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二氢吡啶类钙通道阻滞剂与豚鼠心室肌细胞的电压依赖性结合。

Voltage-dependent binding of dihydropyridine calcium channel blockers to guinea pig ventricular myocytes.

作者信息

Kamp T J, Sanguinetti M C, Miller R J

机构信息

Department of Pharmacological and Physiological Sciences, University of Chicago, Illinois.

出版信息

J Pharmacol Exp Ther. 1988 Dec;247(3):1240-7.

PMID:2849670
Abstract

The voltage dependence of the binding of dihydropyridine Ca channel blockers (+)-[3H]PN200-110 and [3H]nitrendipine to enzymatically isolated guinea pig ventricular myocytes was examined. The equilibrium saturation binding of (+)-[3H]PN200-110 could be well described by a simple 1:1 binding scheme under all conditions tested. The results demonstrated that the effect of depolarization induced by high extracellular K+ (50 mM) compared to normal K+ (4.8 mM) was an increase in the observed number of binding sites (Bmax) with no change in the measured affinity of binding (Kd). Similarly, depolarization induced by a combination of Na channel toxins in the presence of normal extracellular K+ caused an increase in the observed binding of (+)-[3H]PN200-110 comparable to that observed with high K+. [3H]Nitrendipine binding was likewise increased by depolarization in the presence of 50 mM K+ compared to 4.8 mM K+. Percoll density gradient centrifugation was found to enrich the cell preparation with viable myocytes and increased the measured voltage-dependent change in binding. In agreement with the predictions from previous studies (Kamp and Miller, 1987a), the magnitude of the observed change in Bmax was directly related to the fraction of cells which were viable in a given experiment. These results are discussed in comparison to the modulated receptor hypothesis proposed from electrophysiological studies.

摘要

研究了二氢吡啶类钙通道阻滞剂(+)-[3H]PN200-110和[3H]尼群地平与酶分离的豚鼠心室肌细胞结合的电压依赖性。在所有测试条件下,(+)-[3H]PN200-110的平衡饱和结合都可以用简单的1:1结合模式很好地描述。结果表明,与正常钾离子浓度(4.8 mM)相比,高细胞外钾离子浓度(50 mM)诱导的去极化作用是使观察到的结合位点数量(Bmax)增加,而测得的结合亲和力(Kd)没有变化。同样,在正常细胞外钾离子存在的情况下,钠通道毒素组合诱导的去极化导致(+)-[3H]PN200-110的观察结合增加,与高钾离子浓度下观察到的情况相当。与4.8 mM钾离子浓度相比,在50 mM钾离子存在的情况下,去极化同样增加了[3H]尼群地平的结合。发现Percoll密度梯度离心可使细胞制剂中活心肌细胞富集,并增加测得的结合电压依赖性变化。与先前研究(坎普和米勒,1987a)的预测一致,观察到的Bmax变化幅度与给定实验中活细胞的比例直接相关。与电生理研究提出的调节受体假说相比,对这些结果进行了讨论。

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