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钼辅因子生物合成中的共享功能和兼职蛋白

Shared function and moonlighting proteins in molybdenum cofactor biosynthesis.

作者信息

Leimkühler Silke

机构信息

.

出版信息

Biol Chem. 2017 Aug 28;398(9):1009-1026. doi: 10.1515/hsz-2017-0110.

Abstract

The biosynthesis of the molybdenum cofactor (Moco) is a highly conserved pathway in bacteria, archaea and eukaryotes. The molybdenum atom in Moco-containing enzymes is coordinated to the dithiolene group of a tricyclic pyranopterin monophosphate cofactor. The biosynthesis of Moco can be divided into three conserved steps, with a fourth present only in bacteria and archaea: (1) formation of cyclic pyranopterin monophosphate, (2) formation of molybdopterin (MPT), (3) insertion of molybdenum into MPT to form Mo-MPT, and (4) additional modification of Mo-MPT in bacteria with the attachment of a GMP or CMP nucleotide, forming the dinucleotide variants of Moco. While the proteins involved in the catalytic reaction of each step of Moco biosynthesis are highly conserved among the Phyla, a surprising link to other cellular pathways has been identified by recent discoveries. In particular, the pathways for FeS cluster assembly and thio-modifications of tRNA are connected to Moco biosynthesis by sharing the same protein components. Further, proteins involved in Moco biosynthesis are not only shared with other pathways, but additionally have moonlighting roles. This review gives an overview of Moco biosynthesis in bacteria and humans and highlights the shared function and moonlighting roles of the participating proteins.

摘要

钼辅因子(Moco)的生物合成在细菌、古菌和真核生物中是一条高度保守的途径。含Moco的酶中的钼原子与三环吡喃蝶呤单磷酸辅因子的二硫烯基团配位。Moco的生物合成可分为三个保守步骤,第四步仅存在于细菌和古菌中:(1)环状吡喃蝶呤单磷酸的形成,(2)钼蝶呤(MPT)的形成,(3)钼插入MPT形成Mo-MPT,以及(4)细菌中Mo-MPT通过连接GMP或CMP核苷酸进行额外修饰,形成Moco的二核苷酸变体。虽然参与Moco生物合成各步骤催化反应的蛋白质在各门类中高度保守,但最近的发现揭示了与其他细胞途径的惊人联系。特别是,FeS簇组装途径和tRNA的硫修饰通过共享相同的蛋白质成分与Moco生物合成相连。此外,参与Moco生物合成的蛋白质不仅与其他途径共享,而且还具有兼职功能。本综述概述了细菌和人类中Moco的生物合成,并强调了参与蛋白质的共享功能和兼职作用。

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