首页> 外文OA文献 >Competition of bacteriophage polypeptides with native replicase proteins for binding to the DNA sliding clamp reveals a novel mechanism for DNA replication arrest in Staphylococcus aureus.
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Competition of bacteriophage polypeptides with native replicase proteins for binding to the DNA sliding clamp reveals a novel mechanism for DNA replication arrest in Staphylococcus aureus.

机译:噬菌体多肽与天然复制酶蛋白竞争与DNA滑动钳的结合揭示了一种金黄色葡萄球菌中DNA复制停滞的新机制。

摘要

Bacteriophages have evolved specific mechanisms that redirect bacterial metabolic pathways to the bacteriophage reproduction cycle. In this study, we characterized the bactericidal mechanism of two polypeptides from bacteriophages Twort and G1 that target the DNA sliding clamp of Staphylococcus aureus. The DNA sliding clamp, which tethers DNA polymerase to its template and thereby confers processivity upon the enzyme, was found to be essential for the viability of S. aureus. Expression of polypeptides TwortORF168 and G1ORF240 in S. aureus selectively inhibited DNA replication which in turn resulted in cell death. Both polypeptides specifically inhibited the S. aureus DNA replicase that was reconstituted in vitro but not the corresponding replicase of Streptococcus pyogenes. We demonstrated that inhibition of DNA synthesis is multifaceted and occurs via binding the DNA sliding clamp: TwortORF168 and G1ORF240 bound tightly to the DNA sliding clamp and prevented both its loading onto DNA and its interaction with DNA polymerase C. These results elucidate the impact of bacteriophage polypeptide expression upon DNA replication in the growing cell.
机译:噬菌体已进化出特定的机制,可将细菌代谢途径重定向至噬菌体繁殖周期。在这项研究中,我们表征了噬菌体Twort和G1的两个多肽的杀菌机理,该多肽靶向金黄色葡萄球菌的DNA滑动钳。发现将DNA聚合酶束缚在其模板上并由此赋予该酶以可加工性的DNA滑动夹具对于金黄色葡萄球菌的生存力至关重要。金黄色葡萄球菌中多肽TwortORF168和G1ORF240的表达选择性抑制DNA复制,进而导致细胞死亡。两种多肽都特异性抑制体外重构的金黄色葡萄球菌DNA复制酶,但不抑制化脓性链球菌的相应复制酶。我们证明了对DNA合成的抑制作用是多方面的,并且是通过结合DNA滑动夹而发生的:TwortORF168和G1ORF240与DNA滑动夹紧密结合,并阻止了其装载到DNA上以及与DNA聚合酶C相互作用。这些结果阐明了噬菌体的影响DNA在生长细胞中复制后表达。

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