Combined dose‐ratio analysis of cholecystokinin receptor antagonists, devazepide, lorglumide and loxiglumide in the guinea‐pig gall bladder

Abstract

1 Interactions between cholecystokinin octapeptide (CCK-8) and CCK_A-receptor antagonists derived from benzodiazepines (devazepide) and glutamic acid (lorglumide and loxiglumide) have been examined in an improved bioassay using the guinea-pig, isolated, gall bladder preparation. 2 The presence of CCK_B-receptors in the assay was provisionally-ruled out on the basis of the low potency of pentagastrin in the assay. By applying analyses of both agonism and antagonism, pentagastrin was shown to behave as a partial agonist at the CCK_A-receptor. 3 Devazepide, lorglumide and loxiglumide behaved as simple competitive antagonists of CCK_A-receptors and pK_B values of 9.98, 7.59 and 7.07 were estimated, respectively. 4 Application of a combined dose-ratio analysis to the interactions between CCK-8 and combinations of devazepide/lorglumide and devazepide/loxiglumide indicated that these molecules behave as syntopic, competitive, antagonists at the CCK_A-receptor. 5 We conclude that the guinea-pig gall bladder assay contains a homogeneous population of CCK_A-receptors and offer an explanation for the differences between our results and those obtained recently by Maubach et al. (1991) which were taken as preliminary evidence for CCK_A-receptor heterogeneity.