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RECQ5 helicase associates with the C-terminal repeat domain of RNA polymerase II during productive elongation phase of transcription

机译:RECQ5解旋酶在转录的生产延伸阶段与RNA聚合酶II的C末端重复域关联

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摘要

It is known that transcription can induce DNA recombination, thus compromising genomic stability. RECQ5 DNA helicase promotes genomic stability by regulating homologous recombination. Recent studies have shown that RECQ5 forms a stable complex with RNA polymerase II (RNAPII) in human cells, but the cellular role of this association is not understood. Here, we provide evidence that RECQ5 specifically binds to the Ser2,5-phosphorylated C-terminal repeat domain (CTD) of the largest subunit of RNAPII, RPB1, by means of a Set2–Rpb1-interacting (SRI) motif located at the C-terminus of RECQ5. We also show that RECQ5 associates with RNAPII-transcribed genes in a manner dependent on the SRI motif. Notably, RECQ5 density on transcribed genes correlates with the density of Ser2-CTD phosphorylation, which is associated with the productive elongation phase of transcription. Furthermore, we show that RECQ5 negatively affects cell viability upon inhibition of spliceosome assembly, which can lead to the formation of mutagenic R-loop structures. These data indicate that RECQ5 binds to the elongating RNAPII complex and support the idea that RECQ5 plays a role in the maintenance of genomic stability during transcription.
机译:已知转录可以诱导DNA重组,从而损害基因组稳定性。 RECQ5 DNA解旋酶通过调节同源重组来促进基因组稳定性。最近的研究表明,RECQ5在人细胞中与RNA聚合酶II(RNAPII)形成稳定的复合物,但这种结合的细胞作用尚不清楚。在这里,我们提供证据表明RECQ5通过位于C的Set2-Rpb1相互作用(SRI)母题与RNAPII最大的亚基RPB1的Ser2,5-磷酸化的C末端重复域(CTD)特异性结合-RECQ5的终点。我们还显示,RECQ5以依赖于SRI主题的方式与RNAPII转录的基因相关联。值得注意的是,转录基因上的RECQ5密度与Ser2-CTD磷酸化的密度相关,而后者与转录的生产延伸期有关。此外,我们显示,RECQ5抑制剪接体组装后对细胞活力产生负面影响,这可能导致诱变R环结构的形成。这些数据表明RECQ5与延长的RNAPII复合物结合,并支持RECQ5在转录过程中维持基因组稳定性中起作用的观点。

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