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Rrp5p, Noc1p and Noc2p form a protein module which is part of early large ribosomal subunit precursors in S. cerevisiae

机译:Rrp5p,Noc1p和Noc2p形成一个蛋白质模块,该模块是酿酒酵母中早期大型核糖体亚基前体的一部分

摘要

Eukaryotic ribosome biogenesis requires more than 150 auxiliary proteins, which transiently interact with pre-ribosomal particles. Previous studies suggest that several of these biogenesis factors function together as modules. Using a heterologous expression system, we show that the large ribosomal subunit (LSU) biogenesis factor Noc1p of Saccharomyces cerevisiae can simultaneously interact with the LSU biogenesis factor Noc2p and Rrp5p, a factor required for biogenesis of the large and the small ribosomal subunit. Proteome analysis of RNA polymerase-I-associated chromatin and chromatin immunopurification experiments indicated that all members of this protein module and a specific set of LSU biogenesis factors are co-transcriptionally recruited to nascent ribosomal RNA (rRNA) precursors in yeast cells. Further ex vivo analyses showed that all module members predominantly interact with early pre-LSU particles after the initial pre-rRNA processing events have occurred. In yeast strains depleted of Noc1p, Noc2p or Rrp5p, levels of the major LSU pre-rRNAs decreased and the respective other module members were associated with accumulating aberrant rRNA fragments. Therefore, we conclude that the module exhibits several binding interfaces with pre-ribosomes. Taken together, our results suggest a co- and post-transcriptional role of the yeast Rrp5p-Noc1p-Noc2p module in the structural organization of early LSU precursors protecting them from non-productive RNase activity.
机译:真核生物的核糖体生物合成需要150多种辅助蛋白,这些蛋白与核糖体前颗粒瞬时相互作用。先前的研究表明,这些生物发生因子中的几个共同作为模块起作用。使用异源表达系统,我们显示酿酒酵母的大核糖体亚基(LSU)生物发生因子Noc1p可以同时与LSU生物发生因子Noc2p和Rrp5p相互作用,这是大小核糖体亚基的生物发生所必需的因子。 RNA聚合酶I相关染色质的蛋白质组分析和染色质免疫纯化实验表明,该蛋白质模块的所有成员和一组特定的LSU生物发生因子均被转录转录为酵母细胞中新生的核糖体RNA(rRNA)前体。进一步的离体分析表明,在发生最初的pre-rRNA加工事件后,所有模块成员都主要与早期的LSU早期颗粒相互作用。在消耗Noc1p,Noc2p或Rrp5p的酵母菌株中,主要LSU pre-rRNA的水平降低,并且各个其他模块成员与异常rRNA片段的积累有关。因此,我们得出结论,该模块展示了与核糖体前体的几种结合界面。两者合计,我们的结果表明,酵母Rrp5p-Noc1p-Noc2p模块在早期LSU前体的结构组织中具有共转录和转录后作用,可保护它们免受非生产性RNase活性的影响。

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