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无关蛋白质三级结构中序列相似五肽的分析。蛋白质折叠策略及定点诱变指南。

Analysis of sequence-similar pentapeptides in unrelated protein tertiary structures. Strategies for protein folding and a guide for site-directed mutagenesis.

作者信息

Argos P

机构信息

European Molecular Biology Laboratory, Heidelberg, Federal Republic of Germany.

出版信息

J Mol Biol. 1987 Sep 20;197(2):331-48. doi: 10.1016/0022-2836(87)90127-6.

Abstract

From the most recent Brookhaven Protein Co-ordinate Databank, 229 sequence-identical pentapeptide pairs, each found in two unrelated protein structures, were collected; 9115 such pairs differing in only one residue were also gathered. For both samples the main-chain fold was conserved about 20% of the time, despite the different atomic environments presented by the unrelated protein architectures. An analysis of the substituted residues as well as the composition of the sequence-similar pentapeptides allowed several suggestions regarding protein folding mechanisms. An examination of the most frequently observed residue substitutions and their correlation with structural changes in the oligopeptide pairs yields a possible guide for site-directed mutagenesis experiments, especially when no tertiary structural information is at hand.

摘要

从最新的布鲁克海文蛋白质坐标数据库中,收集了229对序列相同的五肽对,每对都存在于两个不相关的蛋白质结构中;还收集了9115对仅一个残基不同的此类五肽对。对于这两个样本,尽管不相关的蛋白质结构呈现出不同的原子环境,但主链折叠在约20%的时间内是保守的。对取代残基以及序列相似的五肽组成进行分析,得出了一些关于蛋白质折叠机制的建议。检查最常观察到的残基取代及其与寡肽对结构变化的相关性,可为定点诱变实验提供可能的指导,尤其是在没有三级结构信息的情况下。

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