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辅因子依赖性磷酸甘油酸变位酶的磷酸蛋白磷酸酶同源物中意外的催化位点变异。

Unexpected catalytic site variation in phosphoprotein phosphatase homologues of cofactor-dependent phosphoglycerate mutase.

作者信息

Rigden Daniel J

机构信息

Embrapa Genetic Resources and Biotechnology, Cenargen/Embrapa, Parque Estação Biológica, Final W3 Norte, 70770-900 Brasília, Brazil.

出版信息

FEBS Lett. 2003 Feb 11;536(1-3):77-84. doi: 10.1016/s0014-5793(03)00014-0.

Abstract

The cofactor-dependent phosphoglycerate mutase (dPGM) superfamily contains, besides mutases, a variety of phosphatases, both broadly and narrowly substrate-specific. Distant dPGM homologues, conspicuously abundant in microbial genomes, represent a challenge for functional annotation based on sequence comparison alone. Here we carry out sequence analysis and molecular modelling of two families of bacterial dPGM homologues, one the SixA phosphoprotein phosphatases, the other containing various proteins of no known molecular function. The models show how SixA proteins have adapted to phosphoprotein substrate and suggest that the second family may also encode phosphoprotein phosphatases. Unexpected variation in catalytic and substrate-binding residues is observed in the models.

摘要

依赖辅因子的磷酸甘油酸变位酶(dPGM)超家族除了变位酶之外,还包含多种磷酸酶,底物特异性既有宽泛的也有狭窄的。在微生物基因组中显著丰富的远缘dPGM同源物,对仅基于序列比较的功能注释构成了挑战。在此,我们对两类细菌dPGM同源物进行了序列分析和分子建模,一类是SixA磷蛋白磷酸酶,另一类包含各种分子功能未知的蛋白质。模型显示了SixA蛋白如何适应磷蛋白底物,并表明第二类蛋白也可能编码磷蛋白磷酸酶。在模型中观察到催化和底物结合残基存在意外变异。

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