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膜蛋白折叠:来自膜β-折叠寡聚体中子衍射研究的见解

Protein folding in membranes: insights from neutron diffraction studies of a membrane beta-sheet oligomer.

作者信息

Han Xue, Hristova Kalina, Wimley William C

机构信息

The Johns Hopkins University, Department of Materials Science and Engineering, Baltimore, Maryland 21218, USA.

出版信息

Biophys J. 2008 Jan 15;94(2):492-505. doi: 10.1529/biophysj.107.113183. Epub 2007 Sep 14.

Abstract

Studies of the assembly of the hexapeptide Acetyl-Trp-Leu(5) (AcWL(5)) into beta-sheets in membranes have provided insights into membrane protein folding. Yet, the exact structure of the oligomer in the lipid bilayer is unknown. Here we use neutron diffraction to study the disposition of the peptides in bilayers. We find that pairs of adjacent deuterium-labeled leucines have no well-defined peak or dip in the transmembrane distribution profiles, indicative of heterogeneity in the depth of membrane insertion. At the same time, the monomeric homolog AcWL(4) exhibits a homogeneous, well-defined, interfacial location in neutron diffraction experiments. Thus, although the bilayer location of monomeric AcWL(4) is determined by hydrophobicity matching or complementarity within the bilayer, the AcWL(5) molecules in the oligomer are positioned at different depths within the bilayer because they assemble into a staggered transmembrane beta-sheet. The AcWL(5) assembly is dominated by protein-protein interactions rather than hydrophobic complementarity. These results have implications for the structure and folding of proteins in their native membrane environment and highlight the importance of the interplay between hydrophobic complementarity and protein-protein interactions in determining the structure of membrane proteins.

摘要

关于六肽乙酰基 - 色氨酸 - 亮氨酸(5)(AcWL(5))在膜中组装成β - 折叠的研究为膜蛋白折叠提供了见解。然而,脂质双层中寡聚体的确切结构尚不清楚。在此,我们利用中子衍射研究肽在双层中的分布情况。我们发现,相邻的氘标记亮氨酸对在跨膜分布图谱中没有明确的峰或谷,这表明膜插入深度存在异质性。同时,单体同系物AcWL(4)在中子衍射实验中呈现出均匀、明确的界面位置。因此,尽管单体AcWL(4)在双层中的位置由双层内的疏水性匹配或互补性决定,但寡聚体中的AcWL(5)分子在双层内处于不同深度,因为它们组装成了交错的跨膜β - 折叠。AcWL(5)的组装主要由蛋白质 - 蛋白质相互作用而非疏水互补性主导。这些结果对蛋白质在其天然膜环境中的结构和折叠具有启示意义,并突出了疏水互补性与蛋白质 - 蛋白质相互作用之间的相互作用在决定膜蛋白结构中的重要性。

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