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原核生物中硫胺素生物合成的比较基因组学。新基因与调控机制。

Comparative genomics of thiamin biosynthesis in procaryotes. New genes and regulatory mechanisms.

作者信息

Rodionov Dmitry A, Vitreschak Alexey G, Mironov Andrey A, Gelfand Mikhail S

机构信息

State Scientific Center GosNIIGenetika, Moscow 113545, Russia.

出版信息

J Biol Chem. 2002 Dec 13;277(50):48949-59. doi: 10.1074/jbc.M208965200. Epub 2002 Oct 9.

Abstract

Vitamin B(1) in its active form thiamin pyrophosphate is an essential coenzyme that is synthesized by coupling of pyrimidine (hydroxymethylpyrimidine; HMP) and thiazole (hydroxyethylthiazole) moieties in bacteria. Using comparative analysis of genes, operons, and regulatory elements, we describe the thiamin biosynthetic pathway in available bacterial genomes. The previously detected thiamin-regulatory element, thi box (Miranda-Rios, J., Navarro, M., and Soberon, M. (2001) Proc. Natl. Acad. Sci. U. S. A. 98, 9736-9741), was extended, resulting in a new, highly conserved RNA secondary structure, the THI element, which is widely distributed in eubacteria and also occurs in some archaea. Search for THI elements and analysis of operon structures identified a large number of new candidate thiamin-regulated genes, mostly transporters, in various prokaryotic organisms. In particular, we assign the thiamin transporter function to yuaJ in the Bacillus/Clostridium group and the HMP transporter function to an ABC transporter thiXYZ in some proteobacteria and firmicutes. By analogy to the model of regulation of the riboflavin biosynthesis, we suggest thiamin-mediated regulation based on formation of alternative RNA structures involving the THI element. Either transcriptional or translational attenuation mechanism may operate in different taxonomic groups, dependent on the existence of putative hairpins that either act as transcriptional terminators or sequester translation initiation sites. Based on analysis of co-occurrence of the thiamin biosynthetic genes in complete genomes, we predict that eubacteria, archaea, and eukaryota have different pathways for the HMP and hydroxyethylthiazole biosynthesis.

摘要

维生素B1的活性形式焦磷酸硫胺素是一种必需辅酶,由细菌中的嘧啶(羟甲基嘧啶;HMP)和噻唑(羟乙基噻唑)部分偶联合成。通过对基因、操纵子和调控元件的比较分析,我们描述了现有细菌基因组中的硫胺素生物合成途径。先前检测到的硫胺素调控元件thi框(米兰达-里奥斯,J.,纳瓦罗,M.,和索贝龙,M.(2001年)美国国家科学院院刊98,9736-9741)得到扩展,形成了一种新的、高度保守的RNA二级结构,即THI元件,它广泛分布于真细菌中,也存在于一些古细菌中。对THI元件的搜索和操纵子结构分析在各种原核生物中鉴定出大量新的候选硫胺素调控基因,其中大多数是转运蛋白。特别是,我们将硫胺素转运蛋白功能赋予芽孢杆菌/梭菌属中的yuaJ,将HMP转运蛋白功能赋予一些变形菌门和厚壁菌门中的ABC转运蛋白thiXYZ。类似于核黄素生物合成的调控模型,我们提出基于涉及THI元件的替代RNA结构形成的硫胺素介导的调控。转录或翻译衰减机制可能在不同的分类群中起作用,这取决于是否存在作为转录终止子或隔离翻译起始位点的假定发夹结构。基于对完整基因组中硫胺素生物合成基因共现情况的分析,我们预测真细菌、古细菌和真核生物在HMP和羟乙基噻唑生物合成方面具有不同的途径。

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