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Traveling Rocky Roads: The Consequences of Transcription-Blocking DNA Lesions on RNA Polymerase II

机译:旅行岩石道路:转录阻断DNA病变对RNA聚合酶II的后果

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Abstract The faithful transcription of eukaryotic genes by RNA polymerase II (RNAP2) is crucial for proper cell function and tissue homeostasis. However, transcription-blocking DNA lesions of both endogenous and environmental origin continuously challenge the progression of elongating RNAP2. The stalling of RNAP2 on a transcription-blocking lesion triggers a series of highly regulated events, including RNAP2 processing to make the lesion accessible for DNA repair, R-loop-mediated DNA damage signaling, and the initiation of transcription-coupled DNA repair. The correct execution and coordination of these processes is vital for resuming transcription following the successful repair of transcription-blocking lesions. Here, we outline recent insights into the molecular consequences of RNAP2 stalling on transcription-blocking DNA lesions and how these lesions are resolved to restore mRNA synthesis. Graphical Abstract Display Omitted Highlights ? Stalling of RNA polymerase II (RNAP2) on damaged DNA is cytotoxic. ? RNAP2 stalling activates DNA damage signaling. ? RNAP2 needs to be processed to allow repair. ? Transcription-coupled repair resolves DNA lesions. ? After DNA repair, transcription needs to restart.
机译:摘要RNA聚合酶II(RNAP2)对真核基因的忠实转录对适当的细胞功能和组织稳态至关重要。然而,内源性和环境原点的转录阻断DNA病变连续地攻击伸长RNAP2的进展。 RNAP2对转录阻断病变的停止触发了一系列高度调节的事件,包括RNAP2处理,以使DNA修复,R环介导的DNA损伤信号传导的病变和转录偶联的DNA修复的启动。对这些方法的正确执行和协调对于在成功修复转录障碍病变后恢复转录至关重要。在这里,我们概述最近的洞察力进入RNAP2停滞在转录阻断DNA病变上的分子后果以及这些病变如何解决以恢复mRNA合成。图形抽象显示省略了亮点? RNA聚合酶II(RNAP2)在受损DNA上停滞是细胞毒性的。还是RNAP2停滞激活DNA损伤信号。还是RNAP2需要处理以允许修复。还是转录耦合修复解决了DNA病变。还是在DNA修复后,转录需要重新启动。

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