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膜内的功能竞争:脂质识别与跨膜螺旋寡聚化

Functional competition within a membrane: Lipid recognition vs. transmembrane helix oligomerization.

作者信息

Stangl Michael, Schneider Dirk

机构信息

Department of Pharmacy and Biochemistry, Johannes-Gutenberg-University Mainz, Johann-Joachim-Becher-Weg 30, 55128 Mainz, Germany.

Department of Pharmacy and Biochemistry, Johannes-Gutenberg-University Mainz, Johann-Joachim-Becher-Weg 30, 55128 Mainz, Germany.

出版信息

Biochim Biophys Acta. 2015 Sep;1848(9):1886-96. doi: 10.1016/j.bbamem.2015.03.011. Epub 2015 Mar 16.

DOI:10.1016/j.bbamem.2015.03.011
PMID:25791349
Abstract

Binding of specific lipids to large, polytopic membrane proteins is well described, and it is clear that such lipids are crucial for protein stability and activity. In contrast, binding of defined lipid species to individual transmembrane helices and regulation of transmembrane helix monomer-oligomer equilibria by binding of distinct lipids is a concept, which has emerged only lately. Lipids bind to single-span membrane proteins, both in the juxta-membrane region as well as in the hydrophobic membrane core. While some interactions counteract transmembrane helix oligomerization, in other cases lipid binding appears to enhance oligomerization. As reversible oligomerization is involved in activation of many membrane proteins, binding of defined lipids to single-span transmembrane proteins might be a mechanism to regulate and/or fine-tune the protein activity. But how could lipid binding trigger the activity of a protein? How can binding of a single lipid molecule to a transmembrane helix affect the structure of a transmembrane helix oligomer, and consequently its signaling state? These questions are discussed in the present article based on recent results obtained with simple, single-span transmembrane proteins. This article is part of a Special Issue entitled: Lipid-protein interactions.

摘要

特定脂质与大型多结构域膜蛋白的结合已有充分描述,显然此类脂质对于蛋白质的稳定性和活性至关重要。相比之下,特定脂质种类与单个跨膜螺旋的结合以及通过不同脂质的结合来调节跨膜螺旋单体 - 寡聚体平衡,这一概念是最近才出现的。脂质可与单跨膜结构域膜蛋白结合,既可以在近膜区域,也可以在疏水的膜核心区域。虽然一些相互作用会抑制跨膜螺旋的寡聚化,但在其他情况下,脂质结合似乎会增强寡聚化。由于许多膜蛋白的激活都涉及可逆的寡聚化,特定脂质与单跨膜结构域蛋白的结合可能是一种调节和/或微调蛋白质活性的机制。但是脂质结合如何触发蛋白质的活性呢?单个脂质分子与跨膜螺旋的结合如何影响跨膜螺旋寡聚体的结构,进而影响其信号传导状态?本文将基于最近对简单的单跨膜结构域蛋白所获得的结果来讨论这些问题。本文是名为“脂质 - 蛋白质相互作用”的特刊的一部分。

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