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字母表大小和可折叠性要求对蛋白质结构可设计性的影响。

Effect of alphabet size and foldability requirements on protein structure designability.

作者信息

Buchler N E, Goldstein R A

机构信息

Biophysics Research Division, Ann Arbor, Michigan, USA.

出版信息

Proteins. 1999 Jan 1;34(1):113-24.

Abstract

A number of investigators have addressed the issue of why certain protein structures are especially common by considering structure designability, defined as the number of sequences that would successfully fold into any particular native structure. One such approach, based on foldability, suggested that structures could be classified according to their maximum possible foldability and that this optimal foldability would be highly correlated with structure designability. Other approaches have focused on computing the designability of lattice proteins written with reduced two-letter amino acid alphabets. These different approaches suggested contrasting characteristics of the most designable structures. This report compares the designability of lattice proteins over a wide range of amino acid alphabets and foldability requirements. While all alphabets have a wide distribution of protein designabilities, the form of the distribution depends on how protein "viability" is defined. Furthermore, under increasing foldability requirements, the change in designabilities for all alphabets are in good agreement with the previous conclusions of the foldability approach. Most importantly, it was noticed that those structures that were highly designable for the two-letter amino acid alphabets are not especially designable with higher-letter alphabets.

摘要

一些研究人员通过考虑结构可设计性来探讨为何某些蛋白质结构特别常见,结构可设计性定义为能够成功折叠成任何特定天然结构的序列数量。一种基于可折叠性的方法表明,结构可以根据其最大可能的可折叠性进行分类,并且这种最佳可折叠性与结构可设计性高度相关。其他方法则专注于计算用简化的双字母氨基酸字母表编写的晶格蛋白质的可设计性。这些不同的方法表明了最具可设计性的结构的不同特征。本报告比较了在广泛的氨基酸字母表和可折叠性要求范围内晶格蛋白质的可设计性。虽然所有字母表的蛋白质可设计性都有广泛的分布,但分布形式取决于蛋白质“生存能力”的定义方式。此外,在不断增加的可折叠性要求下,所有字母表的可设计性变化与可折叠性方法的先前结论高度一致。最重要的是,人们注意到那些对于双字母氨基酸字母表具有高度可设计性的结构,对于更高字母表而言并非特别具有可设计性。

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