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The Prokaryotic Antecedents of the Ubiquitin-Signaling System and the Early Evolution of Ubiquitin-Like β-Grasp Domains

机译:泛素-信号系统的原核前体和泛素样β-抓域的早期进化

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摘要

A systematic analysis of prokaryotic ubiquitin-related beta-grasp fold proteins provides new insights into the Ubiquitin family functional history. BACKGROUND. Ubiquitin (Ub)-mediated signaling is one of the hallmarks of all eukaryotes. Prokaryotic homologs of Ub (ThiS and MoaD) and E1 ligases have been studied in relation to sulfur incorporation reactions in thiamine and molybdenum/tungsten cofactor biosynthesis. However, there is no evidence for entire protein modification systems with Ub-like proteins and deconjugation by deubiquitinating enzymes in prokaryotes. Hence, the evolutionary assembly of the eukaryotic Ub-signaling apparatus remains unclear. RESULTS. We systematically analyzed prokaryotic Ub-related β-grasp fold proteins using sensitive sequence profile searches and structural analysis. Consequently, we identified novel Ub-related proteins beyond the characterized ThiS, MoaD, TGS, and YukD domains. To understand their functional associations, we sought and recovered several conserved gene neighborhoods and domain architectures. These included novel associations involving diverse sulfur metabolism proteins, siderophore biosynthesis and the gene encoding the transfer mRNA binding protein SmpB, as well as domain fusions between Ub-like domains and PIN-domain related RNAses. Most strikingly, we found conserved gene neighborhoods in phylogenetically diverse bacteria combining genes for JAB domains (the primary de-ubiquitinating isopeptidases of the proteasomal complex), along with E1-like adenylating enzymes and different Ub-related proteins. Further sequence analysis of other conserved genes in these neighborhoods revealed several Ub-conjugating enzyme/E2-ligase related proteins. Genes for an Ub-like protein and a JAB domain peptidase were also found in the tail assembly gene cluster of certain caudate bacteriophages. CONCLUSION. These observations imply that members of the Ub family had already formed strong functional associations with E1-like proteins, UBC/E2-related proteins, and JAB peptidases in the bacteria. Several of these Ub-like proteins and the associated protein families are likely to function together in signaling systems just as in eukaryotes.
机译:对原核遍在蛋白相关的β-抓握折叠蛋白的系统分析为泛素家族的功能史提供了新的见解。背景。泛素(Ubquitin)(Ub)介导的信号传导是所有真核生物的标志之一。已经研究了Ub(ThiS和MoaD)和E1连接酶的原核同源物,与硫胺素中的硫掺入反应和钼/钨辅助因子的生物合成有关。但是,没有证据表明完整的蛋白质修饰系统具有类似Ub的蛋白质,并且通过原核生物中的去泛素化酶进行解偶联。因此,真核Ub信号装置的进化组装仍不清楚。结果。我们使用灵敏的序列图谱搜索和结构分析系统地分析了与原核Ub相关的β-抓握折叠蛋白。因此,我们鉴定了特征性的ThiS,MoaD,TGS和YukD域以外的新型Ub相关蛋白。为了了解它们的功能关联,我们寻求并恢复了几个保守的基因邻域和域结构。这些包括涉及各种硫代谢蛋白,铁载体的生物合成和编码转移mRNA结合蛋白SmpB的基因以及Ub样结构域和PIN结构域相关的RNA酶之间的结构域融合的新型关联。最令人惊讶的是,我们在系统发育多样的细菌中发现了保守的基因邻域,这些细菌结合了JAB域的基因(蛋白酶体复合物的主要去泛素化异肽酶),以及类似E1的腺苷酸化酶和不同的Ub相关蛋白。在这些邻域中其他保守基因的进一步序列分析揭示了几种与Ub结合的酶/ E2-连接酶相关的蛋白质。在某些尾状噬菌体的尾部装配基因簇中也发现了Ub样蛋白和JAB结构域肽酶的基因。结论。这些观察结果表明,Ub家族成员已经与细菌中的E1样蛋白,UBC / E2相关蛋白和JAB肽酶形成了强大的功能关联。这些Ub样蛋白中的几种以及相关的蛋白家族可能像真核生物一样在信号系统中一起发挥作用。

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