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蛋白质四级结构的分析与预测

Analysis and prediction of protein quaternary structure.

作者信息

Poupon Anne, Janin Joel

机构信息

Yeast Structural Genomics, IBBMC UMR 8619 CNRS, Université Paris-Sud, Orsay, France.

出版信息

Methods Mol Biol. 2010;609:349-64. doi: 10.1007/978-1-60327-241-4_20.

Abstract

The quaternary structure (QS) of a protein is determined by measuring its molecular weight in solution. The data have to be extracted from the literature, and they may be missing even for proteins that have a crystal structure reported in the Protein Data Bank (PDB). The PDB and other databases derived from it report QS information that either was obtained from the depositors or is based on an analysis of the contacts between polypeptide chains in the crystal, and this frequently differs from the QS determined in solution.The QS of a protein can be predicted from its sequence using either homology or threading methods. However, a majority of the proteins with less than 30% sequence identity have different QSs. A model of the QS can also be derived by docking the subunits when their 3D structure is independently known, but the model is likely to be incorrect if large conformation changes take place when the oligomer assembles.

摘要

蛋白质的四级结构(QS)是通过测量其在溶液中的分子量来确定的。数据必须从文献中提取,甚至对于那些在蛋白质数据库(PDB)中有晶体结构报道的蛋白质,数据也可能缺失。PDB以及从中衍生的其他数据库报告的QS信息,要么是从 depositors 那里获得的,要么是基于对晶体中多肽链之间接触的分析,而这常常与在溶液中确定的QS不同。蛋白质的QS可以使用同源性或穿线法从其序列中预测。然而,大多数序列同一性低于30%的蛋白质具有不同的QS。当亚基的三维结构已知时,也可以通过对接亚基来推导QS模型,但如果寡聚体组装时发生大的构象变化,该模型可能是不正确的。

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