首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Herpes simplex virus 1 activates cdc2 to recruit topoisomerase IIα for post-DNA synthesis expression of late genes
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Herpes simplex virus 1 activates cdc2 to recruit topoisomerase IIα for post-DNA synthesis expression of late genes

机译:单纯疱疹病毒1激活cdc2以募集拓扑异构酶IIα用于后期基因的DNA合成后表达

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摘要

A subset (γ2) of late herpes simplex virus 1 genes depends on viral DNA synthesis for its expression. For optimal expression, a small number of these genes, exemplified by US11, also requires two viral proteins, the α protein infected cell protein (ICP) 22 and the protein kinase UL13. Earlier we showed that UL13 and ICP22 mediate the stabilization of cdc2 and the replacement of its cellular partner, cyclin B, with the viral DNA polymerase processivity factor UL42. Here we report that cdc2 and its new partner, UL42, bind a phosphorylated form of topoisomerase IIα. The posttranslational modification of topoisomerase IIα and its interaction with cdc2–UL42 proteins depend on ICP22 in infected cells. Although topoisomerase II is required for viral DNA synthesis, ICP22 is not, indicating a second function for topoisomerase IIα. The intricate manner in which the virus recruits topoisomerase IIα for post-DNA synthesis expression of viral genes suggests that topoisomerase IIα also is required for untangling concatemeric DNA progeny for optimal transcription of late genes.
机译:单纯疱疹病毒1基因的一个子集(γ2)取决于病毒DNA的表达。为了获得最佳表达,这些基因中的少数基因(例如US11)还需要两种病毒蛋白,即被α蛋白感染的细胞蛋白(ICP)22和蛋白激酶UL13。先前我们显示,UL13和ICP22用病毒DNA聚合酶加工性因子UL42介导了cdc2的稳定及其细胞伴侣cyclin B的替代。在这里我们报告cdc2及其新的伙伴UL42结合了磷酸化形式的拓扑异构酶IIα。拓扑异构酶IIα的翻译后修饰及其与cdc2-UL42蛋白质的相互作用取决于感染细胞中的ICP22。尽管拓扑异构酶II是病毒DNA合成所必需的,但ICP22不是必需的,这表明拓扑异构酶IIα具有第二种功能。病毒招募拓扑异构酶IIα进行病毒基因的DNA后合成表达的复杂方式表明,拓扑异构酶IIα也是解开串联DNA后代以使晚期基因最佳转录所必需的。

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