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周质细菌分子伴侣SurA会调整其结构以结合不同构象的肽,从而表现出对芳香族残基的序列偏好。

The periplasmic bacterial molecular chaperone SurA adapts its structure to bind peptides in different conformations to assert a sequence preference for aromatic residues.

作者信息

Xu Xiaohua, Wang Shuying, Hu Yao-Xiong, McKay David B

机构信息

Department of Structural Biology, Stanford University School of Medicine, Stanford, CA 94305, USA.

出版信息

J Mol Biol. 2007 Oct 19;373(2):367-81. doi: 10.1016/j.jmb.2007.07.069. Epub 2007 Aug 15.

DOI:10.1016/j.jmb.2007.07.069
PMID:17825319
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2040117/
Abstract

The periplasmic molecular chaperone protein SurA facilitates correct folding and maturation of outer membrane proteins in Gram-negative bacteria. It preferentially binds peptides that have a high fraction of aromatic amino acids. Phage display selections, isothermal titration calorimetry and crystallographic structure determination have been used to elucidate the basis of the binding specificity. The peptide recognition is imparted by the first peptidyl-prolyl isomerase (PPIase) domain of SurA. Crystal structures of complexes between peptides of sequence WEYIPNV and NFTLKFWDIFRK with the first PPIase domain of the Escherichia coli SurA protein at 1.3 A resolution, and of a complex between the dodecapeptide and a SurA fragment lacking the second PPIase domain at 3.4 A resolution, have been solved. SurA binds as a monomer to the heptapeptide in an extended conformation. It binds as a dimer to the dodecapeptide in an alpha-helical conformation, predicated on a substantial structural rearrangement of the SurA protein. In both cases, side-chains of aromatic residues of the peptides contribute a large fraction of the binding interactions. SurA therefore asserts a recognition preference for aromatic amino acids in a variety of sequence configurations by adopting alternative tertiary and quaternary structures to bind peptides in different conformations.

摘要

周质分子伴侣蛋白SurA促进革兰氏阴性菌外膜蛋白的正确折叠和成熟。它优先结合具有高比例芳香族氨基酸的肽段。噬菌体展示筛选、等温滴定量热法和晶体结构测定已被用于阐明结合特异性的基础。肽段识别由SurA的第一个肽基脯氨酰异构酶(PPIase)结构域赋予。已解析了序列为WEYIPNV和NFTLKFWDIFRK的肽段与大肠杆菌SurA蛋白的第一个PPIase结构域形成的复合物的晶体结构,分辨率为1.3 Å,以及十二肽与缺乏第二个PPIase结构域的SurA片段形成的复合物的晶体结构,分辨率为3.4 Å。SurA以单体形式与七肽以伸展构象结合。它以二聚体形式与十二肽以α-螺旋构象结合,这基于SurA蛋白的大量结构重排。在这两种情况下,肽段芳香族残基的侧链在结合相互作用中占很大比例。因此,SurA通过采用不同的三级和四级结构来结合不同构象的肽段,从而对各种序列构型中的芳香族氨基酸表现出识别偏好。

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Binding of phage-display-selected peptides to the periplasmic chaperone protein SurA mimics binding of unfolded outer membrane proteins.噬菌体展示筛选出的肽与周质伴侣蛋白SurA的结合模拟了未折叠外膜蛋白的结合。
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