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Formation of the complex of bovine papillomavirus E1 and E2 proteins is modulated by E2 phosphorylation and depends upon sequences within the carboxyl terminus of E1.

机译:牛乳头瘤病毒E1和E2蛋白复合物的形成受E2磷酸化的调节,并取决于E1羧基末端内的序列。

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摘要

The 68-kDa bovine papillomavirus (BPV) type 1 replication protein E1 and the 48-kDa transactivator protein E2 form a complex that specifically binds DNA [Mohr, I.J., Clark, R., Sun, S., Androphy, E.J., MacPherson, P. & Botchan, M.R. (1990) Science 250, 1694-1699]. We have confirmed this observation and shown that the E1-E2 complex binds to DNA fragments that contain the BPV plasmid maintenance sequence 1 and a site for the initiation of bidirectional BPV DNA synthesis. The E1 protein was found to bind preferentially to non- or underphosphorylated species of E2, suggesting that the phosphorylation state of E2 modulates the association of the two proteins. Replication-deficient E1 mutants with single amino acid substitutions and deletions in the carboxyl terminus failed to interact with E2, indicating that a region in the E1 carboxyl terminus is required for E1 to interact with E2. Our results suggest that the replication deficiency of some E1 mutants reflects their inability to associate with E2.
机译:68 kDa牛乳头瘤病毒(BPV)1型复制蛋白E1和48 kDa反式激活蛋白E2形成特异性结合DNA的复合物[Mohr,IJ,Clark,R.,Sun,S.,Androphy,EJ,MacPherson, P.&Botchan,MR(1990)Science 250,1694-1699]。我们已经证实了这一观察结果,并表明E1-E2复合物与包含BPV质粒维持序列1和双向BPV DNA合成起始位点的DNA片段结合。发现E1蛋白优先与E2的非磷酸化或磷酸化不足的物种结合,这表明E2的磷酸化状态调节了这两种蛋白的结合。在羧基末端具有单个氨基酸取代和缺失的复制缺陷型E1突变体无法与E2相互作用,这表明E1与E2相互作用需要E1羧基末端的区域。我们的结果表明,某些E1突变体的复制缺陷反映了它们无法与E2相关联。

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  • 作者

    Lusky, M; Fontane, E;

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  • 年度 1991
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  • 原文格式 PDF
  • 正文语种 en
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