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K2P钾离子通道中的门控、调节与结构:求同存异?

Gating, Regulation, and Structure in K2P K+ Channels: In Varietate Concordia?

作者信息

Niemeyer María Isabel, Cid L Pablo, González Wendy, Sepúlveda Francisco V

机构信息

Centro de Estudios Científicos (CECs), Valdivia, Chile (M.I.N., L.P.C., F.V.S.), Centro de Bioinformática y Simulación Molecular (CBSM), Universidad de Talca, Talca, Chile (W.G.).

Centro de Estudios Científicos (CECs), Valdivia, Chile (M.I.N., L.P.C., F.V.S.), Centro de Bioinformática y Simulación Molecular (CBSM), Universidad de Talca, Talca, Chile (W.G.)

出版信息

Mol Pharmacol. 2016 Sep;90(3):309-17. doi: 10.1124/mol.116.103895. Epub 2016 Jun 6.

DOI:10.1124/mol.116.103895
PMID:27268784
Abstract

K2P K(+) channels with two pore domains in tandem associate as dimers to produce so-called background conductances that are regulated by a variety of stimuli. Whereas gating in K2P channels has been poorly understood, recent developments have provided important clues regarding the gating mechanism for this family of proteins. Two modes of gating present in other K(+) channels have been considered. The first is the so-called activation gating that occurs by bundle crossing and the splaying apart of pore-lining helices commanding ion passage. The second mode involves a change in conformation at the selectivity filter (SF), which impedes ion flow at this narrow portion of the conduction pathway and accounts for extracellular pH modulation of several K2P channels. Although some evidence supports the existence of an activation gate in K2P channels, recent results suggest that perhaps all stimuli, even those sensed at a distant location in the protein, are also mediated by SF gating. Recently resolved crystal structures of K2P channels in conductive and nonconductive conformations revealed that the nonconductive state is reached by blockade by a lipid acyl chain that gains access to the channel cavity through intramembrane fenestrations. Here we discuss whether this novel type of gating, proposed so far only for membrane tension gating, might mediate gating in response to other stimuli or whether SF gating is the only type of opening/closing mechanism present in K2P channels.

摘要

具有两个串联孔结构域的K2P钾通道以二聚体形式结合,产生所谓的背景电导,该电导受多种刺激调节。尽管人们对K2P通道的门控机制了解甚少,但最近的进展为该蛋白家族的门控机制提供了重要线索。人们考虑了其他钾通道中存在的两种门控模式。第一种是所谓的激活门控,它通过束交叉和引导离子通过的孔内衬螺旋的张开而发生。第二种模式涉及选择性过滤器(SF)处的构象变化,这会阻碍离子在传导途径的这个狭窄部分流动,并解释了几种K2P通道的细胞外pH调节。尽管有一些证据支持K2P通道中存在激活门,但最近的结果表明,也许所有刺激,即使是那些在蛋白质中远处感知到的刺激,也同样由SF门控介导。最近解析的处于导电和非导电构象的K2P通道晶体结构表明,非导电状态是由一条脂质酰基链阻断而达到的,该脂质酰基链通过膜内小孔进入通道腔。在这里,我们讨论这种迄今为止仅针对膜张力门控提出的新型门控是否可能介导对其他刺激的门控,或者SF门控是否是K2P通道中唯一存在的开/关机制类型。

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