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The Rtr1p CTD phosphatase autoregulates its mRNA through a degradation pathway involving the REX exonucleases

机译:Rtr1p CTD磷酸酶通过涉及REX核酸外切酶的降解途径自动调节其mRNA

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Rtr1p is a phosphatase that impacts gene expression by modulating the phosphorylation status of the C-terminal domain of the large subunit of RNA polymerase II. Here, we show that Rtr1p is a component of a novel mRNA degradation pathway that promotes its autoregulation through turnover of its own mRNA. We show that the 3'UTR of the RTR1 mRNA contains a cis element that destabilizes this mRNA. RTR1 mRNA turnover is achieved through binding of Rtr1p to the RTR1 mRNP in a manner that is dependent on this cis element. Genetic evidence shows that Rtr1p-mediated decay of the RTR1 mRNA involves the 5'-3' DExD/H-box RNA helicase Dhh1p and the 3'-5' exonucleases Rex2p and Rex3p. Rtr1p and Rex3p are found associated with Dhh1p, suggesting a model for recruiting the REX exonucleases to the RTR1 mRNA for degradation. Rtr1p-mediated decay potentially impacts additional transcripts, including the unspliced BMH2 pre-mRNA. We propose that Rtr1p may imprint its RNA targets cotranscriptionally and determine their downstream degradation mechanism by directing these transcripts to a novel turnover pathway that involves Rtr1p, Dhh1p, and the REX family of exonucleases.
机译:Rtr1p是一种磷酸酶,通过调节RNA聚合酶II大亚基的C端结构域的磷酸化状态来影响基因表达。在这里,我们显示Rtr1p是新型的mRNA降解途径的组成部分,该途径通过自身mRNA的更新来促进其自动调节。我们显示RTR1 mRNA的3'UTR包含使该mRNA不稳定的顺式元件。 RTR1 mRNA的更新是通过Rtr1p与RTR1 mRNP的结合而实现的,该方式取决于该顺式元件。遗传证据表明,Rtr1p介导的RTR1 mRNA降解涉及5'-3'DExD / H-box RNA解旋酶Dhh1p和3'-5'外切核酸酶Rex2p和Rex3p。发现Rtr1p和Rex3p与Dhh1p相关,这表明了将REX外切酶募集到RTR1 mRNA进行降解的模型。 Rtr1p介导的衰变可能影响其他转录本,包括未剪接的BMH2 pre-mRNA。我们建议Rtr1p可能会共转录其RNA靶标并通过将这些转录本引导至涉及Rtr1p,Dhh1p和REX核酸外切酶家族的新型更新途径来确定其下游降解机制。

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