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钙通道阻滞剂与血管平滑肌异质性

Calcium entry blockers and vascular smooth muscle heterogeneity.

作者信息

Van Nueten J M, Vanhoutte P M

出版信息

Fed Proc. 1981 Dec;40(14):2862-5.

PMID:7308496
Abstract

Inasmuch as the cytoplasmic level of activator Ca2+ governs the contractile activity of vascular smooth muscle cells, the efficacy of calcium entry blockers in curtailing vasoconstriction is determined by the dependency of this level on the influx of extracellular Ca2+ into the cells; this dependency varies with the trigger to contraction as well as with the anatomical origin of the vascular preparation tested. Certain calcium entry blockers (e.g., flunarizine and lidoflazine) tested in experimental conditions triggering the influx of the activator ion exhibit a pronounced tissue selectivity, presumably because the characteristics and accessibility of the Ca2+ channels vary among different vascular smooth muscle cells. The time of onset and duration of calcium entry blockade are not identical for all calcium entry blockers, which must reflect their permeation in the tissue as well as their individual pharmacological properties at the molecular level.

摘要

鉴于激活剂Ca2+的细胞质水平控制着血管平滑肌细胞的收缩活动,钙通道阻滞剂抑制血管收缩的效果取决于该水平对细胞外Ca2+流入细胞的依赖性;这种依赖性随收缩触发因素以及所测试血管标本的解剖学来源而变化。在触发激活离子流入的实验条件下测试的某些钙通道阻滞剂(如氟桂利嗪和利多氟嗪)表现出明显的组织选择性,这可能是因为不同血管平滑肌细胞中Ca2+通道的特性和可及性不同。所有钙通道阻滞剂的钙通道阻滞起效时间和持续时间并不相同,这必定反映了它们在组织中的渗透情况以及它们在分子水平上的个体药理学特性。

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