Sep 1, 1985

Experimental testing of Mackay's model for functional antagonism in the isolated costo-uterus of the rat

British Journal of Pharmacology
P J HenryJ W Paterson

Abstract

Several key predictions of a recently developed model for functional antagonism (Mackay, 1981) were experimentally tested using the rat isolated costo-uterine preparation. In the presence of the functional antagonist fenoterol (Fen), the functional constants (KAF) for carbachol and oxotremorine (Oxo) were respectively 9.9 and 3.4 fold greater than their corresponding affinity constants (KA). According to Mackay's model for functional antagonism, the higher KAF/KA ratio for carbachol indicates that this cholinoceptor agonist has a greater efficacy than Oxo. This was confirmed by using conventional pharmacological methods. As predicted from the model of functional antagonism, the plot of KAF/KA-1 against the fraction of cholinoceptors not irreversibly blocked by phenoxybenzamine (Pbz) was linear for both carbachol and Oxo and the lines of best fit crossed the axes at a point not significantly different from the origin. The value of 4.6 for the relative efficacy of carbachol to Oxo estimated from functional antagonism studies was comparable to the value of 5.6 calculated using the method of irreversible antagonism proposed by Furchgott (1966).

Mentioned in this Paper

Study
Carboptic
Entire Uterus
CFI
Phenoxybenzamine Hydrochloride
Neoplasm of Uncertain or Unknown Behavior of Uterus
Uterus
August Rats
Antagonist Muscle Action
Fenoterol Hydrobromide

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