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首页> 外文期刊>Nucleic Acids Research >Full shut-off of Escherichia coli RNA-polymerase by T7 phage requires a small phage-encoded DNA-binding protein
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Full shut-off of Escherichia coli RNA-polymerase by T7 phage requires a small phage-encoded DNA-binding protein

机译:通过T7噬菌体完全关闭大肠杆菌RNA聚合酶需要小噬菌体编码的DNA结合蛋白

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摘要

Infection of Escherichia coli by the T7 phage leads to rapid and selective inhibition of the bacterial RNA polymerase (RNAP) by the 7 kDa T7 protein Gp2. We describe the identification and functional and structural characterisation of a novel 7 kDa T7 protein, Gp5.7, which adopts a winged helix-turn-helix-like structure and specifically represses transcription initiation from host RNAP-dependent promoters on the phage genome via a mechanism that involves interaction with DNA and the bacterial RNAP. Whereas Gp2 is indispensable for T7 growth in E. coli, we show that Gp5.7 is required for optimal infection outcome. Our findings provide novel insights into how phages fine-tune the activity of the host transcription machinery to ensure both successful and efficient phage progeny development.
机译:T7噬菌体感染大肠杆菌导致通过7kDa T7蛋白GP2快速和选择性抑制细菌RNA聚合酶(RNAP)。 我们描述了一种新型7kDa T7蛋白GP5.7的鉴定和功能性和结构表征,其采用翼状的螺旋转向螺旋状结构,并特别抑制来自噬菌体RNAP依赖性启动子的转录开始通过a 涉及与DNA和细菌RNAP相互作用的机制。 虽然GP2对于大肠杆菌中的T7生长是必不可少的,但我们表明最佳感染结果需要GP5.7。 我们的调查结果提供了对噬菌体的微调的微调,以确保成功和高效的噬菌体后代发育的新颖洞察。

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