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单链 DNA 是 SOS 非依赖性 DNA 损伤反应转录激活因子 DriD 的别构调节剂。

ssDNA is an allosteric regulator of the SOS-independent DNA damage response transcription activator, DriD.

机构信息

Department of Biology, Massachusetts Institute of Technology. Cambridge, Massachusetts 02139, USA.

Department of Biochemistry, Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

Genes Dev. 2022 May 1;36(9-10):618-633. doi: 10.1101/gad.349541.122. Epub 2022 May 26.

Abstract

DNA damage repair systems are critical for genomic integrity. However, they must be coordinated with DNA replication and cell division to ensure accurate genomic transmission. In most bacteria, this coordination is mediated by the SOS response through LexA, which triggers a halt in cell division until repair is completed. Recently, an SOS-independent damage response system was revealed in This pathway is controlled by the transcription activator, DriD, but how DriD senses and signals DNA damage is unknown. To address this question, we performed biochemical, cellular, and structural studies. We show that DriD binds a specific promoter DNA site via its N-terminal HTH domain to activate transcription of genes, including the cell division inhibitor A structure of the C-terminal portion of DriD revealed a WYL motif domain linked to a WCX dimerization domain. Strikingly, we found that DriD binds ssDNA between the WYL and WCX domains. Comparison of apo and ssDNA-bound DriD structures reveals that ssDNA binding orders and orients the DriD domains, indicating a mechanism for ssDNA-mediated operator DNA binding activation. Biochemical and in vivo studies support the structural model. Our data thus reveal the molecular mechanism underpinning an SOS-independent DNA damage repair pathway.

摘要

DNA 损伤修复系统对于基因组完整性至关重要。然而,它们必须与 DNA 复制和细胞分裂相协调,以确保准确的基因组传递。在大多数细菌中,这种协调是通过 LexA 介导的 SOS 反应来实现的,LexA 会触发细胞分裂停止,直到修复完成。最近,在 中揭示了一种 SOS 不依赖的损伤反应系统。该途径由转录激活因子 DriD 控制,但 DriD 如何感知和信号 DNA 损伤尚不清楚。为了解决这个问题,我们进行了生化、细胞和结构研究。我们表明,DriD 通过其 N 端 HTH 结构域结合特定的启动子 DNA 位点,激活包括细胞分裂抑制剂 在内的基因转录。A 结构的 C 端部分揭示了一个与 WCX 二聚化结构域相连的 WYL 基序结构域。引人注目的是,我们发现 DriD 结合在 WYL 和 WCX 结构域之间的 ssDNA 上。apo 和 ssDNA 结合的 DriD 结构的比较表明,ssDNA 结合顺序和定向 DriD 结构域,表明 ssDNA 介导的操纵子 DNA 结合激活的机制。生化和体内研究支持结构模型。我们的数据因此揭示了 SOS 不依赖的 DNA 损伤修复途径的分子机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9be1/9186387/783063f62c49/618f01.jpg

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