anomalies related to the convergence of the
Minimally invasive techniques to manage biliary pathology left and right hepatic ducts and the insertion of cystic duct.
have reduced the need for open operative intervention. Although Although the left biliary system is fairly consistent, the right
open exploration for biliary disease has become less common, biliary system is prone to anatomic variation; the most common
specific situations, such as obstructive common duct stones not variants include the right anterior or posterior sector ducts
amenable to endoscopic therapy or restoration of biliary-enteric traversing a longer extrahepatic course before joining the left
continuity following resection of bile duct tumors, remain indi- biliary system (Blumgart et al, 1984).
cations for more invasive approaches. It is important to have a
thorough understanding of biliary anatomy and familiarity with BILE DUCT EXPLORATION
various options for operative exposure and management. Oper-
ative techniques encompassing bile duct exploration and Overview
biliary-enteric bypass will be the focus of this chapter. It is estimated that approximately 10% of the adult U.S. popula-
tion is affected by cholelithiasis, with nearly one third of these
ANATOMY patients requiring cholecystectomy over their lifetime (see
Chapter 32). Approximately 10% to 15% of patients undergo-
Knowledge of extrahepatic biliary anatomy and an appreciation ing cholecystectomy have choledocholithiasis; thus common
of anatomic variants are essential for safe operative conduct (see bile duct (CBD) stones remain the most common etiology for
Chapter 2). The intrahepatic bile ducts draining the various biliary exploration (Costi et al, 2014) (see Chapters 36 and 37).
sectors ultimately coalesce into the right hepatic duct draining There are a number of techniques available for evaluation and
the right hemiliver and the left hepatic duct draining the left clearance of the common bile duct, including percutaneous,
hemiliver, which then converge at the liver hilum to form the endoscopic, laparoscopic, and open methods. Open common
common hepatic duct, the most anterior structure of the portal bile duct exploration (CBDE) is only necessary in a small
triad at this location. In approximately 80% to 90% of cases, subset of patients. This subset includes patients undergoing
the right hepatic artery courses posterior to the common an open cholecystectomy (or a laparoscopic cholecystectomy
hepatic duct toward the right liver, whereas in the minority of converted to open) in which choledocholithiasis is suspected,
cases, it can be found anterior to the duct. The right hepatic patients with large or multiple stones, and patients requiring
duct has a short extrahepatic segment (approximately 1.5 to transduodenal sphincteroplasty. Although it is more invasive,
2 cm) compared with the left, which traverses beneath segment open CBDE is highly effective and safe. A recent analysis dem-
IVB for approximately 3 to 4 cm after exiting the liver paren- onstrated equivalent duct clearance, morbidity, and mortality
chyma. When segment IVB is broad, the left hepatic duct between endoscopic measures and open surgical techniques
assumes a longer extrahepatic course with a transverse orienta- (Clayton et al, 2006). Because percutaneous, endoscopic, and
tion, as opposed to a shorter and more oblique orientation laparoscopic modalities are discussed in other chapters, open
when segment IVB is narrow (Fig. 31.1). The left hepatic duct bile duct exploration will be the focus of the next section.
and left portal vein travel within a peritoneal reflection of the
gastrohepatic ligament; exposure of these structures is facili- Incision and Exposure
tated by lowering the hilar plate at the base of segment IVB A right subcostal incision affords satisfactory exposure of the
(Fig. 31.2). As the left hepatic duct and left portal vein enter gallbladder, portal structures, and duodenum; alternatively, an
the umbilical fissure, they are joined by the left hepatic artery, upper midline incision may be equally effective, particularly in
and vascular branches to segments II, III, and IV travel with thin patients. Division of the lateral peritoneal attachments of
biliary drainage from these segments. To maximize access to the right colon, followed by mobilization of transverse colon
these structures, a bridge of hepatic tissue at the base of the mesentery off of the duodenum, provides visualization of the
umbilical fissure (bridging segment III and IV) must often be duodenum. A generous Kocher maneuver facilitates access to
divided (Fig. 31.3). The ligamentum teres (obliterated umbili- the CBD located in the lateral border of the hepatoduodenal
cal vein) at the base of the falciform ligament runs across the ligament. Cephalad retraction of the undersurface of the liver
umbilical fissure, separating segment IV from segment II and at the base of segment IVB will optimize visualization of the
III. Segment I hepatic ducts flow into both the right and left extrahepatic biliary system (Fig. 31.4). Additionally, cholecys-
biliary systems, with the majority of drainage entering the left tectomy can enhance exposure of the hepatoduodenal ligament
hepatic duct just proximal to common hepatic duct. and can facilitate intraoperative transcystic cholangiography,
Safe operative conduct requires a close familiarity with ana- which can help to delineate biliary anatomy. Dissection of the
tomic variations of biliary drainage, as they occur in up to 25% gallbladder and cystic duct also identifies the confluence of
537
538 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
VIII II
I
VII
III
Segment IV
Anterior
CL
A B C
FIGURE 31.2. Sagittal section showing the relationship of segment IV
and caudate lobe (CL) to the left portal triad, which is encased within a
reflection of the lesser omentum that fuses with the Glisson capsule at
the base of segment IV. The arrow indicates the point of incision for the
dissection to lower the hilar plate (see also Fig. 31.5). A, Left hepatic
duct; B, left branch, portal vein. Note the left hepatic artery (C) joins the
FIGURE 31.4. To optimize exposure of the extrahepatic biliary system,
left duct and left branch of the portal vein at the umbilical fissure.
the undersurface of the liver at segment IVB is retracted cephalad. Also
depicted here is the initial line of incision for an approach to the left
hepatic duct by lowering of the hilar plate. The incision is made at pre-
cystic duct and CBD. Once the CBD has been successfully cisely the point at which the Glisson capsule reflects to the lesser
identified, the overlying peritoneal tissue can be dissected free omentum (see Fig. 31.2).
to allow access to the anterior portion of the duct.
Supraduodenal Exploration caution should be taken to avoid injuring the posterior wall of
The anterior aspect of the CBD is exposed, and two stay the duct. The length of the choledochotomy will depend upon
sutures are placed on either side of the midpoint of the planned the diameter of the duct and size of stones present with the
longitudinal incision. The choledochotomy should be located lumen but is generally 1 to 2 cm. Another consideration regard-
anteriorly to avoid compromising blood vessels that typically ing the location of this incision is proximity to duodenum; in
run along the medial and lateral aspects of the CBD and the event that a choledochoduodenostomy should be required
common hepatic duct. To avoid injury to the cystic duct, the for appropriate drainage, every effort should be made to posi-
site of cystic duct insertion should be identified, as this may tion the incision distally enough to permit a tension-free anas-
occur in a medial or posterior location. During the incision, tomosis to the proximal duodenum.
Chapter 31 Bile duct exploration and biliary-enteric anastomosis 539
After choledochotomy, flushing of the duct (distally toward traverse into the left or right hepatic duct proximally or into the
the ampulla) with saline irrigation can result in expulsion of duodenum distally, and by excising the back wall of the hori-
stones. Following this, a deflated Fogarty balloon catheter is zontal portion of the T (to minimize the risk of tube occlusion
passed distally through the ampulla into the duodenum. Once and to facilitate tube removal). The tube is inserted through
the tip of the catheter is palpated within the duodenal lumen, the choledochotomy, and the remainder of the duct is closed
the balloon is inflated and the catheter is withdrawn until resis- with fine absorbable sutures around the tube. Care should be
tance is encountered, indicating that the balloon is positioned taken to leave enough redundancy in the intraperitoneal portion
against the sphincter of Oddi. The balloon is slowly and par- of the tube to avoid tension (and possible tube dislodgement)
tially deflated while applying continuous tension, allowing in the event of significant postoperative abdominal distension.
passage into the distal CBD. At this point, the balloon is care- Postoperatively, the T-tube is placed to dependent drainage
fully reinflated, and the catheter is swept proximally, sweeping until resolution of postoperative papillary edema allows physi-
retained stones up toward the cholodochotomy. This process ologic flow of bile into the duodenum. If persistently elevated
is repeated until no stones return. The catheter is then passed output or drainage around the tube occurs, investigation via
proximally to retrieve any stones within the common hepatic cholangiography can identify malfunction, dislodgement, or
duct and intrahepatic biliary tree. Rigid instruments such as distal obstruction secondary to retained stone. If a repeat chol-
clamps or stone forceps can cause injury to the bile duct and angiogram at approximately 2 to 3 weeks is normal, the T-tube
are therefore generally best avoided. Rather, a choledochoscope may be removed. If choledocholithiasis persists, the T-tube can
can be utilized to visualize remnant stones. These can be cap- be clamped to promote stone passage. If signs or symptoms of
tured with basket retrieval, in which the basket is passed beyond cholangitis occur, the tube can be unclamped and repeat
the stone, opened, and pulled back to ensnare the stone. The imaging is obtained. Residual obstruction may be amenable to
choledochoscope and associated basket with stone are then stone extraction via T-tube or endoscopic or percutaneous
withdrawn. At the conclusion of duct exploration, confirmation access.
of proximal and distal duct clearance is performed either using
choledochoscopy or completion cholangiography (Verbesey Outcomes
et al, 2008). Open CBDE has been shown to be a safe procedure, with
favorable mortality and morbidity rates. A recent analysis of
Transduodenal Exploration multiple trials comparing open CBDE with endoscopic retro-
When an impacted stone at the distal CBD cannot be cleared grade cholangiopancreatography (ERCP) identified similar
via choledochotomy, a transduodenal approach can be used. A rates of mortality (1% vs. 3%) and morbidity (20% vs. 19%)
2- to 4-cm longitudinal incision on the lateral aspect of the in the open surgery versus endoscopy groups, respectively
second portion of the duodenum can allow visualization of the (Dasari et al, 2013). Even in high-risk patients, open surgical
ampulla. Stay sutures are placed on either side of the incision intervention has comparable mortality (4% vs. 6%) and mor-
to maximize exposure. If there is difficulty visualizing the bidity (23% vs. 16%) versus ERCP (Targarona et al, 1996).
ampulla, a small catheter can be passed through the choledo- The rate of retained stones was historically lower after open
chotomy into the duodenum. A sphincterotomy is performed CBD exploration than after ERCP (6% vs. 20%) (Suc et al,
at the 10 to 11 o’clock position, and the sphincter is incised to 1998). However, more recently, studies have demonstrated
the level of the impacted stone or probe (catheter). Placing rates of retained stones after ERCP to be approximately 2% to
the incision at this location in the ampulla minimizes the chance 10%, although higher rates are reported for difficult scenarios
of pancreatic duct injury, which is generally located opposite (i.e., larger stones, cholangitis) (Rogers et al, 2010; Wan et al,
the planned sphincterotomy site. The stone is then extracted, 2011) (see Chapter 29). For instance, a recent study of retained
and the CBD mucosa is approximated to the duodenal mucosa stones after ERCP in a high-volume center demonstrated clear-
with absorbable sutures (sphincteroplasty) to avoid postopera- ance of the CBD in 91.7% of patients with stones less than
tive papillary stenosis. Once again, a catheter is passed to 2 cm in diameter versus 77.8% successful clearance in patients
ensure resolution of obstruction, and choledochoscopy or with stones greater than 2 cm in diameter (Wan et al, 2011).
cholangiography is used to confirm the absence of residual There is a relative paucity of recent data encompassing open
stones. The duodenotomy is typically closed in one layer CBDE due to options of ERCP and laparoscopic CBDE.
(Verbesey et al, 2008). If sphincteroplasty is not successful, the However, given the safety profile and necessity when less inva-
obstruction can be bypassed with a choledochoduodenostomy sive alternatives fail, open CBDE remains an important option
(discussed in Choledochoduodenostomy later). for CBD stones.
cholangiography is no longer necessary to delineate biliary Kocher maneuver, will further enhance exposure for biliary-
anatomy in the great majority of cases. Cross-sectional imaging enteric bypass.
with magnetic resonance imaging/magnetic resonance cholan- Caution must be exercised in the setting of long-standing
giopancreatography, or even thin-cut computed tomography biliary obstruction or conditions associated with ipsilateral
scans, can accurately characterize the anatomy of the biliary tree hepatic atrophy and contralateral hypertrophy. In the scenario
and underlying pathology (see Chapter 19). Invasive imaging of of marked right hemiliver atrophy, the liver hilum and portal
the biliary tree with endoscopic or percutaneous cholangiogra- structures will become rotated in a counterclockwise manner.
phy allows stent placement, which can facilitate intraoperative Consequently, the portal vein will assume a more anterior loca-
identification of right and left hepatic ducts (see Chapters 20, tion, and the CBD or common hepatic duct will be posteriorly
29, and 30). However, it should be stressed that utilization of displaced. Hypertrophy of segment IV protrudes over the porta
an intrabiliary catheter should not be necessary in most cases hepatis and may provide additional complexity for access to the
for duct identification in the hands of an experienced biliary hilum and left biliary system (Pottakkat et al, 2009). In cases
surgeon. It is also important to recognize that instrumentation of very profound right liver atrophy, access to the biliary conflu-
of the biliary tree introduces bacterial contamination that, in a ence may require a thoracoabdominal incision.
setting of biliary stasis, can result in cholangitis, periductal
inflammation, and a higher risk of postoperative infections. Hepaticojejunostomy
Caution must also be exercised to avoid percutaneous drainage Despite the need for an additional anastomosis (at the jeju-
if it is unlikely that the stent can be passed across the obstructing nojejunostomy), Roux-en-Y hepaticojejunostomy is the most
lesion. Insertion of a percutaneous drain into an excluded biliary common surgical reconstruction for biliary obstruction. The
segment will result in bacterial colonization of static bile; if that jejunum is typically anastomosed to the common hepatic
hepatic segment cannot be decompressed by a subsequent oper- duct just distal to the confluence of the right and left hepatic
ative intervention, it will not be possible to remove that external ducts. If this approach is not feasible due to tumor infiltra-
drain without risking refractory cholangitis. These complexities tion or a high stricture, drainage can be obtained via the right
underscore the critical importance of an experienced multidis- hepatic duct or left hepatic duct. Moreover, ducts draining
ciplinary team reviewing and treating complex biliary obstruc- segment III can be utilized when the left hepatic duct is not
tion, particularly at the biliary confluence. accessible (Blumgart et al, 1984). Disadvantages include
Depending on the underlying pathology, there are a number necessity for two anastomoses and exclusion of bile from the
of options for restoration of biliary continuity with the duodenum.
alimentary tract. For instance, choledocholithiasis refractory
to local exploration may require choledochoduodenostomy. Approach to Right Hepatic Duct
Other benign etiologies, such as iatrogenic bile duct injury, As the portal pedicles enter the liver parenchyma, they remain
strictures from previous biliary-enteric operations, choledochal enclosed within a fibrous sheath derived from Glisson’s capsule.
cysts, or inflammatory strictures, may require restoration with Access to the right portal pedicle containing the right hepatic
Roux-en-Y choledochojejunostomy or hepaticojejunostomy. duct can be achieved by isolating the pedicle in an extrahepatic
Additionally, benign proximal biliary strictures as well as malig- location or by exposing the pedicle via intrahepatic dissection.
nancy (cholangiocarcinoma) may require anastomosis between The extrahepatic approach begins by lowering the hilar plate;
intrahepatic ducts and jejunum. Finally, the gallbladder may the peritoneum along the posterior aspect of segment IV is
also be utilized to facilitate drainage (cholecystoduodenostomy divided, allowing separation of Glisson’s capsule from the peri-
and cholecystojejunostomy). Although nonoperative measures toneal reflection enveloping the porta hepatis. By reflecting the
can be utilized in most situations, familiarity with the various base of segment IV in a cephalad direction, this dissection
surgical techniques can enable appropriate restoration of effectively exposes the confluence of the right and left hepatic
biliary-enteric continuity when the situation demands (see duct. By continuing this plane of dissection to the right
Chapter 42). (onto the cystic plate), the right hepatic duct may be exposed
(Strasberg et al, 2008). If the extrahepatic portion of the right
Incision and Exposure hepatic duct is too short to be visualized in this way (as is often
A right subcostal incision with or without an upper midline the case), the intrahepatic approach may be used. This requires
extension or a left subcostal extension followed by upward hepatotomies in the caudate process just posterior to the porta
elevation and cephalad retraction of the costal margin provides hepatis and along the base of the gallbladder fossa. A blunt
adequate exposure for construction of any biliary-enteric anas- right angle clamp may be passed between these hepatotomies
tomosis. The ligamentum teres is ligated and divided, and the to encircle the right pedicle, which can then be delivered for
falciform ligament is divided to its most cephalad extent on the further dissection to identify the right hepatic duct, or the
diaphragm. Retraction of the ligamentum teres is helpful for anterior or posterior sectional ducts (Fig. 31.5) (Jamieson &
optimal visualization of the vascular inflow and biliary drainage Launois, 1992).
of segments II, III, and IV. If direct decompression of the gall-
bladder is not to be undertaken, cholecystectomy can be advan- Approach to Left Hepatic Duct
tageous for identification of the cystic duct, which can be The left hepatic duct traverses an extrahepatic course below
dissected to its point of insertion onto the common hepatic segment IVB from the umbilical fissure to the porta hepatis.
duct. Cholecystectomy will also expose the cystic plate, which Because of its longer extrahepatic course, the left hepatic duct
runs in continuity with the hilar plate. By lowering the hilar is the preferred target. After ligation of the ligamentum teres
plate, the left hepatic duct may be exposed as it runs against with a firm tie, retraction is applied to elevate the left hemiliver.
the base of segment IVB (Blumgart, 1987). Mobilization of The bridge of tissue at the base of the umbilical fissure contains
the right colon with caudal retraction, followed by generous no large vessels and can be divided to provide mobility of the
Chapter 31 Bile duct exploration and biliary-enteric anastomosis 541
A B
FIGURE 31.5. A, Exposure of the right hepatic pedicle in the setting of a cholangiocarcinoma, extending into the left hepatic duct. Intrahepatic
exposure of the right hepatic duct is accomplished initially by controlling the right portal pedicle. After performing hepatotomies in the caudate process
just posterior to the porta hepatis and along the base of the gallbladder fossa, a blunt right angle can be used to facilitate encircling and delivery of
the right pedicle. The overlying hepatic parenchyma is further dissected, which allows identification of the right hepatic duct, as well as the anterior
or posterior sectional ducts. B, The relevant duct, usually the anterior sectoral duct, is opened, and anastomosis is carried out.
C D
FIGURE 31.7. A, The liver is held up so that its inferior surface is seen. The bridge of liver between segment IV and the left lobe of the liver has
been divided. The base of the ligamentum teres is seen. B, The ligamentum teres is then pulled downward. The peritoneum of its upper surface on
the left side is incised, and the extensions passing into the liver are exposed. The left sides of these extensions are divided between ligatures, which
must be passed carefully using aneurysm needles. This part of the dissection is tedious and should be carried out meticulously because hemorrhage
within the recess adjacent to the segment III duct can be difficult to control. C, The segment III duct is exposed. D, The duct is opened longitudinally
for anastomosis, which is carried out by the technique illustrated in Figure 31.13.
A B
FIGURE 31.8. A, The liver is split to the left of the ligamentum teres in the umbilical fissure, and it may be necessary to remove a small wedge of
liver tissue. B, The segment III duct is exposed at the base of the liver split above and behind its accompanying vein and is ready for
anastomosis.
Chapter 31 Bile duct exploration and biliary-enteric anastomosis 543
Construction of Anastomosis
For the purposes of Roux-en-Y reconstruction, the most proxi-
mal loop of jejunum that can be brought to lie against the
planned site of anastomosis without tension is selected. The
jejunum is transected, and a Roux limb of 50 to 70 cm is passed
in a retrocolic fashion through the avascular portion of the
transverse mesocolon to the right of the middle colic artery. A
The jejunojejunostomy may be fashioned in a sutured or stapled
manner. We do not typically use transanastomotic stent;
however, if a stent is to be used, it is preferable to pass the stent
through the cut hepatic duct prior to construction of the anas-
tomosis. The stent may be affixed against the duct wall with a
single 4-0 or 5-0 absorbable catgut suture that is tied on the
outside of the duct wall (Fig. 31.9); this maneuver helps to
avoid inadvertent dislodgment of the tube during placement of
the anastomotic sutures. When more than one biliary duct
orifice is present, it is preferable to create a single-duct orifice
by approximating the two ducts with a single row of 4-0 or 5-0
absorbable sutures (Fig. 31.10).
The hepaticojejunostomy may be performed in an end-to-
side or side-to-side anastomosis (see Chapter 42). For an end-
to-side hepaticojejunstomy, the bile duct segment is transected,
and an adjacent jejunotomy is fashioned at a safe distance from
the mesenteric margin of the bowel approximately 2 cm from
the staple line. The jejunotomy length should be shorter than
the ductotomy, as the bowel is more pliable than the duct. An
anterior row of full-thickness, single interrupted 4-0 or 5-0
absorbable sutures is placed in the bile duct, passed from inside B
to outside, and working from the patient’s left to right. This
FIGURE 31.11. A, The initial step in the creation of hepaticojejunos-
row of sutures, with needles intact, is retracted and elevated;
tomy Roux-en-Y. The anterior layer of suture (3-0 Vicryl) on the bile duct
this maneuver effectively pulls the anterior aspect of the duct is inserted first, and the sutures are passed from the inside out, starting
away, facilitating exposure and placement of the posterior row from the patient’s left and working toward the right. The needles are
of sutures (Fig. 31.11). A single full-thickness posterior row of retained, and the sutures are kept in order. B, The anterior layer of
interrupted 4-0 or 5-0 absorbable sutures is used to approxi- sutures is elevated. This displays the posterior ductal wall, and the
mate the inferior edge of the biliary duct to the superior edge posterior row of sutures is now placed, again from left to right.
544 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
of jejunum, also working from patient’s left to right. These generally completed with a single layer to avoid narrowing.
sutures are tied and cut short except for the two corner sutures, Placement of a sponge circumferentially around the anastomo-
which are secured with clamps. The previously placed row of sis allows an intraoperative test to confirm absence of a large
anterior sutures is then used to complete the anastomosis. Each bile leak.
needle is passed through the jejunum, tied, and cut short; the The alternative approach of constructing a side-to-side anas-
corner stay sutures are then cut. tomosis offers the advantages of less devascularization, with the
A side-to-side anastomosis may be appropriate in the setting use of a nontransected duct, and preservation of biliary-
of left hepatic duct or segment III duct hepaticojejunostomy duodenal continuity, in case future ERCP should be desirable
(see Fig. 31.6). Additionally, benign strictures (e.g., iatrogenic) (Winslow et al, 2009). To perform this anastomosis, the ante-
can be approached in this fashion. When decompression is rior surface of the duct is exposed and opened longitudinally
undertaken at the level of the proximal hepatic duct, increased for a distance of 2.5 to 3.0 cm, avoiding the medial and lateral
length may be achieved by extending the incision onto the left locations of periductal vasculature. The biliary-enteric anasto-
hepatic duct. A longitudinal ductomy of approximately 2.5 to mosis can then be completed in a similar manner as described
3.0 cm is performed, with a corresponding jejunotomy on the for side-to-side hepaticojejunostomy (see earlier). A single
antimesenteric border, 2 cm from the staple line. An anterior interrupted anterior (or right) row of sutures allows exposure
row of full-thickness, single interrupted 4-0 or 5-0 absorbable for placement of the posterior (or left) row, approximating duct
sutures, passed from outside to inside, are retracted to allow to jejunum, followed by completion of the anterior row
exposure for placement of the posterior row. Full-thickness, (Winslow et al, 2009).
single interrupted 4-0 or 5-0 absorbable sutures approximate
the inferior edge of the duct to the superior edge of jejunum. Choledochoduodenostomy
Following placement, the posterior row of sutures is tied with Although choledochoduodenostomy has the physiologic advan-
knots on the inside. Subsequently, the preplaced anterior row tage of enabling bile flow into the duodenum, this procedure is
of sutures are used to complete the anastomosis; they are effective only for distal strictures or impacted stone(s) in the
passed from inside to outside on the jejunum, and the knots distal CBD. After mobilization of hepatic flexure of the colon,
are tied on the outside (Winslow et al, 2009). a generous Kocher maneuver is performed to allow sufficient
mobility of the duodenum to enable construction of a tension-
Choledochojejunostomy free anastomosis. The gallbladder is removed and the cystic
Decompression of the biliary tree utilizing the common duct ligated. A 2.5- to 3.0-cm longitudinal incision is made
hepatic or CBD is typically undertaken in the setting of distal on the anterior surface of the supraduodenal CBD. Corre-
obstruction. Impacted ampullary stone(s), iatrogenic injuries, spondingly, the duodenum adjacent to the CBD is incised
stricture formation in which a more durable drainage procedure longitudinally along its superior-lateral border (Fig. 31.13).
is required, and irresectable periampullary tumors in which This produces incisions that are perpendicular to one another
biliary stenting is not effective are clinical scenarios where cho- (unlike the parallel configuration used during hepaticojejunos-
ledochojejunostomy may be utilized. Advantages of a surgical tomy). As with the hepaticojejunostomy, the duodenotomy is
approach versus nonoperative decompressive modalities are generally shorter in length than the ductotomy. The anastomo-
long-term patency and durability without the uncommon need sis is then constructed in a manner that anastomoses the bile
for repeat stent placement or revisions. duct transversely to the longitudinally-oriented duodenotomy.
Choledochojejunostomy can be performed as an end-to-side Three corner 4-0 or 5-0 absorbable sutures are placed: The
or side-to-side anastomosis. For the end-to-side technique, a first two are positioned between the midpoints of the ductot-
cholecystectomy with cystic duct ligation is performed, fol- omy and proximal and distal aspects of the duodenotomy, and
lowed by ligation of the CBD or common hepatic duct (hepati- the third is placed between the distal aspect of the CBD incision
cojejunostomy) at the level of planned transection. The duct is and midpoint of the superior lip of the duodenotomy. Traction
opened at the level of the planned anastomosis, and the endo- on the three corner sutures reorients the distal portion of the
biliary stent, if present, is removed. If desired, bile cultures may ductotomy transversely, facilitating placement of the posterior
also be collected at this time. The remainder of the CBD is row of absorbable sutures between the superior edge of the
transected, and the distal stump is oversewn with 3-0 absorb- duodenotomy and the distal half of the CBD. Full-thickness
able suture. It is important to identify healthy, well-vascularized sutures are made to approximate the ductal mucosa to duode-
duct proximal to the level of injury or pathology to avoid isch- nal mucosa. A fourth corner suture can then be placed between
emic stricture. Similarly, care should be taken to avoid excessive the proximal end of the ductotomy and the midpoint of the
circumferential dissection of the duct, as this can compromise anterior duodenal wall. Retraction of this fourth corner suture
its blood supply. A 50- to 70-cm Roux-en-Y limb of jejunum tents the remaining anterior wall of the anastomosis forward,
is passed retrocolic and to the right of the middle colic vessels facilitating placement of the remaining anterior row of sutures
and positioned to reside adjacent to the proximal bile duct in (Fig. 31.14). As before, use of a single row of sutures minimizes
a tension-free manner. The posterior wall of the duct is sutured the risk of anastomotic narrowing.
to the jejunum with a running 3-0 or 4-0 absorbable suture.
The tail of the suture and needle are left intact. A jejunotomy Cholecystoduodenostomy and Cholecystojejunostomy
is fashioned along the duct, and single interrupted 3-0 or 4-0 Loss common approaches to biliary bypass are cholecystoduo-
absorbable sutures are used to approximate the jejunal mucosa denostomy or cholecystojejunostomy. The cholecystoenteric
to the duct mucosa with the knots tied on the inside of the bypass is relatively easy to construct, but long-term patency
lumen. The anterior portion of the anastomosis is then com- rates are suboptimal compared with maneuvers that directly
pleted using the running suture used to construct the posterior decompress the extrahepatic biliary ducts. As a result, use of
row (Fig. 31.12). Due to the small lumen, the anastomosis is cholecystoduodenostomy or cholecystojejunostomy is limited
Chapter 31 Bile duct exploration and biliary-enteric anastomosis 545
II
I
III IV
FIGURE 31.12. A, Technique for end-to-side anastomosis of the bile duct below the hilus to jejunum. I, A 3-0 Vicryl suture is used, and the serosa
of the jejunum is sutured to the full thickness of the bile duct. II, This suture is developed as the posterior wall of the bile duct is attached to the
jejunal serosa. The dotted line marks the point of incision in the jejunum, which is made after the posterior layer is attached. III, The suture is now
developed either as a continuous or an interrupted suture on the anterior layer. The posterior layer of the jejunal mucosa is not sutured directly to
the bile duct mucosa. Several interrupted sutures may be inserted before completing the anterior layer, however, to approximate the mucosa (inset).
IV, The anastomosis is completed. The inset shows the posterior layer with mucosal apposition. B, Alternatively, the jejunum may be opened, and
a mucosa-to-mucosa anastomosis may be performed with a continuous polydioxanone suture as illustrated.
FIGURE 31.13. After the gallbladder is removed, the common bile duct is
removed through a conventional longitudinal incision following a Kocher inci-
sion (1), freeing the lateral duodenum around the common duct. Routine
common duct exploration is carried out. If indications for a choledochoduo-
denostomy exist, the anastomosis is performed. The incision in the common
duct (2) is extended to 2.5 cm by direct measurement. In almost all instances,
the incision in the duct carries into the common hepatic duct. The incision in
the postbulbar duodenum (3) is slightly smaller because the stoma in the
duodenum stretches to approximate the choledochal incision.
C D
Chapter 31 Bile duct exploration and biliary-enteric anastomosis 547
A B
C
FIGURE 31.15. Technique of cholecystojejunostomy. A, The cystic duct should join the common bile duct above the tumor. If it enters at the
level of the tumor (dashed line), the procedure is contraindicated. B, The posterior layer of the anastomosis is performed with a running suture
between the openings at the fundus of the gallbladder and the jejunum. C, The anterior layer of the side-to-side anastomosis is completed. (We do
not use an associated enteroenterostomy.)
to circumstances of advanced malignancy that require simple performed and the gallbladder evacuated of stones and bile; a
operative interventions and only short-term palliation (Dayton, bile specimen can be sent for analysis. Continuity with the
et al, 1980). Cholecystoenterostomy may be suitable in situa- common hepatic duct is confirmed, and a corresponding
tions where major tumoral obstruction obscures access to the enterotomy mirroring the cholecystotomy is fashioned. An
porta hepatis; however, the obstruction must not extend to the anterior row of sutures is then placed to complete the anasto-
level of the cystic duct insertion. The presence of cholelithiasis mosis (Fig. 31.15).
is another consideration, as significant stone burden within the
gallbladder makes this operative strategy less attractive. OUTCOMES
Operatively, the gallbladder and cystic duct are evaluated
to ensure their suitability for biliary decompression; specifi- A recent single institution retrospective analysis of 45 patients
cally, a patent cystic duct is required for this technique to undergoing reconstruction after biliary injury measured a
provide effective drainage. To construct a cholecystoduodenos- postoperative biliary fistula rate of 3% and a biliary stricture
tomy, a Kocher maneuver is used to provide enough duodenal rate of less than 5% over 4 years (Winslow et al, 2009) (see
mobility for a tension-free anastomosis. If cholecystojejunos- Chapter 42). Other analyses have also confirmed the safety
tomy is performed, the most proximal loop of jejunum that will and longevity of biliary decompression, with low rates of
easily lie adjacent to the gallbladder is selected; a Roux-en-Y fistula and stricture formation necessitating subsequent opera-
is not routinely performed. The gallbladder fundus is secured tive intervention (Chapman et al, 1995; Jarnagin et al, 1998;
to the antimesenteric border of duodenum or jejunum with Murr et al, 1999; Tocchi et al, 1996). Although the limited
interrupted 3-0 absorbable sutures. A cholecystotomy is number of patients requiring biliary-enteric bypass prohibits
548 PART 4 TECHNIQUES OF BILIARY TRACT INTERVENTION: RADIOLOGIC, ENDOSCOPIC, AND SURGICAL
comparative analysis of the various techniques, the larger decompression, cholangiocarcinoma developed in 5.8% of
series demonstrate low perioperative morbidity and mortality patients after transduodenal sphincteroplasty, 7.6% of patients
and adequate long-term patency. In patients undergoing after choledochoduodenostomy, and 1.9% of patients after
bypass for benign disease, consideration should be given to hepaticojejunostomy after an interval of 132 to 218 months
prolonged clinical monitoring, as there appears to be both a (Tocchi et al, 2001).
risk of delayed stricture and an elevated risk of cholangiocar-
cinoma. In a review of 1003 patients undergoing biliary References are available at expertconsult.com.
Chapter 31 Bile duct exploration and biliary-enteric anastomosis 548.e1
CHAPTER 32
Natural history of gallstones and
asymptomatic gallstones
Pierre F. Saldinger and Omar Bellorin-Marin
551
552 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
North America
Everhart et al, 1999, 2001, 2002 American Indians 64.1 29.5
Hispanic 8.9 27
Shaffer, 2005 Non-Hispanic White 8.6 16.6
Non-Hispanic Black 5.3 13.9
South America
Miguel et al, 1998; Covarrubias Chilean Indians 12.6 49.4
et al, 1995; Moro et al, 2000
Palermo et al, 2013 Argentina 18.2 25
Europe
Glambek et al, 1987 Norway 17 21
Loria et al, 1994 Italy 2.7 8.4
Mellström et al, 1988 Sweden NR 27
Kratzer et al, 1998 Germany 5.8 6.3
Martinez et al, 1997 Spain 7.8 11.5
Asia
Khuroo et al, 1989 Kashmir 3.07 9.6
Unisa et al, 2011 India 2 5.6
Chen et al, 1998 Taiwan 5.3 2.4
Shen et al, 2014 China 9.3 9.8
Kono et al,1992 Japan 3.6 NR
Chapman et al, 2000 New Zealand 18.1 23.1
Africa
Walker et al, 1989; South Africa NR 10
Bagi Abdel, 1991 Sudan 5.6 5.1
NR, Not reported.
absorption, and gallbladder hypokinesia, which leads to bile can be in part explained by a hormonal effect; estrogen decreases
cholesterol supersaturation and nucleation (see Chapter 8). bile salts secretion and increases cholesterol, whereas progestins
Bacterial infection and an increase in bilirubin load play a role act by impairing gallbladder emptying, causing stasis. Preg-
in the development of black and brown gallstones. The follow- nancy is associated with up to 30% risk of developing biliary
ing is an overview of the most common risk factors for the sludge. Oral contraceptive use and low-dose estrogen therapy
development of gallstones. in postmenopausal women also increase the risk of gallstone
formation (Hulley et al, 1998; Maringhini, et al, 1993).
Age
The incidence of gallstones increases with age across all ethnic Obesity, Diet, Physical Activity, and Weight Loss
groups, becoming 4 to 10 times more likely in individuals older Obesity is a well-established major risk factor for the develop-
than 40 years, with a very low rate among infants and children ment of gallstones, with an incidence of 25% in morbidly obese
(Chen et al, 1998; Einarsson et al, 1985). In a population- patients (Li et al, 2009).The association with simple obesity is
based study, the prevalence of gallstones in children was 1.9% important in females, whereas in males it is mostly associated
(Wesdorp et al, 2000). As previously mentioned, some specific with intraabdominal (central) obesity and metabolic syndrome
populations, such as American Indians (Pima), have an (De Santis et al, 1997; Heaton et al, 1991; Maclure et al, 1989;
increased incidence of gallstones (up to 70% by 30 years of Tsai et al, 2004).
age), implicating hereditary metabolic factors (Sampliner et al, The frequency of detection of gallstones has almost doubled
1970). Pediatric populations with chronic hemolytic condi- in the last 60 years, in parallel with a changed composition of
tions, such as sickle cell anemia, also represent another distinct stones from pigment to cholesterol. In humans, most choles-
group in whom gallstones develop early. In a study of 82 chil- terol found in gallstones is from the diet because de novo
dren (0 to 18 years of age) with cholelithiasis, gallstone disease hepatic synthesis is only about 20% (Paigen & Carey, 2002).
was associated to a hemolytic disease in 39% of cases (Wesdorp This emphasizes the importance of high caloric and carbohy-
et al, 2000). drate intake as risk factors for the development of gallstones in
modern society.
Gender Bariatric patients are at a high risk for the development of
Female gender is a risk factor for developing gallstones, surpass- cholelithiasis after weight-reduction surgery. Sludge and gall-
ing males in the incidence of gallstones and the chance of having stones form in 30% to 71% of patients following bariatric
surgery by 2 : 1 or 3 : 1 in most studies (see Table 32.1). This procedures, with weight loss more than 1.5 kg/week being a risk
A. Gallstones and Gallbladder Chapter 32 Natural history of gallstones and asymptomatic gallstones 553
factor (Shiffman et al, 1991; Weinsier et al, 1995). The stones control subjects (van der Linden et al, 1973), suggesting a
are likely to become apparent 6 weeks after surgery and symp- familial component for gallstone formation. Concordance rates
tomatic in 7% to 16% of patients. This presentation is associ- of gallstones in monozygotic twins of both genders are signifi-
ated with weight loss that exceeds more than 25% of initial cantly higher than for dizygotic twins, representing conclusive
body weight (Li et al, 2009). evidence for a genetic predisposition in developing gallstone
Patients receiving total parenteral nutrition (TPN) are disease (Katsika et al, 2005). Hepatic cholesterol hypersecre-
another group with a high incidence of gallstone and sludge tion, resulting in bile supersaturation and cholesterol stone
development. Biliary sludge appears as early as 5 to 10 days formation, may be caused by increased hepatic uptake and
after fasting, with all patients developing sludge after 6 weeks synthesis of cholesterol, decreased hepatic synthesis of bile
of TPN therapy. Sludge usually resolves within 4 weeks of ces- salts, decreased hepatic synthesis of cholesterol esters for inclu-
sation of TPN when the patient has resumed oral intake. After sion in very-low-density lipoprotein (VLDL), and derange-
3 months of TPN therapy, approximately 45% of patients will ments in the intestinal absorption of cholesterol and bile
develop gallstones (Messing et al, 1983; Murray et al, 1992; salts. Genes controlling hepatic cholesterol metabolism have
Shaffer, 2001). Low levels of physical activity are associated been implicated in the pathogenesis of gallstone formation in
with development of gallstones in large observational and popu- transgenic/knockout mouse models and in humans (Table
lation studies. These patients also typically have related obesity 32.2). Excess cholesterol load in the smooth muscle of the
and typical dietary risk factors (Leitzmann et al, 1999). Finally, gallbladder can affect signaling via the cholecystokinin A recep-
patients receiving long-term somatostatin analogue therapy tor and contribute to the development of gallstones by inducing
for various disorders (acromegaly, neuroendocrine tumors) bile stasis. Intestinal cholesterol/bile salt absorption is tightly
are at increased risk for gallstone formation as a result of controlled, and genes responsible for cholesterol absorption
reduced gallbladder motility and reduced bile flow (Bornschein (NPC1L1, Niemann-Pick C1–like protein) or cholesterol efflux
et al, 2009). (ABCG5/G8) have been implicated in the development of gall-
stones in certain populations because of intestinal bile salt loss.
