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Time-Dependent Interaction of a New H2-Receptor Antagonist, IT-066, with the Receptor in the Atria of Guinea Pig

3-Amino-4-[4-[4-(l-piperidinomethyl)-2-pyridyloxy]-cis-2-butenylamino]-3-cyclobutene-l,2-dione hydrochloride (IT-066) showed a highly potent and long lasting H2-receptor blocking action in guinea pig atria. The inhibitory effect of IT-066 on the histamine-induced positive chronotropic response incre...

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Bibliographic Details
Published in:Japanese journal of pharmacology 1991, Vol.57(1), pp.13-23
Main Authors: Muramatsu, Makoto, Hirose-Kijima, Haruko, Aihara, Hironaka, Otomo, Susumu
Format: Article
Language:English
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Summary:3-Amino-4-[4-[4-(l-piperidinomethyl)-2-pyridyloxy]-cis-2-butenylamino]-3-cyclobutene-l,2-dione hydrochloride (IT-066) showed a highly potent and long lasting H2-receptor blocking action in guinea pig atria. The inhibitory effect of IT-066 on the histamine-induced positive chronotropic response increased concentration- and time-dependently. A short period of treatment with IT-066 shifted the concentration-response curve of histamine to the right in parallel, without decreasing the maximal response to histamine. With prolongation of the treatment, the concentration-response curve shifted further to the right with time-dependent suppression of the maximal response to histamine. The inhibitory effect of IT-066 was irreversible. The dissociation constant for histamine (KA) was not changed by prolongation of the time of incubation with IT-066. The dissociation constant for IT-066 (Kb) was decreased with the prolongation of the treatment. Kinetic analysis of the time-dependent inhibition showed a two-step reaction: the first was reversible and the second was irreversible. Preincubation of the atria with ranitidine, however, protected the H2-receptor from the apparently irreversible antagonism of IT-066. These results suggest that IT-066 has a time-dependent and irreversible interaction with the H2-receptor and that the interaction may be responsible for the potent and long lasting H2-receptor blocking action of IT-066.
ISSN:0021-5198
1347-3506
DOI:10.1254/jjp.57.13