Pharmacological analysis of the muscarinic receptors involved when McN‐A 343 stimulates acid secretion in the mouse isolated stomach

Abstract

1 In view of the recent M₁ and M₂ subclassification of muscarinic receptors and the suggestion of separate populations of muscarinic receptors on oxyntic and histamine cells in the gastric mucosa, we have analysed the effects of McN-A 343, classified as an M₁-selective agonist, on gastric acid secretion by the mouse, isolated, lumen-perfused stomach assay. 2 Acid secretion stimulated by McN-A 343 was not inhibited by tetrodotoxin pretreatment, although it was competitively antagonized by atropine (pK_B 7.90), suggesting a muscarinic site of action between postganglionic neurones and the final secretory event. 3 Acid secretion stimulated by McN-A 343 was more sensitive than 5-methylfurmethide-stimulated secretion to H₂-receptor blockade: the profile of inhibition was consistent with expectations for a model of indirect agonism, suggesting that McN-A 343 preferentially stimulated the release of endogenous histamine from mucosal histamine cells. 4 In view of this selective action the McN-A 343-pirenzepine interaction was studied, the latter being classified as an M₁-selective antagonist. Results were consistent with expectations for a competitive interaction but the pK_B (6.69) was not significantly different from the value obtained at the oxyntic cell, using 5-methylfurmethide as agonist in the presence of H₂-receptor blockade, in a previous study. 5 We suggest that there is no need to postulate differences in oxyntic and histamine cell muscarinic receptors to account for the selective stimulant activity of McN-A 343 observed in this study and the relatively selective inhibition of gastric acid secretion by pirenzepine in vivo. McN-A 343 selectivity may be accounted for by a higher muscarinic receptor density on the histamine cell and pirenzepine selectivity by a smaller degree of loss into the gastric secretion compared to atropine.