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Correct intranuclear localization of herpes simplex virus DNA polymerase requires the viral ICP8 DNA-binding protein.

机译:单纯疱疹病毒DNA聚合酶的正确核内定位需要病毒ICP8 DNA结合蛋白。

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摘要

We used indirect immunofluorescence to examine the factors determining the intranuclear location of herpes simplex virus (HSV) DNA polymerase (Pol) in infected cells. In the absence of viral DNA replication, HSV Pol colocalized with the HSV DNA-binding protein ICP8 in nuclear framework-associated structures called prereplicative sites. In the presence of viral DNA replication, HSV Pol colocalized with ICP8 in globular intranuclear structures called replication compartments. In cells infected with mutant viruses encoding defective ICP8 molecules, Pol localized within the cell nucleus but showed a general diffuse intranuclear distribution. In uninfected cells transfected with a plasmid expressing Pol, Pol similarly showed a diffuse intranuclear distribution. Therefore, Pol can localize to the cell nucleus without other viral proteins, but functional ICP8 is required for Pol to localize to prereplicative sites. In cells infected with mutant viruses encoding defective Pol molecules, ICP8 localized to prereplicative sites. Thus, Pol or the portions of Pol not expressed by the mutant viruses are not essential for the formation of prereplicative sites or the localization of ICP8 to these structures. These results demonstrate that a specific nuclear protein can influence the intranuclear location of another nuclear protein.
机译:我们使用间接免疫荧光来检查决定感染的细胞中单纯疱疹病毒(HSV)DNA聚合酶(Pol)的核内位置的因素。在没有病毒DNA复制的情况下,HSV Pol与HSV DNA结合蛋白ICP8共同定位在核框架相关结构中,称为复制前位点。在存在病毒DNA复制的情况下,HSV Pol与ICP8共同定位在称为复制区隔的球状核内结构中。在感染编码有缺陷的ICP8分子的突变病毒的细胞中,Pol位于细胞核内,但显示出普遍的弥散性核内分布。在用表达Pol的质粒转染的未感染细胞中,Pol同样显示出弥散的核内分布。因此,Pol可以定位到细胞核而无需其他病毒蛋白,但是功能化的ICP8是Pol定位到复制前位点所必需的。在感染编码有缺陷的Pol分子的突变病毒的细胞中,ICP8定位于复制前的位点。因此,Pol或不由突变病毒表达的Pol部分对于形成复制前位点或ICP8定位于这些结构不是必需的。这些结果表明,特定的核蛋白可以影响另一种核蛋白的核内位置。

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