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The ribosome assembly gene network is controlled by the feedback regulation of transcription elongation

机译:通过转录伸长率的反馈调节来控制核糖体组装基因网络

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Ribosome assembly requires the concerted expression of hundreds of genes, which are transcribed by all three nuclear RNA polymerases. Transcription elongation involves dynamic interactions between RNA polymerases and chromatin. We performed a synthetic lethal screening in Saccharomyces cere-visiae with a conditional allele of SPT6, which encodes one of the factors that facilitates this process. Some of these synthetic mutants corresponded to factors that facilitate pre-rRNA processing and ribosome biogenesis. We found that the in vivo depletion of one of these factors, Arb1, activated transcription elongation in the set of genes involved directly in ribosome assembly. Under these depletion conditions, Spt6 was physically targeted to the up-regulated genes, where it helped maintain their chromatin integrity and the synthesis of properly stable mRNAs. The mRNA profiles of a large set of ribosome biogenesis mutants confirmed the existence of a feedback regulatory network among ribosome assembly genes. The transcriptional response in this network depended on both the specific malfunction and the role of the regulated gene. In accordance with our screening, Spt6 positively contributed to the optimal operation of this global network. On the whole, this work uncovers a feedback control of ribosome biogenesis by fine-tuning transcription elongation in ribosome assembly factor-coding genes.
机译:核糖体组件需要由所有三种核RNA聚合酶转录的数百个基因的齐齐异的表达。转录伸长率涉及RNA聚合酶和染色质之间的动态相互作用。我们在Saccharomyces Cere-Visia中进行了合成的致死筛选,其条件等位基因为SPT6,它们编码了促进该过程的一个因素。这些合成突变体中的一些对应于促进rRNA加工和核糖体生物发生的因素。我们发现,在这些因素中的一个,ARB1,直接在核糖体组件中涉及的基因中的激活转录伸长的体内耗尽。在这些耗竭条件下,SPT6物理靶向上调基因,在那里它有助于保持其染色质完整性和合成适当稳定的MRNA的合成。一大组核糖体生物生物生物体的mRNA谱证实了核糖体组装基因中反馈调节网络的存在。该网络中的转录响应依赖于特定的故障和调节基因的作用。按照我们的筛选,SPT6积极贡献了这一全球网络的最佳运行。总的来说,通过核糖体组装因子编码基因的微调转录伸长,该工作揭示了核糖体生物发生的反馈控制。

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