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来自两种嗜热生物的钼辅因子生物合成蛋白MogA的晶体结构、动力学及功能意义

Crystal structures, dynamics and functional implications of molybdenum-cofactor biosynthesis protein MogA from two thermophilic organisms.

作者信息

Kanaujia Shankar Prasad, Jeyakanthan Jeyaraman, Shinkai Akeo, Kuramitsu Seiki, Yokoyama Shigeyuki, Sekar Kanagaraj

机构信息

Bioinformatics Centre, Centre of Excellence in Structural Biology and Bio-computing, Indian Institute of Science, Bangalore 560 012, India.

出版信息

Acta Crystallogr Sect F Struct Biol Cryst Commun. 2011 Jan 1;67(Pt 1):2-16. doi: 10.1107/S1744309110035037. Epub 2010 Dec 21.

DOI:10.1107/S1744309110035037
PMID:21206014
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3079962/
Abstract

Molybdenum-cofactor (Moco) biosynthesis is an evolutionarily conserved pathway in almost all kingdoms of life, including humans. Two proteins, MogA and MoeA, catalyze the last step of this pathway in bacteria, whereas a single two-domain protein carries out catalysis in eukaryotes. Here, three crystal structures of the Moco-biosynthesis protein MogA from the two thermophilic organisms Thermus thermophilus (TtMogA; 1.64 Å resolution, space group P2(1)) and Aquifex aeolicus (AaMogA; 1.70 Å resolution, space group P2(1) and 1.90 Å resolution, space group P1) have been determined. The functional roles and the residues involved in oligomerization of the protein molecules have been identified based on a comparative analysis of these structures with those of homologous proteins. Furthermore, functional roles have been proposed for the N- and C-terminal residues. In addition, a possible protein-protein complex of MogA and MoeA has been proposed and the residues involved in protein-protein interactions are discussed. Several invariant water molecules and those present at the subunit interfaces have been identified and their possible structural and/or functional roles are described in brief. In addition, molecular-dynamics and docking studies with several small molecules (including the substrate and the product) have been carried out in order to estimate their binding affinities towards AaMogA and TtMogA. The results obtained are further compared with those obtained for homologous eukaryotic proteins.

摘要

钼辅因子(Moco)生物合成是几乎所有生命王国(包括人类)中一条进化上保守的途径。两种蛋白质,MogA和MoeA,催化细菌中该途径的最后一步,而在真核生物中,一种单一的双结构域蛋白质进行催化。在这里,已经确定了来自嗜热栖热菌(TtMogA;分辨率1.64 Å,空间群P2(1))和嗜热栖热放线菌(AaMogA;分辨率1.70 Å,空间群P2(1)和分辨率1.90 Å,空间群P1)这两种嗜热生物的Moco生物合成蛋白MogA的三种晶体结构。基于这些结构与同源蛋白结构的比较分析,确定了蛋白质分子寡聚化所涉及的功能作用和残基。此外,还对N端和C端残基的功能作用提出了建议。此外,还提出了MogA和MoeA可能的蛋白质 - 蛋白质复合物,并讨论了参与蛋白质 - 蛋白质相互作用的残基。已经确定了几个不变水分子以及存在于亚基界面的水分子,并简要描述了它们可能的结构和/或功能作用。此外,还进行了与几种小分子(包括底物和产物)的分子动力学和对接研究,以估计它们对AaMogA和TtMogA的结合亲和力。将所得结果与同源真核蛋白的结果进一步进行比较。