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Structural Basis for Transcript Elongation Control by NusG Family Universal Regulators

机译:NUSG家族普遍监管机构转录伸长控制的结构基础

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NusG/RfaH/Spt5 transcription elongation factors are the only transcription regulators conserved across all life. Bacterial NusG regulates RNA polymerase (RNAP) elongation complexes (ECs) across most genes, enhancing elongation by suppressing RNAP backtracking and coordinating r-dependent termination and translation. The NusG paralog RfaH engages the EC only at operon polarity suppressor (ops) sites and suppresses both backtrack and hairpin-stabilized pausing. We used single-particle cryoelectron microscopy (cryo-EM) to determine structures of ECs at ops with NusG or RfaH. Both factors chaperone base-pairing of the upstream duplex DNA to suppress backtracking, explaining stimulation of elongation genome-wide. The RfaHopsEC structure reveals how RfaH confers operon specificity through specific recognition of an ops hairpin in the single-stranded nontemplate DNA and tighter binding to the EC to exclude NusG. Tight EC binding by RfaH sterically blocks the swiveled RNAP conformation necessary for hairpin-stabilized pausing. The universal conservation of NusG/RfaH/Spt5 suggests that the molecular mechanisms uncovered here are widespread.
机译:NUSG / RFAH / SPT5转录伸长因子是唯一在所有生命中保存的转录监管机构。细菌NUSG在大多数基因中调节RNA聚合酶(RNAP)伸长率复合物(ECS),通过抑制RNAP反向和协调依赖于终止和翻译来增强伸长率。 NUSG ParaRog ​​RFAH仅在Operon Polyity抑制器(OPS)站点上互动,并抑制回溯和发夹稳定的暂停。我们使用单粒子冷冻电子显微镜(Cryo-EM)来确定与NUSG或RFAH的OPS的ECS结构。两种因素伴随上游双相DNA的伴侣碱基配对,以抑制回溯,解释伸长基因组的刺激。 Rfahopsec结构揭示了RFAH如何通过在单链的Nontemplate DNA中的OPS发夹和与EC的更严格结合以排除NUSG来赋予RFAH的特异性。 RFAH空间的紧张EC绑定块块旋转的发夹稳定的暂停所需的旋转的RNAP构象。 NUSG / RFAH / SPT5的普遍保护表明这里未发现的分子机制是普遍的。

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