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一种简化蛋白质折叠字母表的计算方法。

A computational approach to simplifying the protein folding alphabet.

作者信息

Wang J, Wang W

机构信息

National Laboratory of Solid-State Microstructure and Department of Physics, Nanjing University, Nanjing 210093, People's Republic of China.

出版信息

Nat Struct Biol. 1999 Nov;6(11):1033-8. doi: 10.1038/14918.

Abstract

What is the minimal number of residue types required to form a structured protein? This question is important for understanding protein modeling and design. Recently, an experimental finding by Baker and coworkers suggested a five-residue solution to this problem. We were motivated by their results and by the arguments of Wolynes to study reductions of protein representation based on the concept of mismatch between a reduced interaction matrix and the Miyazawa and Jernigan (MJ) matrix. We find several possible simplified schemes from the relationship of minimized mismatch versus the number of residue types (N = approximately 2-20). As a specific case, an optimal reduction with five types of residues has the same form as the simplified palette of Baker and coworkers. Statistical and kinetic features of a number of sequences are tested. Comparison of results from sequences with 20 residue types and their reduced representations indicates that the reduction by mismatch minimization is successful. For example, sequences with five types of residues have good folding ability and kinetic accessibility in model studies.

摘要

形成一个结构化蛋白质所需的最小残基类型数量是多少?这个问题对于理解蛋白质建模和设计很重要。最近,贝克及其同事的一项实验发现为此问题提出了一个五残基的解决方案。他们的结果以及沃利恩斯的观点激发了我们基于简化相互作用矩阵与宫泽和杰尔尼根(MJ)矩阵之间的不匹配概念来研究蛋白质表示的简化。我们从最小化不匹配与残基类型数量(N约为2 - 20)的关系中找到了几种可能的简化方案。作为一个具体例子,具有五种残基类型的最优简化与贝克及其同事的简化调色板具有相同的形式。测试了许多序列的统计和动力学特征。对具有20种残基类型的序列及其简化表示的结果进行比较表明,通过最小化不匹配进行简化是成功的。例如,在模型研究中,具有五种残基类型的序列具有良好的折叠能力和动力学可及性。

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