Pharmacological profile of the novel .ALPHA.-adrenoceptor antagonist KT-611(naftopidil).
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概要
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The pharmacological profile of a new alpha-adrenoceptor antagonist, KT-611 (naftopidil), was studied in vitro. In the dog mesenteric and carotid arteries and in the rabbit, guinea pig and rat thoracic aortae, KT-611 competitively inhibited α<SUB>1</SUB>-adrenoceptor-mediated contractions induced by noradrenaline with pA<SUB>2</SUB> values ranging from 6.73 to 8.15. KT-611 also inhibited the postjunctional α<SUB>2</SUB>-adrenoceptormediated contractions in the dog saphenous vein (pA<SUB>2</SUB> = 6.77) or dog basilar artery. However, the responses mediated through prejunctional α<SUB>2</SUB>-adrenoceptors (rat vas deferens), β-adrenoceptors (rat atria), muscarinic receptors (guinea pig ileum) and 5-HT<SUB>2</SUB> receptors (dog mesenteric artery) were little affected by KT-611. KT-611 also inhibited the sympathetic adrenergic contraction evoked by electrical transmural stimulation in the dog mesenteric artery, and the inhibition was not relieved upon repetitive washing for 1 hour with the drug-free solution. <SUP>3</SUP>H-prazosin and <SUP>3</SUP>H-clonidine binding to the rat cortex membranes was inhibited by KT-611 with pK<SUB>i</SUB> values of 7.69 and 5.75, respectively. These results suggest that KT-611 is an α<SUB>1</SUB>-adrenoceptor antagonist with a weak antagonistic activity to postjunctional α<SUB>2</SUB>-adrenoceptors.
著者
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Muramatsu Ikunobu
Department Of Pharmacology Faculty Of Medicine Kyoto University And Department Of Zoology And Its Ca
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Kigoshi Shigeru
Department Of Pharmacology Fukui Medical School
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YAMANAKA Kyozo
Department of Pharmacology, Fukui Medical School
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