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螺旋结构在膜中的形成和稳定性。

Helix formation and stability in membranes.

机构信息

Department of Chemistry and Biochemistry, University of Arkansas, Fayetteville, AR 72701, USA.

Department of Chemistry and Biochemistry, University of Arkansas, Fayetteville, AR 72701, USA.

出版信息

Biochim Biophys Acta Biomembr. 2018 Oct;1860(10):2108-2117. doi: 10.1016/j.bbamem.2018.02.010. Epub 2018 Feb 13.

Abstract

In this article we review current understanding of basic principles for the folding of membrane proteins, focusing on the more abundant alpha-helical class. Membrane proteins, vital to many biological functions and implicated in numerous diseases, fold into their active conformations in the complex environment of the cell bilayer membrane. While many membrane proteins rely on the translocon and chaperone proteins to fold correctly, others can achieve their functional form in the absence of any translation apparatus or other aides. Nevertheless, the spontaneous folding process is not well understood at the molecular level. Recent findings suggest that helix fraying and loop formation may be important for overall structure, dynamics and regulation of function. Several types of membrane helices with ionizable amino acids change their topology with pH. Additionally we note that some peptides, including many that are rich in arginine, and a particular analogue of gramicidin, are able passively to translocate across cell membranes. The findings indicate that a final protein structure in a lipid-bilayer membrane is sequence-based, with lipids contributing to stability and regulation. While much progress has been made toward understanding the folding process for alpha-helical membrane proteins, it remains a work in progress. This article is part of a Special Issue entitled: Emergence of Complex Behavior in Biomembranes edited by Marjorie Longo.

摘要

本文综述了目前对膜蛋白折叠基本原理的理解,重点介绍了更为丰富的α-螺旋类膜蛋白。膜蛋白对于许多生物功能至关重要,并与许多疾病有关,它们在细胞双层膜的复杂环境中折叠成其活性构象。虽然许多膜蛋白依赖于易位子和伴侣蛋白来正确折叠,但其他蛋白可以在没有任何翻译装置或其他辅助物的情况下达到其功能形式。然而,自发折叠过程在分子水平上还没有得到很好的理解。最近的发现表明,螺旋磨损和环形成可能对整体结构、动力学和功能调节很重要。带有可电离氨基酸的几种类型的膜螺旋其拓扑结构会随 pH 值变化而变化。此外,我们注意到,包括富含精氨酸的许多肽在内的一些肽,以及一种特定的短杆菌肽类似物,能够被动地穿过细胞膜。这些发现表明,脂质双层膜中的最终蛋白质结构是基于序列的,脂质有助于稳定和调节。虽然在理解α-螺旋膜蛋白的折叠过程方面已经取得了很大进展,但这仍然是一个正在进行的工作。本文是由 Marjorie Longo 编辑的特刊“生物膜中复杂行为的出现”的一部分。

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