Genetics Single-gene mutations resulting in hemolysis increase the inci-
Population studies indicate a 30% genetic component in the dence of black stones because of an excess of unconjugated bile
development of gallstone disease. Family and twin studies have acids forming polymerized calcium bilirubinate stones. A
contributed to the understanding of gallstone formation. Cho- summary of genes found to be involved in gallstone pathogen-
lesterol gallstones are found at a ratio of 3 : 1 in family members esis can be found in Table 32.2 (Chuang et al, 2013; Grünhage
of the affected person, compared with spouses or unrelated & Lammert, 2006).
554 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
cholecystectomy is before or during renal transplantation or 10-year period. As a result, cholecystectomy to prevent the
during bariatric surgery (Bonatsos et al, 2001; Graham et al, development of gallbladder cancer in patients with gallstones is
1995; Shiffman et al, 1993). not recommended. Some populations, such as Pima Indians,
Chileans, and Pakistani women with gallstones, have an unusu-
ally high incidence of gallbladder cancer (12 to 21 per 100,000)
GALLSTONES, PORCELAIN GALLBLADDER, (Goldin & Roa, 2009). In these unique populations, prophy-
AND GALLBLADDER CARCINOMA lactic cholecystectomy to prevent the development of gallblad-
(SEE CHAPTER 49) der cancer is probably justified.
Calcification of the gallbladder is encountered in up to
Gallstones are closely associated with gallbladder cancer, with 0.8% of all gallbladder pathology specimens. Porcelain gall-
a pooled relative risk (compared with patients without gall- bladder or diffuse gallbladder calcification was long considered
stones) of 4.9 and a calculated risk of 0.02% per year (Randi to be a significant risk factor for the presence of gallbladder
et al, 2006). Chemical exposure, tobacco, family history of cancer, with a risk of cancer ranging from 12% to 62%
gallbladder cancer, and duration of cholelithiasis are all poten- (Cunningham & Alexander, 2007; Stephen & Berger, 2001;
tial risk factors for the development of gallbladder cancer (Kajal Towfigh et al, 2001). Two studies from the United States ana-
et al, 2012; Miyazaki et al, 2008). Gallstones are present in lyzed large databases of cholecystectomy specimens and
60% to 90% of gallbladder cancer cases (Goldin & Roa, 2009), reported a much lower incidence of cancer in porcelain gall-
although no direct causal relationship between gallstones and bladder than in previous studies (Stephen & Berger, 2001;
gallbladder cancer has been proven. Gallstones larger than Towfigh et al, 2001). In a more recent study, calcification-
3 cm have been associated with a higher risk of gallbladder associated gallbladder cancer was found in only 6% compared
cancer; however, the presence of large gallstones may simply with 1% in a matched cohort of patients without gallbladder
reflect the duration of cholelithiasis and inflammation rather wall calcification (Schnelldorfer, 2013). Based on these data, at
than a direct causal relationship with cancer. Also, a significant least in Western populations, the incidence of cancer in porce-
difference in prevalence of gallbladder cancer worldwide points lain gallbladder should be considered to be increased but not
to the influence of other factors. The risk of developing carci- as high as reported previously. Given the small but significantly
noma has been estimated to be 1% of calculous gallbladders higher risk of gallbladder cancer associated with porcelain gall-
20 years after the initial diagnosis of gallstones, with the risk bladder, compared with the general population, and the lethal-
increased mainly in men (Maringhini et al, 1987); however, ity of this cancer, cholecystectomy is generally indicated in
given the high incidence of gallstones and the rarity of gallblad- patients with a calcified gallbladder.
der cancer, this estimate would seem to be high. In some series,
no patients with gallstones developed gallbladder cancer over a References are available at expertconsult.com.
A. Congenital Disorders Chapter 32 Natural history of gallstones and asymptomatic gallstones 555.e1
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CHAPTER 33
Cholecystitis
Kaitlyn J. Kelly and Sharon Marie Weber
556
A. Gallstones and Gallbladder Chapter 33 Cholecystitis 557
Hepatobiliary scintigraphy is not useful in patients with poor cholecystitis are the same as those seen on US and include wall
hepatic function because it requires hepatic excretion of bile, thickening, pericholecystic stranding, distension of the gallblad-
but it is accurate in approximately 90% of patients and may be der, high-attenuation bile, pericholecystic fluid, and subserosal
more accurate than US alone. Hepatobiliary scintigraphy is edema. CT is generally less sensitive than US for diagnosing
more involved, more expensive, and requires a longer time than acute cholecystitis, particularly early in the course, when the
US; however, it should be reserved for selected cases (Chatzi- imaging findings may be subtle (Fidler et al, 1996; Harvey &
ioannou et al, 2000; Kalimi et al, 2001). Mahid and colleagues Miller, 1999).
(2009) have suggested a diagnostic approach that starts with
US for patients with biliary symptoms. If no gallstones are Treatment
definitively identified, this should be followed by esophagogas- Initial treatment with antibiotics active against enteric bacteria
troduodenoscopy to exclude alternative causes of symptoms, should begin as soon as the patient is diagnosed with acute
such as peptic ulcer disease or gastritis. If this test result is cholecystitis. In addition, oral intake should be held, and appro-
negative, hepatobiliary scintigraphy should follow. priate intravenous (IV) fluid resuscitation should be started in
Computed tomography (CT; see Chapter 18) can also help preparation for surgery with parenteral analgesics administered
diagnose acute cholecystitis and provides more detailed ana- as needed.
tomic information than US. CT is particularly useful in patients The definitive treatment for acute cholecystitis is cholecys-
whose symptoms suggest a complication such as pericholecystic tectomy (see Chapter 35). From the time this operation was
abscess or an alternative diagnosis. The CT findings of acute first performed in 1882 by Langenbuch, open cholecystec-
tomy has been the standard of care for patients with acute
cholecystitis. With the advent of laparoscopic cholecystectomy
in the 1980s, the standard approach has changed such that
cholecystectomy is now routinely performed laparoscopically.
The benefits of laparoscopic cholecystectomy are discussed in
depth elsewhere (see Chapter 35), but they include a shorter
TRANS RT GB
postoperative stay and decreased analgesia requirements (Cox
et al, 1993). Although the laparoscopic approach is now stan-
dard for most cases, it is interesting to note that two prospec-
tive, randomized studies suggested little or no difference in
several outcome measures between laparoscopic versus small-
incision open cholecystectomy (Keus et al, 2008; Majeed
et al, 1996).
Early analysis of the results of laparoscopic cholecystectomy
in patients with acute versus chronic cholecystitis showed
increased morbidity and mortality rates for patients with simple
or complicated acute cholecystitis. Because of the increased
morbidity and mortality, acute cholecystitis initially was consid-
ered a relative contraindication to laparoscopic cholecystectomy
(Flowers et al, 1991). Subsequent reports, however, have shown
FIGURE 33.1. Transverse view of the gallbladder on ultrasound in a the improved safety of this technique in the acute setting (Chan-
patient with calculous cholecystitis, revealing gallstones and gallbladder dler et al, 2000; Johansson et al, 2003; Lai et al, 1998; Lo et al,
wall thickening. 1998). The conversion rate to an open procedure is higher for
A B
FIGURE 33.2. A, Normal hepatoiminodiacetic acid (HIDA) scan demonstrating contrast-filled gallbladder (arrow). B, Abnormal HIDA scan demon-
strating nonfilling of the gallbladder consistent with cystic duct obstruction. (Courtesy Dr. Scott Perlman, University of Wisconsin Hospital and Clinics.)
558 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
patients with acute cholecystitis compared with patients under- compared with those treated conservatively with IV antibiotics
going elective operations for simple biliary colic (Schirmer et al, and bowel rest, followed by delayed cholecystectomy. In high-
1991), but most patients with acute cholecystitis (>80%) can risk patients in whom general anesthesia is contraindicated,
undergo laparoscopic cholecystectomy successfully (Papi et al, percutaneous stone extraction has been used successfully
2004). Retrospective series have reported that risk factors for (Gibney et al, 1987; Wong et al, 1999). More recently, single
conversion to open cholecystectomy include obesity (Rosen and repeated percutaneous transhepatic gallbladder aspiration
et al, 2002), elevated white blood cell count (Alponat et al, has been shown to be successful in high-risk patients with acute
1997; Kanaan et al, 2002), and male gender (Kanaan et al, cholecystitis who do not respond to conservative therapies
2002). (Tsutsui et al, 2007). This treatment modality is not widely
Other novel surgical approaches to cholecystectomy have practiced, however.
been proposed to treat patients’ symptomatic gallstones,
including so-called mini-laparoscopic cholecystectomy (see Chapter Timing of Surgery
35), which uses 2- to 3-mm ports (Hsieh, 2003); mini- The optimal interval of time between the diagnosis of acute
cholecystectomy (Assalia et al, 1997), in which a small (mean, cholecystitis and definitive treatment with cholecystectomy has
5.5 cm) incision is used to remove the gallbladder; single-incision been the subject of many prospective randomized trials, nine
laparoscopic cholecystectomy; and natural orifice transluminal evaluating open cholecystectomy and five evaluating laparo-
endoscopic (NOTES) cholecystectomy with transvaginal extrac- scopic cholecystectomy (Papi et al, 2004; Siddiqui et al,
tion. Prospective, randomized studies evaluating the safety of 2008). The concern in operating on patients with early chole-
these techniques are lacking, but existing data suggest decreased cystitis (typically defined as <3 days) is the potential for
postoperative pain and improved cosmesis at the expense of increased postoperative complications, including common bile
slightly longer operating times with these techniques. duct injury. The risk of performing cholecystectomy late
Laparoscopic subtotal cholecystectomy (LSC) has also (weeks after the diagnosis of cholecystitis) is that a subset of
been evaluated as a means of decreasing the conversion rate patients has recurrent symptoms during the period between
to open procedure in patients with acute cholecystitis (Horiu- diagnosis and surgical treatment, which leads to recurrent hos-
chi et al, 2008; Singhal et al, 2009) (see Chapter 35). This pital admissions and urgent surgery (Papi et al, 2004). In mul-
procedure involves leaving the posterior wall of the gallbladder tiple randomized prospective trials evaluating the timing of
when it is significantly difficult to dissect from the liver bed, open cholecystectomy, patients undergoing early operation
with cauterization of the remnant mucosa and suturing or sta- experienced no increased perioperative morbidity or mortality
pling of the gallbladder neck in cases of severe inflammation and had a shorter length of hospital stay compared with
of the triangle of Calot. Indeed, in the face of severe inflam- patients undergoing delayed operation (Norrby et al, 1983;
matory change, such an approach is safer than risking injury Van der Linden & Edlund, 1981). In addition, a meta-analysis
to the common hepatic duct by pursuing dissection within the of these trials demonstrated that more than 20% of patients
porta hepatis. Horiuchi and colleagues (2008) demonstrated a did not respond to medical management while awaiting defini-
significant decrease in conversion rate to open procedure with tive treatment, and approximately half of these patients
the use of this technique, with no increase in postoperative required urgent surgical treatment as a result (Papi et al,
complications. In this study, all patients undergoing LSC had 2004). In this same analysis, no increase in morbidity was seen
temporary subhepatic drains placed. This technique, although in patients undergoing early definitive treatment with laparo-
innovative, does not have wide clinical applicability because of scopic (p = 0.6) or open (p = 0.2) cholecystectomy compared
limited availability of instruments, specialist surgeons trained with delayed treatment, but a clear difference was seen in
in their use, or both. Laparoscopic cholecystectomy remains length of hospital stay, with patients undergoing delayed treat-
the standard therapy for definitive treatment of patients with ment requiring a more prolonged hospitalization (Papi et al,
acute cholecystitis, with conversion to an open procedure if 2004). Although it is safe to perform cholecystectomy either
necessary. early or late after an episode of acute cholecystitis, patients
In patients with a high perioperative risk related to sepsis or benefit when surgery is performed early.
other underlying medical comorbidities, initial treatment of Performing laparoscopic cholecystectomy in patients with
acute cholecystitis with percutaneous cholecystostomy tube acute cholecystitis poses unique challenges to surgeons because
placement is preferred (see Chapter 34). These tubes can be of the potential for increased morbidity, including the most
placed percutaneously using either US or CT guidance (Hat- feared complication—common bile duct injury (see Chapter
zidakis et al, 2002). This procedure effectively decompresses 42). The concern is that the acute inflammation may obscure
the gallbladder by evacuating the infected bile and relieving the the anatomy, leading to an increase in postoperative complica-
pain associated with gallbladder distension from outlet obstruc- tions. Multiple prospective randomized trials have evaluated the
tion, and it is associated with a low complication rate (Akyürek outcome of patients with acute cholecystitis undergoing early
et al, 2005; Byrne et al, 2003; Spira et al, 2002; Werbel et al, versus late laparoscopic cholecystectomy (Table 33.1). Although
1989). In addition, most patients (>80%) improve clinically a significant increase in operation time was experienced for
within a short time (Byrne et al, 2003; Hatzidakis et al, 2002; those undergoing early compared with delayed cholecystecomy
Vauthey et al, 1993). After stabilization of the patient, and if (p = 0.002), the results of these trials uniformly showed no
the clinical situation otherwise warrants, a delayed interval significant difference in postoperative morbidity or mortality,
cholecystectomy should be performed, which often can be including common bile duct injury, when surgery is performed
accomplished laparoscopically (Spira et al, 2002). Akyürek early (Siddiqui et al, 2008). Additionally, no significant differ-
and colleagues (2005) demonstrated decreased hospital stay ence was found in the conversion rate to open cholecystectomy,
and cost in high-risk patients undergoing percutaneous chole- although it was clearly higher (20% to 30%) in patients with
cystostomy, followed by early laparoscopic cholecystectomy cholecystitis compared with prior studies evaluating patients
A. Gallstones and Gallbladder Chapter 33 Cholecystitis 559
TABLE 33.1 Results of Prospective, Randomized Trials Comparing Early versus Delayed Laparoscopic Cholecystectomy for Acute
Cholecystitis
Length of Conversion to Open
Reference N Definition Morbidity Rate Stay (days) Cholecystectomy
undergoing elective laparoscopic cholecystectomy in the non- surgery was more cost effective because of reduced overall
acute setting. Perhaps the most important finding was that in length of hospital stay and avoidance of readmissions for recur-
all but one study, patients randomly assigned to late cholecys- rent cholecystitis or biliary colic.
tectomy did not respond to conservative management in 15%
to 30% of cases. Although patients in the early group generally CHRONIC CHOLECYSTITIS
experienced a longer postoperative hospitalization (p = 0.004),
most of these trials demonstrated a decrease in overall length Pathogenesis and Clinical Manifestations
of hospital stay in the early group versus the delayed group Chronic cholecystitis may result after one or more episodes of
(cumulative p < 0.001) (Chandler et al, 2000; Johansson et al, acute cholecystitis, or it may evolve, initially without symptoms,
2003; Kolla et al, 2004; Lai et al, 1998; Lo et al, 1998). Early merely from the presence of gallstones. In most cases, patients
laparoscopic cholecystectomy is therefore the preferred surgical describe one or more episodes of abdominal pain that is clini-
technique for patients with acute cholecystitis. Catena and col- cally consistent with biliary colic. The term colic is a misnomer
leagues (2009) have proposed the use of a harmonic scalpel for because the pain from chronic cholecystitis is usually constant
improved hemostasis and biliostasis in laparoscopic cholecys- in nature and is similar to that seen initially with acute chole-
tectomy, and preliminary data suggested it may decrease the cystitis, although it is self-limited and often less severe. The
conversion rate to open procedure in patients undergoing lapa- pain associated with chronic cholecystitis seems to be the result
roscopic cholecystectomy for acute cholecystitis. A prospective, of intermittent obstruction of the gallbladder outflow.
randomized controlled trial subsequently confirmed these find- There are numerous well-described risk factors for the
ings (Catena et al, 2009). development of gallstones and subsequent chronic cholecystitis.
The majority of trials of early versus delayed laparoscopic Patients at particularly high risk include obese women, in whom
cholecystectomy define “early” as within 72 hours of symptom pathologic changes of chronic inflammation are found even in
onset. A nonrandomized, prospective study by Tzovaras and the absence of gallstones (Calhoun & Willbanks, 1987; Csendes
colleagues (2006) assessed 129 patients undergoing laparo- et al, 2003); this may be due to an increase in the cholesterol
scopic cholecystectomy for acute cholecystitis during the index saturation of bile in obese patients (St. George & Shaffer, 1993;
admission. The patients were divided into three groups regard- see Chapter 8). These patients are often asymptomatic. Xan-
ing the timing of their surgery from symptom onset: within 3 thogranulomatous cholecystitis is a subtype of chronic chole-
days, between 4 and 7 days, and after 7 days. They found no cystitis that can mimic gallbladder cancer (Agarwal, et al. 2013)
significant difference in conversion rate, morbidity, or postop- (see Chapter 49). It is characterized by the presence of destruc-
erative hospital stay among these groups and thus suggest that tive inflammation of the gallbladder wall, often accompanied
the benefits of early cholecystectomy are not limited to patients by proliferative fibrosis. The histologic appearance is that of
who are seen within 72 hours of symptom onset. foamy histiocytes in a background of acute and chronic inflam-
Another factor to consider is whether early or delayed lapa- matory cells. This process can result in the appearance of asym-
roscopic cholecystectomy for acute cholecystitis is more cost metric gallbladder wall thickening and/or mass formation in the
effective. A meta-analysis of randomized and other studies per- gallbladder wall and can be difficult or impossible to distinguish
formed by Lau and colleagues (2006) concluded that early from gallbladder cancer (Fig. 33.3). Further confusing this
560 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
A B
FIGURE 33.3. A, Coronal image of a patient seen with chronic right upper quadrant pain and a distended gallbladder with asymmetric wall thick-
ening concerning for malignancy. B, Gross image of the resected gallbladder, which was firm and markedly abnormal. Final pathology demonstrated
xanthogranulomatous cholecystitis.
picture, serum cancer antigen 19-9 levels can be elevated in burns, or in those undergoing a prolonged recovery from major
xanthogranulomatous cholecystitis (Clarke et al, 2007). operations who are unable to tolerate oral intake (Gu et al,
2014). It has been speculated that in such situations, there is no
Diagnostic Imaging stimulus for gallbladder contraction, the bile becomes inspis-
US examination of the gallbladder most often reveals circum- sated, and biliary sludge forms. The exact pathogenesis is
ferential thickening of the gallbladder wall with cholelithiasis unknown but likely involves some combination of ischemia,
(see Chapter 15). In advanced cases, a small, shrunken gall- biliary stasis, and sepsis (Hakala et al, 1997; Warren, 1992), and
bladder with a thickened wall and multiple gallstones are seen. inspissated bile and sludge seem to play some causative role.
Discomfort may be reproduced with direct pressure on the Although this condition traditionally has been described in the
gallbladder with the US probe. Commonly, particularly in patient groups mentioned earlier, several reports suggest an
obese patients and in those with mild symptoms, the US exami- increase in the de novo presentation of acalculous cholecystitis
nation shows no particular gallbladder wall abnormalities in the outpatient population, including patients with atheroscle-
(Calhoun & Willbanks, 1987). rotic vascular disease, such as seen in hypertension and diabetes
(Parithivel et al, 1999; Ryu et al, 2003; Savoca et al, 1990).
Treatment Overall, acalculous cholecystitis represents approximately 5%
Elective cholecystectomy is the treatment of choice for patients to 15% of all cases of acute cholecystitis. A male predominance
with symptoms of chronic cholecystitis (see Chapter 35). In is seen in cases of acalculous cholecystitis, in contrast to acute
most (≥ 90%) cases, cholecystectomy can be accomplished calculous cholecystitis, which occurs more commonly in women
laparoscopically. Patients occasionally are seen with atypical (Kalliafas et al, 1998; Ryu et al, 2003; Wang et al, 2003).
pain (left hypochondrium) or with minimal or no pain but, A prospective study evaluating trauma patients with serial
rather, intermittent nausea or bloating. In such cases, evalua- US examinations found that the incidence of acalculous chole-
tion for other possible causes of symptoms should be under- cystitis in severely injured patients (injury severity score ≥ 12,
taken, particularly if US shows gallstones but no sequelae of requiring intensive care for > 4 days) was 11% (Pelinka et al,
chronic cholecystitis are seen. In cases where there is asym- 2003), which is similar to other reports (Imhof et al, 1992). In
metric gallbladder wall thickening or mass formation concern- addition, three factors were correlated with an increased risk
ing for malignancy, a laparoscopic exploration is reasonable but for acalculous cholecystitis in this high-risk population: (1) high
with a low threshold for conversion to an open operation. The injury-severity score, (2) increased heart rate, and (3) transfu-
surgeon should be prepared to perform a definitive gallbladder sion requirement at the time of admission. This study suggests
cancer operation, including liver resection and regional lymph- that more acutely injured patients, who are expected to require
adenectomy. In these cases, it is critical to avoid gallbladder prolonged ventilatory and nutritional support, are at higher risk
perforation or spillage intraoperatively. Frozen-section analysis for acalculous cholecystitis (Pelinka et al, 2003).
of any grossly abnormal tissue can be considered, but it is often
appropriate to proceed with a cancer operation if gross findings Clinical Manifestations
are suspicious for malignancy (see Chapter 49). Part of the difficulty in making the diagnosis of acalculous
cholecystitis is that many patients seen with this condition are
ACUTE ACALCULOUS CHOLECYSTITIS critically ill and require ventilatory support and sedation. The
symptoms and signs are often masked by the patient’s underly-
Pathogenesis ing condition or the interventions used to treat it (Kalliafas
Acalculous cholecystitis usually occurs in patients with coexist- et al, 1998). In the outpatient population seen with acalculous
ing major illnesses, such as generalized sepsis, major trauma, or cholecystitis, the diagnosis is more straightforward, mimicking
A. Gallstones and Gallbladder Chapter 33 Cholecystitis 561
the signs and symptoms of acute calculous cholecystitis (Ryu assessed 255 severely injured trauma patients with serial US
et al, 2003). examinations. In this trial, all patients with US findings consis-
The most frequent physical and laboratory findings are tent with acalculous cholecystitis and major clinical symptoms—
fever, right upper quadrant pain, leukocytosis, and hyperbiliru- abdominal pain or distension or both, hemodynamic instability,
binemia. These findings are often nonspecific, however, in the or organ failure—underwent cholecystectomy, and all had acal-
setting of sepsis and critical illness (Kalliafas et al, 1998). The culous cholecystitis on final pathology. A few patients had posi-
incidence of gangrene and perforation seems to be increased in tive US findings, but no major clinical symptoms were observed.
patients with acalculous cholecystitis compared with acute cal- In this group, all US findings returned to normal within 3 weeks.
culous cholecystitis, likely because of the delay in diagnosis that In addition, 15% of patients experienced hydrops of the gall-
is common with this disease. Severe gallbladder complications bladder without clinical symptoms, and subsequent normaliza-
such as gangrene, perforation, and empyema occur more com- tion of the US was observed in all (Pelinka et al, 2003). These
monly in older patients with an elevated white blood cell count findings suggest that although many critically ill patients may
(Ryu et al, 2003; Wang et al, 2003). In many series, the risk develop US abnormalities consistent with acalculous cholecys-
of severe gallbladder complications was found to be 50% to titis, the combination of clinical symptoms and positive imaging
60% (Kalliafas et al, 1998; Swayne, 1986; Wang et al, 2003). findings will identify most patients who require intervention.
This high risk may be the result of the disturbance in capillary Because of the difficulty establishing a diagnosis in these
microcirculation that has been shown in pathologic studies on critically ill patients, CT has been used as an additional imaging
gallbladder specimens after cholecystectomy for acalculous test. The advantage of CT is that imaging of the entire chest,
cholecystitis (Hakala et al, 1997; Warren, 1992). In addition, abdomen, and pelvis can be obtained; this is particularly impor-
partly as a result of the severity of the patient’s underlying tant in this patient cohort, in whom clinical signs and symptoms
condition, the mortality rates are high—15% in some series may be misleading or whose signs and symptoms may result
(Wang et al, 2003). from other causes. CT may be more sensitive and specific than
US (Blankenberg et al, 1991; Mirvis et al, 1986), but it has the
Diagnostic Evaluation and Imaging disadvantage of requiring transport of the patient outside of the
Imaging algorithms for patients with suspected acalculous cho- intensive care unit.
lecystitis are similar to algorithms for patients with acute cho- When a patient’s diagnosis is questionable based on physical
lecystitis. The initial imaging test is usually US, which classically findings or US evaluation or both, hepatobiliary scintigraphy
reveals gallbladder distension, a thickened gallbladder wall, and may be used. In past reports, a high rate of false-positive results
biliary sludge without stones (Fig. 33.4; Wang et al, 2003) (see was seen in patients with acalculous cholecystitis (Mirvis et al,
Chapter 15). The difficulty with interpreting these findings is 1986), but more recent evaluation of this modality has shown
that many critically ill, parenteral nutrition–dependent patients improved accuracy in diagnosing acalculous cholecystitis (Kal-
have these findings. Partly because of this difficulty, the accu- liafas et al, 1998; Ryu et al, 2003). In some series, scintigraphy
racy of US to diagnose acalculous cholecystitis has been highly has been found to be more sensitive than CT or US in diagnos-
institution dependent, with some series showing it to be highly ing acalculous cholecystitis (Kalliafas et al, 1998; Prevot et al,
sensitive and specific (Pelinka et al, 2003) and others showing 1999; Puc et al, 2002; Ryu et al, 2003). The specificity of
it to be less accurate (Kalliafas et al, 1998). US is widely avail- hepatobiliary scintigraphy can be improved by administering
able and easy to use, even in acutely ill patients, because it can morphine to cause constriction of the sphincter of Oddi and
be performed at the bedside, and it is inexpensive. US should improve gallbladder filling (see Chapter 17). This maneuver
be performed as the initial imaging modality for suspected decreases the incidence of false-positive studies and improves
acalculous cholecystitis. specificity, but it does not result in improvements in sensitivity
Evaluating the natural history of abnormalities visualized on compared with conventional scintigraphy (Cabana et al, 1995;
US in acutely injured patients is problematic; a prospective trial Flancbaum et al, 1989; Kalliafas et al, 1998).
Treatment
The definitive treatment for acalculous cholecystitis is chole-
cystectomy, which can be performed laparoscopically in most
cases. In patients who are critically ill, placement of a percuta-
neous cholecystostomy tube allows decompression of the gall-
bladder and drainage of contained, infected bile (see Chapter
34); this allows time for the patient to recover from the acute
illness before considering proceeding with cholecystectomy
(Akyürek et al, 2005; McClain et al, 1997). Percutaneous cho-
lecystostomy may be the definitive treatment for acalculous
cholecystitis because there is no chronic obstruction of the
gallbladder outlet as in acute cholecystitis (Davis et al, 1999;
Vauthey et al, 1993) (see Chapters 28 and 32).
COMPLICATIONS OF CHOLECYSTITIS
Gangrenous Cholecystitis
FIGURE 33.4. Ultrasound of a patient with acalculous cholecysti- Gangrenous cholecystitis is a more common finding in diabetic
tis reveals marked thickening of the gallbladder wall (arrows). patients with acute cholecystitis who present with a leukocytosis
562 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
Emphysematous Cholecystitis
Emphysematous cholecystitis is a rare entity that results from
the presence of gas-forming bacteria in the bile. Emphysema-
tous cholecystitis may be seen in association with acute or
gangrenous cholecystitis, and it is more common in men and
patients with diabetes (Tellez et al, 1999). The diagnosis occa-
FIGURE 33.6. Computed tomography scan (noncontrast) in a
sionally can be made by simple abdominal radiographs, but
patient with emphysematous cholecystitis showing gallbladder
more often it is diagnosed on US (Fig. 33.5) or CT scan (Fig.
filled with air.
33.6)(Bennett & Balthazar, 2003; Gill et al, 1997; Konno et al,
2002). Patients should receive IV antibiotics to include coverage
for Clostridium species, followed by emergent cholecystectomy. any stones may be all that is possible and usually resolves the
condition. In the acute setting, the biliary obstruction often
Mirizzi Syndrome resolves after cholecystectomy and resolution of the inflamma-
Mirizzi syndrome is defined as biliary obstruction secondary to tory process. In some cases, however, the chronic inflamma-
cholecystitis. It occurs in 0.3% to 3% of patients undergoing tion leads to fistulation from the gallbladder to the bile duct,
cholecystectomy (Lai & Lau, 2006). An impacted stone in the or a biliary stricture results, both of which will complicate the
gallbladder infundibulum or cystic duct can compress the bile operative procedure and may require biliary reconstruction
duct, usually at the level of the common hepatic duct (type I), (see Chapter 42).
or a stone can erode from the gallbladder or cystic duct into
the common hepatic duct, resulting in a cholecystocholedochal Cholecystoenteric Fistula
fistula (type II). Patients are seen with symptoms of acute Cholecystoenteric fistula, or perforation of the gallbladder into
cholecystitis but with the additional finding of hyperbilirubine- an adjacent hollow organ, is a rare complication of acute cho-
mia and elevated alkaline phosphatase. A laparoscopic approach lecystitis. The duodenum and the transverse colon are the most
to this condition has been shown to result in high conversion common sites of fistulation, which results in decompression of
and complication rates and is generally not recommended the gallbladder and may result in brief symptomatic improve-
(Antoniou et al, 2009; Lai & Lau, 2006). Open cholecystec- ment. This complication occurs most frequently in women in
tomy is the gold standard for treatment when this condition is their sixth to seventh decades and has been shown to be associ-
identified preoperatively. If inflammation has obliterated the ated with Mirizzi syndrome or an additional hepatobiliary
triangle of Calot, a partial cholecystectomy with removal of abnormality such as gallbladder cancer (Beltran et al, 2008;
A. Gallstones and Gallbladder Chapter 33 Cholecystitis 563
Chowbey et al, 2006; Costi et al, 2009). Contamination of the concomitant Mirizzi syndrome should be considered. Patients
biliary tree by enteric organisms may result, and patients may with gallstone ileus require removal of the obstructing stone
be seen with cholangitis and pneumobilia. Approximately 10% via enterotomy (Chowbey et al, 2006), and it is important to
to 15% of patients with cholecystoenteric fistulae will pass perform a thorough examination of the bowel for any other
gallstones into the small intestine and be seen with small bowel stones. Fistula takedown and cholecystectomy can be performed
obstruction, termed gallstone ileus. In patients with cholecysto- at the same procedure or at a second, delayed procedure if the
colonic fistula, chronic diarrhea is the most common presenting patient is too unstable to tolerate a prolonged initial operation,
symptom in nonemergent cases (Costi et al, 2009). or if the pericholecystic inflammation is so severe as to make
Patients with cholecystoenteric fistula require cholecy initial cholecystectomy unsafe.
stectomy with takedown and closure of the fistula. When cho-
lecystoenteric fistula is encountered at the time of surgery, References are available at expertconsult.com.
A. Gallstones and Gallbladder Chapter 33 Cholecystitis 563.e1
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Saber A, Hokkam EN: Operative outcome and patient satisfaction in in acute acalculous cholecystitis, World J Gastroenterol 9:2821–2823,
early and delayed laparoscopic cholecystectomy for acute cholecys- 2003.
titis, Minim Invasive Surg 2014:162643, 2014. Warren BL: Small vessel occlusion in acute acalculous cholecystitis,
Savoca PE, et al: The increasing prevalence of acalculous cholecystitis Surgery 111:163–168, 1992.
in outpatients: results of a 7-year study, Ann Surg 211:433–437, Werbel GB, et al: Percutaneous cholecystostomy in the diagnosis and
1990. treatment of acute cholecystitis in the high-risk patient, Arch Surg
Schirmer BD, et al: Laparoscopic cholecystectomy: treatment of choice 124:782–786, 1989.
for symptomatic cholelithiasis, Ann Surg 213:665–676, 1991. Wong SK, et al: Percutaneous cholecystostomy and endoscopic chole-
Siddiqui T, et al: Early versus delayed laparoscopic cholecystectomy cystolithotripsy in the management of acute cholecystitis, Surg
for acute cholecystitis: a meta-analysis of randomized clinical trials, Endosc 13:48–52, 1999.
Am J Surg 195(1):40–47, 2008.
Singhal T, et al: Laparoscopic subtotal cholecystectomy: initial experi-
ence with laparoscopic management of difficult cholecystitis, Surgeon
7(5):263–268, 2009.
CHAPTER 34
Percutaneous treatment of gallbladder disease
Jad Abou Khalil, George Zogopoulos, and Jeffrey Stewart Barkun
OVERVIEW and illustrate some of its technical aspects and potential com-
plications. We will place a particular emphasis on the quality of
The first reports of an operative cholecystostomy are attribut- the evidence available in the literature and propose guidelines
able to Johannes Fabricius (1618) and Stalpert Von Der Wiel for the management of patients considered for PC.
(1667), who described the procedure as occurring almost by
happenstance (Hardy, 1993). The following two centuries only
revealed further sporadic reports, until Marion Sims, an Ameri- INDICATIONS AND CONTRAINDICATIONS FOR
can surgeon in Paris, performed a clearly intentional cholecys- PERCUTANEOUS CHOLECYSTECTOMY
tostomy in 1878. Bobbs had previously performed an inadvertent
kitchen-table cholecystostomy. Kocher and Tait (Traverso, Acute Calculous Cholecystitis in High-Risk Patients
1976) formalized the procedure in 1878, many months after Despite its prevalent use, there is a dearth of data from high-
Sims but independent of his efforts. quality clinical trials to support the use of PC in patients with
At a time when cholecystectomy (see Chapter 35) became acute calculous cholecystitis (ACC) who also have significant
the gold standard for the management of most acute gallblad- medical comorbidities (see Chapter 33). Despite this lack of
der diseases, operative cholecystostomy remained an attractive supporting data, this procedure is relatively common. In reviews
alternative in situations of significant patient comorbidity or of surgical databases, patients who receive PC are demonstrably
intraoperative risk, often as a bridge to cholecystectomy (Glenn, older and have greater medical comorbidity than those receiv-
1977; Skillings et al, 1980). ing LC (Anderson et al, 2013; Smith et al, 2013).
The first description of an ultrasound-guided percutaneous A systematic review of cohort studies comparing PC with
cholecystostomy (PC) for acute cholecystitis followed the open and/or LC for ACC identified 53 studies examining the
development of percutaneous biliary drainage for the manage- question; however, differences in outcome reporting, biases in
ment of obstructive jaundice and dates back to 1980 (Radder, control selection, and significant heterogeneity of study popula-
1980; van Sonnenberg et al, 1992). Early case series showed tions made it impossible to draw conclusive recommendations
encouraging results in patients who were not candidates for on clear indications in high-risk surgical patients (Winbladh
open cholecystectomy (Eggermont et al, 1985), and ensuing et al, 2009). The review confirmed that mortality rates after PC
cohort studies popularized its use in circumstances in which are high (15.4% vs. 4.5% with cholecystectomy). Aside from
cholecystectomy was not feasible. The popularity of this pro- the obvious selection bias, this rate of mortality is also likely
cedure has persisted into the laparoscopic era. In the absence inflated by the high mortality in early cohorts. The review
of comparative data, PC has supplanted open and laparoscopic reported a combined mortality following PC of 22.1% and
alternatives to cholecystostomy and become widely accepted as 13.3% in cohorts before and after 1995, respectively (P <.001).
a treatment for cholecystitis in situations in which surgical In one of the only matched studies comparing PC and
intervention is not feasible or deemed too risky (Fig. 34.1). A LC, Smith and colleagues (2013) reported a single-institution
review of nationwide medicoadministrative data shows that the retrospective analysis during two time periods: 1989-1998
number of PCs performed in the United States for all indica- and 1998-2009 (143 vs. 286 PC and LC, respectively). Patients
tions has increased sixfold between 1994 and 2004. The vast were matched for time period alone rather than any clinical
majority of PCs, 97% in that time period, have been performed patient factor. The authors demonstrated changing trends
by interventional radiologists (Duszak & Behrman, 2012) (see in the characteristics of patients receiving PC for acute chole-
Chapter 30). An examination of the National Inpatient Sample cystitis: From 1989-1998, 100% of patients were American
database shows that between 1998 and 2010, 1.5% of calculous Society of Anesthesiologists (ASA) 3 and 4, whereas from
and 7.5% of acalculous cholecystitis in the United States were 1998 to 2009, that proportion dropped to 82%. The use of PC
treated with PC (Anderson et al, 2013) rather than by open or in patients with ASA scores of 1 and 2 is therefore increasing
laparoscopic cholecystectomy (LC). with time.
In addition to its use for the management of acute cholecys- A retrospective cohort comparing 51 patients undergoing
titis, the PC technique also provided its early practitioners with PC with 151 undergoing LC for ACC and acute acalculous
the opportunity to investigate the management of gallstone cholecystitis (AAC) within the Veteran’s Affairs Boston Health
disease nonsurgically by chemical dissolution, mechanical System demonstrated again that patients selected for PC were
extraction, or lithotripsy of gallbladder calculi (van Sonnenberg older, had higher Charlson Comorbidity Index (CCI) scores,
et al, 1990, 1992). However, these approaches are not curative ASA classifications, white blood cell counts, and alkaline phos-
and have largely been abandoned due to the high rate of recur- phatase levels. The authors performed a multivariate logistic
rence of cholecystitis and the superiority of LC. In this chapter, regression and demonstrated that high CCI was the only inde-
we will examine the indications and contraindications for PC pendent predictor of receiving a PC.
564
A. Gallstones and Gallbladder Chapter 34 Percutaneous treatment of gallbladder disease 565
A B
FIGURE 34.1. Computer tomography–guided percutaneous cholecystostomy for acute acalculous cholecystitis in a patient with severe arterioscle-
rosis and ischemic heart disease. A, Percutaneously placed drainage catheter. B, Pigtail catheter in the gallbladder. The gallbladder wall is thickened,
and there is hyperdense sludge within the gallbladder.
