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2,4,6-三氨基嘧啶鎓(TAP)对胆囊紧密连接阳离子选择性通道的阻断作用。

Blockage of gallbladder tight junction cation-selective channels by 2,4,6-triaminopyrimidinium (TAP).

作者信息

Moreno J H

出版信息

J Gen Physiol. 1975 Jul;66(1):97-115. doi: 10.1085/jgp.66.1.97.

Abstract

The organic cation 2,4,6-triaminopyrimidinium (TAP) specifically inhibits Na+ passive permeation (PNa) across gallbladder, small intestine, and choroid plexus without detectable effect on the Cl(-) permeability, indicating that Na+ and Cl(-) follow different permeation pathways. In bullfrog gallbladder, where it was examined in greater detail, the effect of TAP was shown to be: (a) completely reversible, (b) due only to the protonated form of 2,4,6-triaminopyrimidine, (c) effective when added to either one or both sides of the membrane (the rate limiting for the delay in the response being the diffusion through the unstirred layers), and (d) exhibiting a typical saturation kinetics, best fitted with the parameters "Km" = 2.6 mM and maximal effect = 100% inhibition. These data, along with the fact that the PNa blocking action of chemical analogs of TAP increases with their ability to donate protons to form hydrogen bonds, suggest that TAP blocks the cation permeation of the channels by strongly associating, via hydrogen bonds, with the anionic ligands within the channel.

摘要

有机阳离子2,4,6-三氨基嘧啶(TAP)可特异性抑制跨胆囊、小肠和脉络丛的Na⁺被动通透(PNa),而对Cl⁻通透性无明显影响,这表明Na⁺和Cl⁻遵循不同的通透途径。在牛蛙胆囊中进行了更详细的研究,结果显示TAP的作用为:(a)完全可逆;(b)仅归因于2,4,6-三氨基嘧啶的质子化形式;(c)添加到膜的一侧或两侧均有效(响应延迟的限速因素是通过未搅动层的扩散);(d)呈现典型的饱和动力学,最适合的参数为“Km” = 2.6 mM,最大效应为100%抑制。这些数据,以及TAP化学类似物的PNa阻断作用随其提供质子形成氢键的能力增加这一事实,表明TAP通过与通道内的阴离子配体通过氢键强烈结合来阻断通道的阳离子通透。

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