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Ficha 51
Ficha 51
frequency among patients with the syndrome L = Low frequency among patients with the syndrome
1.
Nephrotic Syndrome (NS) Primary Nephrotic Syndrome Minimal change disease - H Focal segmental glomerulosclerosis - H Membranous glomerulopathy - L Systemic Nephrotic Syndrome Diabetes mellitus - H Amyloidosis - L Systemic lupus erythematosus (WHO Class V)
2A
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Membranoproliferative GN - L
Systemic Nephritic Syndrome Systemic lupus erythematosus (WHO Class III, WHO Class IV) - H
Hereditary Nephritis (Alport syndrome) - L Rapidly progressive GN (RPGN), ANCA associated, pauciimmune
Systemic Nephritic Syndrome Lupus nephritis (WHO Class II) - H
Anti-basement membrane disease (Goodpasture's Syndrome) - L Systemic vasculitis: Polyarteritis nodosa microscopic polyarteritis Wegener's granulomatosis Henoch Schoenlein Purpura Thrombotic thrombocytopenic purpura / Hemolytic uremic syndrome
Pauci-immune RPGN, ANCA-associated Anti-glomerular basement membrane disease (Goodpasture) - L Immune complex mediated RPGN:Systemic lupus erythematosus, IgANephropathy, etc. Acute tubulointerstitial diseases: Acute tubular necrosis (ATN) - H Acute interstitial nephritis (AIN) - H
Post Renal - Obstruction
Morphology MCD
By light microscopy the glomeruli are normal. By electron microscopy, the basement membrane appears normal. Principal lesion: visceral epithelial cells show a uniform, and diffuse effacement of foot processes, Fusion of foot processes, represents simplification of the epithelial cell architecture with flatening, retraction and swelling of foot processes.
Glomeruli are normal by light microscopy in minimal change disease, as shown in this biopsy. The glomerular basement membrane is thin and delicate, and mesangial cellularity and matrix are within normal limits. (Jones' silver stain, X200).
In this electron micrograph, overlying epithelial cell foot processes are effaced (giving the appearance of fusion) and run together.
Morphology MCD
This changes are reversible after corticosteroid therapy and remission of the proteinuria. The cells of the proximal tubules are often laden with lipid, reflecting tubular reabsorotion of lipoproteins passing through diseased glomeruli: Lipoid nephrosis. Immunofluorescence studies show no immunoglobulin or complement deposits.
Clinical Course
Nephrotic syndrome:
Proteinuria (albumin) > 3.5 g/day. Hipoalbuminemia Edema Hyperlipidemia Lipiduria Thromboembolic events Slow decrease of the glomerular filtrate
Type I: Inmune complexes and activation of alternative and classic pathways of complement Type II:Alternative pathway of complement. Autoantibodies IgG (Nephritic factor C3) which joins with C3 convertase and inactivate C3.
Morphology MPGN
As seen here, the glomerulus has increased overall cellularity, mainly mesangial.
Extensive double contours of the glomerular basement membranes, stained by silver, in membranoproliferative glomerulonephritis type 1, caused by mesangial interposition and new basement membrane formation in response to subendothelial immune complex deposits. The deposits are PAS positive and globular-to-sausage shaped (Jones' silver stain; original magnification, x400).
Type I MPGN
2/3 of cases Subendothelial electrodense deposits under transmission electronic mycroscopy. Immnunofluorescence
Membranoproliferative glomerulonephritis type 1. The marked endocapillary proliferation (proliferating endothelial and mesangial cells) appears to occlude the capillary lumen. Numerous large subendothelial and occasional mesangial-dense immune complex-type deposits (bottom middle) are present (transmission electron microscopy; original magnification, x4,700
Segmental, coarsely granular-to-globular or elongated capillary wall IgG deposits in membranoproliferative glomerulonephritis type 1 (immunofluorescence with anti-IgG; origina magnification, x200).
This electron micrograph demonstrates the dense deposits in the basement membrane of MPGN type II. There are dark electron dense deposits within the basement membrane that often coalesce to form a ribbon-like mass of deposits.
Type I
Clinical Course: Massive proteinuria, Nephrotic sd. Treatment: Elimination of the infection. Prognosis: Good, 70 85% without clinical alterations.
Clinical Course: Nephrotic and Nephritic sd. Prognosis: Most patients progress to endstage renal disease within 10 years.
In both types: Hipocomplementemia, cause of the comsumption in the glomeruli.