Only two randomized studies examining the use of PC in the proportion of conversion to open cholecystectomy at opera-
acute cholecystitis have been published; however, they ask dif- tion. The authors did not define inclusion or exclusion criteria,
ferent questions, and both have significant methodologic limi- and no definition was provided for “a high-risk” surgical
tations. Hatzidakis and colleagues (2002) randomly assigned patient. The study was also not adequately powered to detect
123 high-risk patients (Acute Physiology and Chronic Health meaningful differences in the outcomes it compared. Further-
Evaluation [APACHE] score > 12) with ultrasound-proven more, the trial did not state how randomization was performed,
ACC or AAC to ultrasound-guided PC versus conservative lacked blinding or allocation concealment, and analysis was
medical therapy (63 and 60 patients, respectively). In this trial, performed strictly per-protocol despite the high drop-out rate.
ultrasound-guided PC was unsuccessful in 5% of patients who Such methodologic shortcomings make it difficult to make
had to undergo computed tomography (CT)-guided PC. Early recommendations based on this study.
in the series, the investigators used a nephrostomy tube instead A Cochrane Collaboration Systematic Review (Gurusamy
of a more secure pigtail catheter, resulting in a 15% (9/63) rate et al, 2013) on the use of PC in high-risk patients with ACC
of tube dislodgment, with 3 (5%) patients requiring operative identified the aforementioned two randomized trials (Akyürek,
intervention. These 3 patients all had a transperitoneal route 2005; Hatzidakis et al, 2002), grading their quality as very low
of entry. Only 3 (5%) of the PC patients required cholecystec- and their risk of bias as very high. The group was unable to
tomy within 30 days of failure of PC to control symptoms. The generate a recommendation on the usefulness of PC compared
authors were unable to demonstrate a difference in symptom with conservative therapy, calling for higher-quality random-
resolution after 3 days or in 30-day mortality and concluded ized trials. The largest multicenter randomized trial to date, the
that PC was indicated if symptoms failed to resolve after 3 days CHOCOLATE trial, has published its protocol but is currently
of conservative medical management. The study, however, had still recruiting (Kortram et al, 2012).
significant methodologic flaws. There was no power analysis, In conclusion, despite the absence of convincing high-level
no measures taken to conceal allocation, and no attempt to evidence, and based mainly on retrospective unmatched
blind the investigators, the patients, or the care providers. cohorts, PC is frequently recommended for patients with ACC
Moreover, an evolving procedural learning curve within the who do not respond to medical therapy and who are deemed
study period makes PC appear more morbid than it likely is in unfit for surgery due to age or medical comorbidity.
more experienced hands. The second randomized trial by
Akyürek and colleagues (2005) randomly assigned 70
Acute Calculous Cholecystitis With
ultrasound-proven AAC patients to PC, followed by early LC Delayed Presentation
3 to 4 days later (37 patients), compared with conservative PC, followed by interval LC, has been used in the specific
management and delayed LC 8 weeks following recovery (33 context of ACC late in the course of the disease, hoping that
patients). The investigators aimed to compare hospital length conversion to open cholecystectomy would be less than during
of stay, cost, and treatment success. Treatment success was LC at the index presentation (see Chapters 33 and 35). This
defined as resolution of signs and symptoms of cholecystitis, as was the subject of a retrospective cohort study of ASA one half
well as a decrease in white blood cell count. Six of 37 patients patients seen with ACC after more than 72 hours of symptoms
in the PC group did not go on to have early LC because they and not responding to nonoperative treatment for 48 hours. It
persistently had an APACHE score greater than 12 for 120 compared PC with delayed LC 4 weeks later (48 patients) to
hours after PC. Three of 33 patients in the delayed LC group LC (43 patients). The authors found a lower frequency of
were excluded—1 because of death from sepsis and 2 because conversion to open surgery, shorter hospital stay, and fewer
of refusal to undergo LC. In this study, PC followed by early total complications with PC and delayed LC (40% vs. 19%;
LC decreased hospital length of stay and costs compared with P = .029 in the early LC vs. early PC and delayed LC group)
delayed LC after conservative management but did not decrease (Karakayali et al, 2014). The main methodologic limitation of
566 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
A B
C
FIGURE 34.2. Percutaneous transhepatic cholecystostomy for acute acalculous hemorrhagic cholecystitis. After an initial gallbladder puncture
under ultrasound guidance with a 22-gauge needle, the procedure was continued under fluoroscopic control. A, Direct cholecystography showed
a large filling defect in the infundibulum of the gallbladder. B, The 22-gauge access was converted to a larger caliber, and a guidewire was introduced
into the gallbladder. A 6.5-Fr self-retaining pigtail catheter was placed in the gallbladder lumen. There was no opacification of the cystic duct at the
time of the initial procedure. C, Repeat cholangiography was done 1 week after emergency cholecystostomy. The cystic duct was patent, and there
was unimpeded flow of contrast material into the duodenum. Most of the debris within the gallbladder had disappeared. The cholecystostomy
catheter was removed 1 week after cholecystostomy; elective cholecystectomy was not required.
the study was selection bias: It is unclear how patients in the trend toward higher 30-day mortality in the PC group (13%).
early cholecystectomy group were selected, and no attempt was The deaths in the PC group were due to advanced cancer,
made at multivariate adjustment for baseline differences illustrating the significant selections bias that went into treat-
between the groups. Zehetner and colleagues (2014) compared ment attribution, a bias that remains uncorrected by matching
23 patients with ultrasound-confirmed ACC presenting more on basic demographic characteristics. It is also difficult to draw
than 72 hours after symptom onset and treated with PC with a statistically sound conclusion from such a small sample size.
controls treated by LC. The authors pair-matched patients for
age, sex, race, body mass index, diabetes, and sepsis. Contrary Acute Acalculous Cholecystitis in High-Risk Patients
to the previous study, the authors demonstrated increased The use of PC in high-risk patients with AAC is supported by
length of hospital stay (LOS) with PC and no difference in many cohort studies demonstrating decreased morbidity and
major morbidity; however, there was a significant proportion of mortality when compared with LC or open cholecystectomy
conversion to open surgery in the no-PC group (17%) and a (OC) (Simorov et al, 2013) (Fig. 34.2). However, when
A. Gallstones and Gallbladder Chapter 34 Percutaneous treatment of gallbladder disease 567
compared with conservative medical therapy, different studies mortality or serious morbidity. These case reports and case
reach different conclusions, with some large studies showing no series suggest that PC is feasible during pregnancy and may be
benefit attributable to PC (see Chapter 33). used as a safe alternative to operative intervention after failure
An examination of 43,341 patients with AAC and severe of medical management in the first or third trimesters.
sepsis or shock within the California Office of Statewide Health
Planning and Development Patient Discharge Database (1995- Sepsis of Unknown Origin in the Intensive Care
2009) demonstrated that patients undergoing PC had the In the critically ill patient with persistent sepsis of unknown
greatest number of comorbidities and were the sickest. However, origin, PC affords a safe and rapid therapeutic intervention in
no improvement in survival was associated with PC versus the event of suspected AAC or ACC, and it can be used to
medical management after extensive multivariate adjustment exclude the gallbladder as the septic focus. Two case series
(Anderson et al, 2014), and this remained true even in the describe such an approach: In 24 (Lee et al, 1991) and 82
subgroup of patients with severe sepsis or shock and those patients (Boland et al, 1994), cholecystostomy resulted in reso-
dependent on mechanical ventilation. In fact, patients seemed lution of sepsis in 58% and 51% of patients, respectively. These
to fare best when they could undergo cholecystectomy alone or case series were, however, not followed by controlled trials.
treated with PC followed by cholecystectomy. The study did Moreover, it is possible that the incidence of AAC was higher
not consider short-term outcomes, length of stay, symptom compared with contemporary practice due to different intensive
control, and quality-of-life measures. This large study of medi- care practices, such as prolonged enteric starvation. We postu-
coadministrative data is the strongest evidence that PC might late that “diagnostic PC” has less utility in the modern intensive
not offer a mortality benefit over medical management in care setting.
patients with AAC who are deemed unfit for surgery.
An analysis of 58,518 patients with AAC from another med- Conclusion
icoadministrative database, the National Inpatient Sample PC should be reserved for patients who are not medically fit to
(Anderson et al, 2013), demonstrated that, after multivariate undergo open or LC (Abi-Haidar et al, 2012). It may be used
adjustment (for sex, age, race, Charlson index, and hospital as a bridge to cholecystectomy in patients failing medical
teaching status), PC remained associated with increased odds therapy for ACC and not fit for surgery at the time of presenta-
of death, increased length of stay, and decreased odds of tion, and it can be used as definitive therapy in patients with
gallbladder-specific and total complications, indicating that in AAC.
both ACC and AAC its use was reserved for selected patients.
The study did not compare PC with nonoperative manage- TECHNICAL ASPECTS AND COMPLICATIONS
ment, and there is no doubt that residual statistical confound-
ing is a concern in such large retrospective databases. Insertion Technique
Therefore whether or not PC in critically ill patients with 1. Drainage versus aspiration: Drainage has been demonstrated
ACC offers a survival advantage over the absence of gallbladder- to be superior to simple aspiration of the acutely inflamed
directed interventions remains unclear, as our knowledge is gallbladder in a single randomized trial (Ito et al, 2004) and
derived from retrospective cohort studies with varying degrees is currently most widely used.
of risk adjustment and significant residual confounding 2. Operator: Most commonly, PC is performed by radiologists
(Mansour & Yopp, 2014). (Duszak & Behrman, 2012) (see Chapter 30) under ultra-
sonographic guidance, but a single publication reports on a
Special Populations series performed by surgeons (Silberfein et al, 2007), with
Pregnancy acceptable results and improved access times, although this
Although the safety of LC is well established in the second experience may not be generalizable to most institutions.
trimester (Lu et al, 2004; Swisher et al, 1994), most surgeons Either way, it is advisable that only individuals highly facile
are reluctant to operate in the first and third trimesters due to with ultrasonographic or CT-guided interventional tech-
fear of spontaneous abortion and preterm labor, respectively. niques perform PC and that there be regular institutional
PC may thus provide a safe temporizing measure for pregnant quality monitoring, according to proposed procedure-
patients seen with severe biliary colic or cholecystitis in the first specific quality-control benchmarks (Saad et al, 2010).
and third trimester who fail conservative medical therapy. The 3. Approach: Patient preparation consists of skin disinfection
evidence to support this approach is scarce, and no large cohort and standard sterile precautions, procedural sedation, and
or controlled trials has examined this question. Two small either prophylactic administration or ready availability of
studies have reported the feasibility and safety of PC in preg- atropine, as vagal reactions have been documented (Little
nancy for acute cholecystitis and biliary colic in a limited et al, 2013). PC is performed under direct ultrasound or CT
number of patients. Allmendinger and colleagues (1995) pub- guidance, with equivalent success and complication rates
lished a case report of two pregnant patients who underwent (Loberant et al, 2010). After the planned anatomic course
PC for cholecystitis at 30 and 32 weeks of gestation, respec- is identified, the gallbladder is entered using a finder needle,
tively, followed by elective cholecystectomy in the postpartum and a guidewire is inserted into it, with a size 7- to 10-Fr
phase. Chiappetta Porras and colleagues (2009) described a pigtail catheter inserted over the guidewire using a Seldinger
cohort of 122 (Technical Aspects and Complications) for biliary technique. Other catheters, such as a central venous cathe-
colic in the first trimester, four cholecystostomies in the first ter, can be used in lieu of a pigtail catheter and may be of
trimester for cholecystitis, and four gallbladder aspirations in use in certain institutional settings, but data on catheter
the third trimester (three for biliary colic and one for cholecys- displacement and patency times with these other options
titis.) In this series, patients seen with biliary disease were are limited (Park et al, 2005). A catheter placed by transhe-
treated exclusively with LC, with no reported fetal or maternal patic access is preferred to the transperitoneal route. The
568 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
transhepatic tract matures faster than the transperitoneal 22% at 1 year but also a 1 year mortality of 37% following
tract (2 weeks vs. 3 weeks, respectively), allowing faster index admission, mainly from medical causes unrelated to gall-
removal of the catheter as well as less bile leaks and stone disease (Sanjay et al, 2013). Although cholecystectomy
bile peritonitis (Hatjidakis et al, 1998). The transhepatic may be desirable after PC for ACC, a review of a large medi-
approach is safer because it avoids the peritoneum in patients coadministrative database demonstrates that PC is, in fact, only
with significant ascites or bowel interposition (Ginat & Saad, followed by elective cholecystectomy in 40% of patients at 1
2008). However, it is associated with the potential for pneu- year, whereas an additional 18% die without undergoing cho-
mothorax, bleeding, and hemobilia (van Sonnenberg, 1990). lecystectomy (de Mestral et al, 2013). It is therefore prudent
to weigh the risk of interval LC with the patient’s concurrent
Complications medical comorbidities, evolving surgical risks, and life expec-
In experienced hands, PC has both a high technical success rate tancy against the risk of recurrence and ensuing morbidity and
(>98.9%) (Winbladh et al, 2009) and a low complication rate. mortality.
This includes hemorrhage (2.5%), pneumothorax (0.5%), and
postprocedural catheter dislodgement (<1%) (Saad et al, PERCUTANEOUS TREATMENT OF GALLSTONES:
2010). Following catheter withdrawal, 3% of patients experi- TECHNIQUES OF HISTORIC INTEREST
ence severe bile peritonitis, and another 3% experience a mild
symptomatic biliary leak (Wise et al, 2005). Bile leaks are asso- Many techniques have been developed in an attempt to avoid
ciated with transperitoneal access (Sanjay et al, 2013) and may the need for elective cholecystectomy. The 1980s saw the rise
require operative therapy or repeat PC. In a systematic review in popularity of extracorporeal shock-wave lithotripsy (ESWL),
of 35 papers, displacement of the PC catheter was reported in which in association with oral bile salt therapy, promised to
8.57%; however, this may be an underestimation in an outpa- clear the gallbladder of gallstones without resorting to surgery.
tient population (Winbladh et al, 2009). In the cohort described However, its use was limited to patients with less than three
by Smith and colleagues (2013), catheter-related complications cholesterol stones of size 2 cm or less, and it required multi-
occurred in 14.5% of patients, including tube dislodgement in ple treatments over months. The proportion of patients with
10 of 143 (7%), extra-abdominal peritube bile leak in 7 of 143 recurrent cholelithiasis at 6 years was 69%, making ESWL an
(5%), pain in 4 of 143 (3%), and occlusion in 4 of 143 (3%). unacceptable option for most patients (Cesmeli et al, 1999).
These complications were managed mostly with tube reposi- Moreover, it has been proven to not be a cost-effective
tioning or upsizing, and none required operation. approach (Barkun et al, 1997), and its use has been largely
abandoned.
Management of the Percutaneous Cholecystectomy Methyl tert-butyl ether (MTBE), a cholesterol solvent, has
Catheter and the Gallbladder been used to dissolve gallbladder calculi after the placement of
As already stated, the catheter tract usually matures after 2 a PC. However, its use is cumbersome, requires specialized
weeks for transhepatic catheters and after 3 weeks for transperi- equipment and tubing that will not be destroyed by MTBE, as
toneal drains. A cholecystogram can be obtained prior to well as a bothersome, prolonged administration over many days
removal of the catheter 3 to 6 weeks after insertion, but imaging (Thistle et al, 1989). Its use is mainly of historic interest.
is not necessary in cases where a small-bore catheter was placed A publication has suggested the use of PC as an adjunct to
and where the cystic duct was patent at insertion. In AAC, cystic duct stenting in patients deemed unfit for LC (Elmunzer
assuming the resolution of precipitating factors, PC is consid- et al, 2011). Only four patients were described in this study,
ered curative, and LC is usually not necessary. There remains and no information on long-term patency of this technique was
a debate as to whether PC can be considered curative after described. A small series has described the feasibility of endo-
ACC (Chung et al, 2012). Recurrence rates of cholecystitis scopic ultrasound-guided transduodenal drainage of the gall-
after PC in ACC without interval cholecystectomy vary between bladder; however, this experience has not been reproduced to
studies: from 4.1% at 1 year in one study (Li et al, 2013) to date (Lee et al, 2007).
11.7% at 38 months in another (Chang et al, 2014). A cohort
from the United Kingdom shows a recurrence rate as high as References are available at expertconsult.com.
A. Gallstones and Gallbladder Chapter 34 Percutaneous treatment of gallbladder disease 568.e1
569
570 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
Gallbladder Laparoscope
Liver
A
A B
FIGURE 35.1. Positions for insertion of trocars during laparoscopic cholecystectomy. The laparoscope (A) is positioned in the periumbilical region,
the graspers for gallbladder retraction (B) and manipulation (C) are positioned in the RUQ along the subcostal region, while the subxyphoid region
(D) is used for the dissector, diathermy, and clip appliers.
A. Triangle of
cholecystectomy
B. Triangle of
FIGURE 35.2. The omentum and adhesions are divided with cautery
Calot
or by carefully pulling them away with atraumatic grasping forceps
(shown here). FIGURE 35.3. A, Triangle of cholecystectomy limited by the common
hepatic duct, right hepatic duct, cystic duct, and inferior liver edge.
B, The triangle of Calot limited by the common hepatic duct, cystic duct,
trocar, and the peritoneum is opened along the gallbladder wall and cystic artery.
at the neck. This dissection is continued superiorly along both
sides of the gallbladder 1 to 2 mm from the liver edge. Medial attachments surrounding the neck of the gallbladder are dis-
retraction of the gallbladder is helpful to facilitate this dissec- sected free until only two structures remain: the cystic duct and
tion on the lateral wall. cystic artery. It may be useful to alternatively retract the infun-
Once the peritoneum is opened on the gallbladder wall, dibulum either medially or laterally to expose both sides of the
attention is then turned again to the triangle of Calot to develop gallbladder and dissect the adhesions free (Fig. 35.4). There is
a “window” of dissection and obtain the critical view of no need to continue dissection to the level of the CBD, because
safety (Strasberg et al, 1995). This technique has been widely this may only increase the risk of injury. Blunt dissection using
adopted and demonstrated to reduce the incidence of iatrogenic a Maryland grasper or a laparoscopic right-angle grasper may
bile duct injuries during cholecystectomy (Strasberg & Brunt, be performed to create a window behind the cystic duct by
2010). Using a combination of blunt dissection and cautery, all gently spreading the avascular tissue. The gallbladder is
A. Gallstones and Gallbladder Chapter 35 Technique of cholecystectomy: open and minimally invasive 573
A B
FIGURE 35.4. Proper gallbladder retraction for exposure of triangle of Calot (A) and reverse triangle of Calot (B). (Courtesy Quality Medical Publish-
ing, St. Louis, MO.)
first, and additional dissection off the cystic plate may be per-
formed to confirm the location and course of the cystic duct.
FIGURE 35.5. Critical view. Hepatocystic triangle is dissected free of Completion of Cholecystectomy
all tissue except for the cystic duct and artery, and the cystic plate on After anatomy is confirmed, the cystic artery and duct are
the liver bed is exposed. When this view is achieved, the two structures
clipped and divided. We prefer to use clips, either metallic or
entering the gallbladder can only be the cystic duct and artery.
plastic. Before each clip is secured, it is important to properly
visualize the posterior jaw of the clip applier to avoid injury to
dissected off of the liver’s edge, exposing the cystic plate. Once the surrounding structures and ensure proper deployment of the
the cystic artery and duct can clearly be identified entering the clip. The clips should not be placed too distally so that the CBD
gallbladder and only the cystic plate is seen behind these struc- is “tented up” into the clip. Occasionally, a large or inflamed
tures, the critical view of safety is achieved, and it is considered duct may hinder the ability to sufficiently secure clips across the
safe to divide the duct and artery (Figs. 35.5 and 35.6). If there entire lumen, and in these cases, an Endoloop preformed suture
is a question regarding anatomy at this time, a cholangiogram can be used on the distal cystic duct. Although used by some
may be performed. Additionally, the cystic artery may be divided surgeons, we strongly discourage the use of a linear stapler for
574 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
being introduced for these purposes and may contribute to an not be justified for routine use in simple cases due to significant
improvement in outcomes. Until that time, larger studies are cost and resource burden, performing robotic surgery on more
needed to demonstrate a true effect. straightforward cases, such as cholecystectomy, has been pro-
posed as an ideal way for surgeons to acquire experience, skill,
Single-Incision Laparoscopic Surgery and confidence (Jayaraman et al, 2009). Cholecystectomy is
Single-incision laparoscopic surgery (SILS) cholecystectomy is often the first procedure that a general surgeon attempts with
an extension of the attempt to reduce the number and size of robotic assistance. This is due to many factors, including rela-
laparoscopic ports. SILS is performed through one small trans- tive ease and frequency with which cholecystectomy is per-
abdominal incision, usually at the umbilicus, rather than the formed in the modern era and familiarity with the operation.
standard multiple trocar sites. The theoretical benefits include To date, few studies have compared robotic cholecystectomy
less pain and a better esthetic result. Similar to three-port and with the laparoscopic approach, and there are no RCTs to
two-port cholecystectomy, SILS is often assisted with needle- compare them. A recent Cochrane Review concluded that
scopic graspers and/or sutures placed on the gallbladder for although robotic cholecystectomy is safe, there are no obvious
retraction and exposure. However, no widely accepted standard benefits over laparoscopic cholecystectomy (Gurusamy et al,
technique currently exists. Because it requires the same basic 2012). This review was significantly limited by the small
skill set and instruments of a traditionally laparoscopic chole- number of trials and the high risk of systemic errors and bias
cystectomy, SILS can be readily implemented. Several specifi- within these trials.
cally designed single-port systems and instruments have now Although outcomes are no different, there is a significantly
been approved by the U.S. Food and Drug Administration. higher cost associated with robotic surgery. This is due not only
There have been several RCTs comparing SILS with either to the significant upfront cost of initially acquiring a robotic
standard- or reduced-port cholecystectomy. However, all of console (2 million US dollars), but also the cost of maintenance
these trials have relatively small numbers of patients and a low and replacement of disposable instruments. Economic analyses
overall rate of complications. The largest such trial randomly have demonstrated significantly higher costs in the robotic
assigned 200 patients to SILS or standard four-port laparo- group, both in single-institution studies as well as large national
scopic cholecystectomy. The total rate of adverse events was samples, ranging from $1730 to $8182 more than laparoscopic
not significantly different in either group, but the incidence of cholecystectomy (Breitenstein et al, 2008; Kamiński et al, 2014;
wound complications, including postoperative hernia, was Rosemurgy et al, 2015). With the recent focus on cost savings
higher in the SILS group (Marks et al, 2013). The hernia rate and responsible spending becoming more pervasive in the
in this study was 1.2% for the laparoscopic group, compared medical system, these costs may be prohibitive for all but when
with 8.4% in the SILS group (P = .03). Operative times are robotic surgery is considered absolutely necessary.
also often longer for a SILS cholecystectomy compared with a A recent trend has been to combine robotics with SILS.
standard laparoscopic approach (Marks et al, 2013; Tsimoyi- Combining the two approaches allows the robotic console’s
annis et al, 2010). Two RCTs evaluating postoperative scars improved dexterity and ergonomics to offset the inherent limi-
found improved cosmetic scores in the SILS group (Lai et al, tations in the single-site technique. The robotic platform
2011; Marks et al, 2013). is thought to improve visualization, reduce instrument colli-
Although SILS appears to be feasible and safe, patient selec- sions, and restore intuitive instrument manipulation that limits
tion is a crucial factor. The primary benefit—that of improved standard single-site surgery. Initial studies suggest that single-
cosmetic results—appears to come at the cost of increased incision robotic surgery is not only safe and effective but
wound complications and hernia rate. This trade-off must be also requires less of a learning curve than traditional SILS
thoroughly addressed with the patient during the consent (Spinoglio et al, 2012). Although initially considered in highly
process. Although other benefits are yet to be determined, the selected patients, recent data suggest that liberally applying
true safety profile is also yet to be established. It is most impor- the technique to a wider population can also be safe and effec-
tant to maintain appropriate surgical principles, including visu- tive (Svoboda et al, 2015; Vidovszky et al, 2014).
alization of the critical view of safety, regardless of the approach
used. Although four-port cholecystectomy still remains the gold CONTRAINDICATIONS
standard treatment, SILS may play a role in selected patients.
Contraindications to cholecystectomy can be considered in two
Robotic Cholecystectomy groups: contraindications to cholecystectomy and contraindica-
Robotic surgery has significantly increased in popularity and tions to laparoscopy. Absolute contraindications to operative
availability during the last decade. While technology has cholecystectomy, open or laparoscopic, include refractory coag-
advanced, both the surgical community and public have become ulopathy, inability to tolerate general anesthesia for any reason,
more aware of its existence, and robotic consoles have become and severe sepsis causing hemodynamic instability or end-
prominent at most major medical centers. Much of this has organ failure. In the latter case, considered grade III acute
arguably been driven by a combination of patient demand cholecystitis based on the 2013 Tokyo Guidelines for the diag-
and company marketing. However, the perceived benefits of nosis and management of acute cholecystitis and cholangitis,
improved visualization, ergonomics, and a gentler learning the patient may be better served by emergent gallbladder
curve have made robotic surgery an attractive alternative to decompression via a percutaneous cholecystostomy tube (see
traditional laparoscopy for the general surgeon. Although there Chapter 34) (Mayumi et al, 2007). Once the patient is stabi-
is a paucity of data to demonstrate objective improvements in lized, an interval cholecystectomy can be considered. However,
measurable outcomes when using a robotic approach in general if the patient has diffuse peritonitis with hemodynamic instabil-
surgery, its rapid adoption is becoming more widespread. Some ity and the diagnosis is unclear, an open procedure is then
groups have recommended that although robotic surgery may recommended. Laparotomy offers the ability to confirm the
576 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
diagnosis and rapidly correct the disorder. Relative contraindi- experience, and comfort with both laparoscopic and open tech-
cations to surgery can include cirrhosis with portal hyperten- niques, as well as the patient’s anatomy and pathology. A
sion, severe cardiopulmonary disease, and pregnancy, but are surgeon whose primary experience is with open cholecystec-
ultimately at the surgeon’s discretion. tomy may more liberally convert, whereas many younger sur-
Contraindications to laparoscopy continue to decrease while geons today have only a limited experience with the open
surgeons gain expertise and technology advances. Any contra- approach and feel more comfortable using advanced laparo-
indication to open cholecystectomy would also obviously be scopic techniques to troubleshoot problems or accomplish the
considered a contraindication to laparoscopic cholecystectomy. procedure. No one attitude is correct, as long as patient safety
In the case of hemodynamic instability, pneumoperitoneum is the ultimate goal. Although conversion rates are generally
may reduce venous return and exacerbate hypotension; thus greater with less experienced surgeons, a nationwide study
laparoscopy should not be used in these situations. In addition reported a conversion rate to open procedure of 5% to 10%
to the previous, absolute contraindications unique to laparo- (Livingston & Rege, 2004).
scopic cholecystectomy are dictated primarily by the surgeon’s Primary reasons to consider a conversion include unclear
philosophy and experience and include suspicion for gallblad- anatomy, intraoperative complications, failure to progress in a
der cancer, previous abdominal operations with extensive adhe- timely manner, and pathology, including choledocholithiasis
sions, morbid obesity, and pregnancy. not amenable to laparoscopic or postoperative endoscopic tech-
Previous lower abdominal or pelvic operations rarely inter- niques (see Chapters 36 and 37). Although conversion has been
fere with cholecystectomy. Ideally, an unscarred area around considered a “complication” by some, it should be regarded as
the umbilicus is used to gain entry, but if this is not possible, mature judgement, accepting a potentially longer hospital stay
a Veress needle to the left upper or right upper quadrant can to avoid a disastrous complication. Often the complications
be a safe and effective method to insufflate the abdomen. A requiring conversion to open laparotomy are obvious, including
5 mm camera can then be inserted at this site to better evaluate massive hemorrhage, bowel perforation, or major injury to the
any adhesions that may be present along the midline. If neces- bile duct. An open procedure offers the advantage of palpation
sary, right upper quadrant or subxiphoid ports may be inserted and tactile sensation to the surgeon. This may be beneficial
next to free adhesions from the midline before a trocar and when the anatomy is unclear from inflammation, adhesions, or
camera are inserted in that position. anomalies. Although rare, the discovery of a fistula between the
biliary system and bowel may require laparotomy for definitive
Cirrhosis management.
Cirrhosis is considered by many to be a contraindication to at
least laparoscopic cholecystectomy, and possibly to cholecys- OPEN TECHNIQUE
tectomy in general (see Chapter 77). This is due to concerns
over the ability to retract a heavy, friable liver, and the risk of Incision
coagulopathy. A recent population-based study demonstrated The traditional incision used during an open cholecystectomy
that the laparoscopic technique is well tolerated by patients is a right subcostal or Kocher incision. This incision is made 2
with cirrhosis and associated with significantly lower rates of cm below the costal margin and generally extends from the
infection, bleeding, transfusion, liver failure, and overall mor- midline to the edge of the rectus muscle laterally. The length
tality compared with an open procedure, making it the proce- of the incision should be tailored to the exposure required and
dure of choice for cholecystectomy (Chmielecki et al, 2012). A body habitus of the patient. The incision is carried down to the
meta-analysis also demonstrated that the laparoscopic tech- anterior fascia. The rectus muscle is divided with cautery,
nique is preferred in Child’s A and B cirrhotics, with a shorter ensuring appropriate hemostasis by any perforating vessels in
hospital stay and fewer overall postoperative complications the muscle. The posterior rectus sheath is incised, and the
compared with an open technique (de Goede et al, 2013). To abdomen is entered
successfully perform a cholecystectomy in a patient with cir-
rhosis, any coagulopathy should be reversed before surgery. Exposure and Placement of Retractors
Careful attention should be made to observe for any aberrant Exposure during open cholecystectomy is paramount to per-
portosystemic venous collateralization, either in the liver bed, forming the procedure adequately and safely. The round
porta hepatis, or even in the abdominal wall. Liberal use of ligament is divided between ties or, occasionally, with an
hemostatic agents can be used, and energy sources, including energy-sealing device near the anterior abdominal wall. The
the argon beam cautery should be readily available if needed. falciform ligament is incised with cautery for several centime-
If bleeding is unusual or cannot be controlled laparoscopically, ters superiorly to further facilitate exposure. A circular plastic
prompt conversion to an open procedure should be performed. wound edge protector can be inserted and has been demon-
Once the procedure is complete, attention should be placed to strated in RCTs to prevent wound infections (Mihaljevic et al,
carefully ensure that all incision closures are made watertight 2014). A major retractor such as a Thompson- or Bookwalter-
to minimize postoperative ascitic leak (Poggio et al, 2000). type retractor is then attached to the operating room table and
properly set up.
CONVERSION TO OPEN Two abdominal wall retractors are placed on the superior
edge of the incision, one medially and one laterally, and secured
Although laparoscopy is the preferred approach in the majority to the retractor system. Moist sponges are used to pack the
of patients, there are many situations the surgeon may encoun- bowel out of the operative field inferiorly, and additional packs
ter that necessitate conversion to an open procedure. The placed behind the liver often help elevated the gallbladder into
choice and timing of intraoperative conversion to open depends the field for easier dissection. A large malleable retractor may
on a variety of factors and are often based on the surgeon’s skill, be placed on the sponge to maintain this exposure, but it is not
A. Gallstones and Gallbladder Chapter 35 Technique of cholecystectomy: open and minimally invasive 577
always needed in a small patient. An additional retractor is then Once all the avascular attachments are dissected in this area
placed on the undersurface of the liver to the left of the gallblad- and only two structures are seen going into the gallbladder with
der to retract the liver edge out of the way and bring the porta the cystic plate behind, the critical view is confirmed. The cystic
hepatis into view. duct is then palpated to evaluate for stones and “milked” back
into the gallbladder (Fig. 35.10). The cystic artery is then
Dissection ligated and transected between sutures or clips close to the
Retrograde Cholecystectomy gallbladder wall (Fig. 35.11).
When performing a retrograde cholecystectomy, the critical If a cholangiogram is necessary, it is performed at this time
view of safety is first identified before removal of the gallbladder by placing a clip at the junction of the gallbladder and cystic
from the liver. This technique is the usual technique used duct and then opening the cystic duct via a small transverse
during laparoscopic cholecystectomy but may be more chal- incision 2 to 3 mm distally for insertion of a cholangiocatheter
lenging for a novice surgeon in the open setting without the (see Chapters 23 and 36). The cystic duct is then ligated and
magnification of laparoscopy and when exposure is difficult transected between sutures or clips. The gallbladder is then
secondary to inflammation or obesity. However, it is important dissected from its fossa by using cautery. Gentle traction is
to maintain the same principles to avoid inadvertent biliary placed to facilitate dissection. This dissection plane is kept close
injury. to the gallbladder wall while the cystic plate is left behind to
The fundus of the gallbladder is identified and grasped with avoid deeper dissection into the liver parenchyma and resultant
a Kelly or similar-type clamp (Fig. 35.9A). The peritoneum injury. In the case of acute cholecystitis, this dissection may be
overlying the infundibulum is incised. The incision is carried best done by using sharp or suction dissection. After the gall-
along anteriorly and posteriorly to exposure the cystic triangle. bladder is removed, the gallbladder fossa is inspected to ensure
Care should be made to keep this dissection close to the gall- hemostasis. Any small bleeding points are controlled with
bladder. Once the cystic duct is identified, a suture ligature can cautery. If available, the argon beam coagulator may be valu-
be passed around it and left untied to place tension on the duct able here. If there is more brisk bleeding from a lacerated area
for better exposure and to prevent any stone migration into the of the liver bed, a gauze pack should be held in place with
CBD. The cystic artery is identified as it usually lies just above constant pressure for 5 to 10 minutes. Hemostatic agents may
the cystic duct (Fig. 35.9B). The artery is dissected toward the also be used at this time. This is often sufficient to stop most
gallbladder, visualizing its termination at the gallbladder wall venous bleeding. If hemorrhage is not controlled after simple
to avoid ligating an aberrant or anterior right hepatic artery. pressure, deep hemostatic sutures can be placed with care taken
The gallbladder should be freed along the cystic plate for not to injury the right portal pedicle, which may lie in close
greater exposure and to visualize the critical view of safety. proximity at the base of the gallbladder fossa.
A B
FIGURE 35.9. A, The gallbladder is grasped with a clamp, and dissection of the cholecystectomy triangle is started. B, The cystic artery is in its
normal position, above the cystic duct.
578 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
fossa. The anterior and posterior fascial layers are then closed
separately, followed by staples or sutures on the skin.
FIGURE 35.10. Palpation reveals a stone in the cystic duct, which
may be “milked” back into the gallbladder.
Anterograde, or Fundus-Down, Cholecystectomy
In some cases, an anterograde approach may be necessary. This
technique should not be used in the presence of severe inflam-
mation obstructing visualization of the cystic duct, however.
There is still significant risk of biliary injury in these cases unless
proper visualization of the cystic duct and artery are obtained.
First, a large Kelly clamp is used to grasp the fundus of
the gallbladder. Another clamp, such as a right-angle clamp is
then used to grasp the peritoneum on the liver edge. An incision
in the gallbladder serosa is made approximately 0.5 cm away
from the liver edge by using cautery. A plane is developed
between the gallbladder wall and the cystic plate; the surgeon
should ensure not to dissect too deeply into liver parenchyma,
because this may risk injury. This plane is created medially and
laterally toward the fundus while the gallbladder is dissected
away from the fossa. Occasionally, an energy-sealing device may
be used if the peritoneal covering is edematous and excessively
vascular. Dissection is performed in a posterolateral manner to
free the gallbladder and best expose the cystic duct and artery.
The cystic artery is encountered while the dissection is contin-
ued medially toward the cystic triangle. The cystic artery is then
ligated and transected as it enters the gallbladder wall (Fig.
35.12). The infundibulum is next dissected free while it courses
down toward the gallbladder neck. Careful palpation should
identify any stones that may have migrated into the cystic or
CBDs. The cystic duct is dissected free for a length of no more
than 1 cm to avoid injury to the common hepatic or CBD. At
this point, the only attachment to the gallbladder should be the
cystic duct. Once the anatomy is confirmed, the cystic duct is
FIGURE 35.11. The cystic artery is ligated close to the gallbladder
ligated and transected between sutures or clips, and the speci-
wall.
men is removed from the field. The abdomen is closed as
described earlier.
The gallbladder can be opened and inspected on the back
table for the presence of stones, tumors, and to evaluate the PARTIAL OR SUBTOTAL CHOLECYSTECTOMY
cystic duct. A drain is rarely necessary after an uncomplicated
cholecystectomy, but if there is concern for bile leakage, then it A severely inflamed gallbladder may be encountered at the time
may be left postoperatively, positioned close to the gallbladder of operation that limits the ability to safely achieve the critical
A. Gallstones and Gallbladder Chapter 35 Technique of cholecystectomy: open and minimally invasive 579
view of safety (see Chapter 33). Fibrosis or inflammation may the case or after the gallbladder has been inadvertently injured
cause the surgeon to mistake the CBD for the cystic duct (Fig. or entered. In these cases, a partial or subtotal cholecystectomy,
35.13). In these cases, the surgeon is urged not to proceed in which a portion of the gallbladder is removed and gallstones
boldly but instead to err on the side of caution. Cholecystitis extracted while the posterior wall is left behind, is the procedure
can often be managed safely until inflammation has had a of choice for source control and surgical management.
chance to subside, but bile duct injuries have the potential to This approach can be used during either open or laparo-
cause significant long-term harm or even death. If the difficulty scopic surgery, and the technique is similar. The gallbladder is
of the operation and risk for injury is identified early and the drained and opened with hook diathermy at the fundus or
gallbladder has not been perforated, a cholecystostomy tube occasionally at the infundibulum. Bile, stones, and debris are
may be placed, the patient closed, and surgery may be delayed suctioned out and removed. During laparoscopy, this may be
until a period of medical management has occurred. Unfortu- facilitated by placing an Endobag to collect the contents of
nately, this is often difficult to recognize until further along in the gallbladder. The incision may need to be extended to the
gallbladder neck without dissecting the cystic duct or artery. If
this is performed via laparotomy, a finger may be inserted
into the gallbladder and be useful to guide dissection (Fig
35.14A). The anterior wall is then excised with cautery
with a small strip of the posterior wall left attached to the liver
(Fig. 35.15). The remnant mucosa can then be either removed
A B
FIGURE 35.14. A, The fundus of the gallbladder has been opened, and a finger is introduced into the gallbladder for palpation. B, Partial chole-
cystectomy. The superficial part of the fundus and body of the gallbladder has been excised, leaving in place its attachment to the liver. The remaining
mucosa is removed by curettage and/or fulgurated with electrocoagulation, and a closed-suction drain is placed near the infundibulum.
580 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
INTRAOPERATIVE PROBLEMS
Anatomic Variations
An intimate knowledge of gallbladder and biliary anatomy and
the common variations is essential to safely performing chole-
cystectomy, laparoscopic or open. Normal anatomy of the gall-
bladder and biliary system is discussed in detail in Chapters 1
and 2. Hepatobiliary anatomy can present with anomalies
and variations. Duplicated, left-sided, bilobed, or congenitally
absent gallbladder is considerably rare, predominantly identi-
fied preoperatively, and not associated with postoperative injury
or complications. Our focus instead will be on relevant biliary
anatomy and variations that can potentially lead to inadvertent FIGURE 35.16. Variations in the confluence of the cystic duct and
injury. common hepatic duct.
