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不同的脂质双层组成对 K+ 通道功能具有普遍和蛋白特异性的影响。

Distinct lipid bilayer compositions have general and protein-specific effects on K+ channel function.

机构信息

Membrane Biophysics, Technische Universität Darmstadt, Darmstadt, Germany.

Department of Structural Biology, Christian-Albrechts-Universität, Kiel, Germany.

出版信息

J Gen Physiol. 2021 Feb 1;153(2). doi: 10.1085/jgp.202012731.

Abstract

It has become increasingly apparent that the lipid composition of cell membranes affects the function of transmembrane proteins such as ion channels. Here, we leverage the structural and functional diversity of small viral K+ channels to systematically examine the impact of bilayer composition on the pore module of single K+ channels. In vitro-synthesized channels were reconstituted into phosphatidylcholine bilayers ± cholesterol or anionic phospholipids (aPLs). Single-channel recordings revealed that a saturating concentration of 30% cholesterol had only minor and protein-specific effects on unitary conductance and gating. This indicates that channels have effective strategies for avoiding structural impacts of hydrophobic mismatches between proteins and the surrounding bilayer. In all seven channels tested, aPLs augmented the unitary conductance, suggesting that this is a general effect of negatively charged phospholipids on channel function. For one channel, we determined an effective half-maximal concentration of 15% phosphatidylserine, a value within the physiological range of aPL concentrations. The different sensitivity of two channel proteins to aPLs could be explained by the presence/absence of cationic amino acids at the interface between the lipid headgroups and the transmembrane domains. aPLs also affected gating in some channels, indicating that conductance and gating are uncoupled phenomena and that the impact of aPLs on gating is protein specific. In two channels, the latter can be explained by the altered orientation of the pore-lining transmembrane helix that prevents flipping of a phenylalanine side chain into the ion permeation pathway for long channel closings. Experiments with asymmetrical bilayers showed that this effect is leaflet specific and most effective in the inner leaflet, in which aPLs are normally present in plasma membranes. The data underscore a general positive effect of aPLs on the conductance of K+ channels and a potential interaction of their negative headgroup with cationic amino acids in their vicinity.

摘要

越来越明显的是,细胞膜的脂质组成会影响跨膜蛋白(如离子通道)的功能。在这里,我们利用小病毒 K+通道的结构和功能多样性,系统地研究了双层组成对单个 K+通道孔模块的影响。体外合成的通道被重建到磷脂酰胆碱双层中±胆固醇或阴离子磷脂(aPL)。单通道记录显示,饱和浓度为 30%的胆固醇对单位电导和门控只有较小的、蛋白特异性的影响。这表明通道具有有效的策略来避免蛋白质与周围双层之间的疏水性不匹配对结构的影响。在测试的所有七种通道中,aPL 都增加了单位电导,这表明这是阴离子磷脂对通道功能的普遍影响。对于一种通道,我们确定了有效半最大值浓度为 15%的磷脂酰丝氨酸,这是 aPL 浓度的生理范围内的值。两种通道蛋白对 aPL 的不同敏感性可以用脂质头部基团和跨膜结构域之间的界面处存在/不存在阳离子氨基酸来解释。aPL 还会影响某些通道的门控,这表明电导和门控是解耦的现象,aPL 对门控的影响是蛋白特异性的。在两种通道中,后一种情况可以用孔衬跨膜螺旋的取向改变来解释,这种改变阻止了苯丙氨酸侧链翻转到离子渗透途径,从而导致通道长时间关闭。不对称双层实验表明,这种效应是双层特异性的,在正常存在于质膜中的内层中最为有效。这些数据强调了 aPL 对 K+通道电导的普遍正效应,以及它们的负电荷头部基团与附近阳离子氨基酸的潜在相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/397e/7809880/8be35a8df49c/JGP_202012731_FigS1.jpg

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