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通过电压依赖性钾通道的关闭捕获有机阻滞剂:激活门控的活板门机制的证据。

Trapping of organic blockers by closing of voltage-dependent K+ channels: evidence for a trap door mechanism of activation gating.

作者信息

Holmgren M, Smith P L, Yellen G

机构信息

Department of Neurobiology, Harvard Medical School and Massachusetts General Hospital, Boston 02114, USA.

出版信息

J Gen Physiol. 1997 May;109(5):527-35. doi: 10.1085/jgp.109.5.527.

Abstract

Small organic molecules, like quaternary ammonium compounds, have long been used to probe both the permeation and gating of voltage-dependent K+ channels. For most K+ channels, intracellularly applied quaternary ammonium (QA) compounds such as tetraethylammonium (TEA) and decyltriethylammonium (C10) behave primarily as open channel blockers: they can enter the channel only when it is open, and they must dissociate before the channel can close. In some cases, it is possible to force the channel to close with a QA blocker still bound, with the result that the blocker is "trapped." Armstrong (J. Gen. Physiol. 58:413-437) found that at very negative voltages, squid axon K+ channels exhibited a slow phase of recovery from QA blockade consistent with such trapping. In our studies on the cloned Shaker channel, we find that wild-type channels can trap neither TEA nor C10, but channels with a point mutation in S6 can trap either compound very efficiently. The trapping occurs with very little change in the energetics of channel gating, suggesting that in these channels the gate may function as a trap door or hinged lid that occludes access from the intracellular solution to the blocker site and to the narrow ion-selective pore.

摘要

长期以来,像季铵化合物这样的有机小分子一直被用于探究电压依赖性钾离子通道的通透和门控机制。对于大多数钾离子通道而言,细胞内施加的季铵(QA)化合物,如四乙铵(TEA)和癸基三乙铵(C10),主要表现为开放通道阻滞剂:它们只有在通道开放时才能进入通道,并且在通道关闭之前必须解离。在某些情况下,有可能在QA阻滞剂仍然结合的情况下迫使通道关闭,结果导致阻滞剂被“困住”。阿姆斯特朗(《普通生理学杂志》58:413 - 437)发现,在非常负的电压下,鱿鱼轴突钾离子通道从QA阻滞中恢复表现出一个缓慢的阶段,这与这种困住现象一致。在我们对克隆的Shaker通道的研究中,我们发现野生型通道既不能困住TEA也不能困住C10,但在S6中有一个点突变的通道能够非常有效地困住这两种化合物中的任何一种。困住现象发生时通道门控的能量学变化很小,这表明在这些通道中,门可能起到活板门或铰链盖的作用,从而阻止细胞内溶液进入阻滞剂位点和狭窄的离子选择性孔道。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d4df/2217058/3ab6865ee64a/JGP.holmgren1.jpg

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