Significant variation of the junction between the cystic duct
and common hepatic duct can exist (Fig. 35.16). The common
hepatic duct can range in length from 1 to 7.5 cm. In 22% of
patients, the cystic duct is seen to run parallel to the common
hepatic duct for an average of 17 mm before forming the CBD
(Newman & Northrup, 1963). The cystic duct can be signifi-
cantly shortened or absent secondary to inflammation and scar-
ring from repeated bouts of cholecystitis (Dorrence et al, 1999).
This is usually not predicted or identified until at the time of
the operation.
Large series of cholangiographic studies have demonstrated
anatomic variations and congenital abnormalities of the biliary
tree in nearly half of patients (Puente et al, 1983). The cystic
duct may drain directly into the right hepatic duct or even a
low right sectoral duct (Fig. 35.17). Anomalous extrahepatic
bile ducts can occur in as many as 12% of patients, with the
most common being an anomalous right sectoral duct that
empties into either the common hepatic duct or cystic duct
(Berci, 1981). Fig. 35.18 demonstrates the common anatomic
biliary variations of the right sectoral ducts. When these varia-
tions do occur, they are often replaced ducts and represent the
only biliary drainage from the corresponding segment(s) of the
liver. Therefore if these ducts are occluded, biliary obstruction
will ensue with resultant liver atrophy and/or obstructive chol-
angitis. Ligation of the cystic duct may need to occur distal to
an aberrant duct insertion site, to preserve proper biliary drain-
age (Fig. 35.19). Although it may be suspected when encoun-
tering an anatomic anomaly during surgery, true duplication of
the cystic duct is exceedingly rare. It is essential to be aware FIGURE 35.17. High insertion of the cystic duct demonstrated on
of the common anatomic variations and have a high index of endoscopic retrograde cholangiopancreatography.
A. Gallstones and Gallbladder Chapter 35 Technique of cholecystectomy: open and minimally invasive 581
Gallbladder Perforation
Gallbladder perforation is likely the most common intraopera-
tive problem or complication encountered by most surgeons,
especially during the learning curve of cholecystectomy.
Although the leakage of bile or stones can be troublesome, it
rarely requires conversion to an open procedure. Perforation
primarily occurs either secondary to traction of forceps or from
electrocautery thermal injury. Although it is difficult to accu-
rately measure the rates worldwide, perforation may occur in
as many as one third of patients during cholecystectomy (Jones
et al, 1995). When it does occur, the loss of gallstones and their
retention in the abdominal cavity should be noted in the
description of the surgical procedure (Gerlinzani et al, 2000).
It is unclear what consequences, if any, are secondary to
FIGURE 35.18. Variations in the confluence of the extrahepatic bile gallbladder perforation during surgery. For most patients, per-
ducts and cystic duct. foration does not result in any immediate complications or
clinical difference (Jones et al, 1995; Memon et al, 1999). If
gallstones are spilled into the abdomen and not retrieved, prob-
lems may occur. Pigmented stones often harbor bacteria and
may cause postoperative infection. There are several case
reports and series of such complications, including intraab-
dominal (Horton & Florence, 1998) and abdominal wall
(Eisenstat, 1993) abscess formation secondary to gallstone
spillage during cholecystectomy. A recent prospective analysis
of clinical outcomes after accidental gallbladder spillage sug-
gests that it may cause more postoperative pain, ileus, and
infection when compared with uncomplicated cases (Suh et al,
2012).
Biliary Injury
Although fortunately quite rare, biliary injury remains one of
the most dreaded complications of cholecystectomy (see Chap-
ters 38 and 42). Not only can bile duct injury be fatal in the
short or long term, but it can cause disturbances in quality of
life and need for prolonged medical care (Cates et al, 1993;
Landman et al, 2013). Additionally, it commonly results in
litigation (Asbun et al, 1993; Perera et al, 2010). Although they
are infrequent, and designing adequate studies to evaluate
proper management and treatment can be difficult, much has
been learned about the etiology of iatrogenic bile duct injuries.
FIGURE 35.19. An aberrant duct draining directly into the cystic duct Interestingly, the majority of bile duct injuries are caused by
as demonstrated on endoscopic retrograde cholangiopancreatography. attending surgeons and are not recognized at the time of opera-
tion (Bingham et al, 2000). Injuries are more often due to
suspicion during surgery. Intraoperative cholangiogram may be misperceptions of normal anatomy than lack of knowledge,
useful in identifying or confirming abnormal biliary anatomy. skill, or judgment (Way et al, 2003). In experienced hands, the
Arterial anatomic variations are also common and can con- rate of iatrogenic biliary is likely 0.3% or less in both open and
tribute to or be the direct cause of significant morbidity if laparoscopic cholecystectomy.
injured. The cystic artery originates from the right hepatic Routine use of cholangiography was initially proposed to
artery most commonly (76%) but may also come from the left, reduce injury after the widespread and rapid adoption of lapa-
common, or proper hepatic arteries (Chen et al, 2000). A roscopic cholecystectomy was found to result in a higher inci-
double cystic artery can be found in 12% to 25% of patients. dence of biliary injuries (Fletcher et al, 1999; Flum et al,
Additionally, when the cystic artery originates from an aberrant 2003). However, risk of injury to the CBD or a segmental duct
source, it frequently traverses outside the triangle of Calot while performing cholangiography can occur if proper anatomic
(Ding et al, 2007). Although not technically an anatomic varia- identification is not accomplished. Additionally, the ability to
tion, the right hepatic artery may frequently loop onto the properly interpret the images intraoperatively can remain a
infundibulum of the gallbladder and become misidentified as challenge and lead to bile duct injury even with a reported
the cystic artery. Arterial injury may accompany bile duct injury “normal” cholangiogram (Chapman et al, 2003).
(vasculobiliary injury), with the right hepatic artery involved in The critical view of safety, as described earlier and developed
92% of cases, and can significantly add to the morbidity of the by Strasberg, remains the current standard technique to reduce
582 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
the incidence of bile duct injury during cholecystectomy. Often, a biliary injury may not be identified until postopera-
Although no level I data exist to prove that this technique defi- tively. In these cases, the surgeon must have a high index of
nitely lowers the rate of bile duct injury, a large body of evi- suspicion and make every effort to avoid a delay in diagnosis.
dence does support it (Strasberg & Brunt, 2010). Due to the Symptoms of worsening abdominal pain, fevers, and abdominal
rare frequency of iatrogenic biliary injury, a RCT proving the distention that persist for several days after surgery warrant
efficacy of this technique may not be feasible. further investigation. Initial diagnostic tests include ultrasonog-
Common circumstances that are thought to risk iatrogenic raphy and computed tomography of the abdomen. If fluid is
injury include misidentification of anatomy, a short cystic duct, seen in the gallbladder fossa, right paracolic gutter, hepatorenal
significant inflammation, previous scar or adhesions, obesity, recess, or subdiaphragmatic space, it should be percutaneously
or bleeding obscuring the field of view (Adams et al, 1993; drained and sampled. Biliary injuries have been well described
Asbun et al, 1993; Soper et al, 1993). The “classic injury” and classified by the Strasberg scheme (Fig. 35.21) (Strasberg
occurs when the CBD is mistaken for the cystic duct and et al, 1995). Evaluation of the extent of injury can be deter-
clipped, thought to occur if the cystic duct is pulled too vigor- mined with magnetic resonance cholangiopancreatography or
ously laterally, causing the cystic duct and CBD to stretch into cholangiogram via either endoscopic retrograde cholangiopan-
alignment and appear as one. If this mistake is not immediately creatography (ERCP) or percutaneous transhepatic cholangi-
identified, dissection often continues along the CBD postero- ography. A majority of simple postoperative bile leaks can be
superiorly until an “aberrant” or “duplicated” duct is encoun- managed with drainage alone or with drainage and ERCP
tered also entering toward the gallbladder. If this is then ligated, placement of a biliary stent (Kozarek et al, 1994), but more
a more proximal bile injury will then occur (Fig 35.20). complex injuries require multidisciplinary management and
If a bile duct injury is identified at the time of surgery, the may require operative repair. Repair of biliary injuries and
surgeon must make an assessment of not only the extent of biliary-enteric anastomoses are discussed in more detail else-
injury and their own ability to potentially repair it, but the where in this text (see Chapter 31).
patient’s current condition, resources of the hospital, and
the availability of specialized hepatobiliary expertise. Often, the Bleeding
most prudent action is to terminate the operation, leave a drain, The incidence of uncontrollable bleeding from laparoscopic
and close the patient with immediate referral to a specialized cholecystectomy is 0.1% to 1.9% and can occur from three
hepatobiliary center. Early referral to a specialist has been dem- distinct sites: (1) the liver, (2) arterial sources, and (3) port-
onstrated to result in better long-term outcomes (Perera et al, insertion sites. Significant bleeding from the liver bed is fairly
2011). As noted previously, if an attempt is made to forge ahead common and is now appreciated to be from the close proximity
and remove the gallbladder, there is significant risk in worsen- of the middle hepatic vein and its terminal branches, which run
ing the bile duct injury and/or creating a vascular injury (Stras- close to the gallbladder fossa in as many as 10% to 15% of
berg & Helton, 2011). patients. Major bleeding usually occurs during the final aspects
of the removal of the gallbladder from the hepatic fossa and
generally requires immediate conversion to open surgery to
control profuse hemorrhage through stitch ligation if initial
attempts at laparoscopic hemostatic control fail. Bleeding from
the cystic artery can be controlled with clips, but only if ana-
tomic landmarks can be safely confirmed. Caution must be
exercised in this setting because of a high association with right
hepatic arterial injury with injudicious placement of clips or
sutures. Significant bleeding may also first be evident postop-
3 eratively as an acute hemodynamic decline requiring resuscita-
tion, transfusions, and often reoperation. The culprit in this
2 scenario is usually a dislodged clip.
When a trocar injury to a major blood vessel is suspected,
the patient must be opened immediately without removing the
1 trocar, and the involved blood vessel must be isolated and
controlled. In contrast, if the small-bore Veress needle enters a
viscus or blood vessel, the operation generally can be com-
pleted, and the patient is monitored closely for signs of com-
plications in the postoperative period. Additionally, bleeding
may occur if a trocar lacerates a blood vessel within the abdomi-
FIGURE 35.20. Pathogenesis of the “classic” injury. 1. The common nal wall, such as the epigastric artery or one of its branches.
bile duct is mistaken as the cystic duct and is clipped and divided. 2. Before removal, each trocar should be visualized from the peri-
The dissection is carried up along the left side of the common hepatic toneal aspect by using the laparoscope. If significant hemor-
duct in the belief that this is the underside of the gallbladder. 3. The rhage is seen, it generally can be controlled with cautery or a
common hepatic duct is transected while the surgeon tries to dissect
through-and-through suture on each side of the trocar insertion
what he or she believes is the gallbladder from the liver bed. If the struc-
ture is recognized as a bile duct at this point, it is often thought to be a
site.
second cystic duct or an accessory duct. While the common hepatic
duct is divided, the right hepatic artery is often injured. (From Strasberg
Bowel Injury
SM, Helton WS: An analytical review of vasculobiliary injury in laparo- Bowel injury is a rare complication but can be potentially fatal
scopic and open cholecystectomy. HPB (Oxford) 13:1-14, 2011.) if unrecognized. It is most likely to occur at two common
A. Gallstones and Gallbladder Chapter 35 Technique of cholecystectomy: open and minimally invasive 583
A B C
>2 cm <2 cm E3
E1 E2
E4
E5
FIGURE 35.21. Strasberg classification of biliary injuries. Type A injuries are leaks from the cystic duct or small ducts in the liver bed. Type B and
C injuries almost always involve aberrant right hepatic ducts. Type D injuries are lateral injuries to the major bile ducts. Type E injuries are subdivided
according to the Bismuth classification system. (From Strasberg SM, et al: An analysis of the problem of biliary injury during laparosopic cholecys-
tectomy. J Am Coll Surg 180:101-125, 1995.)
points: during laparoscopic entry or during dissection of the indolent course, presenting with an enterocutaneous fistula,
cystic structures near the porta hepatis. Bowel injury has been standard drainage and nutritional support is appropriate.
described in approximately one to four patients in 1000 lapa-
roscopic procedures and is slightly more common with an open POSTOPERATIVE MANAGEMENT
cut-down technique than with a Veress needle, but it can occur
with both. Immediately after insufflation occurs and the The majority of patients who undergo elective laparoscopic
abdomen is entered, a brief but thorough inspection of the cholecystectomy are discharged the same day, both for patient
abdomen should be performed to ensure that no injury occurred preference and to reduce hospital costs. A patient admitted
during initial entry. All additional trocars should be placed from the clinic or emergency department with acute cholecys-
under direct laparoscopic visualization to avoid injury or per- titis is often observed in the hospital overnight postoperatively.
foration to nearby bowel. The trocar should be grasped in such Other patients who may benefit from an overnight stay include
a manner that a hand can be used as a “brake” to prevent elderly patients, those with significant comorbid illnesses, those
inadvertently introducing the trocar too far. Although some requiring substantial analgesia postoperatively, and patients
injuries may be reparable laparoscopically, conversion to open with complications. The patient is allowed a diet shortly after
should not be delayed if necessary for an adequate repair. surgery, usually beginning with clear liquids then advanced as
Another feared postoperative complication of cholecystec- tolerated to a regular diet without any specific restrictions.
tomy is that of a missed enterotomy. Severe abdominal pain Incisional and referred should pain is common. The patient is
and distention, fevers, diarrhea, persistent radiographic free air, often prescribed oral narcotics for postoperative pain control,
and, potentially, even sepsis and subsequent hemodynamic but many patients are able to recover with only over-the-coun-
instability should alert the surgeon to this serious complication. ter pain medications. It is unnecessary to prescribe a course of
These symptoms usually occur within the first 3 to 4 days antibiotics postoperatively except in unusual circumstances.
postoperatively. An immediate laparotomy is usually indicated Minimal activity restrictions are placed on the patient postop-
to diagnose and treat the condition. If the patient has a more eratively if they undergo laparoscopic surgery. Due to a risk of
584 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
hernia formation, heavy lifting is discouraged for 4 to 6 weeks operation in an ambulatory setting. Attempts at improving out-
after an open procedure. The patient may return to work once comes from laparoscopic cholecystectomy will continue to
their pain is well controlled, usually by postoperative day 2 or drive the development of novel surgical tools and techniques.
3. Routine follow-up by the surgeon in clinic can occur between Due to the relative safety and low number of complications,
1 and 4 weeks after surgery. further improvement may be difficult and much of the recent
technology has been focused on cosmetic or other ancillary
CONCLUSION improvements. These newer approaches to cholecystectomy,
including single-incision laparoscopy and robotics must be held
Cholecystectomy remains the gold standard for the manage- to the current standard of laparoscopic cholecystectomy in the
ment of gallbladder disease in the developed world, with face of growing patient and industry pressure.
the vast majority now performed minimally invasively with
excellent results. Many patients are now able to undergo this References are available at expertconsult.com.
A. Gallstones and Gallbladder Chapter 35 Technique of cholecystectomy: open and minimally invasive 584.e1
Nenner R, et al: Increased cholecystectomy rates among Medicare Steck T, et al: Prevalence and management of cholelithiasis in heart
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J Community Health 19(6):409–415, 1994. Steele RJ, et al: Introduction of laparoscopic cholecystectomy in a large
Newman HF, Northrup JD: Extrahepatic biliary tract anatomy, West J teaching hospital: independent audit of the first 3 years, Br J Surg
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Perera MT, et al: Risk factors for litigation following major transec- Steiner CA, et al: Surgical rates and operative mortality for open and
tional bile duct injury sustained at laparoscopic cholecystectomy, laparoscopic cholecystectomy in Maryland, N Engl J Med 330(6):
World J Surg 34(11):2635–2641, 2010. 403–408, 1994.
Perera MT, et al: Specialist early and immediate repair of post- Strasberg SM, Brunt LM: Rationale and use of the critical view of
laparoscopic cholecystectomy bile duct injuries is associated with an safety in laparoscopic cholecystectomy, J Am Coll Surg 211(1):132–
improved long-term outcome, Ann Surg 253(3):553–560, 2011. 138, 2010.
Pesce A, et al: Bile duct injury during laparoscopic cholecystectomy Strasberg SM, Helton WS: An analytical review of vasculobiliary injury
without intraoperative cholangiography: a retrospective study on in laparoscopic and open cholecystectomy, HPB (Oxford) 13:1–14,
1,100 selected patients, Dig Surg 29(4):310–314, 2012. 2011.
Poggio JL, et al: A comparison of laparoscopic and open cholecystec- Strasberg SM, et al: An analysis of the problem of biliary injury during
tomy in patients with compensated cirrhosis and symptomatic gall- laparosopic cholecystectomy, J Am Coll Surg 180:101–125, 1995.
stone disease, Surgery 127(4):405–411, 2000. Suh SW, et al: Accidental gallbladder perforation during laparoscopic
Puente SG, et al: Radiological anatomy of the biliary tract: variations cholecystectomy: does it have an effect on the clinical outcomes?,
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Ransohoff D, Gracie W: Treatment of gallstones, Ann Intern Med Sun S, et al: Three-port versus four-port laparoscopic cholecystectomy:
119:606–619, 1993. meta-analysis of randomized clinical trials, World J Surg 33(9):1904–
Ransohoff D, et al: Prophylactic cholecystectomy or expectant manage- 1908, 2009.
ment for silent gallstones: a decision analysis to assess survival, Ann Svoboda S, et al: Robotic single-site cholecystectomy in the obese:
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Coll Surg 217(6):1038–1043, 2013. ment of cholelithiasis in children with sickle cell disease, J Pediatr
Ros A, et al: Laparoscopic cholecystectomy versus mini-laparotomy Surg 29:209–212, 1994.
cholecystectomy: a prospective, randomized, single-blind study, Ann Tsimoyiannis EC, et al: Different pain scores in single transumbilical
Surg 234(6):741–749, 2001. incision laparoscopic cholecystectomy versus classic laparoscopic
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Rosenmüller MH, et al: Expertise-based randomized clinical trial of Tuveri M, Tuveri A: Laparoscopic cholecystectomy: complications and
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Soper N, et al: Diagnosis and management of biliary complications of Way LW, et al: Causes and prevention of laparoscopic bile duct injuries:
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Spinoglio G, et al: Single-site robotic cholecystectomy (SSRC) versus tive, Ann Surg 237(4):460–469, 2003.
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CHAPTER 36A
Stones in the bile duct: clinical features and open
surgical approaches and techniques
Kevin N. Shah and Bryan Marshall Clary
585
586 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
will pass spontaneously without incident. During the era of clinical evidence of ascending cholangitis, and bilirubin greater
open cholecystectomy, the practice of routine cholangiography than 4 mg/dL were identified as “very strong” predictors;
was common, and studies from this period demonstrated an dilated CBD on TUS (>6 mm) and bilirubin between 1.8 and
incidence of choledocholithiasis approaching 10% to 15% in 4 mg/dL were “strong” predictors; abnormal LFTs other than
patients without any clinically evident common duct involve- bilirubin, age older than 55 years, and clinical gallstone pan-
ment (Coelho et al, 1984; DenBesten & Berci, 1986; Doyle creatitis were “moderate” factors. Using these factors, patients
et al, 1982; Ganey et al, 1986; Girard, 2000; Hampson et al, are stratified into high, intermediate, and low likelihood for
1981; Lygidakis, 1983; McSherry & Glenn, 1980). This has choledocholithiasis groups. Presence of any “very strong” or
caused some to advocate for the utility of routine intraoperative both “strong” predictors leads to classification as high likeli-
cholangiography, even in patients without clinical signs of cho- hood for choledocholithiasis. Patients with no predictors are
ledocholithiasis. Proponents of a more selective approach to low likelihood, and all others are intermediate.
cholangiography, however, note that the percentage of clinically In patients identified to be at elevated risk for having CBD
significant stones is lower than the 10% to 15% of patients who stones, a thoughtful and efficient approach to subsequent
will have cholangiographic findings of CBD stones when imaging and intervention is required. TUS is the most com-
routine cholangiography is used. monly used initial diagnostic tool for suspected biliary stones
The use of selective intraoperative cholangiography in lapa- because it is noninvasive, widely available, and inexpensive (see
roscopic cholecystectomy series demonstrates similar findings Chapter 15). If CBD stones are detected, specificity is high
(Fogli et al, 2009). Collins and colleagues (2004) identified (95% to 100%); however, TUS has low sensitivity (25% to
filling defects consistent with stones in 4.6% of patients on 60%) for detection of CBD stones and is highly operator
intraoperative cholangiogram. In these patients, access was dependent (Amouyal et al, 1994; Sugiyama & Atomi, 1997).
maintained for the performance of postoperative cholangio- As mentioned previously, indirect evidence such as the pres-
grams. At 48 hours, 26% of patients had a normal cholangio- ence of gallstones or biliary ductal dilation with a CBD diam-
gram, and an additional 26% had evidence for passage of the eter greater than 6 mm in the appropriate clinical setting can
stones by 6 weeks. Twenty-two patients (2.2%) had persistent be predictive of bile duct stones.
CBD stones at 6 weeks after laparoscopic cholecystectomy and Like TUS, standard computed tomography (CT) scanning
underwent ERCP for retrieval (Collins et al, 2004). has a low sensitivity for the detection of bile duct stones and is
most useful in documenting biliary dilation or excluding mass
PREOPERATIVE DIAGNOSIS lesions as a cause of biliary obstruction (see Chapter 18).
Newer techniques of CT cholangiography use contrast agents
In the absence of clinical signs such as cholangitis or pancre- excreted in the biliary tree, which combined with high-resolution
atitis, preoperative identification of choledocholithiais typically helical scans and three-dimensional reconstructions can give
relies on serum liver function tests (LFTs) and imaging studies. accurate and detailed information about the biliary tree (Cabada
The utility of LFTs in predicting the presence of CBD stones Giadàs et al, 2002; Maniatis et al, 2003). The sensitivity of this
has been demonstrated by a number of groups (Peng et al, technique can be as high as 97%, and the specificity is 75% to
2005; Sgourakis et al, 2005). Serum bilirubin and alkaline 96% (Anderson et al, 2008; Cabada Giadàs et al, 2002; Gibson
phosphatase are typically the most commonly used laboratory et al, 2005; Kim et al, 2007; Kondo et al, 2005; Maniatis et al,
values; however, a raised γ-glutamyltransferase level has been 2003; Polkowski et al, 1999; Soto et al, 2000; Zandrino et al,
suggested to be the most sensitive and specific laboratory indi- 2005). Although these data suggest accuracy comparable to
cator of CBD stones. A value greater than 90 U/L has been magnetic resonance cholangiopancreatography (MRCP) (see
proposed to indicate a high risk of choledocholithiasis, with Chapter 19), helical CT cholangiography is limited by several
sensitivity and specificity of 86% and 74.5%, respectively (Peng issues: (1) possible allergic reactions to the contrast agents (as
et al, 2005). high as 15% in one series using intravenous iotroxate) (Gibson
When used in conjunction, clinical examination, laboratory et al, 2005); (2) suboptimal ductal contrast opacification in the
studies, and ultrasonography (typically the first-line imaging presence of significant jaundice (Polkowski et al, 1999; Soto
modality) (see Chapter 15) are sensitive in 96% to 98% and et al, 1999); and (3) limited visualization of intrahepatic duct
specific in 40% to 75% for identification of patients with cho- branches (Chopra et al, 2000; Gibson et al, 2005).
ledocholithiasis (Alponat et al, 1997; Koo & Traverso, 1996; MRCP has been the gold standard for noninvasive biliary
Trondsen et al, 1998). Liu and colleagues (2001) stratified imaging since its introduction in 1991 (Wallner et al, 1991) and
precholecystectomy patients into four groups of descending risk has been recommended by some as the preoperative modality
of choledocholithiasis based on guidelines incorporating clinical of choice for the detection of CBD stones (Hallal et al, 2005;
evaluation, serum chemistry analysis, and transabdominal Shanmugam et al, 2005; Taylor et al, 2002; Topal et al, 2003)
ultrasound (TUS). The occurrence of choledocholithiasis in (see Chapter 17). MRCP provides precise anatomic detail of
these groups (group 1, extremely high risk; group 2, high risk; the biliary tract and has a sensitivity of 81% to 100% and a
group 3, moderate risk; group 4, low risk) was 92.6%, 32.4%, specificity of 92% to 100% in detecting choledocholithiasis
3.8%, and 0.9%, respectively. Triaging patients in this manner (Hallal et al, 2005; Verma et al, 2006). The accuracy of MRCP
resulted in preoperative identification of choledocholithiasis by in diagnosing CBD stones is comparable with that of ERCP
ERCP in 92.3% of the patients who were subsequently referred (see Chapters 19 and 20) and intraoperative cholangiogram
for endoscopic clearance. Similarly, the American Society of (IOC) (see Chapter 23) (Hallal et al, 2005; Vargghese et al,
Gastrointestinal Endoscopy (ASGE) identified several predic- 2000) but may be somewhat less sensitive than endoscopic
tors of choledocholithiasis (ASGE Standards of Practice Com- ultrasound (EUS) for small stones (Verma et al, 2006). As a
mittee, et al, 2010) in their guidelines for the use of endoscopy diagnostic test, MRCP has largely replaced ERCP, once con-
in the evaluation of CBD stones. CBD stones seen on TUS, sidered the gold standard of preoperative bile duct imaging,
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 587
because the nonselective use of ERCP in all patients with sus- management (laparoscopic cholecystectomy and intraoperative
pected choledocholithiasis detects CBD stones in less than 50% cholangiogram; CBD exploration in those with CBD stones)
(Behrns et al, 2008; Petrov et al, 2008). Additionally, indis- over preoperative ERCP, followed by laparoscopic cholecystec-
criminate use of ERCP exposes over half of patients to unneces- tomy. Several prospective randomized controlled trials com-
sary procedure-related morbidity and mortality (Demartines pared these two treatment strategies (Cuschieri et al, 1999;
et al, 2000); thus ERCP is better used as therapeutic interven- Rogers et al, 2010; Sgourakis et al, 2005) and found the two
tion rather than a diagnostic one. Although MRCP is currently groups had equivalent success rates of duct clearance and
the most accurate noninvasive imaging modality for choledo- patient morbidity, but a significantly shorter hospital stay was
cholithiasis, it may miss stones smaller than 5 mm in diameter reported with the single-stage laparoscopic treatment. Cusch-
and can underestimate the number of stones detected (Varg- ieri and colleagues (1999) concluded that precholecystectomy
ghese et al, 2000). Furthermore, it is expensive when compared endoscopic clearance should be reserved for higher-risk patients
with TUS or CT, not readily available at smaller facilities, and (those with multiple comorbidities, cholangitis, severe pancre-
may not be technically feasible in obese patients or those with atitis), whereas fit patients (American Society of Anesthesiolo-
significant claustrophobia. gists categories I and II) should be treated with a single-stage
EUS has also emerged as an alternative to ERCP and MRCP laparoscopic approach.
for preoperative assessment of bile duct stones and was initially When laparoscopic CBD exploration is not part of the sur-
described around 1990 (Amouyal et al, 1989; Edmundowicz geon’s armamentarium, the decision to perform a precholecys-
et al, 1992) (see Chapter 16). The overall diagnostic perfor- tectomy ERCP should be weighed carefully because it is not
mance of EUS has been evaluated in numerous prospective without complications. Although most post-ERCP complica-
studies since then, and in two meta-analyses (Garrow et al, tions are mild to moderate in severity (Andriulli et al, 2007),
2007; Tse et al, 2008) the pooled sensitivity and specificity of the risk of severe complications, such as pancreatitis, bleeding,
EUS were 89% to 94% and 94% to 95%, respectively. Ran- infection, and perforation, need to be weighed against the likeli-
domized controlled trials have also demonstrated that EUS- hood that ERCP will find clinically relevant CBD stones.
guided ERCP can avoid unnecessary ERCP in up to two thirds ERCP has an overall complication rate of 10% and a mortality
of patients when compared with using ERCP alone for diagno- rate less than 0.5% (Cotton, 1993; Davis et al, 1997; Delorio
sis of choledocholithiasis (Petrov & Savides, 2009). Further- et al, 1995; Ponsky, 1992). Additionally, the increased financial
more, selective use of ERCP based on EUS findings resulted cost of preoperative ERCP should be considered when evaluat-
in reduced risk of overall complications and post-ERCP pan- ing its role in treatment of suspected stones.
creatitis. When taken in sum, these data suggest that the ERCP Even using criteria such as elevated LFTs and imaging find-
is best reserved as a therapeutic measure for patients with a ings, accurately predicting which patients will have clinically
high probability of CBD stones, rather than as an initial diag- relevant choledocholithiasis is difficult. Several studies have
nostic test. shown that negative ERCP was performed in 40% to 70% of
patients because most of these biochemical and radiographic
abnormalities were the result of transient biliary obstruction
TIMING AND SEQUENCE OF INTERVENTIONS secondary to stones that ultimately passed into the duodenum
(Cotton, 1993; Cuschieri et al, 1996; Delorio et al, 1995; Stain
Suspected Choledocholithiasis Prior to et al, 1991; Ponsky, 1992). As mentioned earlier in this chapter,
Cholecystectomy the ASGE published a system to grade likelihood of choledo-
In patients with suspected choledocholithiasis, selecting and cholithiasis into high, intermediate, and low likelihood groups
sequencing the most appropriate of laparoscopic, open, and based on risk factors, including LFTs, bile duct size on imaging,
endoscopic therapeutic modalities can be challenging. Prior to and presence of gallstone pancreatitis or cholangitis (ASGE
the popularization of laparoscopy, precholecystectomy endo- Standards of Practice Committee, et al, 2010). Treatment
scopic clearance of the CBD was uncommon. Several studies strategies for patients stratified to the low and high likelihood
did not reveal any morbidity or mortality advantage with pre- groups are generally agreed upon. Patients who are in the low
operative endoscopic sphincterotomy (Heinerman et al, 1989; risk for choledocholithiasis group should go directly to laparo-
Neoptolemos et al, 1988; Stain et al, 1991), and one actually scopic cholecystectomy (with or without IOC) because CBD
showed an increased rate of morbidity in patients who under- clearance is unlikely to be necessary.
went preoperative ERCP, followed by open cholecystectomy, For patients in the high-risk group, particularly those
compared with the group that was treated with single-stage needing biliary decompression for treatment of acute cholangi-
open cholecystectomy and CBD exploration (Stain et al, 1991). tis (Cuschieri et al, 1999; Leung, 2003) and in patients with
A systematic review (Martin et al, 2006) demonstrated that severe gallstone pancreatitis and evidence of persistent choledo-
open surgery resulted in less mortality, lower incidence of cholithiasis, precholecystectomy ERCP is warranted. Patients
primary treatment failure, and fewer procedures required per with multiple medical comorbidities, limited life expectancy, or
patient. Given these data, single-stage cholecystectomy and bile other issues that would make them poor surgical candidates,
duct exploration (as indicated) was the preferred approach in ERCP with endoscopic sphincterotomy (ES) and biliary
the era of open cholecystectomy. decompression can sometimes be used as the definitive man-
The advent of laparoscopy saw a rise in the popularity of agement without cholecystectomy (see Chapter 29). This strat-
preoperative ERCP CBD clearance for patients with suspected egy is not ideal for patients who are acceptable surgical
choledocholithiasis, in part because laparoscopic CBD is more candidates, however, because there is a risk of recurrent biliary
technically challenging (see Chapters 36B and 36C). For sur- symptoms if cholecystectomy is not performed. In a prospective
geons who are comfortable with laparoscopic CBD exploration, randomized trial published in 1995 by Hammarström and col-
there are some data that support a single-stage laparoscopic leagues, an expectant policy after ES was compared with open
588 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
cholecystectomy combined with CBD exploration. It was require further intervention (Roslyn, 1993). Retained calculi
reported that 20% of the patients after ES alone needed cho- occur rarely after open cholecystectomy without CBD explora-
lecystectomy during follow-up (Hammarström et al, 1995). A tion (Bergdahl & Holmlund, 1976), whereas incidence in those
prospective randomized trial of high-risk patients performed by who undergo open cholecystectomy with concomitant CBD
Targarona and colleagues (1996) comparing ES and subse- exploration is slightly higher but still reported to be less than
quent open cholecystectomy to ES alone resulted in similar 5% (Dayton et al, 1984; Kappes et al, 1982; Roslyn, 1993).
findings. They noted patients who underwent elective open Retained CBD stones occur with higher frequency after positive
cholecystectomy had significantly fewer recurrent biliary symp- CBD exploration than after a negative one. The rate of recur-
toms (6% vs. 21%) and needed fewer readmissions (4% vs. rence increases to approximately 20% after a second operation
23%) than patients who did not undergo surgery after ES. on the biliary tract for choledocholithiasis (Saharia et al, 1977;
In contrast to the general consensus of how to treat high- Way, 1973), and this rate increases after subsequent reopera-
and low-likelihood patients, the question of how to treat tion (Allen et al, 1981).
intermediate-risk patients has been the subject of some debate.
A recent randomized clinical trial (Iranmanesh et al, 2014) Treatment
examined an upfront cholecystectomy and IOC strategy against Endoscopic and percutaneous methods remain the preferred
preoperative ERCP and subsequent cholecystectomy for modalities when managing recurrent or retained CBD stones
intermediate-risk patients. Fifty patients were randomized to (see Chapters 30 and 36C). The open surgical approach is
each group, and differences in length of stay, number of sub- reserved for patients who have failed nonoperative treatments.
sequent CBD interventions, morbidity, mortality, and quality Decision making is further influenced by clinical presentation,
of life were analyzed. No significant difference was found in condition of the patient, institutional expertise, and presence
morbidity or quality of life; however, patients who underwent or absence of a T-tube.
cholecystectomy as the initial procedure had a significantly
shorter length of stay (median, 5 days vs. 8 days; P < .001) and RETAINED STONES IN THE PRESENCE OF A T-TUBE. The rise in popu-
fewer common duct investigations. Based on these findings, the larity of laparoscopic biliary surgery has also meant decreasing
authors suggested that initial cholecystectomy with intraopera- use of the T-tube. Even when laparoscopic CBD exploration is
tive cholangiogram may be the preferred approach. In any performed, primary closure has been shown to be safe (Dong
patient being considered for precholecystectomy ERCP, strong et al, 2014; El-Geidie, 2010; Gurusamy et al, 2013), and
consideration should be given to the use of EUS (with selective routine use of postexploration T-tubes is not common (see
ERCP) or MRCP because these studies are less invasive and Chapters 31 and 42). If a T-tube is present, it provides nonin-
have minimal risk compared with that of an ERCP. vasive options for accessing the biliary tree postoperatively. In
the presence of a T-tube, retained CBD stones in the immedi-
Common Bile Duct Exploration at Time of ate postoperative period can be managed with observation,
Open Cholecystectomy mechanical extraction, or ES.
Laparoscopy has become routine in much of the world, and as If choledocholithiasis is noted within the first 4 to 6 weeks
laparoscopic experience has grown, surgeons have become postoperatively, no treatment is typically necessary, assuming
increasingly more comfortable using laparoscopic CBD explo- there is no evidence of obstruction or cholangitis. In the initial
ration when choledocholithiasis is noted intraoperatively. In weeks after CBD exploration, 10% to 25% of retained stones
areas of the developing world, however, where access to endo- found on postoperative cholangiography will pass spontane-
scopic, radiologic, and laparoscopic expertise is limited, open ously into the duodenum, and no further treatment is required.
cholecystectomy and bile duct exploration remains a mainstay If calculi persist after 4 to 6 weeks, treatment options include
of treatment. Even in settings where laparoscopy and endos- radiologic approach through the T-tube tract (see Chapter 30)
copy are readily available, however, there will still be some or ERCP (see Chapter 29). Because of its high success rate and
patients in whom an open approach to CBD exploration may low morbidity and mortality, nonoperative mechanical extrac-
be required (see Chapters 36B and 36C). Principal among tion through the T-tube tract is an attractive treatment choice.
these include (1) patients with large or impacted CBD stones A success rate of 95% has been reported with a morbidity rate
and those who have failed previous endoscopic interventions, of only 4% (Mazzariello, 1978). Burhenne (1980) reported no
in whom biliary enteric drainage is indicated; (2) those with deaths in 661 patients. When complications do occur, they can
anatomic considerations that preclude endoscopic treatment, be treated medically in most instances, and only 0.2% of cases
such as prior gastric resection or duodenal diverticulae; and (3) have required surgery (Mazzariello, 1978).
patients who require an open approach for cholecystectomy, ES also has been shown to be effective in the management
including those with Mirizzi syndrome, biliary-enteric fistula, of retained stones in the early postoperative period after explo-
severe cholecystitis, or a high index of suspicion for cancer. ration of the CBD with a T-tube still in place (Hammarström
et al, 1996; O’Doherty et al, 1986). Although ES has the con-
siderable advantage that it can be carried out as soon as retained
Postcholecystectomy Choledocholithiasis
stones are discovered, treatment may be unnecessary in some
(See Chapter 38) patients because stones may pass spontaneously. Some authors
Incidence (Lambert et al, 1988) have suggested that mechanical stone
The majority of initial operations for gallstone disease, with or extraction through the T-tube tract is superior to ES because
without demonstrated choledocholithiasis, are curative, but of its high success rate and lower morbidity profile, although
some patients will develop sequelae of choledocholithiasis post modern endoscopic equipment may mitigate some of the post-
cholecystectomy. Approximately 1% to 2% of all patients who ERCP hemorrhagic complications seen in earlier series
undergo cholecystectomy have stones left in the CBD that (Christoforidis et al, 2004). Regardless, the safety and efficacy
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 589
of percutaneous intervention through the T-tube makes it an choledocholithotomy. Tompkins and Pitt (1982) and Cameron
ideal choice for initial postoperative interventions, and ES is (1989) emphasized, however, that concomitant biliary drainage
best used in the early postoperative period before a T-tube tract should not be regarded as mandatory procedure in all patients
is well formed, when the patient is clinically unstable, the with retained or recurrent stones. In general, biliary-enteric
T-tube is inappropriate in size and position, or mechanical drainage at reoperation is appropriate in the following scenar-
extraction through the T-tube has failed. If these techniques ios: (1) stricture or stenosis of the distal bile duct or sphincter
fail, operative management can be undertaken with the expec- of Oddi, (2) marked dilation of the duct of 2 cm or more, (3)
tation of a high success rate and acceptable morbidity and multiple or primary bile duct stones, (4) inability to remove all
mortality (Cameron, 1989; Girard & Legros, 1981). stones from the duct, and (5) a third operation.
