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首页> 外文期刊>Nucleic Acids Research >Mismatch Repair proteins are recruited to replicating DNA through interaction with Proliferating Cell Nuclear Antigen (PCNA).
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Mismatch Repair proteins are recruited to replicating DNA through interaction with Proliferating Cell Nuclear Antigen (PCNA).

机译:失配修复蛋白通过与增殖细胞核抗原(PCNA)相互作用而募集到复制DNA中。

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摘要

Mismatch Repair (MMR) is closely linked to DNA replication; however, other than the role of the replicative sliding clamp (PCNA) in various MMR functions, the linkage between DNA replication and MMR has been difficult to investigate. Here we use an in vitro DNA replication system based on simian virus 40, to investigate MMR recruitment to replicating DNA. Both DNA replication and MMR proteins are recruited to replicating DNA in an origin-dependent fashion. Primer synthesis is required for recruitment of both PCNA and MMR proteins, but not for recruitment of the single-stranded DNA-binding protein (RPA). Blocking PCNA recruitment to replicating DNA with a p21-based polypeptide blocks PCNA and MMR, but not RPA recruitment. Once PCNA and subsequent proteins required for replication are loaded onto DNA, addition of p21 leaves PCNA on the replicating DNA, but actively displaces MMR proteins. These findings indicate that the MMR machinery is recruited to replicating DNA through its interaction with PCNA, andsuggests that this occurs via binding of the MMR proteins to the multi-protein interaction sites on PCNA. These studies demonstrate the utility of this system for further investigation of the role of DNA replication in MMR.
机译:错配修复(MMR)与DNA复制密切相关;但是,除了复制性滑动钳(PCNA)在各种MMR功能中的作用外,DNA复制与MMR之间的联系很难进行研究。在这里,我们使用基于猿猴病毒40的体外DNA复制系统,来研究MMR募集到复制DNA。 DNA复制和MMR蛋白均被招募以依赖于起源的方式复制DNA。募集PCNA和MMR蛋白都需要引物合成,但募集单链DNA结合蛋白(RPA)则不需要。使用基于p21的多肽阻止PCNA募集以复制DNA,可以阻止PCNA和MMR,但不能阻止RPA募集。一旦将PCNA和复制所需的后续蛋白质加载到DNA上,添加p21会使PCNA留在复制的DNA上,但会主动置换MMR蛋白。这些发现表明,MMR机制通过其与PCNA的相互作用而被招募来复制DNA,这表明这是通过MMR蛋白与PCNA上多蛋白相互作用位点的结合而发生的。这些研究表明该系统可用于进一步研究DNA复制在MMR中的作用。

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