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Pharmacology of Cholinergic Agonists

Pharmacology of Cholinergic Agonists. Dr. Thomas Abraham PHAR 417: Fall 2005. Cholinergic Agonists. Parasympathomimetic, cholinoceptor agonists. Have predominant actions on: autonomic effector organs innervated by postganglionic parasympathetic nerves.

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Pharmacology of Cholinergic Agonists

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  1. Pharmacology of Cholinergic Agonists Dr. Thomas Abraham PHAR 417: Fall 2005

  2. Cholinergic Agonists • Parasympathomimetic, cholinoceptor agonists. • Have predominant actions on: • autonomic effector organs innervated by postganglionic parasympathetic nerves. • cells containing cholinergic receptors. • Cholinergic agonists primarily divided into: • acetylcholine and synthetic choline esters • cholinomimetic natural alkaloids and analogs • Cholinergic agonists also activate Nicotinic receptors found in the ganglia, neuromuscular junction and CNS

  3. Cholinergic Agonists ACETYLCHOLINE AND CHOLINE ESTERS • ØACETYLCHOLINE • endogenous neurotransmitter; no selectivity for muscarinic vs. nicotinic receptors • rapid metabolism by acetylcholinesterase, butyrylcholinesterase; short half-life • limited therapeutic or diagnostic value

  4. Cholinergic Agonists • ØDERIVATIVES OF CHOLINE ESTERS • resistant to AChE metabolism. Susceptibility to cholinesterase metabolism: Acetylcholine >>> Methacholine >> Carbachol > Bethanechol • mainly muscarinic receptor agonists but Carbachol has significant nicotinic receptor activity.

  5. Cholinergic Agonists • ØActivation of specific muscarinic receptors in various organs elicits physiological response: • Decreased heart rate (negative chronotropy), decreased conduction velocity, decreased atrial contractility (negative inotropy). • Vasodilation of arteries and arterioles: indirectly by the release of • nitric oxide from endothelial cells. • 3. Gastrointestinal: increased intestinal smooth muscle contraction, • motility; relaxation of sphincters, nausea, flatulence, defecation. • 4. Urinary tract: increased detrusor muscle contraction, decreased • trigone, sphincter muscle tone, decreased bladder volume. • 5.     Increased bronchial constriction, increased salivation, lacrimation, • miosis, increased accommodation for near vision.

  6. Cholinergic Agonists Vasodilation of arteries by Muscarinic Agonists Endothelium Vascular Sm. Muscle • These experiments show that endothelial cells on arteries and veins contain muscarinic receptors which when activated would lead to relaxation of vascular smooth muscle and vasodilation.

  7. Cholinergic Agonists Vasodilation of arteries by Muscarinic Agonists Notice that Acetylcholine injection into this “experimental animal” results in decreased BP (blue) and heart rate (HR) but these effects don’t last long.

  8. Cholinergic Agonists • Multiple muscarinic receptors regulate the various physiological effects of endogenous acetylcholine or synthetic analogs:

  9. Cholinergic Agonists • Signal transduction systems of Muscarinic receptors • Coupling of muscarinic receptors to phosphoinositide hydrolysis: • results in initiating various calcium-dependent processes e.g. smooth muscle contraction, secretion of saliva, mucous, release of digestive enzymes, etc

  10. Cholinergic Agonists II. Coupling of muscarinic receptors to effectors via Go/i M2 receptor activation results in decreased heart rate and decreased neurotransmitter release from cholinergic nerves.

  11. Cholinergic Agonists • Therapeutic Uses of Choline esters • To produce miosis during ocular surgery and decrease intraocular pressure: acetylcholine (Miochol®), carbachol (Isopto Carbachol®). • Airway hyperactivity test: methacholine (Provocholine®). • Urinary incontinence and increase GI motility: bethanechol (Urecholine®). • Cautions and contraindications • Use with caution in patients with asthma, hyperthyroidism, coronary insufficiency, peptic ulcer disease. • Toxicity evidenced by hypotension, bradycardia, GI cramps, belching, lack of visual accommodation, headaches, salivation.

  12. Cholinergic Agonists CHOLINOMIMETIC NATURAL ALKALOIDS • ØMore selective for muscarinic vs. nicotinic receptors. • Muscarine from amanita, inocybe, clitocybe sp. of mushrooms; pilocarpine from pilocarpus plant; arecholine from betel nut.

  13. Cholinergic Agonists Mushrooms of Amanita species contain muscarine, which if ingested can cause intoxication “There are many old mushroom pickers and many bold mushroom pickers but there are no old, bold mushroom pickers”

  14. Cholinergic Agonists • ØSystemic administration produces less selective muscarinic effects than • local application: • Cardiovascular system – small doses of muscarine (i.v.) decrease heart rate and blood pressure while pilocarpine can have direct muscarinic effects and indirect (ganglionic) effects. • Smooth muscle effects – pupillary constriction by pilocarpine (miosis), initial increase followed by decreased intraocular pressure, decreased accommodation of lens (for far vision); muscarine increases bronchial and GI muscle contraction while muscarine and pilocarpine promote urination. • Exocrine glands – muscarine and pilocarpine result in sweating, • nausea, vomiting, salivation, lacrimation. • ØTherapeutic uses of pilocarpine for the reduction of intraocular pressure • in open-angle glaucoma; supplied as ophthalmic solution and sustained release delivery system (Occusert Pilo-20®).

  15. Cholinergic Agonists Drainage of Aqueous Humor through the Eye Closed angle Aqueous humor is produced by the ciliary body to maintain shape of the eyeball. Poor drainage through the canal of Schlemm results in elevated intraocular pressure.

  16. Cholinergic Agonists Drainage of Aqueous Humor through the Eye Closed angle Muscarinic agonists cause contraction of the ciliary muscles to relax the trabecular network to allow more fluid movement through the canal. Increasing the thickness of the lens also allows for more movement of aqueous fluid to the anterior chamber. Constriction of the sphincter muscles of the iris also allows proper fluid drainage by pulling away the iris from the closed angle.

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