Transduodenal sphincteroplasty, choledochoduodenos-
RETAINED OR RECURRENT STONES IN THE ABSENCE OF A T-TUBE. ES tomy, and choledochojejunostomy are effective methods of
is the procedure of choice and should be attempted first in biliary enteric drainage (Braasch et al, 1980; Johnson & Harding
patients without a T-tube in place (Cameron, 1989; Sivak, Rains, 1978; Jones, 1978) (see Chapter 31). With the wide
1989) (see Chapters 29 and 36C). Most reports of ES indicate availability of ERCP, operative sphincteroplasty is rarely
a success rate in achieving overall clearance of stones from the required because ES is sufficient in most cases. In the presence
CBD of more than 85% (Cotton, 1984; Dasari et al, 2013; of a long distal CBD stricture, ES is not an appropriate choice
Lambert et al, 1991). Although early complication rates for ES because it does not address the primary obstructive issue. For
range from 5% to 15%, emergency surgery is uncommonly ducts smaller than 1 to 1.5 cm in diameter, sphincteroplasty is
required and most complications can be managed conserva- the preferred operative approach as this avoids possible anas-
tively (Cotton, 1984; Dasari et al, 2013; Escourrou et al, tomotic stricture formation, but it does carry a greater risk of
1984). Hemorrhage, pancreatitis, cholangitis, and perforation postoperative pancreatitis. Occasionally, recurrent or primary
are the most frequent complications, and mortality usually is stones will be seen in patients with dilated ducts and a widely
reported at 0.5% to 2% (Lambert et al, 1991; Sivak, 1989). patent sphincter after sphincteroplasty or sphincterotomy.
Long-term complication rates, mainly from stenosis or new In such cases, choledochoduodenostomy or Roux-en-Y cho-
stones or both, are low (<10%), and most complications can ledochojejunostomy is necessary. Side-to-side or end-to-side
be managed endoscopically (Cotton, 1984; Escourrou et al, choledochoduodenostomy and end-to-side Roux-en-Y cho-
1984; Hammarström et al, 1996; Sivak, 1989). ledochojejunostomy are excellent drainage options for CBDs
If ES is unsuccessful, percutaneous transhepatic rendezvous larger than 1.5 cm and offer better decompression of an
techniques can sometimes aid in duct clearance, particularly if extremely large duct. In the context of previous biliary pancre-
there is difficulty cannulating the ampulla. Often, however, atitis, patients who present for reoperation with multiple stones
failures of endoscopic management will be the result of large and an incompletely cleared proximal biliary system may be
impacted stones or anatomic issues that are not ameliorated by better served with an end-to-side choledochoduodenostomy as
a percutaneous approach. In such settings, operative manage- opposed to a side-to-side technique because it minimizes the
ment is the most reasonable alternative (Cameron, 1989). chance of stones dropping distally and causing recurrent pan-
Reoperation for retained stones can be performed safely, with creatitis. Sump syndrome is an uncommonly observed compli-
operative mortality less than 2% (Girard & Legros, 1981). cation of choledochoduodenostomy and should be managed
Miller and colleagues (1988) reported 237 patients with CBD initially by endoscopic modalities. If ERCP fails to improve
stones treated by CBD exploration or ES. Success was higher symptoms, the choledochoduodenostomy can be converted to
and mortality was lower for the operatively managed group. a Roux-en-Y choledochojejunostomy.
The complication rate was similar, but the complications
tended to be more serious and more apt to require surgery in Clinical Experience With Reoperation
the ES group. A systematic review performed by Dasari and Girard (2000) reviewed all patients who underwent reoperation
colleagues (2013) found that duct clearance in patients under- for retained or recurrent choledocholithiasis at the Maisonneuve-
going open bile duct exploration was superior to ES, but it Rosemont Hospital between 1969 and 1990. Eighty-five patients
should be noted that most series that compare open with preoperatively confirmed choledocholithiasis underwent a
cholecystectomy/CBD exploration to ES are from the era of total of 88 operations. Eighty-five of these operations were
open surgery, which also corresponds to the early days of ERCP second procedures, and three patients required a third opera-
and ES. Therefore caution should be used in extrapolating tion. Three types of bile duct reoperation were performed:
these data to the modern endoscopic experience. Nevertheless, choledocholithotomy with T-tube drainage (64 patients), cho-
these findings reinforce that surgery can be a valuable, effective, ledocholithotomy with side-to-side choledochoduodenostomy
and safe tool in the treatment of recurrent/retained CBD stones, (15 patients), and choledocholithotomy with transduodenal
even if confined to the subset of patients who fail ES. sphincteroplasty (6 patients). Choledocholithotomy with
When reoperation is required for retained CBD stones, the T-tube drainage in 1 patient and choledocholithotomy with
optimal procedure is complete removal of all stones via cho- side-to-side choledochoduodenostomy in 2 patients were per-
ledocholithotomy, choledochoscopy, placement of a T-tube (in formed at a third operation.
many cases), and completion cholangiography. This procedure The average hospital stay was 9.3 days. There were no
is adequate for most patients, and the overall failure rate is deaths in the series despite the fact that 43 of 85 patients were
has been reported as low as 3% (Girard & Legros, 1981). older than age 60 years and 44 patients had associated risk
Others, however, have reported significantly higher failure rates factors. Six minor complications were observed, none of
(Allen et al, 1981; Saharia et al, 1977), which has prompted which necessitated urgent surgery. Two patients (3%) of the
some authors (Allen et al, 1981; Lygidakis, 1982) to recom- 64 who had choledocholithotomy with T-tube drainage devel-
mend biliary-enteric drainage in all patients with previous oped recurrent bile duct stones 4 and 5 years after a second
590 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
TABLE 36A.1 Mortality Rates of Biliary Reoperation for SURGICAL TECHNIQUES FOR EXPLORATION OF
Retained or Recurrent Bile Duct Stones THE COMMON BILE DUCT
Reference No. Operations No. Deaths (%) The principal techniques for open exploration of the CBD will
be detailed in this section. Broadly, the goals of CBD explora-
Saharia et al, 1977 30 0
tion include complete clearance of calculi from the biliary
Jones, 1978 22 0
system and establishment of free flow of bile into the gut. The
McSherry & Glenn, 1980 341 7 (2%) preferred approach to CBD exploration is typically through a
Allen et al, 1981 47 1 (2%) supraduodenal choledochotomy, with the transduodenal/
De Almeida et al, 1982 22 1 (5%) transampullary route reserved for patients with impacted stones
DenBesten & Berci, 1986 86 2 (2.3%) that cannot be removed readily from above. Stones impacted
Girard, 2000 88 0 at the ampulla can be broken down and removed through a
TOTAL 920 15 (1.6%) supraduodenal approach; however, a transduodenal sphinctero-
plasty is generally less traumatic.
Clearance of the biliary tree should be confirmed by per-
forming postexploratory choledochoscopy and cholangiogra-
phy. The value of choledochoscopy has been confirmed by
operation, and side-to-side choledochoduodenostomy was many authors (Dayton et al, 1984; Kappes et al, 1982; Nora
performed. et al, 1977). Postexploratory cholangiography should also be
Taking Girard’s (2000) experience with that of other performed prior to closure of the abdomen, not only because
reported series, there have been 15 deaths among 920 patients it can locate missed stones, but also because it may reveal
submitted for reoperation for recurrent bile duct stones (Table unsuspected disruption of the biliary ductal system. If cholan-
36A.1). In one of these series (McSherry & Glenn, 1980), giography technique is meticulous, issues with false positives
choledocholithotomy was done for retained or recurrent stones from air bubbles and poor opacification of the entire system
in 341 patients; 7 patients died after the procedure, resulting can be largely eliminated to provide consistent and reliable
in a mortality of 2%. If three of these deaths that occurred after cholangiograms.
urgent operations for cholangitis or pancreatitis are excluded, The selective use of biliary-enteric drainage procedures is
however, and only the elective procedures are considered, another method to decrease the incidence of subsequently
only 4 patients died (1%) after repeat choledocholithotomy. symptomatic retained stones. Although we do not recommend
These results show that the overall mortality rate for retained routine biliary-enteric decompression at initial operation, it
or recurrent stones is less than 2%, with most deaths occurring should be considered carefully in patients with multiple duct
in elderly patients. This mortality rate is comparable to that stones, particularly in those with large stones; dilated ducts; and
of ES. in elderly patients. If these conditions pertain in an elderly or
To summarize, ES has become the first-line therapy for poor-risk patient, choledochoduodenostomy may obviate reex-
retained or recurrent bile duct stones, but surgery can be per- ploration. Other indications include (1) the presence of irre-
formed safely with low mortality and morbidity when required. trievable intrahepatic stones, (2) proven ampullary stenosis, or
Surgery remains a critical component of the armamentarium (3) an impacted ampullary stone.
that can be used to treat recurrent bile duct stones. As with
most things in modern medicine, a multidisciplinary approach
Supraduodenal Choledochotomy and Exploration of the
to recurrent CBD stones is important to properly select and
sequence the numerous options now available. Gastroenterolo- Common Bile Duct
gists, radiologists, and surgeons should work together closely Exposure
to assess the most appropriate intervention for an individual The liver is retracted superiorly with a broad-bladed, slightly
patient. In making the choice between open surgery, laparo- curved retractor, such as a Hartmann (“sweetheart”) retractor.
scopic surgery, percutaneous therapies, and ES, the surgeon This retractor should be deep enough to displace the liver but
must consider not only the published data but institutional not so curved as to traumatize it. A pack should be put over
expertise and experience. In a patient with a retained stone and the hepatic flexure of the colon down to the hepatorenal pouch
a T-tube in place, percutaneous extraction through the T-tube and the medial part of the duodenum. This pack is retracted
tract or ES should be attempted first. In the absence of a by a similar, broad-bladed retractor to prevent the colon or
T-tube, ES should be attempted first. If unsuccessful or con- duodenum from obscuring vision (Fig. 36A.1). The lesser
traindicated, operative management is a reasonable alternative. omentum and stomach are retracted to the left after placement
Surgical intervention has a high success rate and acceptable of another pack. The gallbladder is usually removed before
rates of mortality and morbidity. Before operation, the surgeon exploration of the CBD because it may obstruct vision, although
must make an accurate diagnosis of retained stones by using a in some cases it can be a useful aid to retraction. Palpation of
combination of MRCP, ERCP, and US. These findings should the CBD and handling of its lower part during exploration and
be confirmed via intraoperative cholangiography and complete subsequent choledochoscopy cannot be done properly without
clearance of the biliary tree documented with completion chol- having performed a classic Kocher maneuver (Fig. 36A.2).
angiography and choledochoscopy. Most patients do not
require biliary-enteric drainage, but certain patients, particu- Choledochotomy
larly those with multiple or incompletely cleared calculi, large A distal vertical supraduodenal choledochotomy is generally
ducts (>2 cm), and distal CBD strictures, will benefit from preferred for several reasons. First, because a choledochoduo-
drainage procedure. denostomy may be required (see Chapter 31), the opening
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 591
Exploration of the Duct gently withdrawn through the papilla, and then the balloon is
All efforts must be made to minimize trauma related to the reinflated immediately. Passage back through the ampulla can
exploration, and rigid instruments should be avoided if possi- be detected by a sudden easing of the pull on the catheter. At
ble, as false passages into the duodenum and pancreas can be this point, the syringe is held in the surgeon’s nondominant
easily created (Gunn, 1983; Orloff, 1978). Grasping forceps of hand, and the degree of balloon inflation is controlled by the
any type can catch the duct wall and result in delayed stricture thumb and the plunger. With gentle traction superiorly from
formation. Use of the Fogarty balloon catheter can avoid these long forceps held in the surgeon’s dominant hand, the catheter
issues and has been found to be suitable for CBD exploration is gradually pulled up to the choledochotomy site (Fig. 36A.8),
(Fogarty et al, 1968; Fox & Gunn, 1984). with care being taken to prevent any stone slipping into the
The Fogarty probe is held in long forceps with the surgeon’s proximal biliary tree. If the traction is anterior rather than
dominant hand and introduced into the CBD (Fig. 36A.6), superior, there is the risk of lacerating the opening into the duct
The catheter is then passed into the duodenum. The balloon (Fig. 36A.9), and the risk is increased when the opening in the
is inflated, and the catheter is withdrawn until it impinges duct is longitudinal. The procedure is repeated until the distal
against the papilla (Fig. 36A.7). The balloon is identified in the duct is considered to be clear.
second part of the duodenum by palpation, and the location is Next, this procedure is repeated for the proximal ducts by
noted as the site of duodenotomy should a sphincteroplasty reinserting the catheter upward into each of the main hepatic
become necessary. Stones can usually be felt against the shaft ducts. The degree of balloon inflation is of great importance
of the catheter within the duct. The balloon is deflated and here, as overinflation will result in damage to the ducts and
592 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
FIGURE 36A.3. The common bile duct is opened just above the
duodenum to leave room for a choledochoduodenostomy if
necessary. FIGURE 36A.4. Two fine absorbable stay sutures are used to lift and
render the common bile duct (CBD) tense for an incision about 1 to
2 cm long, depending on the size of the duct and the size of the stones.
If the CBD is not made tense, damage can be done to the posterior
wall, or an irregular incision can be made.
A B
FIGURE 36A.5. A, The cystic duct may lie anterior to the common bile duct (CBD) and may be opened in error. B, The cystic duct may run parallel
to the CBD with a low entrance, mimicking a dilated duct.
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 593
A B
FIGURE 36A.6. A Fogarty catheter is fed into the duct with forceps
by using the dominant hand. The operator’s nondominant hand is used
to grasp the mobilized duodenum, which allows palpation of the passage
of the catheter and of any stones within the intrapancreatic portion of
the common bile duct.
Postexploratory Investigations orifices of the smaller biliary radicles. Although flexible scopes
Following exploration, the surgeon must make every effort to carry a higher cost and are more difficult to maintain compared
ensure that the duct system is normal using choledochoscopy with rigid scopes, they allow for less traumatic choledochos-
and cholangiography (see Chapter 23). copy, are more versatile because of their increased length, and
allow introduction of therapeutic instruments through the
Choledochoscopy working channel. Some surgeons experienced in choledochos-
Choledochoscopy is the established method to ensure that the copy recommend exploration of the CBD and removal of
duct system is normal. Modern instruments are small enough stones under direct vision by using the choledochoscope (Berci,
to allow visualization of the major right and left hepatic ducts 2000). This can be facilitated by use of a stone basket through
and intermediate hepatic ducts and to allow visualization of the the working port of a flexible choledochoscope. The use of
594 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
A B
FIGURE 36A.8. A, The balloon is withdrawn gently, revealing the stone. B, Long forceps can be used to obstruct the common hepatic duct to
prevent the stone from slipping upward.
T-Tube Cholangiography T-TUBE PLACEMENT. First, the limbs of the T-tube must be short-
After insertion of a T-tube and closure of the choledochotomy, ened (Fig. 36A.12A). T-tubes can become obstructed, particu-
T-tube cholangiography should be performed to ensure larly if they are tight fitting, and they can be difficult to extract.
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 595
A B
FIGURE 36A.11. A, Faceted retained distal common bile duct (CBD) stone on T-tube cholangiography 1 week after operation. The T-tube is inserted
in the common hepatic duct above the confluence of the cystic duct. B, The retained CBD stone is ensnared in the wire basket before extraction.
This stone measured 5 mm in diameter and was extracted intact through the sinus tract of a 14-Fr T-tube.
596 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
6 cm
A B
FIGURE 36A.12. A, The T-tube is modified by shortening the limbs to prevent proximal obstruction and distal entry into the duodenum. B, A T-tube
is modified by removing half the diameter to prevent obstruction and enable easy removal.
A B C
FIGURE 36A.15. A, The suture must not catch the tube as shown here. B, The T-tube limb should not enter the hepatic duct, as shown here.
C, The distal end of the T-tube should not enter the duodenum, as shown here.
suprasphincteric stricture. It also should not be attempted in PYOGENIC CHOLANGITIS (SEE CHAPTER 43). If papillary stenosis or
the presence of a duodenal diverticulum or where there is severe CBD stones or both exist together with cholangitis, transduo-
periampullary inflammation. denal sphincteroplasty can be an excellent procedure for defini-
tive biliary drainage.
Indications
The most common indications for transduodenal sphinctero- CHRONIC PANCREATITIS AND ACUTE GALLSTONE PANCREATITIS (SEE
plasty relate to bile duct stones and cholangitis (see CHAPTERS 55 TO 58). In chronic pancreatitis, some authors report
Chapter 43). good long-term results with transduodenal sphincteroplasty
alone (Hacaim et al, 1994) or in addition to transpapillary
STONES IMPACTED IN THE DISTAL AMPULLARY REGION. An impacted septectomy (Moody et al, 1983) or with other drainage proce-
stone is often readily palpable, and the incision may be made dures of the duct of Wirsung (Kestens et al, 1996). The pres-
safely using the stone as a guide. In such cases, extraction ence of a stone at the lower end of the CBD or pancreatic duct
through a supraduodenal choledochotomy is often impossible may cause biliary pancreatitis, and transduodenal sphinctero-
without undue risk of creating a false passage and without plasty with clearance of the CBD is a treatment option.
significant risk of postoperative pancreatitis.
Technique
MULTIPLE AND RECURRENT COMMON BILE DUCT STONES. In cases of Sphincteroplasty consists of the incision of the common portion
multiple and recurrent CBD stones, sphincteroplasty should of the sphincter of Oddi (Fig. 36A.18) with partial suture of
provide long-term biliary drainage. When 20 or more stones the incision margin. Using this procedure, the sphincters of the
are removed from the CBD, it is probable that one or more CBD and the duct of Wirsung are not involved, and their func-
stones are still present (Stain et al, 1991). In this situation, tions are not impaired. The procedure also can be called a
choledochoduodenostomy or sphincteroplasty yields excellent subtotal lower sphincteroplasty (Fig. 36A.19) (Stefanini et al,
results. 1977). The approach to the sphincter of Oddi is through a
minimal duodenotomy in the second part of the duodenum.
PAPILLARY STENOSIS. Papillary stenosis is encountered less fre-
quently than in the past. When it is found at operation, trans- Preparation, Position of the Patient, and Incision
duodenal sphincteroplasty ensures good biliary drainage and Preoperative preparation is routine. The patient is placed in a
prevents restenosis (Ramirez et al, 1994). ES is technically suc- supine position on a radiotransparent operating table. A trans-
cessful in only 60% to 80% of cases, and the mortality rate verse incision below the right costal margin is preferred (Vogt
exceeds 1% (Seifert et al, 1982). In addition, sphincterotomy & Hermann, 1981). This incision allows optimal light and
for papillary stenosis is five times more likely to lead to reste- excellent access; it is particularly suitable in obese patients, and
nosis than if the same procedure is performed for calculi the incidence of postoperative incisional hernia is probably
(Tzovaras & Rowlands, 1998). lower than with vertical and oblique incisions. The incision of
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 599
Duodenotomy
Duodenotomy is performed in the lateral duodenal wall by
surgical diathermy. The cut is 10 to 15 mm long immediately FIGURE 36A.21. It is important to expose and mobilize the third
above the inferior knee of the duodenum, with the surgeon portion of the duodenum to easily identify and operate on the papilla
taking account of the fact that the papilla usually is located at and allow facile closure of the duodenotomy.
600 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
2
3
15 mm
1
3
FIGURE 36A.23. If the papilla is not easily seen, it can often be pal-
pated as a small elevation in the medial duodenal wall. If the papilla is
FIGURE 36A.22. The duodenotomy is performed above the junction still not easily seen, a small Nélaton catheter is introduced through the
of the second and third portions of the duodenum; the surgeon takes cystic duct stump until it is seen to protrude from the papillary orifice.
into account that the papilla usually is located at the junction of the upper The forefinger, introduced through the duodenotomy, detects the papilla
two thirds and lower third of the second part of the duodenum. as a small, thick elevation.
the junction of the lower third with the upper two thirds of the (Fig. 36A.24) (Partington, 1977). A Nélaton catheter (4 to 5
second portion of the duodenum (Fig. 36A.22). The duodenal Fr) is introduced from the outside or via the cystic duct. Fol-
incision may be longitudinal or transverse; both types are suit- lowing the line of the catheter—and avoiding plastic catheters,
able, provided that the suture of such incisions is always trans- which melt when surgical diathermy is applied—the surgeon
verse. We prefer a longitudinal incision, because if the retractor makes a cut using surgical diathermy. This cut is made superi-
on the duodenum widens the duodenotomy, this occurs longi- orly (at the 11 o’clock position) for 4 to 5 mm (Fig. 36A.25).
tudinally. In the case of a transverse duodenotomy, any inad- We prefer surgical diathermy because the instrument ensures
vertent extension would cause a transverse enlargement of the good hemostasis. When a sample for biopsy is required, it
wound. should be obtained with a scalpel and be taken only from the
outer margin of the incision. Possible bleeding from the cut,
Identification of the Papilla usually modest, can be arrested with a stitch. After sphincter-
After the duodenal incision, the papilla is readily shown on the otomy, two or three stitches are placed between the duodenal
medial duodenal wall in 15% to 20% of patients. It appears as mucosa and the wall of the CBD on the outer margin by using
a roundish elevation with a central orifice. When the papilla is an atraumatic needle and fine sutures. Traction is applied to
not readily visible, it should be detected by displacement and these sutures, and incision of the sphincter is extended for
flattening of the mucosal folds. This should be done with great another 6 to 7 mm with sutures placed every 2 to 3 mm, all
care to avoid tearing of the mucosa, which would hinder good laterally, until the entire common tract of the sphincter of Oddi
exposure. Identification of the papilla under direct vision is has been incised (Fig. 36A.26). The incision is complete when
possible in 80% of patients. If this is not the case, digital palpa- it is 10 to 12 mm long and an appropriate forceps can be easily
tion can be used running the forefinger, introduced through the introduced (Fig. 36A.27). Its entry into the CBD allows an
duodenotomy, across the medial duodenal wall. The papilla is abundant flow of bile owing to distension of its sphincter.
identified as a small elevation. If digital palpation fails, a small Sutures should be placed only on the outer margin of the
(5 to 6 Fr) Nélaton catheter can be introduced via the cystic sphincterotomy to prevent the risk of damage to the duct of
duct stump and advanced downward to emerge at the papilla Wirsung. The opening of the duct of Wirsung usually is identi-
(Fig. 36A.23). This maneuver should never be performed with fied as a small orifice from which clear, colorless pancreatic
rigid catheters because this may result in the formation of false juice flows.
passages.
Sometimes a very small papilla is detected, and its catheter- Instrumental Exploration of the Common Bile Duct
ization is difficult or impossible. In such cases, the orifice is After sphincteroplasty, instrumental exploration of the CBD
probably that of the duct of Santorini. The major papilla should and extraction of stones is performed (Speranza et al, 1982).
be searched for in a lower position. An angled Randall forceps is introduced into the CBD, and the
bile duct is carefully explored. The maneuver should be
Sphincteroplasty repeated several times to extract all stones. The next step is to
After the papilla has been identified, it is exposed by gentle rinse with saline solution, introduced under slight pressure with
extraction with an Allis or similar clamp. This clamp is applied a Nélaton catheter (8 to 9 Fr) and abruptly withdrawn so that
laterally, never medially, to avoid trauma to the duct of Wirsung small fragments flow downstream with the siphoning (Fig.
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 601
36A.28). Other means to extract stones from the CBD are with
a Fogarty catheter and Dormia basket. The problem of residual
stones is best prevented with choledochoscopy; the endoscope
is introduced via the sphincteroplasty.
Duodenal Closure
As already emphasized, initial longitudinal duodenotomy
always should be closed transversely to avoid stenosis of the
duodenum. First, the superior and inferior margins of the inci-
sions are approximated, and the resulting gaps are sutured with
two extramucosal, nonabsorbable purse-string sutures. Three
or four nonabsorbable seromuscular sutures are added (Fig.
36A.29). The suture should not be under tension, and for this
reason, preliminary extended mobilization of the duodenum
and pancreas is mandatory. The operation is now complete,
and the wound is closed without abdominal drains.
Comment
It is not necessary to perform transduodenal sphincteroplasty
combined with supraduodenal choledochotomy, which has a
higher associated mortality rate (Scheridan et al, 1987). The
cystic duct remnant may be used to introduce a Nélaton cath-
eter to assist recognition of the papilla. There is no need to
insert a T-tube, which lengthens the hospital stay and may
predispose the patient to stenosis and infection of the CBD
(Ratych et al, 1991; Scheridan et al, 1987).
A B C
FIGURE 36A.29. The duodenotomy always should be closed transversely to avoid stenosis of the duodenum. A, The superior and inferior angles
are approximated. B, The resulting lateral gaps are sutured with two extramucosal nonabsorbable purse-string sutures. C, Three to four nonabsorb-
able seromuscular stitches are added as a second layer. The sutures should not be under tension.
A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 603
(but only in 0.9% for sphincterectomy-related complications) with transampullary septectomy (Kelly & Rowlands, 1996)
were age older than 70 years and a bilirubin level greater has led to good long-term results in patients with chronic and
than 85 mmol/L, diabetes, renal failure, and coagulopathy. acute recurrent pancreatitis, even in cases with pancreas divisum
The mortality rate increased when supraduodenal choledo- and in selected patients with abdominal pain of hepatobiliary
chotomy was combined with transduodenal sphincteroplasty origin.
and when a T-tube was used (Sellner et al, 1988). Transduo-
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A. Gallstones and Gallbladder Chapter 36A Stones in the bile duct: clinical features and open surgical approaches and techniques 603.e3
Vargghese JC, et al: Diagnostic accuracy of magnetic resonance Wallner BK, et al: Dilated biliary tract: evaluation with MR cholangi-
cholangio-pancreatography and ultrasound compared with direct ography with a T2-weighted contrast-enhanced fast sequence, Radi-
cholangiography in the detection of choledocholithiasis, Clin Radiol ology 181:805–808, 1991.
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CHAPTER 36B
Stones in the bile duct: minimally invasive
surgical approaches
Zeljka Jutric, Chet W. Hammill, and Paul D. Hansen
OVERVIEW used and the sequence in which they are used depend on the
specific clinical scenario. In addition, the capability and experi-
Choledocholithiasis is identified in 10% to 18% of patients ence of the available personnel will affect the treatment algo-
undergoing cholecystectomy, either preoperatively, intraopera- rithm. The most common clinical scenarios encountered by
tively, or postoperatively (Dasari et al, 2013) (see Chapters 32 surgeons include known or suspected stones prior to cholecys-
and 37). The majority of cases of choledocholithiasis are sec- tectomy, the diagnosis of stones intraoperatively, and stones
ondary, the result of stones that originally formed in the gall- identified subsequent to cholecystectomy.
bladder. Primary choledocholithiasis, 10% to 15% of cases
(with a higher incidence in Asian countries), results from the CLINICAL SCENARIOS
formation of stones within the common bile duct (CBD) (Ko
& Lee, 2002). Choledocholithiasis can lead to a variety of clini- Preoperative Choledocholithiasis
cal manifestations, including biliary colic, obstructive jaundice, Ascending cholangitis (see Chapter 43), gallstone pancreatitis
ascending cholangitis (see Chapter 43), and pancreatitis (see (see Chapters 54 and 55), symptomatic cholelithiasis with evi-
Chapters 54 and 55). These clinical scenarios can vary signifi- dence of choledocholithiasis on imaging or serum liver function
cantly in presentation and morbidity, ranging from minimal to tests, are all potential indicators that CBD stones are present.
critical illness and death. If left untreated, chronic choledocho- For CBD stones suspected at the time of initial clinical presen-
lithiasis can also cause inflammatory strictures, recurrent infec- tation, the decision making is often based on surgeon prefer-
tions, or cirrhosis. ence and institutional capabilities. When CBD stones are highly
The management of choledocholithiasis has changed radi- likely or established with noninvasive imaging, the two primary
cally over the last several decades. Historically, stones in the therapeutic strategies are ERCP followed by laparoscopic cho-
CBD were removed at the time of open surgical exploration. lecystectomy or laparoscopic cholecystectomy with intraopera-
Even after the introduction of endoscopic retrograde cholangio- tive cholangiogram. In the latter case, laparoscopic CBD
pancreatography (ERCP) in the 1970s, laparotomy remained exploration or postoperative ERCP are performed if CBD
the mainstay for CBD exploration (Kroger et al, 1975). At that stones are identified on the cholangiogram.
time, the tools and techniques used for surgical clearance of the In general, ERCP, which is available in essentially all urban
CBD were superior to those available via ERCP, and as long settings and in a growing number of smaller communities, is
as a laparotomy was used to perform the cholecystectomy, more widely available than surgeons skilled at laparoscopic
minimally invasive treatment of choledocholithiasis was unnec- CBD exploration (see Chapters 20 and 29). ERCP is also
essary. It was not until the introduction of the laparoscopic highly effective, with successful clearance of the CBD in more
cholecystectomy in the late 1980s that the role for an associated than 95% of cases (Kum & Goh, 1996). In most centers, CBD
less invasive method of treating choledocholithiasis became a stones up to 1.5 cm can be extracted, and centers that use
priority. lithotripsy can extract stones as large as 3 cm in diameter
During the initial adoption of laparoscopic cholecystectomy, (Lenze et al, 2014). Therefore, in settings where laparoscopic
most general surgeons did not have the skill set, experience, or CBD exploration is not available, the debate centers on preop-
equipment to facilitate a laparoscopic CBD exploration. As the erative versus postoperative ERCP. The central argument
skills, experience, and tools have developed, the advantages and against an ERCP-first strategy is that 80% of known or sus-
disadvantages of laparoscopic CBD exploration versus ERCP pected CBD stones will have passed prior to the intervention,
have been a frequent source of debate. The objective of this making the risks and cost of the intervention unnecessary
chapter is to discuss minimally invasive surgical techniques for (Urbach et al, 2001). The risks of ERCP include acute pancre-
managing choledocholithiasis, including indications and tech- atitis (3% to 7%), bleeding (0.3% to 1.4%), ascending infection
nical aspects of laparoscopic transcystic, transcholedochal, and (1.4%), and perforation (0.6%). The mortality associated with
transduodenal CBD exploration, as well as laparoscopic biliary- ERCP is 0.2% to 0.9% (Orenstein et al, 2014). Proponents of
enteric bypass procedures and laparoscopic-assisted ERCP. performing preoperative ERCP argue that, if ERCP is unsuc-
cessful, a CBD exploration can be performed at the time of
INDICATIONS cholecystectomy without requiring a third procedure.
In most patients, our preferred strategy is laparoscopic cho-
The standard of care for the management of most CBD stones lecystectomy with selective intraoperative cholangiogram (see
is minimally invasive: using either laparoscopic, endoscopic, or Chapter 23). Laparoscopic CBD exploration or ERCP is per-
percutaneous techniques. The minimally invasive techniques formed when CBD stones are identified. However, in patients
604
A. Gallstones and Gallbladder Chapter 36B Stones in the bile duct: minimally invasive surgical approaches 605
with cholangitis, ongoing pancreatitis, or persistent hyperbili- unsuccessful or cannot be performed due to altered anatomy.
rubinemia (>4 U/dL), we recommend preoperative ERCP ERCP fails to cannulate the CBD in 1% to 2% of cases. In this
(Chan et al, 2008). This allows for both clearance of the bile situation, laparoscopic CBD exploration is necessary. Similarly,
duct and assessment of additional or alternative pathologies, if stone extraction fails due to the size of the stones, laparo-
such as impacted stones, strictures, or malignancy. In the case scopic exploration is a reasonable next step. In the case of
of ascending cholangitis, broad-spectrum antibiotics and urgent impacted or large stones that cannot be removed endoscopically
biliary decompression with ERCP is typically the best option, or surgically, biliary-enteric bypass should be considered (see
as it is the least invasive and both diagnostic and therapeutic Chapter 36A).
(Hui et al, 2001). If ERCP is unavailable or not possible (e.g., Laparoscopic CBD exploration or laparoscopic-assisted
history of Roux-en-Y gastric bypass), percutaneous transhe- ERCP may be the only options in patients with a history of
patic biliary decompression should be considered (see Chapter gastrointestinal surgery. With the introduction and rapid expan-
30). Surgical options, laparoscopic or open, are indicated when sion of Roux-en-Y gastric bypass procedures, it is becoming
less invasive methods are not immediately available and the increasingly common to have patients present in whom an
patient’s condition warrants immediate biliary decompression ERCP is either challenging or not possible.
(see Chapter 36A). In both cholangitis and pancreatitis, once
the patient has sufficiently recovered, cholecystectomy should
be completed during the same hospitalization as early recur- TECHNIQUES
rence of symptoms is common, and can lead to significant
morbidity (Chang et al, 2000; Li et al, 2010).
Laparoscopic Transcystic Common Bile
Endoscopic ultrasound (see Chapter 16) and magnetic reso- Duct Exploration
nance cholangiopancreatography (MRCP) (see Chapter 19) The primary method for performing laparoscopic CBD explo-
are additional diagnostic tools that may be helpful in these situ- ration is through the cystic duct. Transcystic exploration is
ations. Endoscopic ultrasound is highly sensitive for CBD typically performed using a standard laparoscopic cholecystec-
stones, without the risk of pancreatitis, allowing ERCP to be tomy trocar configuration. An additional trocar may be placed
used selectively (Artifon et al, 2009). MRCP is a relatively in the midclavicular line to facilitate access to the cystic duct
accurate and noninvasive test that can identify the presence or (Fig. 36B.1A). The gallbladder is left in situ to provide liver
absence of choledocholithiasis, as well as provide anatomic retraction and countertraction on the cystic duct, allowing
delineation prior to surgery. Some centers advocate MRCP to
avoid the risk of unnecessary ERCP; however, this may be
associated with an increase in cost.
Intraoperative Choledocholithiasis (See Chapters 31
and 36A)
When choledocholithiasis is diagnosed on intraoperative chol- Cholangio
angiogram, and the surgeon’s experience and diameter of the scope port
cystic duct are favorable, our preference is to proceed with 5
5
transcystic CBD exploration. If clearance cannot be achieved 5
via the transcystic route, the options are to proceed with tran- 10 mm
5
scholedochal CBD exploration versus a postoperative ERCP.
Intraoperative ERCP, although uncommonly used, is also avail-
able at some institutions (Moreels, 2014; Schreiner et al, 2012).
Our preference is to proceed with postoperative ERCP if the
stones are less than 2 cm and do not appear to be impacted.
ERCP avoids complications associated with a transcholedochal
A
exploration, including biliary stricture and bile leak (Verbesey
& Birkett, 2008). When the probability of endoscopic clearance
is questionable or low, we proceed with a transcholedochal
exploration.
A number of retrospective studies have shown that laparo-
scopic cholecystectomy with CBD exploration as a single oper-
ative procedure is more cost-effective and results in shorter
hospital length of stay than laparoscopic cholecystectomy and
ERCP (Cuschieri et al, 1999; Nathanson et al, 2005; Rogers 5 5
et al, 2010). A recent prospective randomized controlled trial If needed
5
found that both options were highly effective and equivalent in
10 10
overall cost, although the hospital length of stay was lower for
laparoscopic CBD exploration (Rogers et al, 2010).
Postoperative Choledocholithiasis B
Choledocholithiasis identified after a cholecystectomy or when FIGURE 36B.1. A, Trochar placement for transcytic and transchole-
there is not a plan to perform a cholecystectomy is typically dochal common bile duct (CBD) exploration. B, Trochar placement for
managed with ERCP; however, occasionally endoscopy is transduodenal CBD exploration and biliary-enteric bypass.
606 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
easier passage of wires, catheters, and the cholangioscope. The removed, and the duct is again vigorously irrigated. Finally, a
first and easiest step in facilitating passage of stones through cholangiogram is performed to assess for residual stones.
the ampulla is pharmacologic relaxation of the sphincter of If ampullary dilation is unsuccessful, choledochoscopy is the
Oddi by using glucagon (Petelin, 1993). After giving 1 mg of next step. Some surgeons prefer to proceed straight to choledo-
intravenous glucagon and waiting 3 minutes, the duct is vigor- choscopy without attempting ampullary dilation because it
ously irrigated with saline or contrast in an attempt to flush the allows direct visualization of the bile duct and stones. A chol-
stones through the ampulla (Ponce et al, 1989). This technique angioscope or ureteroscope is passed transcystically into the
is most successful for sludge and stones less than 4 mm (Kroh common duct (Fig. 36B.2B). If the cystic duct is too small, the
& Chand, 2008). same balloon used for ampullary dilation can be used to gently
If flushing is unsuccessful, two additional techniques are dilate the cystic duct until it is large enough to allow the chol-
used: dilation of the ampulla and choledochoscopy. Ampullary angioscope to pass. Once the stones are identified, they can be
dilation is performed by passing a wire through the cystic duct gently pushed through the ampulla with the tip of the cholan-
and into the duodenum under fluoroscopic guidance. A 4- to gioscope, or they can be snared. To snare the stones, we recom-
6-mm diameter, 4-cm long ureteral balloon is advanced over mend a helical stone retrieval basket, which is passed through
the wire and positioned across the ampulla. After fluoroscopic the working channel of the cholangioscope. Under direct visu-
confirmation of the balloon’s position, it is inflated, dilating the alization, the basket is passed beyond the stone. Once the
ampulla (Fig. 36B.2A) Following dilation, the balloon is basket is distal to the stone, it is opened and withdrawn until
the stone is captured; the snare is then closed, and the stone is
removed through the cystic duct. Care is taken to avoid causing
injury with the snare, as it is a stiff instrument, and ductal
perforation or penetration into the pancreas is possible. Some
authors recommend blind or fluoroscopically guided wire
basket stone capture and extraction; in our experience, this has
proven less successful and has a higher risk of injury. There are
two options to manage large stones that cannot be extracted
through the cystic duct. Large stones that are soft, can often
be crushed by tightening the snare around them, and the debris
can then be snared individually or pushed through the ampulla
into the duodenum. For large stones that are too hard to crush,
a laser or mechanical lithotripsy catheter can be passed through
the cholangioscope to fracture the stone under direct visualiza-
tion. Finally, in bile ducts with significant inflammation or
strictures, a biopsy should be considered. Malignancy may be
an inciting event in the development of ductal debris or ductal
obstruction. Complications of transcystic CBD exploration, as
observed by Paganini and colleagues (2007), include bile leak
(1%), acute pancreatitis (0.5%), and rupture of the cystic duct
(6.8%).
