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Influence of pHo on calcium channel block by amlodipine, a charged dihydropyridine compound. Implications for location of the dihydropyridine receptor

机译:pHo对氨氯地平(一种带电荷的二氢吡啶化合物)的钙通道阻滞的影响。对二氢吡啶受体位置的影响

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摘要

We have investigated the modulation of L-type calcium channel currents in isolated ventricular cells by the dihydropyridine derivative amlodipine, a weak base with a pKa of 8.6. Under conditions that favor neutral drug molecules, amlodipine block resembles other, previously described, neutral dihydropyridine derivatives: block is more pronounced at depolarized voltages, repetitive pulsing is not needed to promote block, and recovery is complete at hyperpolarized voltages. When the drug is ionized, depolarized voltages still enhance block, however, the time course is slow and speeded by repetitive pulses that open channels. Recovery from block by ionized drug molecules is very slow and incomplete, but can be rapidly modified by changes in external hydrogen ion concentration. We conclude from these observations that the degree of ionization of the drug molecule can affect access to the dihydropyridine receptor and that external protons can interact with the drug-receptor complex even if channels are blocked and closed. These observations place limitations on the location of this receptor in the ventricular cell membrane.
机译:我们已经研究了二氢吡啶衍生物氨氯地平(pKa为8.6的弱碱)在离体心室细胞中对L型钙通道电流的调节。在有利于中性药物分子的条件下,氨氯地平阻滞类似于其他先前描述的中性二氢吡啶衍生物:在去极化电压下阻滞更为明显,不需要重复脉冲来促进阻滞,而在超极化电压下恢复完全。当药物被离子化时,去极化电压仍会增强阻断作用,但是,时间进程很慢,并且通过打开通道的重复脉冲而加快了速度。被离子化的药物分子从阻滞中恢复的过程非常缓慢且不完全,但是可以通过外部氢离子浓度的变化迅速进行修改。从这些观察结果我们得出结论,药物分子的离子化程度会影响对二氢吡啶受体的访问,并且即使通道被阻塞和关闭,外部质子也会与药物受体复合物相互作用。这些观察结果限制了该受体在心室细胞膜中的位置。

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  • 年度 1989
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