首页> 美国卫生研究院文献>The Journal of General Virology >The UL15 protein of herpes simplex virus type 1 is necessary for the localization of the UL28 and UL33 proteins to viral DNA replication centres
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The UL15 protein of herpes simplex virus type 1 is necessary for the localization of the UL28 and UL33 proteins to viral DNA replication centres

机译:1型单纯疱疹病毒的UL15蛋白对于将UL28和UL33蛋白定位到病毒DNA复制中心是必需的

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摘要

The UL15, UL28 and UL33 proteins of herpes simplex virus type 1 (HSV-1) are thought to comprise a terminase complex responsible for cleavage and packaging of the viral genome into pre-assembled capsids. Immunofluorescence studies confirmed that shortly after infection with wild-type HSV-1 these three proteins localize to viral DNA replication compartments within the nucleus, identified by the presence of the single-stranded DNA-binding protein, ICP8. In cells infected with either UL28- or UL33-null mutants, the other two terminase proteins also co-localized with ICP8. In contrast, neither UL28 nor UL33 was detectable in replication compartments following infection with a UL15-null mutant, although Western blot analysis showed they were present in normal amounts in the infected cells. Provision of UL15 in a complementing cell line restored the ability of all three proteins to localize to replication compartments. These data indicate that UL15 plays a key role in localizing the terminase complex to DNA replication compartments, and that it can interact independently with UL28 and UL33.
机译:单纯疱疹病毒1型(HSV-1)的UL15,UL28和UL33蛋白被认为包含一个末端酶复合物,负责将病毒基因组切割和包装成预先组装的衣壳。免疫荧光研究证实,在感染野生型HSV-1后不久,这三种蛋白就定位于细胞核内的病毒DNA复制区室,这是由单链DNA结合蛋白ICP8的存在所确定的。在感染了UL28-或UL33-null突变体的细胞中,其他两个末端酶蛋白也与ICP8共定位。相比之下,在用UL15-null突变体感染后,复制隔室中均未检测到UL28和UL33,尽管Western印迹分析表明它们在感染的细胞中以正常量存在。在补体细胞系中提供UL15恢复了所有三种蛋白质定位于复制区室的能力。这些数据表明,UL15在将末端酶复合物定位于DNA复制区室中起关键作用,并且它可以与UL28和UL33独立相互作用。

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