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维拉帕米和硝普钠对兔主动脉、大鼠主动脉及豚鼠结肠带平滑肌收缩和45钙摄取的比较效应。

Comparative effects of verapamil and sodium nitroprusside on contraction and 45Ca uptake in the smooth muscle of rabbit aorta, rat aorta and guinea-pig taenia coli.

作者信息

Karaki H, Nakagawa H, Urakawa N

出版信息

Br J Pharmacol. 1984 Feb;81(2):393-400. doi: 10.1111/j.1476-5381.1984.tb10091.x.

Abstract

The effects of verapamil and sodium nitroprusside on muscle tension and 45Ca uptake activated in different ways were compared in rabbit aorta, rat aorta and guinea-pig taenia coli. In rabbit aorta, K-induced contraction was specifically inhibited by verapamil and noradrenaline-induced contraction by sodium nitroprusside. In rat aorta, both K-induced and noradrenaline-induced contractions were inhibited by verapamil or by sodium nitroprusside also. In taenia, both K- and histamine-induced sustained contractions were inhibited by verapamil but not by sodium nitroprusside. The effect of verapamil was competitively antagonized by external Ca, while that of sodium nitroprusside was not. High K, noradrenaline and histamine increased the rate of 45Ca uptake in aortae and taenia. In rabbit aorta the increment in response to high K was specifically inhibited by verapamil and the increment induced by noradrenaline was specifically inhibited by sodium nitroprusside. In rat aorta, increments induced by both high K and noradrenaline were inhibited by verapamil and by sodium nitroprusside. In taenia, the increments induced by high K and by histamine were inhibited by verapamil but not by sodium nitroprusside. These results suggest different characteristics of Ca entry systems in these smooth muscles. In rabbit aorta, there seem to be two Ca channels, one of which is activated by high K and inhibited by verapamil, while the other is activated by noradrenaline and inhibited by sodium nitroprusside. In rat aorta, both K- and noradrenaline-activated Ca pathways are sensitive to both verapamil and sodium nitroprusside whereas, in taenia, both K- and histamine-activated Ca pathways are sensitive only to verapamil.

摘要

在兔主动脉、大鼠主动脉和豚鼠结肠带中,比较了维拉帕米和硝普钠对以不同方式激活的肌肉张力和45Ca摄取的影响。在兔主动脉中,维拉帕米特异性抑制钾诱导的收缩,硝普钠特异性抑制去甲肾上腺素诱导的收缩。在大鼠主动脉中,维拉帕米或硝普钠也能抑制钾诱导和去甲肾上腺素诱导的收缩。在结肠带中,维拉帕米抑制钾和组胺诱导的持续性收缩,而硝普钠则无此作用。维拉帕米的作用可被细胞外钙竞争性拮抗,而硝普钠则不受影响。高钾、去甲肾上腺素和组胺可增加主动脉和结肠带中45Ca的摄取率。在兔主动脉中,维拉帕米特异性抑制对高钾反应的增量,硝普钠特异性抑制去甲肾上腺素诱导的增量。在大鼠主动脉中,维拉帕米和硝普钠均抑制高钾和去甲肾上腺素诱导的增量。在结肠带中,维拉帕米抑制高钾和组胺诱导的增量,而硝普钠则无此作用。这些结果表明这些平滑肌中钙内流系统具有不同的特性。在兔主动脉中,似乎存在两种钙通道,其中一种由高钾激活并被维拉帕米抑制,另一种由去甲肾上腺素激活并被硝普钠抑制。在大鼠主动脉中钾和去甲肾上腺素激活的钙途径对维拉帕米和硝普钠均敏感,而在结肠带中,钾和组胺激活的钙途径仅对维拉帕米敏感。

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