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Anticholinergic

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Anticholinergic drugs work by competitively blocking the binding of acetylcholine to muscarinic receptors. The main anticholinergic drugs discussed are atropine, scopolamine, and glycopyrrolate. Atropine has strong effects on the bronchial smooth muscle and heart, making it useful for treating bradycardia. However, it easily crosses the blood-brain barrier and can cause memory deficits. Scopolamine has stronger antisialagogue and CNS effects than atropine. Glycopyrrolate does not cross the blood-brain barrier and has no CNS or ophthalmic effects, but strongly inhibits salivary and respiratory tract secretions.

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Anticholinergic

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Ch.

11 anticholinergic drugs

R1
The pharmacology of drugs that block
muscarinic receptors
cf)nondepol.NM blocking agent-nicotinic Rc.
Antimuscarinic
the mechanism of action and clinical
pharmacology
-atropine
-scopolamine
-glycopyrrolate
<Mechanisms of action>
Anticholinergics are esters of an aromatic
acid an combined with an organic base
The ester linkage competitively blocks
binding by Ach. and prevent Rc.activation
Receptors subgroups
-M1(neuronal)
-M2(cardiac)
-M3(glandular)
<clinical pharmacology>
In clinical doses, only muscarinic Rc.are blocked
The anticholinergic effects depends on the degree of
baseline vagal tone.
Cardiovascular
-tachycardia; useful in reversing bradycardia d/t
vagal reflexes (baroreceptor reflex, peritoneal
stimulation,
or oculocardiac reflex)
-AV node conduction->PR interval
-little effects on ventricular function or
pph.vasculature
-modestly enhance sympathetic activity
-large doses cutaneous blood vessel
dilatation(atropine flush)
Respiratory
-inhibit secretion of the respiratory tract
mucosa, from nose to bronchi
-relaxation of the bronchial smooth
musculature reduces airway resistence and
anatomic dead space(esp. in COPD and
asthma)
Cerebral
-ranging from stimulation to depression
depending on drug choice and dosage
-stimulation as excitation, restlessness, or
hallucinations
-depression as sedation and amnesia
-physostigmine(BBB) reverses these
action
Gastrointestinal
-salivary secretion
-decreased intestinal motility and peristalsis-
>gastric emptying
-lower esophageal sphincter tone
->aspiration pneumonia
Ophthalmic
-mydriasis and cycloplegia
Genitourinary
-urinary retention
Thermoregulation
-sweat gland
(atropine fever)
Immune mediated hypersensitivity
-little efficacy
<specific anticholinergic drugs>
Atropine
Physical structure

Dosage and packaging

-premedication : 0.01-0.02mg/kg(up to 0.4-0.6mg/adult dose) IV,
or IM
-severe bradycardia 2mg
-cholinesterase inhibitors side effect
reverse
Clinical considerations
1) Bronchial smooth muscle heart
-> bradyarrhythmia
2) Coronary artery dis. atropine
tachycardia

3) ipratropium bromide : Atropine
bronchospasm
acute COPD
4) CNS
(1) BBB
(2) Postop. Memory deficit
(3) toxic dose : excitatory reaction
5) 0.01-0.02 mg/kg intramuscular dose
antisialagogue effect
6) Cautious Use
(1) narrow-angle glaucoma
(2) prostatic hypertrophy
(3) bladder-neck obx.
Scopolamine
Physical structure

dosage and packaging

-Premedication : 0.01-0.02mg/kg(up to 0.4-
0.6mg/adult dose) IV, or IM -Atropine
Clinical consideration
-atopine antisialagogue
- CNS effect
-Clinical dose : drowsiness, amnesia
(restlessness, delirium )
-(motion sickness)
-Closed angle glaucoma (best
avoided)
Glycopyrrolate
Physical structure

Dosage and packaging

dose : atropine 1/2
premedication dose : 0.005-0.01mg/kg (up to 0.2-
0.3 mg in adult )
Clinical consideration
BBB
CNS ophthalmic activity
Salivary gland respiratory tract secretion
IV HR ( IM )
Longer duration (2-4h vs atropine 30min)

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