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首页> 外文期刊>Frontiers in Molecular Biosciences >The Transcription-Repair Coupling Factor Mfd Prevents and Promotes Mutagenesis in a Context-Dependent Manner
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The Transcription-Repair Coupling Factor Mfd Prevents and Promotes Mutagenesis in a Context-Dependent Manner

机译:转录修复耦合因子MFD以上下文的方式防止并促进诱变

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The mfd (mutation frequency decline) gene was identified by screening an auxotrophic Escherichia coli strain exposed to UV and held in a minimum medium before plating onto rich or minimal agar plates. It was found that under these conditions, holding cells in minimal (non-growth) conditions resulted in mutations that enabled cells to grow on minimal media. Using this observation as a starting point, a mutant was isolated that failed to mutate to autotrophy under the proscribed conditions, and the gene responsible for this phenomenon (mutation frequency decline) was named mfd. Later work revealed that mfd encoded a translocase that recognizes RNA Polymerase (RNAP) stalled at damage sites and binds to the stalled RNAP, recruits the nucleotide excision repair damage recognition complex UvrA2UvrB to the site, and facilitates damage recognition and repair while dissociating the stalled RNAP from the DNA along with the truncated RNA. Recent single molecule and genome-wide repair studies have revealed time-resolved features and structural aspects of this transcription-coupled repair (TCR) phenomenon. Interestingly, recent work has shown that in certain bacterial species Mfd also plays roles in recombination, bacterial virulence, and development of drug resistance.
机译:通过筛选暴露于UV的疾风养殖大肠杆菌菌株并在电镀到富含或最小琼脂平板上之前鉴定MFD(突变频率下降)基因。发现在这些条件下,保持细胞在最小(非生长)条件下导致使能细胞在最小培养基上生长的突变。使用这种观察结果作为起点,分离突变体,其在被禁止的条件下未能突变为自触发,并且负责这种现象(突变频率下降)的基因被命名为MFD。后来的工作表明,MFD编码了识别在损伤部位的RNA聚合酶(RNAP)并结合停滞的RNAP,促进核苷酸切除修复损伤识别复合UVRA2UVRB,并促进解散停滞的RNAP的损坏识别和修复从DNA以及截短的RNA。最近的单一分子和基因组修复研究揭示了该转录耦合修复(TCR)现象的时间分辨特征和结构方面。有趣的是,最近的工作表明,在某些细菌种类中,MFD也在重组,细菌毒力和耐药性发展中发挥作用。

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