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首页> 外文期刊>Yeast >Yeast RNA viruses as indicators of exosome activity: human exosome hCsl4p participates in RNA degradation in Saccharomyces cerevisiae'
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Yeast RNA viruses as indicators of exosome activity: human exosome hCsl4p participates in RNA degradation in Saccharomyces cerevisiae'

机译:酵母RNA病毒作为外泌体活性的指标:人类外泌体hCsl4p参与酿酒酵母中的RNA降解'

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摘要

The exosome is an evolutionarily conserved 10-mer complex involved in RNA metabolism, located in both the nucleus and the cytoplasm. The cytoplasmic exosome plays an important role in mRNA turnover through its 3'?5' exonucleolytic activity. The superkiller (SKI) phenotype of yeast was originally identified as an increase of killer toxin production due to elevated levels of the L-A double-stranded RNA (dsRNA) Totivirus and its satellite toxin-encoding M dsRNA. Most SKI genes were later shown to be either components of the exosome or modulators of its activity. Variations in the amount of Totivirus are, thus, good indicators of yeast exosome activity, and can be used to analyse its components. Furthermore, if exosome proteins of higher eukaryotes were functional in S. cerevisiae, these viruses would provide a simple tool to analyse their function. In this work, we have found that hCSL4, the human orthologue of SKI4 in the yeast exosome, rescues the null phenotype of the deletion mutant. hCsl4p shares with Ski4p conserved S1 RNA-binding domains, but lacks the N-terminal third of Ski4p. Nevertheless, it interacts with the Dis3p exonuclease of yeast exosome, and partially complements the superkiller phenotype of ski4-1 mutation. The elimination of the N-terminal third of Ski4p does not affect its activity, indicating that it is dispensable for RNA degradation. We have also identified the point mutation G152E in hCSL4, equivalent to the ski4-1 mutation G253E, which impairs the activity of the protein, thus validating our approach of using yeast RNA virus to analyse the exosome of higher eukaryotes. Copyright (c) 2011 John Wiley & Sons, Ltd.
机译:外泌体是一种进化保守的10聚体复合物,参与RNA代谢,位于细胞核和细胞质中。胞质外泌体通过其3'→5'外切核酸活性在mRNA更新中起重要作用。酵母的超级杀手(SKI)表型最初被确定为杀伤性毒素产生的增加,这是由于L-A双链RNA(dsRNA)牛痘病毒及其卫星编码M dsRNA的水平升高所致。后来,大多数SKI基因被证明是外泌体的组成部分或其活性的调节剂。因此,轮状病毒数量的变化是酵母外泌体活性的良好指标,可用于分析其成分。此外,如果高级真核生物的外泌体蛋白在酿酒酵母中起作用,则这些病毒将提供分析其功能的简单工具。在这项工作中,我们发现hCSL4,即酵母外泌体中SKI4的人类直系同源物,可以挽救缺失突变体的无效表型。 hCsl4p与Ski4p保守的S1 RNA结合域共享,但缺少Ski4p的N末端三分之一。然而,它与酵母外泌体的Dis3p外切核酸酶相互作用,并部分互补ski4-1突变的超级杀手表型。 Ski4p的N末端三分之一的消除不影响其活性,表明它可用于RNA降解。我们还鉴定了hCSL4中的点突变G152E,等同于ski4-1突变G253E,这削弱了蛋白质的活性,从而验证了我们使用酵母RNA病毒分析高等真核生物外泌体的方法。版权所有(c)2011 John Wiley&Sons,Ltd.

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