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Rearrangement of structured RNA via branch migration structures catalysed by the highly related DEAD-box proteins p68 and p72

机译:结构化RNA的重排 通过高度相关的催化的分支迁移结构 DEAD-box蛋白p68和p72

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摘要

RNA helicases, like their DNA-specific counterparts, can function as processive enzymes, unwinding RNA with a defined step size in a unidirectional fashion. Recombinant nuclear DEAD-box protein p68 and its close relative p72 are reported here to function in a similar fashion, though the processivity of both RNA helicases appears to be limited to only a few consecutive catalytic steps. The two proteins resemble each other also with regard to other biochemical properties. We have found that both proteins exhibit an RNA annealing in addition to their helicase activity. By using both these activities the enzymes are able in vitro to catalyse rearrangements of RNA secondary structures that otherwise are too stable to be resolved by their low processive helicase activities. RNA rearrangement proceeds via protein induced formation and subsequent resolution of RNA branch migration structures, whereby the latter step is dependent on ATP hydrolysis. The analysed DEAD-box proteins are reminiscent of certain DNA helicases, for example those found in bacteriophages T4 and T7, that catalyse homologous DNA strand exchange in cooperation with the annealing activity of specific single strand binding proteins.
机译:RNA解旋酶和它们的DNA特异性对应物一样,可以充当过程性酶,以单向方式展开具有确定步长的RNA。尽管两种RNA解旋酶的合成能力似乎仅限于几个连续的催化步骤,但据报道重组核DEAD-box蛋白p68及其近亲p72的功能相似。两种蛋白质在其他生化特性方面也相似。我们发现,这两种蛋白质除了其解旋酶活性外,还表现出RNA退火。通过同时使用这两种活性,这些酶可以体外催化RNA二级结构的重排,否则这些二级结构非常稳定,无法通过其低水平的解旋酶活性来解决。 RNA重排通过蛋白质诱导的形成和随后的RNA分支迁移结构的分解而进行,由此后一步取决于ATP水解。分析的DEAD-box蛋白让人想起某些DNA解旋酶,例如在噬菌体T4和T7中发现的那些,它们协同催化同质DNA链交换 具有特定单链结合蛋白的退火活性。

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