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分枝杆菌 HelD 将 RNA 聚合酶回收与转录起始连接起来。

Mycobacterial HelD connects RNA polymerase recycling with transcription initiation.

机构信息

Institute of Biotechnology of the Czech Academy of Sciences, Průmyslová 595, 252 50, Vestec, Czech Republic.

Institute of Microbiology of the Czech Academy of Sciences, Vídeňská 1083, 142 20, Prague, Czech Republic.

出版信息

Nat Commun. 2024 Oct 9;15(1):8740. doi: 10.1038/s41467-024-52891-5.

Abstract

Mycobacterial HelD is a transcription factor that recycles stalled RNAP by dissociating it from nucleic acids and, if present, from the antibiotic rifampicin. The rescued RNAP, however, must disengage from HelD to participate in subsequent rounds of transcription. The mechanism of release is unknown. We show that HelD from Mycobacterium smegmatis forms a complex with RNAP associated with the primary sigma factor σ and transcription factor RbpA but not CarD. We solve several structures of RNAP-σ-RbpA-HelD without and with promoter DNA. These snapshots capture HelD during transcription initiation, describing mechanistic aspects of HelD release from RNAP and its protective effect against rifampicin. Biochemical evidence supports these findings, defines the role of ATP binding and hydrolysis by HelD in the process, and confirms the rifampicin-protective effect of HelD. Collectively, these results show that when HelD is present during transcription initiation, the process is protected from rifampicin until the last possible moment.

摘要

分枝杆菌 HelD 是一种转录因子,通过与核酸(如果存在的话,与抗生素利福平)解离来使停滞的 RNA 聚合酶(RNAP)重新循环。然而,被拯救的 RNAP 必须与 HelD 脱离,才能参与后续的转录循环。释放的机制尚不清楚。我们表明,来自耻垢分枝杆菌的 HelD 与与主要σ因子σ和转录因子 RbpA 相关的 RNAP 形成复合物,但不与 CarD 相关。我们解决了没有和有启动子 DNA 的 RNAP-σ-RbpA-HelD 的几个结构。这些快照在转录起始时捕获 HelD,描述了 HelD 从 RNAP 释放的机制方面以及其对利福平的保护作用。生化证据支持这些发现,定义了 HelD 在该过程中结合和水解 ATP 的作用,并证实了 HelD 对利福平的保护作用。总的来说,这些结果表明,当 HelD 在转录起始时存在时,该过程受到利福平的保护,直到最后一刻。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/efd6/11464796/9704bb49fa6a/41467_2024_52891_Fig1_HTML.jpg

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