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Functional Studies on the Interaction between Human Replication Protein A and Xeroderma pigmentosum Group A Complementing Protein (XPA)

机译:人类复制蛋白A与色干色素A组补充蛋白(XPA)相互作用的功能研究

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The human replication protein A (RPA; also known as human single-stranded DNA binding protein, HSSB) is a multisubunit complex (70, 34 and 11 kDa subunits) involved in the three processes of DNA metabolism; replication, repair, recombination. We found that both 35 and 70 kDa subunits (P34 and p70, respectively), of RPA interacts with the Xerodierma pigmentosum group A complementing protein (XPA), a protein that specifically recognizes UV-damaged DNA. Our mutational analysis indicated that no particular domains of RPA p70 were essential for its interaction with XPA. We also examined the effect of this XPA-RPA interaction on in vitro simian virus 40 (SV40) DNA replication catalyzed by the crude extract and monopolymerase system. XPA inhibited SV40 DNA replication in vitro through its interaction with RPA. Taken together, these results suggest that there is is a role for RPA in the regulation of DNA metabolism through its ability to modulate the interactions of proteins involved in the processes of DNA metabolism.
机译:人复制蛋白A(RPA;也称为人单链DNA结合蛋白,HSSB)是一种多亚基复合物(70、34和11 kDa亚基),参与DNA代谢的三个过程。复制,修复,重组。我们发现RPA的35 kDa和70 kDa亚基(分别为P34和p70)都与色素干性干燥杆菌A互补蛋白(XPA)相互作用,该蛋白专门识别受紫外线损伤的DNA。我们的突变分析表明,RPA p70的任何特定域对其与XPA的相互作用都是必不可少的。我们还检查了该XPA-RPA相互作用对粗提取物和单聚合酶系统催化的体外猿猴病毒40(SV40)DNA复制的影响。 XPA通过与RPA相互作用抑制了SV40 DNA在体外的复制。综上所述,这些结果表明RPA通过调节DNA代谢过程中涉及的蛋白质相互作用的能力而在DNA代谢的调节中发挥作用。

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