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利用氨基酸共进化分析来理解蛋白质的结构和功能。

Using analyses of amino Acid coevolution to understand protein structure and function.

作者信息

Ashenberg Orr, Laub Michael T

机构信息

Department of Biology, Massachusetts Institute of Technology, Cambridge, Massachusetts, USA.

出版信息

Methods Enzymol. 2013;523:191-212. doi: 10.1016/B978-0-12-394292-0.00009-6.

Abstract

Determining which residues of a protein contribute to a specific function is a difficult problem. Analyses of amino acid covariation within a protein family can serve as a useful guide by identifying residues that are functionally coupled. Covariation analyses have been successfully used on several different protein families to identify residues that work together to promote folding, enable protein-protein interactions, or contribute to an enzymatic activity. Covariation is a statistical signal that can be measured in a multiple sequence alignment of homologous proteins. As sequence databases have expanded dramatically, covariation analyses have become easier and more powerful. In this chapter, we describe how functional covariation arises during the evolution of proteins and how this signal can be distinguished from various background signals. We discuss the basic methodology for performing amino acid covariation analysis, using bacterial two-component signal transduction proteins as an example. We provide practical suggestions for each step of the process including assembly of protein sequences, construction of a multiple sequence alignment, measurement of covariation, and analysis of results.

摘要

确定蛋白质的哪些残基对特定功能有贡献是一个难题。通过识别功能耦合的残基,对蛋白质家族内氨基酸共变的分析可以作为一个有用的指导。共变分析已成功应用于几个不同的蛋白质家族,以识别共同作用促进折叠、实现蛋白质-蛋白质相互作用或对酶活性有贡献的残基。共变是一种可以在同源蛋白质的多序列比对中测量的统计信号。随着序列数据库的急剧扩展,共变分析变得更加容易和强大。在本章中,我们描述了功能共变在蛋白质进化过程中是如何产生的,以及如何将这个信号与各种背景信号区分开来。我们以细菌双组分信号转导蛋白为例,讨论进行氨基酸共变分析的基本方法。我们为该过程的每个步骤提供实用建议,包括蛋白质序列的组装、多序列比对的构建、共变的测量以及结果分析。

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