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A Sequence within the Varicella-Zoster Virus (VZV) OriS Is a Negative Regulator of DNA Replication and Is Bound by a Protein Complex Containing the VZV ORF29 Protein▿

机译:水痘带状疱疹病毒(VZV)OriS内的序列是DNA复制的负调节剂,并受含有VZV ORF29蛋白的蛋白复合物的束缚▿

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摘要

The architecture of the varicella-zoster virus (VZV) origin of DNA replication (OriS) differs significantly from that of the herpes simplex virus (HSV) DNA replication origin. Novel aspects of the VZV OriS include a GA-rich region, three binding sites for the VZV origin-binding protein (OBP) all on the same strand and oriented in the same direction, and a partial OBP binding site of unknown function. We have designated this partial binding site Box D and have investigated the role it plays in DNA replication and flanking gene expression. This has been done with a model system using a replication-competent plasmid containing OriS and a replication- and transcription-competent dual-luciferase reporter plasmid containing both the OriS and the intergenic region between VZV open reading frames (ORFs) 62 and 63. We have found that (i) Box D is a negative regulator of DNA replication independent of flanking gene expression, (ii) the mutation of Box D results in a decrease in flanking gene expression, thus a sequence within the VZV OriS affects transcription, which is in contrast to results reported for HSV-1, (iii) there is a specific Box D complex formed with infected cell extracts in electrophoretic mobility shift assay experiments, (iv) supershift assays show that this complex contains the VZV ORF29 single-strand DNA-binding protein, and (v) the formation of this complex is dependent on the presence of CGC motifs in Box D and its downstream flanking region. These findings show that the VZV ORF29 protein, while required for DNA replication, also plays a novel role in the suppression of that process.
机译:DNA复制(OriS)的水痘带状疱疹病毒(VZV)的结构与单纯疱疹病毒(HSV)DNA复制的结构显着不同。 VZV OriS的新颖方面包括一个富含GA的区域,三个VZV起源结合蛋白(OBP)的结合位点都在同一条链上且方向相同,以及功能未知的部分OBP结合位点。我们指定了这个部分结合位点框D,并研究了它在DNA复制和侧翼基因表达中的作用。这是通过使用包含OriS的具有复制能力的质粒以及包含OriS和VZV开放阅读框(ORF)62和63之间的基因间区域的具有复制和转录能力的双重荧光素酶报告基因质粒的模型系统完成的。已经发现(i)Box D是DNA复制的负调控因子,独立于侧翼基因表达,(ii)Box D的突变导致侧翼基因表达降低,因此VZV OriS中的序列影响转录,这是与报告HSV-1的结果相反,(iii)在电泳迁移率变动实验中与感染的细胞提取物形成了特定的Box D复合物,(iv)超转变试验表明该复合物包含VZV ORF29单链DNA- (v)此复合物的形成取决于盒D及其下游侧翼区域中CGC基序的存在。这些发现表明,VZV ORF29蛋白虽然是DNA复制所必需的,但在抑制该过程中也发挥了新的作用。

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