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首页> 外文期刊>RNA biology >Hold on!: RNA polymerase interactions with the nascent RNA modulate transcription elongation and termination.
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Hold on!: RNA polymerase interactions with the nascent RNA modulate transcription elongation and termination.

机译:坚持!:RNA聚合酶与新生RNA的相互作用可调节转录伸长和终止。

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Evolutionary related multisubunit RNA polymerases from all three domains of life, Eukarya, Archaea and Bacteria, have common structural and functional properties. We have recently shown that two RNAP subunits, F/E (RPB4/7)-which are conserved between eukaryotes and Archaea but have no bacterial homologues-interact with the nascent RNA chain and thereby profoundly modulate RNAP activity. Overall F/E increases transcription processivity, but it also stimulates transcription termination in a sequence-dependent manner. In addition to RNA-binding, these two apparently opposed processes are likely to involve an allosteric mechanism of the RNAP clamp. Spt4/5 is the only known RNAP-associated transcription factor that is conserved in all three domains of life, and it stimulates elongation similar to RNAP subunits F/E. Spt4/5 enhances processivity in a fashion that is independent of the nontemplate DNA strand, by interacting with the RNAP clamp. Whereas the molecular mechanism of Spt4/5 is universally conserved in evolution, the added functionality of F/E-like complexes has emerged after the split of the bacterial and archaeoeukaryotic lineages. Interestingly, bacteriophage-encoded antiterminator proteins could, in theory, fulfil an analogous function in the bacterial RNAP.
机译:来自生命的所有三个域的进化相关的多亚基RNA聚合酶具有共同的结构和功能特性,它们来自生命的三个领域,Eukarya,古细菌和细菌。我们最近发现,两个RNAP亚基F / E(RPB4 / 7)-在真核生物和古细菌之间保守,但没有细菌同源物,与新生的RNA链相互作用,从而深刻地调节RNAP活性。总体而言,F / E提高了转录的连续性,但也以序列依赖性的方式刺激了转录的终止。除了RNA结合,这两个明显相反的过程可能涉及RNAP钳位的变构机制。 Spt4 / 5是唯一已知的与RNAP相关的转录因子,在生活的所有三个域中都保守,并且它刺激类似于RNAP亚基F / E的延伸。通过与RNAP夹具相互作用,Spt4 / 5以独立于非模板DNA链的方式增强了合成能力。尽管Spt4 / 5的分子机制在进化中是普遍保守的,但在细菌和古生物的谱系分裂后,出现了F / E样复合物的附加功能。有趣的是,从理论上讲,噬菌体编码的抗终止剂蛋白可以在细菌RNAP中发挥类似的功能。

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