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首页> 外文期刊>Journal of Molecular Biology >THE INTERACTION OF THE F PLASMID KILLER PROTEIN, CCDB, WITH DNA GYRASE - INDUCTION OF DNA CLEAVAGE AND BLOCKING OF TRANSCRIPTION
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THE INTERACTION OF THE F PLASMID KILLER PROTEIN, CCDB, WITH DNA GYRASE - INDUCTION OF DNA CLEAVAGE AND BLOCKING OF TRANSCRIPTION

机译:F质粒杀手蛋白CCDB与DNA旋转酶的相互作用-DNA切割的诱导和转录的阻断。

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We have studied the interaction of the F plasmid killer protein CcdB with its intracellular target DNA gyrase. We confirm that CcdB fan induce DNA cleavage by gyrase anti show that this cleavage reaction requires ATP hydrolysis when the substrate is linear DNA, but is independent of hydrolysis when negatively supercoiled DNA is used. The 64 kDa domain of the gyrase A protein, which can catalyse DNA cleavage in the presence of the B protein and quinolone drugs, is unable to cleave DNA in the presence of CcdB unless the C-terminal 33 kDa domain of the gyrase A protein is also present. CcdB-induced DNA cleavage by gyrase requires a minimum length of DNA (> similar to 160 bp), whereas in the presence of quinolone drugs gyrase can cleave much shorter DNA molecules. We show that CcdB, Like quinolones, can form a complex with gyrase which can block transcription by RNA polymerase. A model for the interaction of CcdB with gyrase involving the trapping of a post-strand-passage intermediate is suggested. We conclude that CcdB can stabilise a cleavage complex between DNA gyrase and DNA in a manner distinct from quinolones but, like the quinolone-induced cleavage complex, the CcdB-stabilised complex can also form a barrier to the passage of polymerases. (C) 1997 Academic Press Limited. [References: 59]
机译:我们已经研究了F质粒杀伤蛋白CcdB及其细胞内靶DNA促旋酶的相互作用。我们证实,CcdB风扇通过反旋酶诱导DNA裂解,表明该裂解反应在底物是线性DNA时需要ATP水解,而在使用负超螺旋DNA时则不依赖于水解。旋转酶A蛋白的64 kDa结构域可以在B蛋白和喹诺酮药物存在下催化DNA裂解,除非存在CcdB,否则无法在CcdB存在下裂解DNA。也存在。旋转酶使CcdB诱导的DNA切割需要最小的DNA长度(>类似于160 bp),而在喹诺酮药物存在下,旋转酶可以切割更短的DNA分子。我们表明,CcdB像喹诺酮一样,可以与回旋酶形成复合物,从而可以阻止RNA聚合酶的转录。提出了一种用于CcdB与回旋酶相互作用的模型,该模型涉及捕获链后通道中间体。我们得出结论,CcdB可以以不同于喹诺酮的方式稳定DNA促旋酶和DNA之间的裂解复合物,但像喹诺酮诱导的裂解复合物一样,CcdB稳定的复合物也可以形成聚合酶通过的障碍。 (C)1997 Academic Press Limited。 [参考:59]

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