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利用局部结构描述符分析蛋白质结构和蛋白质复合物中的残基间接触。

Taking advantage of local structure descriptors to analyze interresidue contacts in protein structures and protein complexes.

作者信息

Martin Juliette, Regad Leslie, Etchebest Catherine, Camproux Anne-Claude

机构信息

INRA UR1077, Unité Mathématique Informatique et Génome, F-78350 Jouy-en-Josas, France.

出版信息

Proteins. 2008 Nov 15;73(3):672-89. doi: 10.1002/prot.22091.

Abstract

Interresidue protein contacts in proteins structures and at protein-protein interface are classically described by the amino acid types of interacting residues and the local structural context of the contact, if any, is described using secondary structures. In this study, we present an alternate analysis of interresidue contact using local structures defined by the structural alphabet introduced by Camproux et al. This structural alphabet allows to describe a 3D structure as a sequence of prototype fragments called structural letters, of 27 different types. Each residue can then be assigned to a particular local structure, even in loop regions. The analysis of interresidue contacts within protein structures defined using Voronoï tessellations reveals that pairwise contact specificity is greater in terms of structural letters than amino acids. Using a simple heuristic based on specificity score comparison, we find that 74% of the long-range contacts within protein structures are better described using structural letters than amino acid types. The investigation is extended to a set of protein-protein complexes, showing that the similar global rules apply as for intraprotein contacts, with 64% of the interprotein contacts best described by local structures. We then present an evaluation of pairing functions integrating structural letters to decoy scoring and show that some complexes could benefit from the use of structural letter-based pairing functions.

摘要

蛋白质结构中以及蛋白质 - 蛋白质界面处的残基间蛋白质接触,传统上是通过相互作用残基的氨基酸类型来描述的,并且如果有接触的局部结构背景,则使用二级结构来描述。在本研究中,我们使用由坎普鲁克斯等人引入的结构字母表所定义的局部结构,对残基间接触进行了另一种分析。这种结构字母表允许将三维结构描述为一系列称为结构字母的原型片段序列,共有27种不同类型。然后,即使在环区,每个残基也可以被指定到一个特定的局部结构。使用基于沃罗诺伊镶嵌定义的蛋白质结构内残基间接触的分析表明,就结构字母而言,成对接触特异性比氨基酸更高。使用基于特异性得分比较的简单启发式方法,我们发现蛋白质结构内74%的长程接触用结构字母比用氨基酸类型能更好地描述。该研究扩展到一组蛋白质 - 蛋白质复合物,表明与蛋白质内接触适用相似的全局规则,64%的蛋白质间接触用局部结构能得到最佳描述。然后,我们对将结构字母整合到诱饵评分中的配对函数进行了评估,并表明一些复合物可能受益于使用基于结构字母的配对函数。

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