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β-突处:β-折叠不规则的广泛结构分析。

β-Bulges: extensive structural analyses of β-sheets irregularities.

机构信息

INSERM, U665, DSIMB, F-75739, Paris, France; University of Paris Diderot, Sorbonne Paris Cité, UMR_S 665, F-75739, Paris, France; Institut National de la Transfusion Sanguine (INTS), F-75739, Paris, France; Laboratoire d'Excellence GR-Ex, F-75739, Paris, France.

出版信息

Protein Sci. 2013 Oct;22(10):1366-78. doi: 10.1002/pro.2324. Epub 2013 Sep 14.

DOI:10.1002/pro.2324
PMID:23904395
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3795495/
Abstract

β-Sheets are quite frequent in protein structures and are stabilized by regular main-chain hydrogen bond patterns. Irregularities in β-sheets, named β-bulges, are distorted regions between two consecutive hydrogen bonds. They disrupt the classical alternation of side chain direction and can alter the directionality of β-strands. They are implicated in protein-protein interactions and are introduced to avoid β-strand aggregation. Five different types of β-bulges are defined. Previous studies on β-bulges were performed on a limited number of protein structures or one specific family. These studies evoked a potential conservation during evolution. In this work, we analyze the β-bulge distribution and conservation in terms of local backbone conformations and amino acid composition. Our dataset consists of 66 times more β-bulges than the last systematic study (Chan et al. Protein Science 1993, 2:1574-1590). Novel amino acid preferences are underlined and local structure conformations are highlighted by the use of a structural alphabet. We observed that β-bulges are preferably localized at the N- and C-termini of β-strands, but contrary to the earlier studies, no significant conservation of β-bulges was observed among structural homologues. Displacement of β-bulges along the sequence was also investigated by Molecular Dynamics simulations.

摘要

β-折叠在蛋白质结构中相当常见,由规则的主链氢键模式稳定。β-折叠中的不规则性,称为β-突环,是两个连续氢键之间的扭曲区域。它们破坏了侧链方向的经典交替,并可以改变β-链的方向性。它们参与了蛋白质-蛋白质相互作用,并被引入以避免β-链聚集。定义了五种不同类型的β-突环。以前对β-突环的研究局限于少数蛋白质结构或一个特定的家族。这些研究引发了进化过程中的潜在保守性。在这项工作中,我们根据局部骨架构象和氨基酸组成分析β-突环的分布和保守性。我们的数据集包含的β-突环数量比上一次系统研究(Chan 等人,《蛋白质科学》1993 年,2:1574-1590)多 66 倍。通过使用结构字母表,突出了新的氨基酸偏好,并强调了局部结构构象。我们观察到β-突环优选定位于β-链的 N-和 C-末端,但与早期的研究相反,结构同源物之间没有观察到β-突环的显著保守性。还通过分子动力学模拟研究了β-突环沿序列的位移。

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