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基于已知三级结构、稳定性概况和序列保守性预测酶中的催化残基。

Prediction of catalytic residues in enzymes based on known tertiary structure, stability profile, and sequence conservation.

作者信息

Ota Motonori, Kinoshita Kengo, Nishikawa Ken

机构信息

National Institute of Genetics, Yata, Mishima, 411-8540, Shizuoka, Japan.

出版信息

J Mol Biol. 2003 Apr 11;327(5):1053-64. doi: 10.1016/s0022-2836(03)00207-9.

DOI:10.1016/s0022-2836(03)00207-9
PMID:12662930
Abstract

The catalytic or functionally important residues of a protein are known to exist in evolutionarily constrained regions. However, the patterns of residue conservation alone are sometimes not very informative, depending on the homologous sequences available for a given query protein. Here, we present an integrated method to locate the catalytic residues in an enzyme from its sequence and structure. Mutations of functional residues usually decrease the activity, but concurrently often increase stability. Also, catalytic residues tend to occupy partially buried sites in holes or clefts on the molecular surface. After confirming these general tendencies by carrying out statistical analyses on 49 representative enzymes, these data together with amino acid conservation were evaluated. This novel method exhibited better sensitivity in the prediction accuracy than traditional methods that consider only the residue conservation. We applied it to some so-called "hypothetical" proteins, with known structures but undefined functions. The relationships among the catalytic, conserved, and destabilizing residues in enzymatic proteins are discussed.

摘要

已知蛋白质的催化或功能重要残基存在于进化受限区域。然而,仅残基保守模式有时信息并不丰富,这取决于给定查询蛋白可获得的同源序列。在此,我们提出一种综合方法,从酶的序列和结构中定位催化残基。功能残基的突变通常会降低活性,但同时往往会增加稳定性。此外,催化残基倾向于占据分子表面孔洞或裂缝中部分埋藏的位点。通过对49种代表性酶进行统计分析证实这些一般趋势后,将这些数据与氨基酸保守性一起进行评估。这种新方法在预测准确性方面表现出比仅考虑残基保守性的传统方法更高的灵敏度。我们将其应用于一些所谓的“假设”蛋白,这些蛋白具有已知结构但功能未明确。文中讨论了酶蛋白中催化、保守和去稳定化残基之间的关系。

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