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hRRN3 is essential in the SL1-mediated recruitment of RNA Polymerase I to rRNA gene promoters

机译:hRRN3在SL1介导的RNA聚合酶I向rRNA基因启动子的募集中至关重要

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摘要

A crucial step in transcription is the recruitment of RNA polymerase to promoters. In the transcription of human rRNA genes by RNA Polymerase I (Pol I), transcription factor SL1 has a role as the essential core promoter binding factor. Little is known about the mechanism by which Pol I is recruited. We provide evidence for an essential role for hRRN3, the human homologue of a yeast Pol I transcription factor, in this process. We find that whereas the bulk of human Pol I complexes (Iα) are transcriptionally inactive, hRRN3 defines a distinct subpopulation of Pol I complexes (Iβ) that supports specific initiation of transcription. Human RRN3 interacts directly with TAFI110 and TAFI63 of promoter-selectivity factor SL1. Blocking this connection prevents recruitment of Pol I β to the rDNA promoter. Furthermore, hRRN3 can be found in transcriptionally autonomous Pol I holoenzyme complexes. We conclude that hRRN3 functions to recruit initiation-competent Pol I to rRNA gene promoters. The essential role for hRRN3 in linking Pol I to SL1 suggests a mechanism for growth control of Pol I transcription.
机译:转录的关键步骤是将RNA聚合酶募集至启动子。在RNA聚合酶I(Pol I)转录人类rRNA基因的过程中,转录因子SL1作为必需的核心启动子结合因子起作用。关于招募Pol我的机制知之甚少。我们提供了证据,证明hRRN3是酵母PolI转录因子的人类同源物在此过程中的重要作用。我们发现,虽然大部分人类Pol I复合物(Iα)在转录上均无活性,但hRRN3定义了支持特定转录起始的Pol I复合物(Iβ)的独特亚群。人RRN3与启动子选择性因子SL1的TAFI110和TAFI63直接相互作用。阻止此连接可防止Pol Iβ募集到rDNA启动子。此外,hRRN3可以在转录自主的Pol I全酶复合物中发现。我们得出结论,hRRN3的功能是将具有启动能力的Pol I募集到rRNA基因启动子。 hRRN3在将PolI与SL1连接中的重要作用提示了一种调控PolI转录生长的机制。

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