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Shared Sulfur Mobilization Routes for tRNA Thiolation and Molybdenum Cofactor Biosynthesis in Prokaryotes and Eukaryotes

机译:原核生物和真核生物中tRNA硫醇化和钼辅因子生物合成的共有硫动员途径。

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摘要

Modifications of transfer RNA (tRNA) have been shown to play critical roles in the biogenesis, metabolism, structural stability and function of RNA molecules, and the specific modifications of nucleobases with sulfur atoms in tRNA are present in pro- and eukaryotes. Here, especially the thiomodifications xm5s2U at the wobble position 34 in tRNAs for Lys, Gln and Glu, were suggested to have an important role during the translation process by ensuring accurate deciphering of the genetic code and by stabilization of the tRNA structure. The trafficking and delivery of sulfur nucleosides is a complex process carried out by sulfur relay systems involving numerous proteins, which not only deliver sulfur to the specific tRNAs but also to other sulfur-containing molecules including iron–sulfur clusters, thiamin, biotin, lipoic acid and molybdopterin (MPT). Among the biosynthesis of these sulfur-containing molecules, the biosynthesis of the molybdenum cofactor (Moco) and the synthesis of thio-modified tRNAs in particular show a surprising link by sharing protein components for sulfur mobilization in pro- and eukaryotes.
机译:已显示转移RNA(tRNA)的修饰在RNA分子的生物发生,代谢,结构稳定性和功能中起关键作用,并且原核生物和真核生物中都存在tRNA中带有硫原子的核碱基的特定修饰。在这里,尤其是在Lys,Gln和Glu的tRNA的摆动位置34处,硫代修饰xm 5 s 2 U特别建议在翻译过程中起重要作用,确保遗传密码的准确破译,以及通过稳定tRNA结构。硫原子核苷的运输和传递是一个复杂的过程,由涉及多种蛋白质的硫中继系统完成,不仅将硫传递到特定的tRNA,而且还传递到其他含硫分子,包括铁硫簇,硫胺素,生物素,硫辛酸和钼蝶呤(MPT)。在这些含硫分子的生物合成中,钼辅因子(Moco)的生物合成和硫修饰的tRNA的合成特别显示出令人惊讶的联系,它们共享原核生物和真核生物中硫移动的蛋白质成分。

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