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Regulation of polymerase exchange between Polη and Polδ by monoubiquitination of PCNA and the movement of DNA polymerase holoenzyme

机译:通过PCNA的单泛素化和DNA聚合酶全酶的移动来调节Polη和Polδ之间的聚合酶交换

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摘要

To ensure efficient and timely replication of genomic DNA, organisms in all three kingdoms of life possess specialized translesion DNA synthesis (TLS) polymerases (Pols) that tolerate various types of DNA lesions. It has been proposed that an exchange between the replicative DNA Pol and the TLS Pol at the site of DNA damage enables lesion bypass to occur. However, to date the molecular mechanism underlying this process is not fully understood. In this study, we demonstrated in a reconstituted system that the exchange of Saccharomyces cerevisiae Polδ with Polη requires both the stalling of the holoenzyme and the monoubiquitination of proliferating cell nuclear antigen (PCNA). A moving Polδ holoenzyme is refractory to the incoming Polη. Furthermore, we showed that the Polη C-terminal PCNA-interacting protein motif is required for the exchange process. We also demonstrated that the second exchange step to bring back Polδ is prohibited when Lys-164 of PCNA is monoubiquitinated. Thus the removal of the ubiquitin moiety from PCNA is likely required for the reverse exchange step after the lesion bypass synthesis by Polη.
机译:为了确保基因组DNA的有效及时复制,生命的所有三个王国中的生物都具有专门的跨病变DNA合成(TLS)聚合酶(Pol),可以耐受各种类型的DNA损伤。已经提出,在DNA损伤部位,复制性DNA Pol和TLS Pol之间的交换使损伤旁路得以发生。然而,迄今为止,尚未完全理解该过程的分子机制。在这项研究中,我们证明了在重组系统中,酿酒酵母Polδ与Polη的交换既需要全酶的停止作用,又需要增殖细胞核抗原(PCNA)的单泛素化作用。移动的Polδ全酶对进入的Polη无效。此外,我们表明,PolηC末端PCNA相互作用蛋白基序是交换过程所必需的。我们还证明,当PCNA的Lys-164单泛素化时,禁止带回Polδ的第二步交换步骤。因此,在通过Polη进行损伤旁路合成之后,逆向交换步骤可能需要从PCNA中去除泛素部分。

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