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Solution structure of Urm1 and its implications for the origin of protein modifiers

机译:Urm1的溶液结构及其对蛋白质修饰物来源的影响

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Protein modifiers are involved in diverse biological processes and regulate the activity or function of target proteins by covalently conjugating to them. Although ubiquitin and a number of ubiquitin-like protein modifiers (Ubls) in eukaryotes have been identified, no protein modifier has been found in prokaryotes; thus, their evolutionary origin remains a puzzle. To infer the evolutionary relationships between the protein modifiers and sulfur carrier proteins, we solved the solution NMR structure of the Urm1 (ubiquitin-related modifier-1) protein from Saccharomyces cerevisiae. Both structural comparison and phylogenetic analysis of the ubiquitin superfamily, with emphasis on the Urm1 family, indicate that Urm1 is the unique "molecular fossil" that has the most conserved structural and sequence features of the common ancestor of the entire superfamily. The similarities of 3D structure and hydrophobic and electrostatic surface features between Urm1 and MoaD (molybdopterin synthase small subunit) suggest that they may interact with partners in a similar manner, and similarities between Urml-Uba4 and MoaD-MoeB establish an evolutionary link between ATP-dependent protein conjugation in eukaryotes and ATP-dependent cofactor sulfuration.
机译:蛋白质修饰剂参与多种生物过程,并通过与目标蛋白共价结合来调节其活性或功能。尽管在真核生物中已鉴定出泛素和许多泛素样蛋白修饰剂(Ubls),但在原核生物中未发现任何蛋白修饰剂。因此,它们的进化起源仍然是一个难题。为了推断蛋白质修饰剂和硫载体蛋白之间的进化关系,我们解决了酿酒酵母中Urm1(泛素相关修饰剂-1)蛋白的溶液NMR结构。泛素超家族的结构比较和系统发育分析(特别是Urm1家族)均表明,Urm1是独特的“分子化石”,具有整个超家族共同祖先最保守的结构和序列特征。 Urm1和MoaD(钼蝶呤合酶小亚基)之间的3D结构以及疏水和静电表面特征的相似性表明,它们可能以相似的方式与伴侣相互作用,并且Urml-Uba4和MoaD-MoeB之间的相似性在ATP-之间建立了进化联系真核生物中的蛋白质依赖性结合和ATP依赖性辅因子硫酸化。

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