Studies on the muscarine receptors in rat gastric smooth muscle
Autor: | Yoshio Goto, Yo Okuno, Hiroaki Ujiie, Kenzo Satake, Yih-Fong Lin, Michio Hongo |
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Rok vydání: | 1988 |
Předmět: |
Male
Agonist medicine.medical_specialty Contraction (grammar) Physiology medicine.drug_class Tetrodotoxin In Vitro Techniques chemistry.chemical_compound Internal medicine Muscarinic acetylcholine receptor medicine Animals Receptor Muscarine Stomach digestive oral and skin physiology Muscle Smooth Muscarinic acetylcholine receptor M2 Pirenzepine Smooth muscle contraction Receptors Muscarinic Acetylcholine Rats Endocrinology chemistry Muscle Contraction medicine.drug |
Zdroj: | Japanese Journal of Smooth Muscle Research. 24:39-45 |
ISSN: | 1884-8788 0374-3527 |
DOI: | 10.1540/jsmr1965.24.39 |
Popis: | It has been reported that the two types of muscarinic receptors, "M1" and "M2", exist in the opossum lower esophageal sphincter. The presence of these muscarinic receptor subtypes had been confirmed with the discovery of the M1 selective antagonist, pirenzepine. But little is known about muscarinic receptor subtypes in gastric smooth muscle. The aim of this study was to identify the muscarinic receptor subtypes on the gastric smooth muscle responsible for the contraction of rat gastric muscle strip. Also, we examined the mechanism of the action of aclatonium napadisilate on rat gastric smooth muscle in vitro. The stimulation of M2 receptor caused the contraction of the gastric smooth muscle. McN-A-343, selective M1 agonist, caused weak contraction of the gastric smooth muscle, and this response was not affected by the selective M1 antagonist, pirenzepine. Aclatonium napadisilate stimulated M2 receptor and caused the gastric smooth muscle contraction. We conclude that the contraction of the gastric smooth muscle is caused by the stimulation of the M2 receptor and this reaction was not affected by tetrodotoxin, suggesting the M2 receptor is located directly on the gastric smooth muscle. The weak contraction of the gastric smooth muscle caused by McN-A-343 was not affected by the selective M1 antagonist, pirenzepine, suggesting that McN-A-343 may not be a pure M1 selective agonist. The action of aclatonium napadisilate is supposed to stimulate the M2 receptor. |
Databáze: | OpenAIRE |
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