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首页> 外文期刊>Nucleic Acids Research >Species specificity of human RPA in simian virus 40 DNA replication lies in T-antigen-dependent RNA primer synthesis.
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Species specificity of human RPA in simian virus 40 DNA replication lies in T-antigen-dependent RNA primer synthesis.

机译:人RPA在猿猴病毒中的种属特异性40 DNA复制取决于T抗原依赖性RNA引物的合成。

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Replication protein A (RPA) is a three-subunit protein complex with multiple functions in DNA replication. Previous study indicated that human RPA (h-RPA) could not be replaced by Schizosaccharomyces pombe RPA (sp-RPA) in simian virus 40 (SV40) replication, suggesting that h-RPA may have a specific function in SV40 DNA replication. To understand the specificity of h-RPA in replication, we prepared heterologous RPAs containing the mixture of human and S.pombe subunits and compared these preparations for various enzymatic activities. Heterologous RPAs containing two human subunits supported SV40 DNA replication, whereas those containing only one human subunit poorly supported DNA replication, suggesting that RPA complex requires at least two human subunits to support its function in SV40 DNA replication. All heterologous RPAs effectively supported single-stranded (ss)DNA binding activity and an elongation of a primed DNA template catalyzed by DNA polymerase (pol) alpha and delta. A strong correlation between SV40 DNA replication activity and large tumor antigen (T-ag)-dependent RNA primer synthesis by pol alpha-primase complex was observed among the heterologous RPAs. Furthermore, T-ag showed a strong interaction with 70- and 34-kDa subunits from human, but poorly interacted with their S.pombe counterparts, indicating that the specificity of h-RPA is due to its role in RNA primer synthesis. In the SV40 replication reaction, the addition of increasing amounts of sp-RPA in the presence of fixed amount of h-RPA significantly reduced overall DNA synthesis, but increased the size of lagging strand, supporting a specific role for h-RPA in RNA primer synthesis. Together, these results suggest that the specificity of h-RPA in SV40 replication lies in T-ag-dependent RNA primer synthesis.
机译:复制蛋白A(RPA)是一种三亚基蛋白复合物,在DNA复制中具有多种功能。先前的研究表明,人猿RPA(h-RPA)在猿猴病毒40(SV40)复制中不能被粟酒裂殖酵母RPA(sp-RPA)取代,这表明h-RPA可能在SV40 DNA复制中具有特定功能。为了了解h-RPA在复制中的特异性,我们制备了包含人和S.pombe亚基混合物的异源RPA,并比较了这些制备物的各种酶活性。包含两个人类亚基的异源RPA支持SV40 DNA复制,而仅包含一个人类亚基的RPA则不支持DNA复制,这表明RPA复合体至少需要两个人类亚基来支持其在SV40 DNA复制中的功能。所有异源RPA有效地支持单链(ss)DNA结合活性以及DNA聚合酶(pol)α和δ催化的引物DNA模板的延长。异源RPAs之间观察到SV40 DNA复制活性和polα-primase复合物合成的大肿瘤抗原(T-ag)依赖的RNA引物合成之间有很强的相关性。此外,T-ag与人类的70-kDa和34-kDa亚基表现出较强的相互作用,但与S.pombe对应物的相互作用较弱,表明h-RPA的特异性是由于其在RNA引物合成中的作用。在SV40复制反应中,在固定量的h-RPA存在下添加数量增加的sp-RPA会显着降低总体DNA合成,但会增加滞后链的大小,从而支持h-RPA在RNA引物中的特定作用合成。总之,这些结果表明h-RPA在SV40复制中的特异性在于T-ag依赖性RNA引物合成。

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