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Y 型结二聚体和黄素模块将多种氧化还原酶结合在一起。

The dyad of the Y-junction- and a flavin module unites diverse redox enzymes.

机构信息

Aix Marseille Univ, CNRS, BIP, 31 Chemin Joseph Aiguier, 13402 Marseille Cedex 09, France.

Aix Marseille Univ, CNRS, BIP, 31 Chemin Joseph Aiguier, 13402 Marseille Cedex 09, France.

出版信息

Biochim Biophys Acta Bioenerg. 2021 Jun 1;1862(6):148401. doi: 10.1016/j.bbabio.2021.148401. Epub 2021 Mar 6.

DOI:10.1016/j.bbabio.2021.148401
PMID:33684340
Abstract

The concomitant presence of two distinctive polypeptide modules, which we have chosen to denominate as the "Y-junction" and the "flavin" module, is observed in 3D structures of enzymes as functionally diverse as complex I, NAD(P)-dependent [NiFe]-hydrogenases and NAD(P)-dependent formate dehydrogenases. Amino acid sequence conservation furthermore suggests that both modules are also part of NAD(P)-dependent [FeFe]-hydrogenases for which no 3D structure model is available yet. The flavin module harbours the site of interaction with the substrate NAD(P) which exchanges two electrons with a strictly conserved flavin moiety. The Y-junction module typically contains four iron-sulphur centres arranged to form a Y-shaped electron transfer conduit and mediates electron transfer between the flavin module and the catalytic units of the respective enzymes. The Y-junction module represents an electron transfer hub with three potential electron entry/exit sites. The pattern of specific redox centres present both in the Y-junction and the flavin module is correlated to present knowledge of these enzymes' functional properties. We have searched publicly accessible genomes for gene clusters containing both the Y-junction and the flavin module to assemble a comprehensive picture of the diversity of enzymes harbouring this dyad of modules and to reconstruct their phylogenetic relationships. These analyses indicate the presence of the dyad already in the last universal common ancestor and the emergence of complex I's EFG-module out of a subgroup of NAD(P)- dependent formate dehydrogenases.

摘要

在结构上截然不同的两个多肽模块(我们将其分别命名为“Y 型接头”和“黄素”模块)共同存在于多种功能不同的酶中,例如复合物 I、NAD(P)-依赖性[NiFe]-氢化酶和 NAD(P)-依赖性甲酸脱氢酶。氨基酸序列的保守性进一步表明,这两个模块也是尚未建立三维结构模型的 NAD(P)-依赖性[FeFe]-氢化酶的一部分。黄素模块包含与底物 NAD(P)相互作用的部位,该部位与严格保守的黄素部分交换两个电子。Y 型接头模块通常包含四个铁硫中心,排列成 Y 形电子传递管道,并介导黄素模块与各自酶的催化单元之间的电子传递。Y 型接头模块是一个电子传递枢纽,有三个潜在的电子进入/退出位点。Y 型接头和黄素模块中存在的特定氧化还原中心的模式与这些酶功能特性的现有知识相关。我们已经在公开可访问的基因组中搜索了同时包含 Y 型接头和黄素模块的基因簇,以综合描绘具有这两个模块对的酶的多样性,并重建它们的系统发育关系。这些分析表明,该二聚体模块存在于最后的普遍共同祖先中,并且复合物 I 的 EFG 模块是从 NAD(P)-依赖性甲酸脱氢酶的一个亚群中出现的。

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