The success rate of a laparoscopic transcystic approach to
choledocholithiasis by experienced surgical teams is 80% to
90% (Kroh & Chand, 2008). There are a number of reasons a
transcystic CBD exploration can fail. In some cases, the cystic
duct is too small, tortuous, or even obliterated, and passage of
a catheter into the CBD is difficult or impossible. Occasionally,
the cystic duct inserts into the very distal common duct or at
an acute angle, making access to the proximal common duct
challenging. Large stones, impacted stones, and significant
inflammation can all increase the difficulty of transcystic bile
duct clearance. In such cases, the surgeon must decide whether
to proceed with transcholedochal exploration or defer to post-
operative ERCP. If the CBD is less than 1 cm in diameter, and
in the absence of large impacted stones, our preference is to
proceed with postoperative ERCP due to the high rate of
success and less potential morbidity.
Laparoscopic Transcholedochal Common Bile
Duct Exploration
Laparoscopic choledochotomy is indicated when the transcys-
tic approach fails or in the presence of multiple, large, or
FIGURE 36B.2. A, Transcystic balloon dilation of the sphincter of impacted stones. Choledochotomy should be avoided if the
Oddi. B, Transcytic examination of the bile duct with the CBD is less than 1 cm in diameter (Verbesey & Birkett, 2008).
choledochoscope. The CBD is accessed by exposing the second portion of the
A. Gallstones and Gallbladder Chapter 36B Stones in the bile duct: minimally invasive surgical approaches 607
duodenum and mobilizing the duodenum down to the level of Our preference is to close the ductotomy with simple inter-
the pancreas. Excessive mobilization of the CBD should be rupted sutures, spaced evenly to avoid duct ischemia. We gener-
avoided to preserve blood supply to the proximal duct. Stay ally use a 5-0 monofilament, slowly absorbable suture. If a
sutures may be placed on either side of the choledochotomy T-tube is used, the ductotomy is closed around the base of the
(preserving the 3 and 9 o’clock blood supply) to allow for trac- tube by using a few sutures adjacent to the side of the T-tube,
tion on the CBD. A longitudinal choledochotomy is then made and the tube is exteriorized through a lateral trocar site. A final
on the distal CBD; the choledochotomy should be long enough cholangiogram through the T-tube is performed at the conclu-
for removal of the largest stone and passage of the choledocho- sion of the case. Tubes are left in place for 3 weeks to promote
scope. Typically, a 1-cm incision is sufficient to meet both of formation of an inflammatory tract around the tube. The
these goals. T-tube can then be gently removed, and the tract will collapse
A choledochoscope is passed directly into the bile duct, and and seal spontaneously. If stones are discovered postopera-
a thorough exploration of the proximal and distal duct is per- tively, percutaneous stone extraction via the T-tube is success-
formed (Fig. 36B.3). Stones may be flushed out of the duc- ful in 95% of cases (Burhenne, 1980). Surgical drains are not
totomy, removed directly with atraumatic graspers, or extracted placed routinely unless there is an increased risk of bile leak or
using a snare passed through the cholangioscope as described when a T-tube is used. Once the patient is tolerating a diet and
in the transcystic approach. There is a mechanical advantage there is no evidence of obstruction, we clamp the T tube. The
to removing impacted stones directly through a choledochot- surgical drain is removed if there is no evidence of a bile leak
omy, although stones impacted in the head of the pancreas may after the T-tube has been clamped.
require a transduodenal approach. The overall success rate of laparoscopic choledochotomy is
After clearance of the duct and completion of the explora- 83% to 96%, with a morbidity rate of 5% to 10%, and mortality
tion, the ductotomy is closed primarily or occasionally over a rate of 1% (Verbesey & Birkett, 2008). As mentioned previ-
T-tube. Historically, T-tubes have been used to decompress the ously, this procedure is not without complications. Bile leak
biliary tree and were thought to minimize bile leaks. They also (reported as high as 14%) and postoperative CBD strictures
allow postoperative percutaneous access to the CBD. T-tubes, are the most feared complications (Nathanson et al, 2005).
however, have potential morbidity, including inadvertent dis- Choledochotomy has similar rates of pancreatitis (7.3% vs.
placement, erosion, cholangitis, nutritional deficiencies from 8.8%), retained stones (2.4% vs. 4.4%), reoperation (7.3% vs.
bile loss (Gurusamy et al, 2013). In addition, T-tubes can cause 6.6%), and overall morbidity (17% vs. 13%) as ERCP (Nathan-
pain and be problematic to manage. son et al, 2005). Major advantages of the transcholedochal
If clearance of the duct has been achieved with confidence approach include easier access to both the upper and lower
and there are no concerns for distal obstruction, our preference ductal systems, and extraction of any size stones. Conversion
is to primarily close the choledochotomy without a T-tube. to an open procedure must be considered in difficult cases,
Several randomized trials have concluded that primary closure although challenging laparoscopic cases are frequently also
of the duct does not result in a higher rate of bile leaks (Zhang challenging open cases; referral to a specialty center should
et al, 2009). These studies have uniformly shown a decreased always be considered before converting to a laparotomy. In
length of hospital stay, shorter operative times, lower hospital patients with a high risk of recurrent stone disease or formation
expenses, and earlier return to normal activity in patients who of a biliary stricture, due to inflammation or a small duct, a
did not have a T-tube (Mangla et al, 2012). In addition, due definitive bypass should be considered.
to the high success rates of duct clearance by choledochotomy,
the need for T-tubes to provide percutaneous access for retained
Laparoscopic Transduodenal Sphincterotomy and
stones is not commonly necessary (Zhang et al, 2009). Common Bile Duct Exploration
For impacted stones refractory to clearance by endoscopy or
CBD exploration, laparoscopic transduodenal exploration with
sphincterotomy is an alternative modality for duct clearance
(see Chapter 36A). This procedure can typically be performed
with a 4 or 5 trocar technique, and we have found it useful to
place the trocars lower than the typical approach to cholecys-
tectomy. An additional camera trocar in the right lower quad-
rant will also provide a better angle for visualization of the
ampullary reconstruction (see Fig. 36B.1B).
To gain access to the duodenum, the right colon is mobi-
lized, and a Kocher maneuver is completed. With the duode-
num elevated, a surgical sponge posterior to the head of the
pancreas may be useful. This will elevate the duodenum and
absorb enteric fluids leaking into the field once the duode-
notomy is created. A longitudinal incision is made in the
antimesenteric wall of the second portion of the duodenum
with electrocautery or ultrasonic shears, to expose the major
duodenal papilla. If the papilla is not easily located, and the
cystic and CBDs are patent, a cholangiogram catheter or
wire can be inserted via the cystic duct and passed through
FIGURE 36B.3. Transcholedochal examination of the bile duct with the ampulla to aid in identification. Once the papilla is identi-
the choledochoscope. Stay sutures are used for retraction. fied, the CBD is intubated with a wire or silicone tube.
608 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
A B
FIGURE 36B.4. A, Transduodenal sphincterectomy at the 11 o’clock
position. B, Suturing of the bile duct mucosa to the duodenal mucosa
after sphincterectomy.
Laparoscopic Biliary-Enteric Bypass FIGURE 36B.5. A, Orientation of the choledochotomy and duodenot-
In patients at moderate to high risk for recurrent CBD stones, omy for anastomosis. B, Creation of the choledochoduodenostomy.
or in patients with distal strictures, biliary-enteric bypass may
provide the most durable result. The two primary options for
bypass are choledochoduodenostomy or Roux-en-Y hepatico- duodenal mobility after kocherization. In these cases, we
jejunostomy. Currently, there are inadequate comparative proceed with laparoscopic Roux-en-Y hepaticojejunostomy.
data to recommend one technique of biliary-enteric anasto- To perform a laparoscopic choledochoduodenostomy we
mosis over another (see Chapters 31 and 36A). There are a use a trocar placement similar to that described for the trans-
number of retrospective studies comparing the two anastomo- duodenal sphincterotomy (see Fig. 36B.1B). A Kocher maneu-
ses that show equivalent outcomes and morbidity (Luu et al, ver is performed to mobilize the duodenum enough to perform
2013; Narayanan et al, 2013; Santore et al, 2011). Choledo- a tension-free anastomosis to the CBD. The degree of kocher-
choduodenostomy has been criticized in the past due to ization ultimately depends on individual anatomy and mobility
concern of reflux of enteric contents into the CBD leading to of the duodenum. Next, approximately 2 cm of the anterior
chronic inflammation and recurring bouts of cholangitis, surface of the distal CBD is exposed. The dissection plane
referred to as the sump syndrome (Khajanchee et al, 2012; should remain anterior to the duct to avoid injury of the blood
Tang et al, 2003). Results of analysis by several authors supply to the proximal duct. A thorough laparoscopic ultra-
suggest that symptoms associated with sump syndrome may sound examination should be performed to identify the CBD
actually be a mechanical problem associated with a narrow and verify the location of any stones. A 1.5-cm supraduodenal,
anastomosis (de Almeida et al, 1996; Degenshein, 1974; longitudinal choledochotomy is made in the anterior wall of the
Madden et al, 1970). duct by using electrocautery or ultrasonic shears. A choledo-
Our current preference is laparoscopic choledochoduode- choscope is then inserted through the choledochotomy, and a
nostomy as it is technically easier, leads to a more physiologic thorough examination is performed. Biopsies should be taken
reconstruction, and importantly, allows direct access to the if there are any concerns for a neoplastic process. A 1-cm lon-
biliary system should further evaluation or manipulation of the gitudinal duodenotomy is made in the adjacent postbulbar
duct be necessary (Moraca et al, 2002; O’Rourke et al, 2004). duodenum. The duodenotomy is created shorter than the duc-
However, choledochoduodenostomy may not be possible in the totomy due to the inevitable stretching of the duodenotomy
setting of significant duodenal inflammation or inadequate (Fig. 36B.5A).
A. Gallstones and Gallbladder Chapter 36B Stones in the bile duct: minimally invasive surgical approaches 609
diagnose biliary stone disease, differentiate it from neoplastic and the capabilities of their team; they also must understand
processes, and treat it with high levels of success and decreasing the tools and talent available within their institutions. Finally,
morbidity. this knowledge must be applied to the particular clinical sce-
We have reviewed a wide range of approaches to the man- nario of each individual patient.
agement of patients with CBD stones. In managing this group
of patients, surgeons must assess their own surgical expertise References are available at expertconsult.com.
C. Biliary Infection and Infestation Chapter 36B Stones in the bile duct: minimally invasive surgical approaches 610.e1
611
612 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
A B
FIGURE 36C.2. Endoscopic retrograde cholangiopancreatography in
a patient with Billroth II partial gastrectomy showing insertion of a cath-
eter (curved arrow) (A) and placement of a guidewire and short biliary
endoprosthesis (solid arrow) (B) immediately before needle-knife sphinc-
terotomy and demonstration of common bile duct stones (open arrows).
FIGURE 36C.1. Endoscopic retrograde cholangiopancreatography
showing cholangiography with dilated bile duct, a single duct stone just
below the endoscope, a guidewire, and a sphincterotome in position
during sphincterotomy (arrows).
Difficult Stones
The most difficult circumstances encountered during endo-
scopic stone removal result from technical difficulties with
achieving deep biliary cannulation or in performing ES. These
difficulties are sometimes because of an inaccessible papilla
related to aberrant anatomy or unfavorable duodenal or papil-
lary structures, such as a periampullary diverticulum, or prior
surgery, such as Bilroth II or Roux-en-Y reconstruction. Tech-
niques have been described for the unique challenge of selective
bile duct cannulation in a patient with a Bilroth II partial gas-
trectomy (Lin et al, 1999). The performance of ES is also a
challenge because the visualized anatomy is inverted. In espe-
cially difficult cases, needle-knife sphincterotomy with a stent, FIGURE 36C.3. Endoscopic retrograde cholangiopancreatography
nasobiliary drain, or guidewire used as a guide for cutting showing large stone in the proximal bile duct (arrows) and basket extrac-
may be an option, or specially designed reverse-direction tion of a distal bile duct stone (chevrons) after endoscopic
accessories. The literature on techniques of cannulation and sphincterotomy.
A. Gallstones and Gallbladder Chapter 36C Stones in the bile duct: endoscopic and percutaneous approaches 613
sphincterotomy in Roux-en-Y reconstructions is limited (Wright to the stones, and the presence of coexisting pathology (e.g.,
et al, 2002), but some success has been reported with balloon stricture or tumor). Stones that are likely to be more difficult
enterosocopy or overtube-assisted ERCP (Kikuyama et al, to extract and may require adjuvant techniques to remove them
2009; Koornstra et al, 2008). are those that appear larger than the endoscope on radiographic
When ES has been successfully performed, extraction may imaging (usually >15 mm); stones that are numerous or hard
be hindered by a variety of stone factors—including size, in consistency; stones that are square, piston shaped, or faceted
number, consistency, shape, and location of stones—and ductal that tightly fit the bile duct or that are packed against each
factors such as contour and diameter at the level of and distal other; intrahepatic stones; or stones located proximal to a stric-
ture or narrowed distal bile duct or in a sigmoid-shaped duct.
Methods that have been developed to dilate the papillary
orifice, reduce stone size, and facilitate endoscopic removal
include endoscopic papillary large balloon dilation (EPLBD),
ML, intracorporeal lithotripsy with laser or electrohydraulic
probes, extracorporeal shock-wave lithotripsy (ESWL), and
chemical contact dissolution therapy. Treatment options
must be discussed jointly by the endoscopist, surgeon, and
interventional radiologist when difficulties are encountered
(Fig. 36C.6).
A B
FIGURE 36C.5. Endoscopic retrograde cholangiopancreatography series showing technique of balloon dilation of the papilla for extraction of small
stones. A, Initial cholangiography with demonstration of three small stones (long arrows, left) and placement of a guidewire and insertion of an 8-mm
dilating balloon located between two radiopaque markers (small arrows, right). B, Inflation of the dilating balloon (left) followed by insertion of an
extraction basket for stone removal (right).
614 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
Mechanical Lithotripsy
Removal of large CBD stones is a challenge for the most skilled
endoscopists. ML (see Chapter 27) (Leung & Tu, 2004; Leung
et al, 2001) remains an excellent option for stones that cannot
be removed by conventional techniques because it can be used
safely and effectively during the initial endoscopic procedure.
Mechanical lithotripters are modifications of standard Dormia
baskets and possess great tensile strength (Fig. 36C.7). The
reinforced basket is opened in the CBD, and the stone is
entrapped within the braided wires. This procedure can be
performed through the endoscope instrumentation channel, or
FIGURE 36C.6. Endoscopic retrograde cholangiopancreatography it can be done after the endoscope has been removed from the
showing a dilated bile duct containing multiple faceted stones in a post patient and a metal sheath has been extended over the inner
cholecystectomy patient positioned such that standard extraction tech- Teflon catheter. The end of the metal sheath is attached to a
niques might be difficult.
winding mechanism, which retracts the basket when cranked
and impales the stone against the rigid distal end of the metal
sheath leading to stone fracturing. The stone fragments can be
Further research has shown that endoscopic sphincterotomy removed with the same basket or a standard retrieval basket or
with EPLBD can obviate the need for ML. A recent review of balloon. In experienced centers, this technique allows removal
seven studies included 902 patients and compared ES with of more than 90% of difficult bile stones that are refractory to
EPBLD versus ES with standard techniques (Madhoun et al, standard extraction techniques, but multiple procedures may
2014). The authors found no differences in ductal clearance be required to achieve complete ductal clearance (Akcakaya
between the EPLBD and standard-techniques groups (98% vs. et al, 2009; Chang et al, 2005; Shaw et al, 1993; Van Dam &
95%, P = .6), but patients in the EPLBD group needed less Sivak, 1993).
ML. The use of EPLBD had a risk reduction of 0.58 (0.32 to
0.74) in terms of adverse events. Other Lithotripsy Modalities
Although the studies mentioned in the previous sections For the 5% of patients with biliary stones resistant to ES and
demonstrate the safety of EPLBD, there has been concern for ML, other methods are available, including intracorporeal tech-
the rare but serious complications, such as bleeding, perfora- niques (laser or electrohydraulic probes) and ESWL (Adamek
tion, and pancreatitis related to stretching the ampullary orifice et al, 1996). The choice between these methods or surgery
to such a large size. A recent review of 33 publications that depends largely on availability and local expertise.
included 2924 total procedures compared the complication
rates of EPLBD with a large ES, with limited ES, and without Electrohydraulic Lithotripsy
ES (Kim et al, 2013). The rate of adverse events was less than Since its development during the 1950s in the former Soviet
10% in each group and not significantly different between the Union as a method to fragment rocks during mining, EHL has
three groups. The rates of severe complications such as pan- been adapted for medical use in the treatment of nephrolithiasis
creatitis (all <4%) and perforation (all <0.5%) were acceptable and, more recently, biliary tract calculi. The electrohydraulic
and also not significantly different among the three groups. The probe consists of two coaxially isolated electrodes at the tip of
rate of bleeding, however, was highest in the large ES group, a flexible catheter, which is capable of delivering electric sparks
at 4.1%, which was significantly higher than the limited-ES and in short, rapid pulses leading to sudden expansion of the sur-
no-ES groups (1.3% vs. 1.9%, respectively). rounding liquid environment and generating pressure waves
A multicenter retrospective study that included 946 patients that result in stone fragmentation (Picus, 1990). Direct chol-
who underwent EPBLD for CBD stones greater than 10 mm angioscopy with either mother-daughter cholangioscopes
in size sought to determine the predictive factors of adverse (Hixson et al, 1992) or single-operator cholangioscopy (SOC)
events in EPLBD (Park et al, 2013). Based on their findings systems, such as the SpyGlass (Boston Scientific, Natick, MA)
authors gave these recommendations for safe EPLBD: (1) Indi- direct visualization system, are used to target the stones to
cation should be patients with a dilated CBD without distal facilitate stone contact with the electrode and to avoid ductal
CBD strictures. (2) Avoid full-ES immediately before LBD to trauma or perforation (Aljebreen et al, 2014; DiSario et al,
A. Gallstones and Gallbladder Chapter 36C Stones in the bile duct: endoscopic and percutaneous approaches 615
A B
FIGURE 36C.7. Endoscopic retrograde cholangiopancreatography sequence showing use of transendoscopic mechanical lithotripsy. A, Positioning
of the mechanical lithotripsy basket with its metallic sheath in the proximal bile duct (left) and its slow withdrawal toward the distally placed stone to
entrap it (right). B, Process of lithotripsy after stone entrapment within the basket (left) as the basket wires cut through the stone (right) to produce
stone fragmentation.
2007). Continuous saline irrigation is used with the bipolar with normal saline is needed to provide a medium for the
electrode placed at the surface of the stone to provide a media transfer of energy and to help clear stone fragments (Lee et al,
for shock-wave energy transmission, to flush away debris, and 2012). Despite the fragmentation of stones, standard tech-
to maintain adequate visualization (DiSario et al, 2007). niques such as balloon sweep or mechanical lithotripsy may still
Reports document complete stone clearance after multiple ses- be required to completely clear the duct of all debris. A study
sions in 86% of patients (Adamek et al, 1996; Arya et al, 2004; published in 2007 described how the holmium laser can frag-
Hixson et al, 1992; Siegel et al, 1990), and in a prospective ment stones regardless of their composition, whether they are
nonrandomized trial, EHL was comparable to ESWL in stone cholesterol, pigment, or calcium stones (Yates et al, 2007). The
clearance (Adamek et al, 1996). holmium laser has a high absorption coefficient in water and
The largest study of EHL performed to date is a retrospec- therefore has a better safety margin and has more than 100
tive review of 94 patients with difficult biliary stones referred times the energy absorption than the neodymium laser (Maydeo
to a tertiary hospital (Arya et al, 2004). The authors used a et al, 2011). Despite the safety profile, to prevent bile duct
mother-daughter cholangioscope and achieved fragmentation injury, it is necessary to use direct visual control while perform-
in 96% of the patients, with an eventual stone clearance rate of ing holmium laser lithotripsy, which also allows real-time
90%. Seventy-six percent of these patients required only one assessment of any biliary injuries (Hochberger et al, 2003;
EHL session, and most patients did not need additional ses- Sauer et al, 2013).
sions to help clear residual stones or debris. Complications Cholangioscopy was classically performed using mother-
included cholangitis (14%), pancreatitis (1%), and hemobilia daughter scopes with two endoscopists, but several recent
(1%) that was successfully treated with epinephrine. Another studies demonstrate the safety and efficacy of the SpyGlass
retrospective review of 26 patients examined EHL for difficult SOC for laser lithotripsy with the holmium :YAG laser. A pro-
biliary stones by using a single-operator duodenoscope-assisted spective study in 2011 examined 60 patients with choledocho-
cholangioscope (Farrell et al, 2005). All of the patients achieved lithiasis who either failed therapy with conventional methods
complete ductal clearance without any complications, and 58% or were referred for management of potentially difficult stone
of the patients only needed one session of EHL. A recent ret- removal (Maydeo et al, 2011). Complete ductal clearance
rospective review studied 13 patients who underwent EHL with using the Spyglass SOC system with the holmium :YAG laser
the SpyGlass SOC and demonstrated a ductal clearance rate of was achieved in 50 patients (83.3%) in one session, and the
100% with a mean number of EHL procedures at 1.6 per remaining patients achieved ductal clearance after one addi-
patient (Aljebreen et al, 2014). There was only one complica- tional session. Complications included fever in 3 patients
tion of cholangitis, treated conservatively with antibiotics. (although these patients were already admitted with cholangi-
tis), postprocedure pain requiring hospital admission in 4
Laser Lithotripsy patients, and a biliary stricture in 1 patient who developed a
Reports of the use of a holmium : yttrium-aluminum-garnet stricture proximal to the stone, which was successfully treated
(holmium :YAG) laser lithotripsy for choledocholithiasis was with dilation using a 10-Fr biliary stent for 3 months. The
first published in 1998 (Burdick et al, 1998; Das et al, 1998). authors were not sure if the stricture was caused by the laser
During holmium laser therapy, continuous ductal irrigation therapy or the stone itself. Holmium laser therapy has also been
616 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
used to treat patients with cystic duct stones (CDS) and Mirizzi
syndrome (MS) using the Spy Glass SOC. A retrospective
study at a single center described 34 patients: 31 with MS, 3
with CDS (Bhandari et al, 2016). All of the Mirizzi syndrome
patients had successful removal in one session, and 2 of the
CDS patients needed a second session for stone removal.
6 months without any complications related to stent placement. 1985; Nakajima et al, 1979; Reiter et al, 1978; Safrany, 1978;
In patients in whom complete ductal clearance is not feasible Schumacher et al, 1998; Seifert et al, 1982; Sherman et al,
on the index ERCP, FC-SEMS placement can greatly improve 1991; Siegel, 1981; Vaira et al, 1989) with individual and col-
the chances of success on the subsequent ERCP while also lected series of 430 to 9041 patients range from 75% to 96%
minimizing the need for advanced lithotripsy techniques. for duct clearance, with a median value of 91%.
Long-Term Morbidity
FIGURE 36C.9. Computed tomographic scan of the stomach, with Long-term follow-up of 1 to 15 years after ERCP with ES in
oral contrast administration showing extensive retroperitoneal, intraperi- postcholecystectomy patients (Cotton, 1984; Escourrou et al,
toneal, and subcutaneous air caused by a perforation from endoscopic 1984; Hawes et al, 1990; Ikeda et al, 1988; Rosch et al, 1981;
sphincterotomy. The patient made an uneventful recovery on conserva-
Seifert et al, 1982; Sivak, 1989) has demonstrated that more
tive treatment.
than 90% of patients are well on symptomatic review, and 7%
to 11% have significant symptoms secondary to recurrent
stones (5%), with or without stenosis of the ES site (1.5% to
tamponade of the sphincterotomy site, injection of dilute epi- 3%) and cholangitis (2%). Most of these long-term complica-
nephrine (1 : 10,000), bipolar cautery, and placement of hemo- tions are amenable to further endoscopic treatment.
static clips (Grimm & Soehendra, 1983; Leung et al, 1995;
Wilcox et al, 2004). Temporary placement of FC-SEMS can LAPAROSCOPIC AND PERCUTANEOUS
provide durable hemostasis through long-term tamponade of APPROACHES TO BILE DUCT STONES
the bleeding site, with efficacy demonstrated in a small case
series (Debenedet et al, 2013). In rare cases of major arterial Laparoscopic Common Bile Duct Exploration
hemorrhage, endoscopic view of the papillary area is obscured Laparoscopic CBD exploration (see Chapter 36B) was first
by blood, precluding any further endoscopic therapies. In these performed in the early 1990s and typically performed at expe-
patients, angiography with superselective embolization of the rienced tertiary referral centers (Khoo et al, 1996; Martin et al,
active bleeding site has been shown to be highly effective 1998; Rhodes et al, 1995). Ductal exploration may be accom-
(Maleux et al, 2014). Accordingly, surgical management for plished through the cystic duct or directly through a choledo-
post-ERCP bleeding has become uncommon in hospitals with chotomy. The transcystic route is the least invasive and generally
interventional radiology services. does not require any ductal manipulation or drainage proce-
Duodenal perforation is relatively rare and is either a small dure, whereas choledochotomy requires either closure of the
retroperitoneal perforation related to the sphincterotomy or a duct over a T-tube or primary closure of the choledochotomy
large duodenal perforation from the shaft of the scope. The with or without a biliary stent placed in an antegrade fashion
perforation may be asymptomatic and noticed only as retroperi- without need for a T-tube (Huang et al, 1996; Rhodes et al,
toneal gas (Fig. 36C.9) or extravasation of radiographic con- 1995). Bile duct clearance rates average 90%, with a median
trast material, but even in a symptomatic patient, conservative rate of conversion to open operation of 4% (Tranter & Thomp-
treatment is often effective, with spontaneous resolution and son, 2002). Complication rate is 2.5%, with a median mortality
avoidance of potentially difficult surgery. Occasionally, this rate of 1% (Strasberg et al, 1995).
complication presents late after ES with a retroperitoneal col- Multiple randomized clinical trials have been performed
lection of bile or pus in the flank or inguinal region (Leese et al, comparing single-stage laparoscopic CBD exploration at the
1985; Neoptolemos et al, 1984) and requires percutaneous or time of cholecystectomy versus a two-stage approach with
surgical drainage. ERCP preceding or following laparoscopic cholecystectomy
Cholangitis is confined almost completely to patients in (Cuschieri et al, 1996; Ding et al, 2014; Rhodes et al, 1998;
whom CBD clearance has not been achieved, and measures Rogers et al, 2010). The results of these trials have been strik-
should be directed at providing adequate bile drainage (e.g., by ingly similar, demonstrating similar ductal clearance rates for
nasobiliary catheter or endoprosthesis) and administering par- both groups (75% to 95%) with comparable rates of complica-
enteral antibiotics. Gallstone ileus is a rare complication, but tions and mortality. In studies that examined hospital param-
its recognition needs to be emphasized because symptoms may eters, the single-stage surgical approach offered lower length of
be obscure in elderly patients, and they occur many days after stay and reduce hospital costs. Length of stay and associated
ERCP and stone release; treatment is along standard surgical hospital costs can be reduced with improved coordination
lines (see Chapter 43). between the surgeon and the endoscopist. Although the single-
The impaction of an extraction basket occurs rarely in expe- stage approach appears at least equivalent to the two-stage
rienced hands because many endoscopic maneuvers have been approach, implementation of this strategy is restricted to centers
A. Gallstones and Gallbladder Chapter 36C Stones in the bile duct: endoscopic and percutaneous approaches 619
with significant expertise in laparoscopic bile duct exploration. 2015). Endoscopic treatment can be performed safely in preg-
Conversely, most facilities have ready access to ERCP services, nant patients (Jamidar et al, 1995; Kahaleh et al, 2004;
and thus a two-stage approach is the most common strategy in Simmons et al, 2004; Tham et al, 2003) using techniques to
the United States. minimize fluoroscopy. A recent retrospective study using the
Nationwide Inpatient Sample demonstrated a higher risk of
Percutaneous Approach post-ERCP pancreatitis in pregnant patients (12%) compared
In the 5% to 10% of patients for whom the endoscopic approach with control patients (5%); multivariable analysis confirmed
is unsuccessful at clearing the CBD of stones, two nonsurgical pregnancy was an independent risk factor for post-ERCP pan-
approaches are available: a rendezvous procedure and a complete creatitis (Inamdar et al, 2016).
percutaneous procedure (see Chapter 30). If the papillary region
can be reached endoscopically, yet deep biliary cannulation is Patients With Gallbladder in Situ
unable to be achieved, then the rendezvous procedure may be In elderly patients or in patients with significant comorbidity,
used. Although typically used for patients with obstructive a deliberate decision often is made to leave the gallbladder in
jaundice from pancreaticobiliary malignancy, this technique situ after ERCP and CBD stone removal. The short- and long-
can be used for choledocholithiasis in patients with surgically term results and complications of ERCP with ES in patients
altered anatomy, such as a Bilroth II, or in patients with chal- with gallbladders do not differ from those in postcholecystec-
lenging papillary anatomy, such as a large periampullary diver- tomy patients (Kaw et al, 2002). The risk of deferring chole-
ticulum. This involves a two-stage procedure with the cystectomy was examined in a study of 120 patients with known
introduction of a percutaneous guidewire through the bile ducts gallstones who underwent successful ERCP with bile duct
and papilla into the duodenum in the first stage, followed by clearance; the study excluded patients who were not surgical
an ERCP (Dowsett et al, 1989; Martin, 1994; Tomizawa et al, candidates, and patients were randomized to laparoscopic cho-
2014; Verstandig et al, 1993). In one report of rendezvous lecystectomy within 6 weeks after ERCP or a wait-and-see
procedures for choledocholithiasis, 0.9% (15/1753) of ERCPs policy with median 2.5-year follow-up. Nearly half the patients
were unsuccessful at biliary cannulation, usually owing to duo- in the wait-and-see group developed biliary-related problems,
denal diverticula or Bilroth II anatomy (Calvo et al, 2001). including biliary pain and cholecystitis, which led to cholecys-
Three patients underwent surgery, and 93% of the remaining tectomy or repeat ERCP or both, whereas none of the patients
patients underwent a successful rendezvous procedure. There in the cholecystectomy group experienced biliary-related prob-
was one complication with a retroperitoneal perforation that lems. The wait-and-see group also had a higher rate of conver-
required surgical management, and during follow-up, only one sion to an open procedure at the time of surgery (Boerma et al,
patient developed recurrent choledocholithiasis, requiring a 2002). A meta-analysis of randomized trials comparing the
repeat rendezvous procedure. In the multicenter prospective wait-and-see approach with elective cholecystectomy confirmed
trial of endoscopic biliary sphincterotomy complications these findings, with a higher risk of biliary pain (relative risk,
(Freeman et al, 1996), the combined endoscopic-percutaneous 14.6), cholangitis (relative risk, 2.5) in patients who deferred
approach was a risk factor for the development of complica- cholecystectomy (McAlister et al, 2007). The risk of these
tions, with a high rate of complications at 22.6% and with 6.5% future biliary complications needs to be balanced with operative
classified as severe. EUS-guided rendezvous procedures are risk in patients with significant underlying comorbidity.
emerging as a viable alternative to percutaneous approaches for
bile duct access in patients with unsuccessful biliary cannula- Suspected Choledocholithiasis
tion (Iwashita et al, 2012) (see Chapter 29). In patients with suspected choledocholithiasis, it is imperative
The complete percutaneous approach is labor intensive and to perform a risk assessment for the presences of CBD stones
typically requires multiple sessions. It has been established as prior to cholecystectomy. The following algorithm accounts for
treatment for hepatolithiasis (Yeh et al, 1995) (see Chapters 39 the relative efficacy, safety, and cost-effectiveness of each pro-
and 44), but it may be used for choledocholithiasis. The pro- cedure and imaging study (Tse et al, 2004). Patients with any
cedure involves initial establishment of a transhepatic fistula, very strong predictor of CBD stones (visualized CBD stone on
followed by stone extraction under fluoroscopy or cholangios- imaging, cholangitis or bilirubin > 4) or two strong predictors
copy 7 to 8 days after the fistula forms. In a series of 31 patients of CBD stones (dilated CBD > 6 mm, bilirubin between 1.8
with failed endoscopic procedures, percutaneous biliary access and 4) should undergo preoperative ERCP. Moderate predic-
was achieved in all patients, and stone clearance was complete tors are any other abnormal liver function tests, age older than
in 87% after a mean of 5.6 sessions (Van der Velden et al, 55 years, and gallstone pancreatitis. Patients without any very
2000). All patients underwent balloon dilation of the papilla, strong, strong, or moderate predictors are deemed low risk for
and most patients required additional means of stone fragmen- CBD stones and should proceed directly to cholecystectomy.
tation, including ML, EHL, and ESWL. Complications includ- All remaining patients are at intermediate risk for CBD stones
ing pancreatitis and bacteremia occurred in 9.7% and did not and should either undergo preoperative MRCP or EUS, fol-
require surgical intervention. The 4 patients who did not lowed by ERCP if CBD stones are visualized. Alternatively,
respond to percutaneous management underwent surgery. depending on local expertise, these intermediate-risk patients
can proceed with laparoscopic cholecystectomy with intraop-
SPECIFIC CLINICAL SCENARIOS erative cholangiogram; patients can then proceed with laparo-
scopic bile duct exploration or undergo postoperative ERCP.
Pregnancy In patients who undergo preoperative ERCP, it is important to
Symptomatic choledocholithiasis during pregnancy poses a minimize the time between the ERCP and cholecystectomy, to
diagnostic and therapeutic challenge. Biliary tract stone disease reduce the risk of recurrent CBD stones prior to surgery. Sub-
occurs in approximately 1.5% of pregnancies (Ellington et al, sequent studies have found this algorithm to be moderately
620 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
accurate (60% to 70%) for predicting the presence of CBD suggesting the possibility that early stone extraction by surgical
stones; the remaining patients did not have CBD stones on or endoscopic techniques would halt progression of the acute
ERCP despite having criteria suggestive of choledocholithiasis event and prevent the development of future attacks in the
(Adams et al, 2015; Sethi et al, 2016). short term.
