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氨氯吡咪及其某些类似物对离体蛙皮和薄脂质膜中阳离子转运的影响。

Effect of amiloride and some of its analogues of cation transport in isolated frog skin and thin lipid membranes.

作者信息

Benos D J, Simon S A, Mandel L J, Cala P M

出版信息

J Gen Physiol. 1976 Jul;68(1):43-63. doi: 10.1085/jgp.68.1.43.

Abstract

The inhibition of short-circuit current (Isc) in isolated frog skin and the induction of surface potentials in lipid bilayer membranes produced by the diuretic drug amiloride and a number of its chemical analogues was studied. The major conclusions of our study are: (a) The charged form of amiloride is the biologically active species. (b) Both the magnitude of Isc and the amiloride inhibitory effect are sensitive to the ionic milieu bathing the isolated skin, and these two features are modulated at separate and distinct regions on the transport site. (c) Amiloride is very specific in its inhibitory interaction with the Na+ transport site since slight structural modifications can result in significant changes in drug effectiveness. We found that substitutions at pyrazine ring position 5 greatly diminish drug activity, while changes at position 6 are less drastic. Alterations in the guanidinium moiety only diminish activity if the result is a change in the spatial orientation of the amino group carrying the positive charge. (d) Amiloride can bind to and alter the charge on membrane surfaces, but this action cannot explain its highly specific effects in biological systems.

摘要

研究了利尿药氨氯吡脒及其一些化学类似物对离体蛙皮短路电流(Isc)的抑制作用以及对脂质双分子层膜表面电位的诱导作用。我们研究的主要结论如下:(a)氨氯吡脒的带电形式是生物活性形式。(b)Isc的大小和氨氯吡脒的抑制作用均对浸泡离体皮肤的离子环境敏感,且这两个特性在转运位点的不同区域受到调节。(c)氨氯吡脒与Na+转运位点的抑制性相互作用具有高度特异性,因为轻微的结构修饰可导致药物效力发生显著变化。我们发现,吡嗪环5位的取代会大大降低药物活性,而6位的变化则不那么剧烈。只有当胍基部分的变化导致携带正电荷的氨基空间取向改变时,才会降低活性。(d)氨氯吡脒可结合并改变膜表面电荷,但这种作用无法解释其在生物系统中的高度特异性作用。

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