Type II
Membranous Glomerulonephritis
Membranous Nephropathy Epimembranous GN Spikes GN
Membranous GN
Most common cause of nephrotic syndrome in adults. Characterized by:
Diffuse thickening of glomerular capillary wall Accumulation of electron-dense, deposits of immunoglobulin. Along the subepithelial side of the basement membrane
Membranous GN
Idiopathic 85% of cases Secondary to:
Drugs: penicillamine, captopril, gold, NSAIDs Underlying malignant tumors: carcinoma of lung, colon and melanoma. Systemic Lupus: Most common type. Infections: chronic hepatitis B/C, syphilis, schistosomiasis, malaria. DM, thyroiditis.
Early Stage: Glomeruli appear normal or exhibit uniform, diffuse thickening of glomerular capillary wall.
BM material is laid down between the deposits, appearing as irregular spikes protruding from the GBM (silver stain is the best)
Electron microscopy: thickening by irregular dense deposits between BM and podocites (subepithelial). Podocites have lost their foot processes.
Clinical Course
Nephrotic syndrome or non-selective proteinuria. Common symptoms: hematuria, hypertension, and symptoms of secondary causes. Course: irregular, indolent. As the glomeruli sclerosis progresses: BUN elevated, hypertension and reduction in severity of proteinuria.
Prognosis:
60% recovers with persistent proteinuria 10% die or progress to renal insufficiency. Spontaneous remission and better prognosis in women with non-nephrotic proteinuria.
Treatment:
NON
Renal Amyloidosis
Amyloidosis
A systemic immune disease characterized by deposition of amyloid (may be localized) Amyloid is a pathologic proteinaceous substance, deposited between cells in various organs and tissues with a wide variety of clinical settings. Tipically involves:
Associated with:multiple myeloma, chronic inflammatory conditions, chronic renal failure, Alzheimers disease, type 2 diabetes.
Amyloidosis
Amyloid is formed by fibril proteins in 95% and by glycloproteins (P component) in 5%. There are 15 biochemically distinct forms of amyloid proteins:
Amyloid Light Chain Amyloid associated protein Ab amyloid in Alzheimers disease All produce the same consequences and give the same pattern in microscopy.
Renal amyloidosis is the most common and potentially the most serious form of organ involvevement.
Gross Pathology
Kidneys may be either : (1)Enlarged, firm with a waxy appearance (2)Shrunken and contracted owing to vascular stenosis.
E A R L Y
S T A G E
Amyloid is deposited in the glomeruli, interstitium, arteries and arterioles. Appear as irregular thickenings of mesangium and capillary basement membranes.
Congo Red Stain - Polarizing microscopy Show diffuse amyloid deposition (green birefringence) in glomerular tufts and mesangial regions.
END STAGE: Glomerular tufts are flooded and replaced by masses or ribbons of amyloid.
Poststreptococcal Glomerulonephritis
(Postinfectious Acute Glomerulonephritis)
Pathogenesis
Glomeruli
Granular immune deposits Endostreptsin and cationic antigens in afected reas
Macro
Micro
Glomeruli: bloodless, hypercelular and enlarged. Proliferating mesangial and endothelial cells oclude the capillary lumina
PMN and monocyte infiltration.
Exudative and difuse (will affect all the lobules)
Interstitium: edema
Electron Microscopy
Clinical Features
Note: adults have a less spontaneous start with HTA. During epidemics, symptoms may be rare. 1% of children develop intense oliguria and progresive glomerulonephritis.
Glomeruli show diffuse hypercellularity due to mesangial and endothelial cell increase and a large number of polymorphonuclear neutrophils (PMNs). H&E
Diffuse proliferative acute postinfectious glomerulonephritis with numerous PMNs with PAS-positive cytoplasm and endocapillary proliferation. PAS
The garland pattern of immune complexes due to large subepithelial deposits in acute postinfectious glomerulonephritis is shown (immunofluorescence
Hump-shaped deposits in acute postinfectious glomerulonephritis with extensive foot process effacement and endocapillary proliferation
General Info
Very uncommon
2 % of all cases presenting with GN
Classification
1.-
3.-
Primary or idiopathic
Pathogenesis
The presence of fibrin in Bowmans space promotes the epithelial proliferation and formation of crescents
Extravasation due to capillary damage
GLOMERULUS
Fibrin Fibrin
The implication of a cellular crescent is that the glomerulus has sustained acute intense injury.
IDIOPATHIC RPGN
Pathogenesis of symptoms
Glomerular tufts adhere to Bowmans capsule Cicatrization of capillaries
OLIGURIA
POST-GLOMERULAR ISCHEMIA
Renal Failure
Electron Microscopy: damage to basal membrane with ruptures but no evidence of immune complex deposition. The urinary space in the top of the photograph shows portion of a crescent with the dark strands representing fibrin (arrow).
Immunofluorescence: positivity with antibody to fibrinogen. With a rapidly progressive GN, the glomerular damage is so severe that fibrinogen leaks into Bowman's space, leading to proliferation of the epithelial cells and formation of a crescent.