Early surgical therapy in cases of acute biliary pancreatitis
Acute Cholangitis (ABP) has been challenged owing to the high operative morbid-
Acute cholangitis (see Chapter 43) resulting from CBD stones ity and mortality. Results and conclusions from numerous
traditionally was managed by supportive measures and paren- series comparing early and late surgical therapy in gallstone
teral antibiotics, followed by early surgery if improvement was pancreatitis are difficult to interpret. The mortality rates range
slow or absent. In early reports, the mortality from emergency from 2% to 67%, studies are retrospective with frequent com-
surgery ranges from 12% to 16%, with higher rates for elderly parisons to historical controls, and stratification for severity of
patients (Boey & Way, 1980; Cotton, 1984; Thompson et al, illness has not been used (Acosta et al, 1978; Kim et al, 1988;
1982). The only randomized trial of emergency endoscopic Osborne et al, 1981; Ranson, 1979). In one study, Kelly and
versus surgical management of severe calculous cholangitis (Lai Wagner (1988) prospectively randomized 165 patients with
et al, 1992) showed a threefold difference in mortality rate gallstone pancreatitis to early or delayed surgery. In the group
(10% vs. 32%; P < .03) in favor of ERCP. In patients who are with severe pancreatitis, mortality was 48% after urgent opera-
hemodynamically stable, it is reasonable to proceed with ES tive intervention compared with 11% mortality rate in patients
during ERCP with removal of all calculi. Care must be taken in whom surgery for gallstones was delayed for more than 48
to minimize aggressive contrast injection (particularly during hours. In contrast, patients with mild pancreatitis had mortality
balloon-occluded cholangiography) to reduce the potential risk rates of 3.3% and 0%, respectively. Another study of moderate
of bacteremia from the procedure. In patients with hemody- to severe gallstone pancreatitis with peripancreatic fluid collec-
namic compromise, procedure duration can be minimized tions confirmed these results, with complications in 44% of
using a two-stage approach, placing a plastic biliary stent patients in the early surgery group compared with 6% in the
without sphincterotomy to achieve biliary decompression, delayed surgery group (Nealon et al, 2004).
which leads to resolution of cholangitis (Hui et al, 2003). After The results of these aforementioned studies favor avoidance
the patient’s clinical status has improved, a second ERCP can of early operative intervention in the acute phase of biliary
be performed with ES, allowing complete ductal clearance of pancreatitis, as the previous surgical dictum was that inflam-
CBD stones. mation and edema from pancreatitis can distort biliary anatomy,
which would complicate surgeries and predispose patients to
Gallstone Pancreatitis bile duct injury (da Costa et al, 2015). However, recent robust
Acute pancreatitis (see Chapters 55 and 56) resulting from clinical data have challenged this thought process, leading to a
gallstones in the ampulla of Vater was first reported by Opie in paradigm shift favoring cholecystectomy during the initial hos-
1901. From his observations in this study, an “obstructive pitalization for ABP, once the acute inflammatory process has
theory” was derived to explain the mechanism responsible for improved.
gallstone pancreatitis. Current evidence suggests that transient A U.K. study retrospectively reviewed admissions to the
stone impaction in the common channel of the pancreatic duct hospital while awaiting an elective outpatient cholecystectomy
and CBD causes increased pancreatic ductal pressure with after an episode of biliary pancreatitis (Cameron et al, 2004).
associated inappropriate activation of pancreatic enzymes Of the 58 patients awaiting laparoscopic cholecystectomy, 21%
(Hirano et al, 1993). In support of the obstructive theory, gall- had unplanned readmissions if waiting for more than 28 days;
stones can be recovered from the feces of 85% to 95% of no patients who had cholecystectomy within 28 days had recur-
patients (Acosta & Ledesma, 1974; Kelly, 1980a, 1980b), and rent admissions. The presence of a sphincterotomy did not
the incidence of CBD stones is 80% in patients undergoing affect readmission rates despite the fact that no patients with
urgent operative or endoscopic intervention compared with a ES returned with ABP, as they instead returned with cholecys-
5% to 30% incidence when the procedure is delayed (Acosta titis or biliary colic. These results were echoed by another
et al, 1978; Kelly, 1980a, 1980b; Ranson, 1979; Stone et al, European study that looked retrospectively at 80 patients with
1981). ABP who had ERCP with ES (Mador et al, 2014). Authors
The Ranson, Imrie, Glasgow, and Acute Physiology, Age, found a 60% rate of recurrent biliary complications (pancreati-
and Chronic Health Evaluation (APACHE II) assessments tis, symptomatic choledocholithiasis, colic) in patients who
provide well-established criteria for assessing the severity of delayed cholecystectomy versus 2% in the group who under-
pancreatitis and predicting local adverse events—such as necro- went early cholecystectomy (P < .0001). A recent multiinstitu-
sis, hemorrhage, infection, and pseudocyst formation—and tional randomized control trial of 266 patients with mild
systemic complications of acute respiratory distress syndrome, gallstone pancreatitis has been performed. In this study, 129
disseminated intravascular coagulation, distant fat necrosis, patients were randomly assigned to same-admission cholecys-
and renal failure (Banks, 1991). Stratifying patients by severity tectomy within 3 days, whereas 137 were randomized to inter-
based on these criteria has been helpful in directing appropriate val cholecystectomy within 25 to 30 days (da Costa et al,
management. Most patients experience mild pancreatitis result- 2015). Readmission for gallstone related complications (pan-
ing from transient impaction of a stone in the ampulla, followed creatitis, cholecystitis, cholangitis, jaundice, colic) were signifi-
by spontaneous migration into the duodenum. These patients cantly more common in the interval group than the
do well with conservative therapy alone and are unlikely to same-admission group (17% vs. 5%, P = .002). These results
benefit from urgent intervention. In contrast, it has been pro- remained significant when comparing patients with endoscopic
posed that more severe cases of pancreatitis result from persis- sphincterotomy in a subgroup analysis. As with the previous
tent stone impaction or choledocholithiasis with infected bile, retrospective studies, there was no difference in length of stay,
A. Gallstones and Gallbladder Chapter 36C Stones in the bile duct: endoscopic and percutaneous approaches 621
difficulty of surgery, conversions from laparoscopic to open Urgent ERCP resulted in a reduction of biliary sepsis from 12%
surgery, or health care use between the two groups. in the conservatively treated patients to 0% in patients undergo-
Because of this paradigm shift in the surgical management ing ERCP. Overall, no significant differences were found in the
of biliary pancreatitis, along with the change in guidelines rec- incidences of either local (10.3% vs. 12.2%) or systemic (10.3%
ommending cholecystectomy on the index admission, a retro- vs. 14.3%) complications. In the subset of patients with severe
spective review recently studied how the implementation of an pancreatitis and CBD stones, urgent ERCP resulted in a
acute-care surgery (ACS) service for biliary disease affected decrease in the combined incidence of local and systemic com-
outcomes in biliary pancreatitis (Murphy et al, 2015; Tenner plications to 21% and mortality rate to 5.3% compared with
et al, 2013). The rate of index cholecystectomy increased from the conservatively managed group, in which the rates were
2.4% to 67% (P < .001) after the implementation of the ACS 68.8% and 25%, respectively. Patients with biliary obstruction
service, which correlated with a decrease in readmission rate and cholangitis were also included in this study. A third ran-
for biliary related disease from 16.8% to 7.3% (P = .04). domized trial (Nowak et al, 1995) studied 280 patients with
Although an ACS service is not a new concept, the study dem- ABP who all underwent urgent ERCP within 24 hours of onset
onstrates the importance of inpatient consultation and prompt of their disease; nearly 25% were found to have impacted stones
evaluation by a surgical service that adheres to the current at the papilla, which were treated by immediate sphincterot-
management guidelines. omy. The remaining 205 patients were randomized to conven-
The data regarding cholecystectomy in patients with severe tional treatment or sphincterotomy regardless of the
ABP with complications such as multiorgan failure or necrosis cholangiographic findings. Compared with conventional treat-
are not as robust, and a recent Cochrane Review states that ment, the authors showed a significant advantage for patients
there is currently no evidence to support or refute early lapa- treated endoscopically with respect to morbidity (17% vs. 36%;
roscopic cholecystectomy for patients with severe acute pancre- P < .001) and mortality (2% vs. 13%; P < .001). Further review
atitis (Gurusamy et al, 2013). Usually a delay in surgery in of these findings is not possible, as the study was only published
these patients is secondary to critical illness or while awaiting in abstract form.
other surgical or endoscopic treatments for complications such Although the aforementioned studies support early ERCP
as a cyst-gastrostomy for a pseudocyst or debridement of in ABP, the patients included in these studies had associated
walled-off pancreatic necrosis. In patients who are too ill or conditions that would require an ERCP (cholangitis, jaundice),
have limiting comorbidities (severe coronary artery disease, and therefore the question of a biliary sphincterotomy in all
cirrhosis) to tolerate any type of surgery, there is a potentially patients with ABP cannot be answered by these data. A ran-
protective effect of an endoscopic sphincterotomy in preventing domized multicenter European study avoided these confound-
further biliary complications, although the data for the role of ing variables by examining the role of early ERCP with
ES in lieu of a cholecystectomy for a high-risk patient in the sphincterotomy in patients with ABP without cholangitis or
absence of choledocholithiasis are limited (May et al, 1991). jaundice (Folsch et al, 1997). Two hundred thirty-eight patients
In the acute setting, an endoscopic approach to biliary pan- were randomly assigned to early ERCP (within 72 hours) or
creatitis offers the theoretical advantage of immediate relief of conservative treatment. The overall mortality and complication
ampullary obstruction and ductal clearance without the risks of rates were similar between the two groups regardless of the
surgery. As animal models and human studies have suggested severity of pancreatitis, but the rate of serious respiratory failure
that the duration of biliary obstruction is a critical factor in was higher in the invasive group (P = .03). A recent meta-
determining the severity of pancreatitis, early resolution of analysis of the seven known well-designed, randomized,
obstruction with ERCP would theoretically ameliorate the controlled trials on this topic confirms these same findings
course of the disease (Kapetanos et al, 2010). The timing of (Uy et al, 2009).
ERCP in ABP has been controversial, and until recently, many According to the most recent high-quality published data,
studies did suggest a role for early ERCP (Fogel et al, 2014). the current practice management guidelines state that early
Three oft-quoted studies in previous guidelines and reviews ERCP is not needed in patients with ABP who lack the labora-
gave the antecedent evidence that early ERCP (within 72 hours) tory or clinical evidence of ongoing biliary obstruction or chol-
and sphincterotomy definitively reduced complications in ABP. angitis. In the absence of jaundice or cholangitis, noninvasive
The Leicester investigators (Neoptolemos et al, 1986) were methods such as MRCP and EUS should be used to screen for
the first to perform a controlled study to evaluate the efficacy choledocholithiasis (Fogel et al, 2014; Tenner et al, 2013).
of early ERCP in biliary pancreatitis. A group of 121 patients
with suspected gallstone pancreatitis was randomized to ERCP CONCLUSIONS
with stone extraction within 72 hours of hospitalization or
conventional nonendoscopic management. Patients with mild Endoscopic management of choledocholithiasis is widely
pancreatitis had similar outcomes regardless of treatment strat- accepted as a highly effective therapy for CBD stones. Endo-
egy. In the group of patients with severe pancreatitis, ERCP scopic techniques are well established, and accessories have
significantly reduced the morbidity from 61% to 24% and been developed to enhance success and safety. ERCP with ES
reduced the length of hospitalization from 17 days to 9.5 days, is the standard of care in the management of CBD stones in
but mortality was not different between the two groups. It is most clinical situations, regardless of the presence or absence
noteworthy that biliary obstruction and jaundice were not of the gallbladder. Advancement in endoscopic techniques
exclusion criteria in this study, and 11 of the patients had con- allows the management of complex bile duct stone disease. The
current cholangitis. A second study (Fan et al, 1993) prospec- endoscopic removal of stones in the perioperative period has
tively randomized 195 consecutive patients with pancreatitis of been shown to be effective, minimizing the need for CBD
any cause to urgent ERCP with ES or initial conservative treat- exploration. Patients with acute cholangitis should be consid-
ment with selective ERCP only if there is clinical deterioration. ered for urgent endoscopic management. ERCP is generally not
622 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
indicated in the management of gallstone pancreatitis in the suggest that the enthusiastic speculations of the early 1970s—
absence of associated obstructive jaundice or cholangitis. Inte- that in stone disease, the surgeon should treat the gallbladder,
grated endoscopic therapy for biliary disease is well established and the endoscopist should treat the bile duct—has come to
in centers where surgeons and endoscopists work closely pass 4 decades later.
together and provide each other with a suitable forum for criti-
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CHAPTER 37
Cholecystolithiasis and stones in the common bile
duct: which approach and when?
Mark P. Callery, Rachel E. Beard, and Lygia Stewart
623
624 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
these cases, obstruction of the cystic duct results in a contained showed a shorter hospital stay for early cholecystectomy patients
infection of the gallbladder. Research on the pathogenesis of and no significant difference in complication rates or conver-
gallstone-associated infections has shown that patients with sion rates between early laparoscopic cholecystectomy (within
bacteria-laden gallstones have more severe biliary infections. In 7 days) versus delayed laparoscopic cholecystectomy (6 to 12
addition, acute cholecystitis can coexist with choledocholithia- weeks) (Gurusamy & Samraj, 2006). Conversion rates, however,
sis, cholangitis, or gallstone pancreatitis. In the general popula- were 45% among patients randomized to the delayed group,
tion, 5% of patients presenting with cholecystitis have coexisting which required a cholecystectomy between 1 and 6 weeks. For
common bile duct (CBD) stones. In the elderly, however, this patients with significant medical problems, cholecystectomy
figure rises to 10% to 20% (Siegel & Kasmin, 1997). may need to be delayed to maximize medical therapy. Most of
The initial treatment for patients with acute cholecystitis is these patients with acute cholecystitis can be safely managed
intravenous hydration, antibiotics, and bowel rest. Many with antibiotics and bowel rest, with resolution of their acute
patients should be offered early cholecystectomy, but others will illness; they can then undergo an elective cholecystectomy once
benefit from delayed intervention, either following conservative their medical problems have been addressed.
therapy or percutaneous gallbladder drainage. Several factors
govern the approach to patients with acute cholecystitis. One GRADE II ACUTE CHOLECYSTITIS. Patients presenting with grade II
consideration is patient comorbidity; emergency cholecystec- acute cholecystitis are a more diverse group. Many will be well
tomy in patients with significant comorbidities can be associ- managed with early cholecystectomy; this is particularly true
ated with high morbidity (20% to 30%) and mortality (6% to for cases with delayed presentation as their only grade II finding.
30%) rates. Guidelines for the management of acute cholecys- In these cases, laparoscopic cholecystectomy should be per-
titis and acute cholangitis were described at an international formed, if possible, within 7 days of the acute illness. In cases
consensus meeting held in Tokyo in 2006, and updated guide- with severe local inflammation, early gallbladder drainage (per-
lines were then published in 2013 (Takada et al, 2007, 2013). cutaneous or surgical) is recommended as the initial treatment
The Tokyo Guidelines define three levels of severity for acute of choice, followed by elective cholecystectomy once the acute
cholecystitis and serve as a useful tool in the management of inflammation resolves (see Chapters 30 and 34). The key is to
acute cholecystitis (Table 37.2) (Yokoe et al, 2013). identify which patients have such an inflammatory process.
Several studies have correlated such findings as age older than
GRADE I ACUTE CHOLECYSTITIS. Patients presenting with mild 50 years, male sex, presence of diabetes, elevated bilirubin level
grade I acute cholecystitis should be offered early cholecystec- (>1.5 mg/dL), and leukocytosis (while blood cell count >
tomy, performed laparoscopically if possible. Several studies 15,000 mm3) with gangrenous cholecystitis (Nguyen et al,
have documented high success rates for laparoscopic cholecys- 2004). These findings are also frequently associated with a
tectomy when the procedure is performed within 72 hours of severe inflammatory process. Other factors suggestive of a sig-
onset of acute cholecystitis (Hadad et al, 2007; Yamashita et al, nificant inflammatory process include symptoms of gastric
2013). Further, a Cochrane Review of five randomized trials outlet obstruction. Patients with such symptoms should have
cross-sectional imaging, with either computed tomography
(CT) or magnetic resonance imaging, to determine whether a
TABLE 37.2 Tokyo Guidelines (TG13) Severity Grading for Acute severe inflammatory process is present (Fig. 37.1), followed by
Cholecystitis percutaneous cholecystostomy if such is found (Takada et al,
Grade Criteria 2007). In the updated 2013 Tokyo Guidelines, percutaneous
transhepatic gallbladder drainage remains the standard
I: Mild Acute cholecystitis that does not meet the criteria
for a more severe grade. Mild gallbladder
inflammation, no organ dysfunction
II: Moderate The presence of one or more of the following:
1. Elevated white blood cell count (>18,000/mm3)
2. Palpable tender mass in the right upper
abdominal quadrant
3. Duration of complaints > 72 hr
4. Marked local inflammation (biliary peritonitis,
pericholecystic abscess, hepatic abscess,
gangrenous cholecystitis, emphysematous
cholecystitis)
III: Severe Associated with dysfunction of any one of the
following:
1. Cardiovascular system: hypotension requiring
dopamine >5 µg/kg/min or any dose of
norepinephrine
2. Nervous system: decreased level of
consciousness
3. Respiratory system: PaO2/FiO2 ratio < 300
4. Renal system: oliguria, serum creatinine >
2.0 mg/dL
5. Hepatic system: PT-INR > 1.5 FIGURE 37.1. Computed tomographic scan demonstrating a severe
6. Hematologic system: platelet count < inflammatory process in the setting of acute cholecystitis. This patient
100,000/mm3 was treated with percutaneous cholecystostomy, followed by elective
FiO2, Forced inspiratory oxygen concentration; PaO2, partial pressure of oxygen in arterial blood; laparoscopic cholecystectomy once the inflammatory process had
PT-INR, prothrombin time/international normalized ratio. resolved.
626 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
drainage method for grade II cholecystitis that does not respond 2006). Biliary injuries are more likely to occur during difficult
to conservative therapy, although techniques such as percutane- laparoscopic operations, no different than with open operations,
ous transhepatic gallbladder aspiration and endoscopic naso- but at a higher incidence (see Chapters 38 and 42). When lapa-
biliary gallbladder drainage were also cited as alternatives roscopic cholecystectomy is performed for acute cholecystitis,
(Tsuyuguchi T, Itoi T, et al, 2013). biliary injuries occur three times more often than during elec-
tive laparoscopic cases and twice as often compared with open
GRADE III ACUTE CHOLECYSTITIS. Patients presenting with grade cholecystectomy for acute cholecystitis. Surgeons should there-
III acute cholecystitis have associated organ dysfunction. fore not hesitate to convert to an open operation if they experi-
Although this occurs rarely, approximately 6% of the time, it ence difficulties with the laparoscopic dissection or are unable
is important because these patients require intensive organ to clearly identify the critical view of safety (Strasberg et al,
support and medical treatment (Yasutoshi et al, 2013). Because 1995). Surgeons should also be aware of certain patient risk
the source of their inflammatory (septic) response and organ factors, including male gender, advanced cholecystitis, the pres-
dysfunction is the severe cholecystitis, percutaneous cholecys- ence of jaundice, and previous abdominal surgery, which are
tostomy (see Chapters 30 and 34) is necessary to treat the associated with an increased risk of conversion to open proce-
severe infection as well as the associated organ dysfunction. dure (Yamashita et al, 2013).
Numerous studies have documented the success of percutane- The decision to perform open cholecystectomy may be dif-
ous cholecystostomy in achieving control of the underlying ficult for some. Over the past 20 years, open cholecystectomy
infection within 24 to 48 hours (Howard et al, 2009). In rare has been far less frequently performed. Trainees during this
cases, urgent cholecystectomy may be required, such as cases period have less experience with open cases (Schulman et al,
with biliary peritonitis as a result of perforation of the gallblad- 2007). The experience and training needed to learn the lapa-
der; but in general, cholecystectomy in the acute phase of grade roscopic operation likely reduces the level of comfort with the
III acute cholecystitis should be avoided (Takada et al, 2007; open technique. Finally, there is the pressure related to patient
Tsuyuguchi et al, 2013). expectation for rapid recovery as well as, perhaps, the hospital
expectation for decreased length of stay and cost, as conversion
UNCOMMON PRESENTATIONS OF ACUTE CHOLECYSTITIS. Acalculous is associated with lengthier stays and increased expense (Lengyel
cholecystitis arises in the absence of cholecystolithiasis, and et al, 2012). Certain scenarios may thus arise that might subtly
associated risk factors include trauma, burns, and gastro- account in part for static biliary injury rates (Khan et al, 2007).
intestinal surgery (Crichlow et al, 2012) (see Chapter 33). Because of inexperience, the surgeon may ignore or resists the
Emphysematous cholecystitis is caused by infection with gas- sensible default option to convert to the open technique, per-
forming anerobes such as Clostridium perfringens. Diabetic sists with the laparoscopic approach, and causes injury. In other
patients are at risk, and the disease can progress quickly to instances, the surgeon overextends laparoscopic experience
profound sepsis. Emergent cholecystectomy is indicated. Gall- when disease severity warrants conversion. To prevent this,
bladder torsion can also occur when the gallbladder is especially patients need to be made fully aware that open cholecystectomy
mobile owing to a connection to the liver by a thin elongated is always a possibility, and the surgeon should not hesitate to
mesentery. Gallbladder perforation can occur as a result of seek help if needed, rather than rely on marginal laparoscopic
gallbladder wall ischemic and resulting necrosis. A localized or open cholecystectomy experience. Conversion from laparo-
perforation can result in formation of a pericholecystic abscess, scopic to open cholecystectomy is not a defeat but rather is
whereas free perforation can lead to biliary peritonitis. A biliary reflective of caution and good judgment (Jenkins et al, 2007;
fistula can also form between the gallbladder and the duode- Wolf et al, 2009).
num as a sequela of cholecystitis, and this can result in a gall- Ideally, a surgeon anticipates the likelihood of conversion on
stone ileus if a stone passes via this fistula and causes a clinical grounds. The anesthesia and operative teams should be
mechanical obstruction at the ileocecal valve (Kimura et al, so notified and prepared. Open-case instruments need to be
2013). readily available, and trocar placement should be along a pre-
drawn right subcostal incision line. Unless there is need to
Cholecystectomy Technique control bleeding, the surgeon enters the RUQ deliberately and
Choosing Laparoscopic Versus Open Techniques is not stressed by the decision to convert. Everyone should be
For typical uncomplicated symptomatic gallstone disease, lapa- ready for what lies ahead, and it should be clear to all that it
roscopic cholecystectomy is the preferred method of removing will be a difficult operation.
the gallbladder (Keus et al, 2006; Yamashita et al, 2013). Since The difficult open cholecystectomy demands adequate expo-
its origin, cholecystectomy rates have increased worldwide, sure, retraction, and identification of anatomy by dissection in
reflecting general acceptance of the laparoscopic technique. the anterior and posterior aspects of the triangle of Calot, fol-
Because the technical aspects of this operation are covered in lowed by dissection of the gallbladder off the liver bed. The
other chapters (see Chapter 35), this section will focus on surgeon achieves conclusive identification of the cystic struc-
concepts of feasibility and safety that relate to disease severity tures as the only two structures entering the gallbladder, elimi-
and the choice between laparoscopic and open cholecystectomy nating the possibility of misidentification (Callery, 2006). As
(Callery, 2006). with the laparoscopic technique, once the critical view is
Laparoscopic cholecystectomy for severe acute and chronic attained, the cystic structures can be ligated and divided. Failure
inflammation is a technically difficult and advanced operation. to achieve this critical view should prompt cholangiography to
Less experienced surgeons must recognize this and seek help define ductal anatomy. Avoidance of ductal injury in the liver
from a more experienced surgeon. Furthermore, the surgeon bed depends upon a combination of patience and staying in the
must understand that conversion to open cholecystectomy may correct plane of dissection, with meticulous technique and expe-
be necessary and is more likely in these cases (Ishizaki et al, rience. In some cases of acute cholecystitis, the gallbladder
A. Gallstones and Gallbladder Chapter 37 Cholecystolithiasis and stones in the common bile duct: which approach and when? 627
“shells out” relatively easily from its edematous hepatic bed. In Silent Common Bile Duct Stones
other cases, and especially in chronic cholecystitis, the dissection Published reports using routine intraoperative cholangiography
of the gallbladder out of the liver bed can be tedious, frustrat- have found that at least 12% of CBD stones are clinically silent
ing, and bloody. Hemostasis can take time and may require an (Murison et al, 1993), and approximately 6% do not exhibit
argon beam, cautery, packing, and topical hemostatics. Subtotal abnormalities in liver function tests (LFTs) or in the diameter
cholecystectomy is always a valid option, especially in patients of the CBD (Majeed et al, 1999). When prospectively followed,
with cirrhosis or in those with severe inflammation that obscures data suggest that more than one third of asymptomatic stones
the anatomy within the porta hepatis. Surgeons should indicate will pass spontaneously after the first 6 weeks after cholecystec-
in operative notes for open and laparoscopic cholecystectomy tomy (Collins et al, 2004).
precisely how they identified the cystic structures for division.
For conversions, they should specify the circumstances, stressing Diagnostic Considerations
safety and surgical judgment. More often than not, the presence of CBD stones is uncertain.
Clinicians use predictive models based on risk factors that
Percutaneous Cholecystostomy include clinical features, abnormal LFTs, jaundice, and CBD
The indications for percutaneous cholecystostomy include dilation. These are very sensitive (96% to 98%) but not very
grade II acute cholecystitis with a severe inflammatory process, specific (0% to 70%) (Koo & Traverso, 1996). The American
grade III acute cholecystitis with associated organ dysfunction, Society of Gastrointestinal Endoscopy (ASGE) provides a
or acute cholecystitis in patients with severe medical morbidity practical strategy that assigns low (<10%), intermediate (10%
that limits surgical options (Hirota et al, 2007; Howard et al, to 50%), or high (>50%) risk of CBD stones by using relevant
2009; Takada et al, 2007; Tsuyuguchi et al, 2013; Yamashita risk factors (ASGE Standards of Practice Committee et al,
et al, 2007). The technical success rate of percutaneous radio- 2010).
logically guided cholecystostomy is 98% to 100% with few
procedure-related complications (mortality and major compli- Imaging Modalities: Why and When
cations, 0% to 6.5%; minor complications, 0% to 20%) Transabdominal Ultrasound
(Howard et al, 2009; Sugiyama et al, 1998). Potential compli- Transabdominal ultrasound (US) is an appropriate initial
cations include intrahepatic hematoma, pericholecystic abscess, modality in the evaluation of CBD stones (Williams et al, 2008)
and biliary peritonitis and pleural effusion caused by puncture (see Chapter 15). US can identify bile duct dilation owing to
of the liver and subsequent migration of the catheter (Yamashita stone obstruction, and it can visualize the actual stone in some
et al, 2013). cases (sensitivity 0.3, specificity 1.0). If the extrahepatic bile
duct diameter is less than 5 mm, CBD stones are exceedingly
Timing of Subsequent Operation for Cholecystitis rare, whereas a diameter greater than 10 mm with signs of
Once the inflammatory process has resolved, elective chole- jaundice predicts the presence of CBD stones in more than
cystectomy can be performed early (within 1 to 7 days) or 90% of cases (Abboud et al, 1996). Axial CT scans have better
delayed (6 to 8 weeks) with excellent success and conversion sensitivity (84%) for choledocholithiasis than US. Helical CT
rates as low as 3% (Akyurek N, 2005). The optimal timing scans outperform conventional nonhelical CT, with 88% sen-
remains controversial due to a lack of randomized controlled sitivity and 73% to 97% specificity (Tseng et al, 2008). In
trials; however, early cholecystectomy following percutaneous terms of availability, cost, and radiation exposure, US prevails
drainage may be preferable if the procedure is free of compli- as the first-line diagnostic.
cations and the patient’s condition improves (Yamashita et al, Magnetic resonance cholangiopancreatography (MRCP) is
2013). Some have reported using percutaneous cholecystos- the most accurate noninvasive modality available. MRCP is the
tomy as definitive treatment for acute cholecystitis in high- standard investigation for CBD stones for patients with inter-
risk, elderly, and debilitated patients. In patients who do not mediate probability or for those who need to be investigated to
have subsequent cholecystectomy, recurrent biliary symptoms exclude other differential diagnoses. MRCP is especially helpful
occur in 9% to 33% (Griniatsos et al, 2008; Sugiyama et al, when anatomic considerations preclude ERCP (status post–
1998). Billroth II gastrectomy, Roux-en-Y biliary bypass, duodenal
stenoses). The drawback of MRCP is its high cost, which chal-
CHOLEDOCHOLITHIASIS lenges its routine use as a more front-line diagnostic modality
(Epelboym et al, 2013).
The clinical clues of CBD stones were recognized during the
Roman Empire by Soranus of Ephesus, who described jaun- Endoscopic Retrograde Cholangiopancreatography
dice, itching, dark urine, and acholic stools. Not all CBD stones ERCP is still considered the gold standard diagnostic modality
render such a classic clinical scenario, but they still carry risk (see Chapters 20, 29, and 36C), although it is invasive, requires
if left unidentified and untreated. More than 85% of CBD radiation, and has significant complications (Andriulli et al,
stones originate in the gallbladder and secondarily migrate into 2007). Observed complications following ERCP include pan-
the CBD. For patients undergoing cholecystectomy for symp- creatitis, hemorrhage, cholangitis, perforation, and a clinically
tomatic gallstones, the prevalence of choledocholithiasis ranges relevant mortality rate (Katsinelos et al, 2014). Routine ERCP
from 10% to 18% (Dasari et al, 2013). Primary CBD stones prior to all laparoscopic cholecystectomies is impractical and
are far less common and are typically associated with conditions unnecessary. When overused, most cholangiograms are normal,
of biliary infection and stasis, such as benign biliary strictures, and costs and complication rates are prohibitive. Even in
sclerosing cholangitis, and choledochal cysts. Primary CBD patients at high risk—those with jaundice, cholestatic LFTs,
stones are more prevalent in Asians and can sometimes be CBD dilation, and a history of pancreatitis—half will not have
related to parasitic infections (Kaufman et al, 1989). CBD stones at the time of ERCP (Daradkeh et al, 2000);
628 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
therefore ERCP is now reserved more for its therapeutic than tolerated in most, a 10% rate of complications remains constant
diagnostic strength. for ERCP (Andriulli et al, 2007), with a serious morbidity rate
of 1.5% and an overall mortality rate of 0.2% to 0.5% (Freeman
Endoscopic Ultrasound et al, 1996). When surgical and endoscopic teams are inexpe-
Endoscopic US (EUS) is very sensitive for choledocholithiasis rienced with CBD stones, the perceived need for preoperative
(Garrow et al, 2007) (see Chapter 16), and a meta-analysis ERCP increases. In this setting, ERCP allows laparoscopic
reveals that EUS can reduce unnecessary diagnostic ERCP cholecystectomy to be performed quickly and with confidence
(Tse et al, 2008). A systematic review reveals that patients who that CBD stones are already managed. If ERCP fails, the surgi-
undergo EUS can avoid ERCP in 67% of cases, with fewer cal plan will need to consider intraoperative management of
complications and less pancreatitis compared with those under- choledocholithiasis. Conversely, in centers where successful
going ERCP initially (Petrov & Savides, 2009). The diagnostic sphincterotomy and stone extraction is almost assured, the rate
efficacy of EUS and MRCP compared with ERCP have revealed of preoperative ERCP will be lower. If the surgeon finds a stone
the tests to be quite comparable (Palmucci et al, 2010; Verma at operation, ERCP becomes a reliable postoperative option.
et al, 2006). Current consensus accepts the use of ERCP prior to laparo-
scopic cholecystectomy for patients with a high probability of
Intraoperative Cholangiography choledocholithiasis. It is recommended that patients with a low
Intraoperative cholangiography (IOC) during cholecystectomy or intermediate index of suspicion for choledocholithiasis
can accurately diagnose CBD stones and both minimize and undergo additional imaging techniques (MRCP, EUS, IOC) to
maximize the need for ERCP. The technique can be performed avoid unnecessary biliary instrumentation (ASGE Standards
safely in both open and laparoscopic approaches. Surgeons can of Practice Committee, 2010; Tse et al, 2004; Williams et al,
respond to such findings, flushing the duct to clear stones or 2008).
debris. Open and laparoscopic IOC can successfully be com-
pleted in about 95% of patients (see Chapters 23, 36A, and PERCUTANEOUS TRANSHEPATIC CHOLANGIOGRAPHY. Compared with
36B), with sensitivity for detecting CBD stones between 80% ERCP, percutaneous transhepatic cholangiography (PTC) is
and 92% and specificity of 93% to 97% (Machi et al, 1999). time consuming, more involved, and likely more stressful
Regardless, an ongoing debate remains whether IOC should be for a patient. It is usually reserved for patients in whom ana-
performed routinely or selectively during cholecystectomy. tomic considerations preclude safe ERCP, such as in the
When used routinely, it has high sensitivity and specificity both case of an impossible ampullary cannulation. Experienced
for suspected CBD stones and for the 3% to 4% of stones that PTC groups have reported successful stone removal rates in
are not clinically suspected but may become symptomatic post- more than 90% of cases, with complication rates around 5%
operatively. Other suggested benefits specifically relate to the (Garcia-Vila et al, 2004), although these are hardly the norms.
prevention of bile duct injuries (Fletcher et al, 1999). The PTC stone removal takes time, involving insertions of catheters
randomized trials that have been performed to address this that are upsized over time, before stones are actually retrieved
question are small, and even a systematic review of these trials with stone baskets. Consequently, there are many reports of
was not sufficiently powered to demonstrate a significant benefit attempts to make it easier. Gil and colleagues (2000) have
(Ford et al, 2012). Because no large prospective randomized reported the safety and utility of balloon dilation of the papilla
trial has answered the question of whether routine IOC is ben- in the clearing of CBD stones using occlusion balloon pushing.
eficial,, most practicing surgeons perform IOC selectively. This is also gaining popularity for the laparoscopic surgeon
during IOC.
Symptomatic Common Bile Duct Stones
The symptoms of CBD stones relate to partial or complete Surgical Approaches: Open and Laparoscopic Techniques
biliary obstruction with and without inflammatory complica- The same issues discussed in choosing open versus laparo-
tions, such as cholangitis, hepatic abscesses, or pancreatitis. In scopic cholecystectomy are accentuated when common bile
chronic scenarios, and depending on the extent and duration duct exploration (CBDE) is considered (see Chapters 31, 35,
of biliary obstruction, choledocholithiasis may also lead to sec- and 36). Today, many trainees will graduate residency having
ondary biliary cirrhosis and portal hypertension. Because of the never performed an open CBDE. Their ability to succeed with
uncertain clinical behavior and potential harmful complications, laparoscopic CBDE is quite variable, as many train with a
it is currently accepted that in the great majority of situations, default dependence on ERCP.
CBD stones should be removed, even if they are asymptomatic
(Williams et al, 2008) (see Chapters 32 and 36). Approach to Recurrent Common Bile Duct Stones
In some instances, even following successful decompression
Definitive Treatment Approaches: Biliary Obstruction and stone removal of the common duct with ERCP, patients
Catheter-Based Approaches will continue to present with recurrent choledocholithiasis.
ERCP (SEE CHAPTERS 20, 29, 36B, AND 36C). Before the laparo- Such patients present a management challenge, with varying
scopic era, ERCP was not commonly used, because open surgi- treatment options. One possible endoscopic approach is
cal bile duct clearance was superior to ERCP in terms of balloon dilation of the papilla with concurrent stone removal,
success and morbidity (Martin et al, 2006). This changed as which has been shown to decrease subsequent CBD stone
laparoscopic cholecystectomy emerged and outpaced the abili- recurrences compared with stone extraction alone (Tsai et al,
ties of most surgeons to perform laparoscopic CBD stone 2015; Yoon et al, 2014). For patients who fail nonoperative
removal. Indeed, ERCP captured and has held its role as the treatments, surgical drainage may be necessary (see Chapters
first-line approach to CBD stones, being successful in more 31 and 36A). Described approaches include choledocholithot-
than 90% of patients (Rieger & Wayand, 1995). Although well omy and T-tube drainage, choledochoduodenostomy, and
A. Gallstones and Gallbladder Chapter 37 Cholecystolithiasis and stones in the common bile duct: which approach and when? 629
choledochojejunostomy, and there is evidence indicating that potential complications of an extra procedure (Clayton et al,
choledochoduodenostomy is the most successful approach for 2006; Martin et al, 2006).
preventing future recurrences (Li et al, 2007; Matsushima Although LCBDE can be safely performed through either
et al, 2012; Uchiyama et al, 2003). transcystic or choledochotomy approaches, most surgeons
prefer the transcystic approach. It is feasible in most cases,
CHOLECYSTECTOMY WITH INTRAOPERATIVE CHOLANGIOGRAPHY. Open saves time, does not violate the CBD, and shows no higher
and laparoscopic IOC can successfully be completed in the morbidity than standard laparoscopic cholecystectomy alone
majority of patients by the majority of surgeons (Machi et al, (Hanif et al, 2010; Tinoco et al, 2008). The most consistent
1999). IOC can be performed through the direct insertion of risk factor for failing transcystic stone clearance is the size of
contrast medium into the gallbladder or more often by intubat- the stone. Once stones exceed 5 mm, the likelihood of tran-
ing the cystic duct. Plain radiographs have largely been replaced scystic extraction falls considerably (Stromberg et al, 2008),
by digital fluoroscopic imaging. IOC is common, and most and laparoscopic choledochotomy becomes necessary. However,
surgeons receive sufficient training. Laparoscopic ultrasound many surgeons do not have the laparoscopic dissection and
cholangiography is also efficacious but not broadly used, and suturing expertise to perform this procedure; they rely instead
its utility is limited by its longer learning curve (Stiegmann on ERCP, or they convert to an open operation. Experienced
et al, 1995). Newer techniques such as hyperspectral cholangi- surgeons can remove larger or multiple CBD stones with
ography and near-infrared fluorescence cholangiography hold reported success rates of up to 90% (Lien et al, 2005).
promise and may become more widely used in the future (Bud- The question of how to close the CBD following exploration
dingh et al, 2011). remains a topic of debate. A 2007 Cochrane Review was not
Since the introduction of laparoscopic cholecystectomy, the able to conclude significant differences in outcomes for primary
debate over routine versus selective IOC has been rekindled closure of the CBD versus the routine use of T-tube drainage
because of the increased incidence of CBD injuries and the after open CBDE (Gurusamy et al, 2009). However, two 2013
inability to palpate the CBD during laparoscopy. IOC accu- Cochrane Reviews reported that T-tube drainage results in
rately defines the biliary anatomy and may protect against intra- longer operating times and hospital stays without any apparent
operative bile duct injuries (Fletcher et al, 1999) and may benefit over primary closure in both open and laparoscopic
reduce their severity (Woods et al, 1995). Opponents claim that CBDE (Gurusamy et al, 2013a, 2013b). Another 2012 meta-
routine IOC may lead to bile duct injury and unnecessary CBD analysis of randomized controlled trials confirmed the superior
explorations because of false positives and that it may add time safety and effectiveness of primary closure over T-tube drainage
and costs unnecessarily. after laparoscopic CBDE (Wu, et al, 2012) (see Chapters 31,
Selective IOC relies upon predicting the probability of cho- 36A, and 36B).
ledocholithiasis. In general, patients with a low probability
(normal LFTs, normal CBD diameter) may undergo cholecys- Gallstone Pancreatitis
tectomy with no further preoperative investigation and selective Acute gallstone pancreatitis is the most frequent form of acute
IOC. Patients with intermediate risk (isolated abnormal LFTs pancreatitis in Western countries (see Chapters 54 and 55). The
or CBD dilation) may undergo further preoperative imaging two most commonly accepted mechanisms for the pathogenesis
(MRCP) and routine IOC at an absolute minimum. Patients of gallstone pancreatitis are reflux of bile into the pancreatic
with high risk (jaundice, cholangitis) warrant confirmatory/ duct and transient ampullary obstruction caused by temporary
therapeutic ERCP (ASGE Standards of Practice Committee, impaction of a stone in the ampulla. The disease is mild in
2010) at most centers. In fact, today many patients are triaged approximately 80% of patients, but 20% experience a more
for this purpose, but in years past, many would undergo open severe clinical course that includes complications such as pan-
CBDE. Ultimately, the choice of modality depends on local creatic necrosis, multisystem organ failure, and even death
availability and expertise in minimally invasive treatments (Acosta et al, 1997; Alexakis et al, 2007; NIH, 2002) (see
coupled with considerations of cost and convenience. Chapters 55 and 56).
In many patients, the biliary obstruction has spontaneously
COMMON BILE DUCT EXPLORATION: TRANSCYSTIC VERSUS CHOLEDO- resolved at the time of presentation, so biliary decompression
CHOTOMY ACCESS. When IOC reveals CBD stones, they can be is not needed. These patients should undergo elective chole-
removed during cholecystectomy. The open choledochotomy cystectomy once the pancreatitis has resolved. At the other end
to allow cholangioscopy, flushing, forceps and balloon clear- of the spectrum are patients with gallstone pancreatitis and
ance, and T-tube placement is rarely performed or taught associated acute cholangitis (see Chapter 43). Clear evidence
today. Instead, laparoscopic common bile duct exploration shows that endoscopic biliary drainage is beneficial in patients
(LCBDE) has evolved as an efficient and more commonly used with acute cholangitis; thus these patients should have early
technique, as described in other chapters(see Chapter 36B). biliary decompression.
Several studies have shown LCBDE to be at least as efficient A secondary question is whether patients with gallstone pan-
as preoperative or postoperative ERCP in terms of stone clear- creatitis, without cholangitis, benefit from biliary decompres-
ance, morbidity, mortality, and short hospital stay, and thus sion. Clinical and experimental studies suggest that impacted
LCBDE is recommended for surgeons with appropriate skills ampullary stones and persistent biliopancreatic obstruction are
and facilities (Martin et al, 2006). A 2013 Cochrane Review of associated with a more severe clinical course. In theory, early
randomized trials actually demonstrated the superiority of both endoscopic removal of obstructing ampullary gallstones should
open and laparoscopic CBDE when compared with ERCP in improve outcomes (Acosta et al, 1997; Alexakis et al, 2007).
clearing the CBD, without any associated increased morbidity Between the late 1970s and mid-1980s, urgent surgery with
(Dasari et al, 2013). For capable surgeons, LCBDE is as safe biliary decompression was studied as a treatment of choice for
and efficient as ERCP, thus avoiding the discomfort, costs, and patients with acute gallstone pancreatitis, but this approach was
630 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
associated with an increased mortality rate among patients with The severity of the patient’s illness guides the timing of
severe pancreatitis. As such, surgical treatment during the acute intervention. Patients whose biliary obstruction has spontane-
phase of the gallstone pancreatitis is not recommended. ously resolved at the time of presentation and those who have
The role of nonsurgical intervention, prior to definitive sur- mild predicted pancreatitis should have early elective cholecys-
gical therapy, has been examined in several prospective ran- tectomy once their pancreatitis has resolved. Patients with
domized studies in which patients with cholangitis were severe predicted pancreatitis and those with associated cholan-
excluded. Integral to any interpretation of treatment approach gitis should undergo early biliary decompression (ERCP or
is the severity of the gallstone pancreatitis. These studies PTC). Among cases of escalating pancreatitis, biliary decom-
defined severe pancreatitis using a number of systems that pression should be performed within 24 to 72 hours of admis-
included the Ranson criteria (>3), Glasgow criteria (>3), or the sion (Moretti et al, 2008). For cases with associated cholangitis,
Acute Physiology and Chronic Health Evaluation (APACHE) biliary decompression should occur within 24 hours of presen-
II score (>8). The Ranson and Glasgow criteria have the advan- tation. Elective cholecystectomy can then be performed once
tage of ease of use and considerable areas of overlap (Table the severe illness has resolved.
