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首页> 外文期刊>Nucleic Acids Research >Deletion of the nuclear exosome component RRP6 leads to continued accumulation of the histone mRNA HTB1 in S-phase of the cell cycle in Saccharomyces cerevisiae
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Deletion of the nuclear exosome component RRP6 leads to continued accumulation of the histone mRNA HTB1 in S-phase of the cell cycle in Saccharomyces cerevisiae

机译:核外泌体成分RRP6的缺失导致酿酒酵母细胞周期S期中组蛋白mRNA HTB1的持续积累

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摘要

The nuclear exosome, a macromolecular complex of 3 to 5 exonucleases, is required for the post-transcriptional processing of a variety of RNAs including rRNAs and snoRNAs. Additionally, this complex forms part of a nuclear surveillance network where it acts to degrade any aberrantly processed mRNAs in the nucleus. The exosome complex has been implicated in the biogenesis pathway of general messenger RNAs through its interaction with the 3-end processing machinery. During the cell cycle, yeast histone mRNAs accumulate in the S-phase and are rapidly degraded as cells enter the G2-phase. To determine if the exosome contributes to the cyclic turnover of yeast histone mRNAs, we examined the pattern of accumulation of HTB1 mRNA during the cell cycle in a deletion strain of RRP6, a component of the nuclear exosome. Our results show that cells lacking Rrp6p continue to accumulate HTB1 mRNA as the cell cycle proceeds. This continued accumulation appears to result from a delay in exit from S-phase in rrp6 cells. The accumulation of HTB1 mRNA in rrp6 cells is influenced by the interaction of the nuclear exosome with the 3-end processing machinery although there is no evidence for differential regulation of histone mRNA 3-end processing during the yeast cell cycle.
机译:核外泌体是3至5个外切核酸酶的大分子复合物,是转录后加工包括rRNA和snoRNA在内的各种RNA所必需的。此外,这种复合物构成了核监视网络的一部分,在该网络中,其作用是降解细胞核中任何异常加工的mRNA。外泌体复合物通过与3末端加工机制的相互作用而参与了一般信使RNA的生物发生途径。在细胞周期中,酵母组蛋白mRNA积累在S期,并随着细胞进入G2期而迅速降解。为了确定外泌体是否有助于酵母组蛋白mRNA的循环更新,我们检查了细胞周期中HTP1 mRNA在核外泌体成分RRP6缺失菌株中的积累模式。我们的结果表明,缺乏Rrp6p的细胞会随着细胞周期的进行而继续积累HTB1 mRNA。这种持续的积累似乎是由于rrp6细胞S期退出延迟所致。尽管没有证据表明在酵母细胞周期中组蛋白mRNA 3末端加工的差异调节,但是rrp6细胞中HTB1 mRNA的积累受核外泌体与3末端加工机制的相互作用的影响。

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