Clinical features
Acute nephritis (Nephritic Sd.) with acute renal failure Hypertension and edema Hematuria, proteinuria, pyuria (nephrotic sd.) Oliguria or anuria The patient may refer a viral syndrome or respiratory infection weeks before onset of renal failure
Goodpastures Syndrome
Goodpastures Syndrome
General Info
Acute and necrotizing RPGN associated to pulmonary hemorraging and hemoptysis Uncommon disease affecting primarily men (4:1) between 20-30 years of age. Autoimmune disease in which there is production of Anti-Basement Membrane Antibodies (ABM) that deposit on alveoli and glomeruli
Goodpastures Syndrome
The Goodpasture antigen resides in the noncollagen portion of the 3-alpha chain of type IV collagen Precipitation factor is unknown, may be:
Pathogenesis
Genetic predisposition: DRW15/DQW6 The lesion consists of deposits of ABM antibody and complement on the basement membrane of glomeruli and alveoli causing their destruction
Goodpastures Syndrome
MACRO: same aspect as RPGN MICRO: crescents composed of epithelial cells and monocytes surrounding capillary tufts in the urinary space
Methenamine silver stain Electron Microscopy: does not show deposits, only architectural damage and epithelial proliferation Immunofluorescence
The lungs show alveolar hemorrage, hemosiderinfilled macrophages and thickening of alveolar septi. The BM shows immune deposits
Silver stain
Immunofluorescence: shows positivity with antibody to IgG has a smooth, diffuse, linear pattern that is PATOGNOMONIC
Goodpastures Syndrome
Typically begins as flu-like illness with evidence of pulmonary compromise Pulmonary hemorrages HEMOPTYSIS Progressive dyspnea Nephritis (Nephritic Sd.) and acute renal failure The disease progresses rapidly with renal failure ocurring within weeks or months
Clinical features
High doses of steroids, with or without cytotoxic agents. Plasmapheresis removes ABM-antibodies Better prognosis than other diseases causing RPGN
Classification
This form of glomerulonephritis is characterized by the presence of prominent IgA deposits in the mesangial regions. Primary glomerular disease Frequent cause of recurrent hematuria Most common Present in children and young adults.
Pathogenesis
Genetic or acquired abnormality of inmune regulation leading to increased mucosal IgA synthesis in response to respiratory or GI exposure to environmental agents. IgA1 and IgA1complexes are entrapped in the mesanguim. They activate the alternative complement pathway and initiate glomerular injury.
MICRO/ H&E
Mesangial widening or proliferation (arrow) Segmental proliferation Overt crescentic glomerulonephritis (rare) Sclerosis (healing of focal proliferative lesion).
Mesangial electron dense deposits and increased mesangial matrix and cellularity in IgA nephropathy (transmission electron microscopy, original magnification x8,500).
MICRO/ Immunofluorescence
Clinical Course
Gross hematuria after GI or respiratory infection. 5-10% develop a typical acute nephritic syndrome. Hematuria lasts several days and then subsides, only to return every few months.
Introduction
SLE-
Classic prototype of the multisystem disease of autoimmune origin, characterized by a bewildering array of autoantibodies, particulary antinuclear antibodies (ANAs). Acute or insidious in its onset, it is a chronic, remitting and relapsing, often febrile illness characterized principally by injury to the skin, joints, kidney, and serosal membranes.
Lupus Glomerulonephritis
Kidney appears to be involved in 60 to 70% of cases.
Classification
According to the WHO (morphologic class.) Class I: Normal by light, electron, and imunofluorescent microscopy Class II: Mesangial lupus glomerulonephritis Class III: focal proliferative glomerulonephritis Class IV: Diffuse proliferative glomerulonephritis Class V: Membranous glomerulonephritis
MICRO/ H&E
Proliferation of mesangial cells and endothelial cells, along with infiltrating mononuclear and polymorphonuclear leukocytes afecting more than 50% of the glomerular area. Extensive peripheral capillary wall subendothelial immune deposition (wire loop), and extracapillary proliferation in the form of crescents. Fibrinoid necrosis, leukocyte infiltration, wireloop deposits, hyaline thrombi, and hematoxylin bodies
MICRO/ Others
Half of the tuft is distorted by marked endocapillary proliferation with occasional infiltrating cells. Segmental areas of basement membrane splitting and eosinophilic subendothelial deposits and mesangial eosinophilic deposits are visualized (Jones' silver stain; original magnification x400).
Clinical Course
Typically have:
high anti-DNA antibody titers low serum complement levels Very active urinary sediment with:
erythrocytes other casts present on urinalysis
Proteinuria
X FIN
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MMI