37.3). A meta-analysis analyzed five prospective randomized
studies that examined the use of early biliary decompression in Cholangitis
cases of gallstone pancreatitis without cholangitis (Moretti Clinical findings associated with acute cholangitis include RUQ
et al, 2008). This study reported a significant reduction in abdominal pain, jaundice, fever, and chills—also known as
pancreatitis-related complications in patients with predicted Charcot’s triad (1877). Charcot’s triad demonstrates high speci-
severe pancreatitis (rate difference of 38.5%; 95% confidence ficity but low sensitivity because not all patients with cholangitis
interval, −53% to −23.9%; P < .0001), but no advantage was manifest all findings: 90% develop fever, but only about 50%
seen in cases with mild pancreatitis, and no difference in mor- to 70% of patients develop all three symptoms (Kiriyama et al,
tality rate was noted. More recently, a 2012 Cochrane Review 2013). Reynolds’ pentad (1959)—Charcot’s triad plus shock and
did not demonstrate any differences between early ERCP and altered mental status—represents a form of severe (grade III)
conservative management in pancreatitis of any severity without cholangitis, which can also manifest with multiorgan dysfunc-
evidence of cholangitis or biliary obstruction. However, in tion. Severe cholangitis is reported in 12% to 30% of patients
patients with concurrent cholangitis or biliary obstruction, early with acute cholangitis (Gouma, 2003; Kiriyama et al, 2013).
ERCP significantly reduced mortality and systemic complica- Cholangitis is a localized infection of the biliary tree, and an
tions (Tse et al, 2012). understanding of the pathophysiology of cholangitis guides
treatment decisions. Research into this disease has shown that
bacteria-laden gallstones are often the source of infection.
TABLE 37.3 Ranson and Glasgow Criteria for Severity of Acute These bacteria exist in a bacterial microcolony (biofilm) within
the pigmented matrix of gallstones (Fig. 37.2) (Stewart et al,
Pancreatitis
2002). The bacteria must detach from the biofilm to cause a
Criterion* Action localized infection, and it must reflux into the cholangiovenous
Ranson circulation to cause a more severe illness, including bacteremia
Admission
and organ dysfunction (Raper et al, 1989; Stewart et al, 2003).
Age > 55 years
Cholangiovenous reflux occurs with biliary pressures greater
WBC count > 16,000/mm 3
Admission
than 20 cm H2O, and even at this pressure, bacterial charac-
Glucose > 200 mg/dL Admission teristics (slime production) influence cholangiovenous reflux.
AST > 250 IU/L Admission In addition, bacterial breakdown by complement releases endo-
LDH > 350 IU/L Admission toxin, and this influences the induction of inflammatory cyto-
Increased BUN > 8 mg/dL 48 hr kines that drive the septic manifestations. It is important to note
PaO2 < 60 mm Hg 48 hr that although choledocholithiasis is a common cause of biliary
Calcium < 8.0 mg/dL 48 hr obstruction, benign and malignant biliary stenosis and biliary
anastomotic strictures are also etiologies (Kiriyama et al, 2013)
Base deficit < 4 mEq/L 48 hr
(see Chapters 42, 49, and 51).
Fluid sequestration≥ 6 L 48 hr
The 2013 updated Tokyo Guidelines describe three grades
Glasgow of acute cholangitis (Table 37.4): grade III is associated with
Age > 55 years Admission organ failure, grade II cases should undergo prompt early biliary
WBC count > 15,000/mm3 Admission drainage, and grade I is all others (Kiriyama et al, 2013). All
Glucose > 200 mg/dL Admission patients with suspected cholangitis should be treated with
AST/ALT > 96 IU/L 48 hr intravenous hydration and antibiotics that cover the most
LDH > 219 IU/L 48 hr common biliary organisms: Escherichia coli, Klebsiella spp.,
Enterococcus, Enterobacter cloacae, Pseudomonas spp., and anaero-
BUN > 45 mg/dL Admission
bic pathogens (see Chapter 12). Patients with severe grade III
PaO2 < 76 mm Hg Admission
cholangitis also require organ support and stabilization of organ
Calcium < 8.0 mg/dL 48 hr dysfunction.
Albumin < 3.4 g/dL 48 hr The critical component of the treatment of cholangitis is
*Mortality rates: 0 to 2 = 2%, 3 to 4 = 15%, 5 to 6 = 40%, >7 = 100%. biliary decompression. Because elevated biliary pressure drives
ALT, alanine aminotransferase; AST, aspartate aminotransferase; BUN, blood urea nitrogen; LDH,
cholangiovenous reflux, decompression of the biliary tree with
lactate dehydrogenase; PaO2, partial pressure of oxygen in arterial blood; WBC, white blood cell ERCP is crucial (see Chapter 29); PTC may be used if ERCP
count. is not available (see Chapter 30). Not only does biliary drainage
A. Gallstones and Gallbladder Chapter 37 Cholecystolithiasis and stones in the common bile duct: which approach and when? 631
A cm B
FIGURE 37.2. A, Black-pigment gallstones. B, Scanning electron micrograph of the black-pigment stones demonstrating bacterial microcolonies.
Note the bacterial bridges and three-dimensional nature of the biofilm. (From Stewart L, et al, 2002: The pathogenesis of pigment gallstones in
Western societies: the central role of bacteria. J Gastrointest Surg 6:891-904.)
is a history of pancreatitis or if more than 6 months have passed historical advances in technology? Patients now benefit from
since sphincterotomy was performed (Archibald et al, 2007). improved imaging and minimally invasive endoscopic and lapa-
roscopic techniques, especially when combined. Indeed, our
CONCLUSION treatment approaches today only occasionally resemble those
of a recent but bygone era in biliary surgery.
In 1970, who could have predicted that the common ailments
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CHAPTER 38
Postcholecystectomy problems
Major Kenneth Lee IV and Charles M. Vollmer Jr.
633
634 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
OVERALL MORBIDITY OF CHOLECYSTECTOMY these issues is therefore mandatory. PCPs include a heteroge-
neous group of issues ranging from traditional complications
Several large series have quantified the morbidity and mortality that are easily identified and quantified in large studies to more
of laparoscopic and open cholecystectomy in the modern era. nebulous, ill-defined issues that are difficult to detect and esti-
In 1995, Jatzko and colleagues (1995) published a multivariate mate. In our view, these diagnoses can be divided into three
comparison of postcholecystectomy complications demonstrat- groups: technical problems apparent in the intraoperative or
ing higher morbidity (7.7% vs. 1.9%) and mortality (5% vs. perioperative setting (immediate technical problems), technical
1%) for open cholecystectomy versus laparoscopic cholecystec- problems that often take months to years to manifest (delayed
tomy. Soon thereafter, a meta-analysis comparing 98 studies of technical problems), and functional problems that are often
laparoscopic cholecystectomy with 28 studies of open cholecys- unrelated to the operation and are sometimes present preopera-
tectomy measured the rate of mortality for laparoscopic chole- tively (functional problems). Notably, overlooked extrabiliary
cystectomy to be 0.086% to 0.16% versus 0.66% to 0.74% for disorders may be the most common cause of postcholecystec-
an open procedure (Shea et al, 1996). An all-cause morbidity tomy pain (Jaunoo et al, 2010). Table 38.1 summarizes diag-
rate was not calculated in this study. More recently, an analysis noses fitting each group of PCPs.
of 65,511 cholecystectomies performed at American College of
Surgeons–National Surgical Quality Improvement Program
(ACS-NSQIP) hospitals found the rates of morbidity, serious IMMEDIATE TECHNICAL PROBLEMS
morbidity, and mortality for laparoscopic cholecystectomy to
be 3.1%, 1.4%, and 0.27%, respectively (Ingraham et al,
Bile Leak and Bile Duct Injury
2010). The same rates for open cholecystectomy were 17.8%, The incidence of bile leak after laparoscopic cholecystectomy
11.1%, and 2.8%, respectively. Rates of major in-hospital com- appears to be higher than for open cholecystectomy (See Chap-
plications (6.8%) and mortality (0.5%) have also been identi- ters 27 and 42). It has been estimated at 1.1% to 4.0% (Agarwal
fied from the U.S. Nationwide Inpatient Sample (Murphy et al, et al, 2006; Barkun et al, 1997; Binmoeller et al, 1991; Bjork-
2010). Although these series report complications rates for all man et al, 1995; Davids et al, 1992; Kim & Kim, 2014). The
patients who underwent cholecystectomy, the Swiss Associa- majority of bile leaks following laparoscopic cholecystectomy
tion of Laparoscopic and Thoracoscopic Surgeons (SALTS) are from two sources: the cystic duct stump and aberrant
database defined the rates of intraoperative complications branches of hepatic ducts, including ducts of Luschka (Barkun
(7%), postoperative local complications (4%), and postopera- et al, 1997; Bergman et al, 1996; Kim & Kim 2014; Rustagi &
tive systemic complications (2.3%) following laparoscopic cho- Aslanian 2014; Ryan et al, 1998; Tewani et al, 2013; Way et al,
lecystectomy for only those patients diagnosed with acute or 2003). Abdominal pain, fever, ascites, and jaundice are the
chronic cholecystitis (Giger et al, 2006). The mortality rate in most common presentations (Agarwal et al, 2006; Barkun et al,
this study was 0.32%. 1997; Bjorkman et al, 1995; Ferriman, 2000; Kim et al, 2010;
Such national database studies have also been used to iden- Kim & Kim, 2014; Pawa & Al-Kawas, 2009). Bilious drainage
tify risk factors for complications following cholecystectomy. from operative drains or percutaneous drains placed postopera-
Murphy and colleagues (2010) showed on multivariate analysis tively typically confirms the diagnosis. The majority of these
that risk factors for complications following laparoscopic cho- leaks can be successfully managed with drainage alone. Endo-
lecystectomy included advanced age, male gender, and comor- scopic procedures aimed at eliminating the pressure gradient
bidities. Surgeon experience and hospital volume were not risk across the sphincter of Oddi to create preferential flow of bile
factors for morbidity. In their analysis, the SALTS group identi- into the duodenum are commonly used in this setting, and
fied patient characteristics (gender, age, comorbidity, body although multiple studies have reported high success rates asso-
weight), clinical findings (acute vs. chronic cholecystitis), and ciated with endoscopic sphincterotomy in the management of
surgeon experience as predictors of perioperative complication minor bile leaks, ranging from 80% to 100% (Katsinelos et al,
(Giger et al, 2006). 2008; Mavrogiannis et al, 2006; Ryan et al, 1998), there is no
clear proof that these procedures are superior to drainage alone.
POSTCHOLECYSTECTOMY PROBLEMS: It is clear, however, that surgery is rarely required to treat most
OVERVIEW bile leaks and is now largely reserved for the most feared com-
plication of cholecystectomy—major bile duct injury.
Persistence or recurrence of symptoms following cholecystec- Despite the clear advantages of laparoscopic versus open
tomy occurs as much as 40% of the time (Jaunoo et al, 2010; cholecystectomy, CBD injuries have traditionally been seen
Zhou et al, 2003). A comprehensive understanding of both more frequently in the laparoscopic setting (0.3% to 0.5% vs.
potential PCPs and strategies for diagnosing and managing 0.1% to 0.2%) (Southern, 1991; Adamsen et al, 1997; Deziel
et al, 1993; Harboe & Bardram, 2011; Nuzzo et al, 2005; junction of the cystic and common hepatic ducts (Duca et al,
Tantia et al, 2008; Vecchio et al, 1998; Waage & Nilsson, 2003).
2006). Advanced minimally invasive procedures such as single- Bile duct injuries in which biliary-enteric continuity persists
incision LC may be associated with even higher rates of bile can be managed endoscopically, but the mainstay of treatment
duct injury (Joseph et al, 2012). This may have to do in part for major bile duct injuries remains surgery (see Chapter 42).
with experience. In a series of 350 laparoscopic cholecystecto- Because bile duct injuries are often unrecognized at the time
mies reviewed by Huang and colleagues (1993), CBD injuries of the index operation, definitive repair is often conducted
more often occurred in the first 10 to 15 operations performed remotely. Multiple reports suggest that surgical repair of these
by the surgeon. Similarly, a multiinstitutional report found that injuries is highly successful in both immediate and delayed
90% of bile duct injuries occurred within an individual sur- cases (Lillemoe et al, 2000; Pekolj et al, 2013; Perera et al,
geon’s first 30 cases (Moore & Bennett, 1995). Universal adop- 2011; Sicklick et al, 2005). Large, single-institution reports
tion of the laparoscopic approach now allows the learning curve have demonstrated success rates as high as 98% with low rates
to be more easily surmounted during surgical training. Indeed, of mortality, major morbidity, reoperation, and anastomotic
the most recent data suggest that the rate of bile duct injury leak. This includes more recent reports focused on repairs
may be decreasing with more laparoscopic experience (Grbas performed immediately (Pekolj et al, 2013; Perera et al, 2011).
et al, 2013) and that laparoscopy is no longer associated with The most frequently used options for repair are hepaticojeju-
an increased risk of bile duct injury (Fullum et al, 2013). nostomy (nearly ubiquitous in the delayed setting) and primary
Regardless, a significant fraction of injuries are purely technical repair versus a T-tube. Multiple studies have shown that bile
and unrelated to experience (Archer et al, 2001). duct injuries should be managed by experienced hepatobiliary
The most common reason for major bile duct injury is surgeons because repairs performed by nonhepatobiliary sur-
failure to identify the anatomy of the triangle of Calot (Stras- geons have significantly increased rates of morbidity and failure
berg et al, 1995). Often, the CBD is mistaken for the cystic (Melton & Lillemoe, 2002; Perera et al, 2011; Stewart & Way,
duct. Less commonly, an aberrant duct is misidentified as the 1995). Surgical management of bile duct injuries and strictures
cystic duct. Bile duct injury has been minimized by application is discussed in greater detail elsewhere in this text.
of the “critical view of safety” in laparoscopic cholecystectomy
(Strasberg et al, 1995; Strasberg & Brunt, 2010). The critical Hemorrhage
view requires clearance of fat and fibrous tissue from the tri- Several large series have defined the risk of perioperative bleed-
angle of Calot, separation of the gallbladder from the lower ing in patients undergoing cholecystectomy. An ACS-NSQIP
third of the cystic plate, and that two and only two structures study of 65,511 North American cholecystectomies quantified
be seen entering the gallbladder. The advantage of applying the the risk of bleeding for laparoscopic and open cholecystectomy
critical view is that the surgeon cannot proceed to the division as 0.08% and 0.54%, respectively. The overall rate of bleeding
of structures if the anatomy is misidentified. However, when requiring transfusion in the series was 0.12% (Ingraham et al,
and whether the critical view has been met can be a matter of 2010). A Swedish registry study of 48,010 cholecystectomies
contention. For this reason, the use of intraoperative photog- found that bleeding necessitating transfusion, reoperation, con-
raphy to document the critical view from both anterior and version to open, and/or other measures prolonging hospital stay
posterior perspectives has been suggested (Fig. 38.1) (Sanford occurred in 2.1% of patients (Persson et al, 2012).
& Strasberg, 2014). In addition to the classic direct CBD inju- Bleeding typically occurs from one of several sites in chole-
ries caused by misidentification of the cystic and CBDs, clip- cystectomy. In a retrospective analysis of 9542 consecu-
ping of a “tented” CBD may occur in LC due to excessive tive laparoscopic cholecystectomies by Duca and colleagues
traction of the CBD into the clip itself. These injuries can lead (2003), intraoperative hemorrhage occurred in 224 patients,
to stricture and obstruction of the CBD, and may be avoided for an incidence of 2.3%. The etiology of bleeding was most
by placing the first clip with visualized distance from the commonly from the gallbladder bed and treated with a
FIGURE 38.1 Doublet photographs of the critical view of safety. This figure demonstrates complete clearance of the hepatocystic triangle, the
presence of only two structures going into the gallbladder, and separation of the gallbladder from the lower one third of the cystic plate. (Image
courtesy Steven M. Strasberg.)
636 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
fibrin-collagen patch in their experience. Tangential lesions of controlled trial of drain use in the setting of acute cholecystitis
the cystic artery or, less commonly, total sectioning of the cystic also showed no difference in intraabdominal infection rates
artery occurred in 95 out of 224 cases of bleeding. In the major- (Park et al, 2015).
ity of cases, the intraoperative bleeding was controlled laparo-
scopically with hemostatic clips. Damage to the hepatic artery Retained Common Bile Duct Stones
occurred in one instance and required immediate conversion The incidence of CBD stones in patients undergoing elective
to an open procedure. Finally, bleeding from the greater cholecystectomy is 5% to 15% (Clayton et al, 2006; Ebner
omentum was seen in 18 cases and controlled laparoscopically et al, 2004; Petelin, 2003; Velanovich et al, 2006a, 2006b;
in 16 cases. Another source of massive intraoperative blood loss Vezakis et al, 2000) (see Chapters 32, 36, and 37). Before lapa-
is from inadvertent incursion into a deep plane of hepatic roscopy became the standard approach to cholecystectomy, the
parenchyma where distal tributaries of the middle hepatic vein presence of CBD stones often had minimal effect on patient
may be encountered. In fact, 10% of patients harbor large management and outcome. This is partly because endoscopic
branches of the middle hepatic vein directly adjacent to the retrograde cholangiopancreatography (ERCP) followed by
gallbladder fossa, which may lead to significant hemorrhage in open cholecystectomy failed to carry significant benefit over
instances of even mild parenchymal dissection (Ball et al, open cholecystectomy with bile duct exploration (Neoptolemos
2006). et al, 1987; Stain et al, 1991; Stiegmann et al, 1992). The shift
It should be recognized that management of profuse bleed- toward laparoscopic cholecystectomy has dramatically altered
ing during cholecystectomy can be fraught with significant the management of patients suspected of having CBD stones.
ramifications. An autopsy study has demonstrated that approxi- Stratified approaches are now generally used in which high-risk
mately 7% of cadavers having undergone cholecystectomy had patients are sent for ERCP, moderate-risk patients for magnetic
evidence of injury to the right hepatic artery or its branches resonance cholangiopancreatography (MRCP), and low-risk
(Halasz, 1991). Although this alone appears to be well toler- patients proceed directly to surgery (Shapey et al, 2012).
ated, combined injuries to the right hepatic artery and bile duct Despite these advances in the identification and clearance of
harbor far more significant consequences (Stewart et al, 2004; CBD stones preoperatively, the incidence of retained CBD
Strasberg & Helton, 2011). Nonetheless, death remains uncom- stones following cholecystectomy still ranges from 0.2% to
mon in this setting. By contrast, extreme vasculobiliary injuries 2.3% (Andrews, 2013; Hamad et al, 2011; Sanjay et al, 2011;
involving injury to a portal vein, hepatic artery, and bile duct Shapey et al, 2012). In these instances, it is often difficult to
are most severe and often result in death (Strasberg & Gouma, decipher whether the retained stones are a consequence of
2012). When seen, these injuries have often occurred despite intraoperative gallbladder manipulation or incorrectly inter-
conversion to an open procedure. The surgeon must be cogni- preted studies.
zant of the fact that the anatomy of the hilum may be severely The majority patients with of retained CBD stones are seen
distorted in the face of severe inflammation, as the fundus- within 6 weeks to 1 year, most commonly with abdominal pain
down technique has been used frequently in these cases. and/or jaundice (Sanjay et al, 2011). Endoscopic sphincterot-
omy is the standard approach for CBD stone extraction, with
Infection a success rate of approximately 87% to 100% (Bergman et al,
Postoperative infection after cholecystectomy is a rare event. In 1997; Granke et al, 1988; Gupta et al, 2008; Kawai et al, 1974;
a 7-year study of 54,504 patients conducted by the Centers for Mo et al, 2002; Ponchon et al, 1989) (see Chapters 29 and
Disease Control and Prevention, the rate of surgical-site infec- 36C). Notably, studies comparing the use of preoperative,
tions (SSI) was significantly lower in the laparoscopic approach intraoperative, and postoperative ERCP in relevant clinical sce-
compared with open cholecystectomy (0.62% vs. 1.82%, narios have not demonstrated superiority of any one approach
respectively) (Richards et al, 2003). The majority of infections (Chang et al, 2000; Wright et al, 2002). Thus no single algo-
in the open approach were seen in superficial spaces, whereas rithm exists for the management of suspected CBD stones.
infections in the laparoscopic setting were less frequent but
were more commonly in organ spaces. As expected, the SSI DELAYED TECHNICAL PROBLEMS
rates were higher in patients taken to the operating room emer-
gently or with an American Society of Anesthesiologists score Spilled Gallstones
of 3 or higher. Few reports of complications from gallstones spilled during
Neither perioperative antibiotic prophylaxis nor routine open cholecystectomy exist (Jacob, et al, 1979; Rothlin et al,
drainage improves the rate of infectious complications follow- 1997). This is because gallbladder spillage during open chole-
ing cholecystectomy. That antibiotic prophylaxis carries no cystectomy is more easily controlled, and dropped gallstones
benefit in lower-risk patients undergoing elective cholecystec- are more likely to be identified and retrieved. Perforation of the
tomy has been shown in multiple studies (Chang et al, 2006; gallbladder during laparoscopic cholecystectomy is more
Harling et al, 2000; Koc et al, 2003; Tocchi et al, 2000; Uludag common and less controlled. Estimates of gallbladder perfora-
et al, 2009). More recently, a gallstone surgery registry was tion and stone spillage range from 6% to 40% in laparoscopic
used to demonstrate that prophylactic antibiotics also carry no cholecystectomy (Brockmann et al, 2002; Helme et al, 2009;
benefit in acute cholecystectomy (Jaafar et al, 2014). Postop- Schafer et al, 1998; Soper & Dunnegan, 1991). It can occur
erative infections occurred in 6.1% of patients who received no for many reasons, including excessive retraction during dissec-
antibiotic prophylaxis compared with 8.4% of patients treated tion, direct puncture with an instrument, and removal of a
with antibiotics. distended gallbladder through a trocar site. This, combined
A Cochrane Review summarizing 12 trials concluded that with increased difficulty in identifying and retrieving spilled
the use of drains in uncomplicated cholecystectomy is unwar- stones, has dramatically increased complications from gallblad-
ranted (Gurusamy et al, 2007), and a recent randomized der perforation in the laparoscopic era.
A. Gallstones and Gallbladder Chapter 38 Postcholecystectomy problems 637
A meta-analysis of eight studies that, with more than 500 et al, 1998; Walsh et al, 2002). In this instance, it is sometimes
laparoscopic cholecystectomies, report on lost gallstones esti- difficult to delineate whether a stone has persisted in a long
mates the incidence of lost stones during LC to be approxi- cystic duct remnant or whether there has been relapse of lithia-
mately 2%; these stones caused complications 8.5% of the time sis in a gallbladder remnant.
(Zehetner et al, 2007). The most frequent complication of The prevalence of remnant cystic duct lithiasis is difficult to
spilled stones is abscess—either intraabdominal or of the estimate. Many reports are surgical series and thus report only
abdominal wall (Dobradin et al, 2013; Horton & Florence, on patients in whom the finding has been managed surgically.
1998; Wilton et al, 1993; Zehetner et al, 2007). Less common However, anecdotal case reports suggest that incomplete gall-
manifestations include fistulas, liver abscesses, and bacteremia. bladder removal is more common in the laparoscopic than open
Stones have even been reported to erode into the chest cavity, era. This may partly reflect the prevalence of subtotal cholecys-
causing empyema and broncholithiasis with expectoration. tectomy in the era of minimally invasive surgery. Laparoscopic
Although the spillage of gallstones is obviously an intraop- subtotal cholecystectomy technique was first reported in the
erative event, complications of spilled gallstones can be termed early 1990s (Bickel & Shtamler, 1993) and has been shown to
a late technical issue in that they often materialize weeks to be relatively safe (Ji et al, 2006; Sharp et al, 2009). However,
months after the procedure. Reoperation for morbidity from a systematic review of the technique used in this procedure
stone spillage has been reported as late as 15 years after chole- shows that a number of surgeons purposefully leave behind a
cystectomy (Arishi et al, 2008; Gooneratne, 2010). Because gallbladder pouch that often is sutured or stapled closed
complications from spilled stones are the exception rather than (Henneman et al, 2013). This tactic is contrary to that described
the rule, we do not recommend converting to an open proce- for open subtotal cholecystectomy in which the posterior wall
dure in the event of gallbladder perforation. However, efforts of the gallbladder is left attached to the liver and the cystic duct
should be made to retrieve stones with suctioning, forceps, and is secured at its origin with a purse-string technique (Bornman
irrigation. It is also a good policy to document the event and & Terblanche, 1985). Although the alternative laparoscopic
to inform the patient that stone spillage occurred in the event approaches to subtotal cholecystectomy are more convenient,
of latent complications and/or confounding imaging findings. they do increase the risk of relapsing lithiasis. In one series, the
Notably, spilled gallstones have even been noted to mimic incidence of cystic duct remnant lithiasis was 4.19% in the
hepatic and peritoneal metastases (Arai et al, 2012; Dasari setting of laparoscopic subtotal cholecystectomy compared
et al, 2009; Rammohan et al, 2012). with 0.02% in conventional laparoscopic cholecystectomy
(Palanivelu et al, 2009).
Gallbladder Remnant and Remnant Cystic Resection of gallbladder and cystic duct remnants due to
Duct Lithiasis lithiasis has been achieved through both laparoscopic and open
It has been suggested that as many as 30% of postcholecystec- approaches. However, advanced endoscopic techniques carry
tomy pain may be related to stone disease in a remnant cystic the potential to manage this problem even less invasively (Ben-
duct or gallbladder following cholecystectomy (Fig. 38.2) (Gui ninger et al, 2004; Phillips et al, 2014). Phillips and colleagues
(2014) recently described their institutional approach to
remnant cystic duct lithiasis, which illustrates the potential for
multidisciplinary management. Twelve patients were described,
and the mean interval from cholecystectomy to discovery of
remnant cystic duct stones was 34.2 months. All patients
reported epigastric and/or right upper quadrant abdominal
pain. Six of the 12 patients underwent reoperation, two of
which were urgent due to acute cystic duct obstruction with
inflammation. All of these procedures were begun laparoscopi-
cally but required conversion to open. The other six patients
were managed nonoperatively with ERCP. Seven of 9 patients
with available follow-up had symptom resolution.
Biliary Strictures
Benign stenosis of the CBD is more common after LC and is
almost always related to iatrogenic injury in the form of partial
sectioning, clipping, or ligation (Kassab et al, 2006) (see
Chapter 42). These postsurgical strictures can also result from
delayed thermal injury or intraoperative ischemic devascular-
ization (Deziel et al, 1993; Genest et al, 1986). The incidence
of stricture after laparoscopic procedures ranges from 0% to
2.7% compared with 0.25 to 0.5% after open cholecystectomy
(Deziel et al, 1993, Strasberg et al, 1996). Strictures most com-
monly present with abdominal pain, fever, and jaundice due to
FIGURE 38.2 Lithiasis of a gallbladder remnant after hazardous cho-
mechanical obstruction. Over time, resultant cholestasis can
lecystectomy. Endoscopic retrograde cholangiopancreatography chol- ultimately lead to choledocholithiasis and recurrent cholangitis
angiogram shows a gallstone noted in a gallbladder remnant in this (Kassab et al, 2006).
patient who had a history of a difficult cholecystectomy. A percutaneous Biliary strictures have historically been treated by surgical
cholecystostomy has been placed in the remnant gallbladder. reconstruction with very good outcomes in experienced hands
638 PART 5 BILIARY TRACT DISEASE Section I Inflammatory, Infective, and Congenital
as detailed earlier (Lillemoe et al, 2000). However, many Oddi manometry (SOM) is the only investigation capable of
studies have more recently reported the safety and efficacy of directly assessing the motor activity at the sphincter. However,
endoscopic or percutaneous balloon dilation and/or stenting as this test is invasive and does carry risk of complication, espe-
a less invasive means of treating such problems (Gouma, 2007; cially in the setting of a normal-caliber bile duct (Freeman et al,
Kassab et al, 2006; Vitale et al, 2008) (see Chapters 27, 29, and 1996; Maldonado et al, 1999; Sherman et al, 1990). There are
30). Although safe and reasonably effective, these methods do noninvasive techniques that are reproducible but less accurate
generally require prolonged courses with repeated stent changes. (Cicala et al, 1991, 2002; Corazziari et al, 1994; Madacsy et al,
Surgery remains the mainstay for treatment of major duct tran- 2000; Sostre et al, 1992; Thomas et al, 2000).
sections, ligations, many sizable strictures, and in cases where Pancreatic SOD characterized by recurrent bouts of pancre-
endoscopic/percutaneous approaches are unsuccessful. More atitis that often occur years after cholecystectomy. Because no
detailed discussion of both benign and malignant strictures can clear etiology is derived from serology, imaging, or history,
be found elsewhere in this text. pancreatitis in this setting is often labeled idiopathic. The diag-
nosis should be considered in patients presenting with recur-
FUNCTIONAL PROBLEMS rent, biochemically proven episodes of pancreatitis without any
alternative etiology. In patients with this presumed diagnosis,
Sphincter of Oddi Dysfunction one prospective cohort study has shown that operative division
The apparatus responsible for directing the flow of biliary and of the sphincter of Oddi prevented recurrent episodes of pan-
pancreatic secretions is termed the sphincter of Oddi. It con- creatitis in a large majority of patients (Toouli et al, 1996).
sists of three segments of smooth muscle: the CBD segment, Whether endoscopic approaches can provide similar efficacy is
which is approximately 10 mm in length; the pancreatic questionable (Behar et al, 2006; Elton et al, 1998; Tarnasky
segment, which is roughly 6 mm in length; and the segment of et al, 1998).
the confluence of both the bile duct and pancreatic duct, which Diagnosis of the biliary variant of SOD is more complex (see
is intraduodenal for close to 6 mm in length (Bistritz & Bain, Table 38.2). Patients are separated into one of three groups
2006). When constricted, this sphincter impairs forward flow based upon whether their typical biliary pain is accompanied
of both bile and pancreatic juices. The sphincter of Oddi has by elevation of liver function tests (LFTs) and/or bile duct dila-
three main functions: regulation of flow into the duodenum, tion. Patients with classic pain, liver function abnormalities,
prevention of reflux from the duodenum into the bile duct and and bile duct dilation are said to have type I biliary SOD.
pancreatic duct, and filling of the gallbladder. The control of Patients with classic pain and either liver function abnormalities
the sphincter’s function is complex and involves both neural or bile duct dilation, but not both, have type II biliary SOD.
and hormonal pathways. Patients with pain alone have type III SOD (Baillie, 2010).
SOD continues to be a diagnostic dilemma. Biliary and Whether SOD can occur with an intact gallbladder is not
pancreatic variants can occur, and diagnostic criteria exist for entirely certain; patients with classic biliary pain and an intact
the diagnosis of SOD and the differentiation of the biliary and gallbladder are often considered to have a functional gallblad-
pancreatic subsets (Behar et al, 2006) (Table 38.2). Patients der disorder, and cholecystectomy is generally performed before
with biliary SOD have stenosis in the biliary sphincter, whereas the diagnosis of SOD is entertained.
those with pancreatic SOD show stenosis in the pancreatic The standard treatment for biliary SOD is endoscopic
segment or both components (Behar et al, 2006). Sphincter of sphincterotomy (Behar et al, 2006; Petersen, 2004). However,
(see Chapter 19). Although there is no therapeutic value, it measured with video recording for subsequent analysis (Csendes
provides a reliable, noninvasive, nonsedating method to evalu- et al, 1979; Geenen et al, 1980). SOD is a dynamic process,
ate various biliary and pancreatic processes. Further, the images and a single normal endoscopic evaluation may not be sufficient
generated can serve as a roadmap for interventional procedures. in patients with persistent symptoms (Khashab et al, 2009;
Patients with abnormal LFTs and dilated CBDs (to >10 mm) Varadarajulu et al, 2003). In a study of 5352 patients who
postcholecystectomy with no evidence of stones or other pathol- underwent SOM during a 13-year period, 1037 had SOM read-
ogy on ultrasound may be candidates for MRCP (Terhaar et al, ings within normal. Of these patients, 30 had repeat ERCP for
2005). persistent symptoms, and 60% of these were given the diagnosis
MRCP has been reported to be 95% to 100% sensitive and of SOD (Khashab et al, 2009).
88% to 97% specific in detecting CBD calculi (Schofer, 2010;
Tse et al, 2006) but does have some limitations in this regard. Hepatobiliary Scintography
The sensitivity falls when detecting stones less than 6 mm in In patients who have undergone cholecystectomy, nuclear scan-
size (Terhaar et al, 2005; Tse et al, 2006), and calculi impacted ning reveals rapid flow of intravenously administered
in the intramural portion of the CBD may not be detectable technetium-99m hepatobiliary radiopharmaceuticals (i.e.,
(Van Hoe et al, 2004). The test is also valuable in delineating hepatic 2,6-dimethyl-iminodiacetic acid [HIDA], ethyl hepatic
a variety of postcholecystectomy issues beyond retained stones. 2,6-dimethyl-iminodiacetic acid [EHIDA], diisopropyl-
Gallbladder remnants, including those harboring stones, are acetanilido-iminodiacetic acid [DISIDA]) from the hepatocytes
readily identified on MRCP. Hepatocyte-specific contrast to the biliary canaliculi, then to the CBD and ultimately the
agents have greatly increased the utility of MRCP in the evalu- duodenum via the sphincter of Oddi (see Chapter 17). In
ation of bile leaks. Sensitivities ranging from 85% to 100% have patients with a suspected bile leak, biliary scintigraphy has a
been reported for detection of bile leaks by MR cholangiogra- sensitivity of as high as 70%. However there are multiple down-
phy by using one of three hepatocyte contrast agents (Park et al, sides to this examination in isolation. First, the study does not
2004; Pilleul et al, 2004; Ratcliffe et al, 2014). Biliary strictures evaluate extrabiliary structures and thus has little to no ability
typically appear as a short-stretch narrowing of the luminal to diagnose complications beyond bile leak. Second, the site of
signal, although MRCP does often tend to overestimate the a bile leak is not usually determinable (Aduna et al, 2005).
length and extent of the stricture (Girometti et al, 2010). The Third, biliary scintigraphy is less sensitive in the setting of
role of MRCP in diagnosing SOD is not well defined, as cor- hepatic dysfunction. Last, biliary scintigraphy carries no thera-
relation with ERCP or biliary manometry has not been well peutic benefit.
evaluated. Furthermore, differentiation between a stenotic and Scintigraphy has also been used in SOD. In patients with
spasmodic papilla is difficult. Secretin-enhanced MRCP may SOD, there is a marked delay in transpapillary transit times,
carry greater diagnostic utility, but data regarding its ability to with stasis seen in the intrahepatic and extrahepatic biliary
predict SOD remain controversial (Aisen et al, 2008). None- system. This sort of quantitative cholescintography may aid in
theless MRCP is reasonable as a first-line noninvasive test for the diagnosis of patients suspected to have SOD following
the evaluation of biliary abnormalities in patients with possible cholecystectomy but is unreliable as a stand-alone test (Coraz-
SOD. ziari et al, 1994, 2003; Madacsy et al, 1999; Shaffer et al,
The gold standard diagnostic and therapeutic procedure in 1986).
patients with biliary obstruction and/or bile leak is ERCP (see
Chapters 20 and 29). It carries a sensitivity and specificity of Axial Imaging
greater than 95% in the detection of obstruction; when pathol- If the aforementioned techniques are unrevealing for causes of
ogy is seen, therapeutic sphincterotomy, stent placement, and/ PCPs, computed tomography (CT) (see Chapter 18) or MRI
or tissue collection for presumed cancer are possible (Buscarini can be used to rule out other sources of pain not suspected
et al, 2003; Palazzo et al, 1995; Prat et al, 1996; Snady et al, preoperatively (e.g., tumors, rib fractures, pneumonia). Post-
1992). As described earlier, ERCP with sphincterotomy/stent cholecystectomy complications such as dropped stones,
is highly successful in the treatment of bile leaks and retained abscesses, hematomas, or hernias can also be readily detected.
stones. However ERCP does carry a legitimate risk of complica- CT is readily available and rapid and thus can carry benefit as
tions. Acute pancreatitis is the most common complication and an early triage test. A “negative” scan is often reassuring to the
occurs in 5% to 40% of low- and high-risk patients, respec- surgeon as it can at least define that postoperative complaints
tively. Additionally, pancreatic necrosis, duodenal or biliary tree are not obviously organic in nature and can lead the workup of
perforation, multiorgan failure, and death may also occur, albeit symptoms in other directions.
less than 1% of the time (Barthet et al, 2002; Dancygier &
Nattermann, 1994; Lieb & Draganov, 2007; Masci et al, 2001).
Algorithm for the Evaluation of
In some cases, endoscopic access to the biliary tree is limited Postcholecystectomy Pain
(e.g., patients who have had diverting gastric bypass surgery), Given the heterogeneity of potential causes of postcholecystec-
and percutaneous transhepatic cholangiography is an alterna- tomy pain, no single algorithm exists to follow when these
tive approach. patients are seen. However, a general approach that allows
In patients with postcholecystectomy pain where SOD is evaluation and exclusion of the majority of diagnoses in con-
suspected, ERCP also allows concurrent SOM. This is consid- sideration is useful. Figure 38.3 details our approach to patients
ered the gold standard for detection of SOD (Khashab et al, who are seen with pain after cholecystectomy. As stated, a full
2010). A triple-lumen catheter connected to external transduc- history, physical examination, and laboratory evaluation should
ers is positioned in the sphincter of Oddi segment of both the commence before any radiographic studies. LFTs are the single
CBD and pancreatic duct separately, and baseline pressure, as best laboratory test; normal LFTs are somewhat reassuring,
well as phasic wave amplitude, duration, and frequencies are because specific patterns of derangement are often seen in the
A. Gallstones and Gallbladder Chapter 38 Postcholecystectomy problems 641
FIGURE 38.3 Algorithm for the evaluation and management of postcholecystectomy pain. CBD, Common bile duct; ERCP, endoscopic retrograde
cholangiopancreatography; EUS, endoscopic ultrasound; GB, gallbladder; LFT, liver function test; MRCP, magnetic resonance cholangiopancreatog-
raphy; poss., possible; r/o, rule out; r/x, treatment.