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猿猴水痘病毒基因28和29启动子共享一个共同的上游刺激因子结合位点,并由IE62反式激活诱导。

Simian varicella virus gene 28 and 29 promoters share a common upstream stimulatory factor-binding site and are induced by IE62 transactivation.

作者信息

Ou Yang, Gray Wayne L

机构信息

Department of Microbiology and Immunology, University of Arkansas for Medical Sciences, 4301 W. Markham Street, Little Rock, AR 72205, USA.

出版信息

J Gen Virol. 2006 Jun;87(Pt 6):1501-1508. doi: 10.1099/vir.0.81645-0.

DOI:10.1099/vir.0.81645-0
PMID:16690914
Abstract

Simian varicella virus (SVV) is a neurotropic alphaherpesvirus that causes a natural, varicella-like disease in non-human primates. After resolution of the primary disease, SVV, like its human counterpart, varicella-zoster virus (VZV), establishes latent infection in the neural ganglia of the host. In this study, gene expression of SVV open reading frames (ORFs) 28 and 29, which encode the viral DNA polymerase and DNA-binding protein, respectively, was characterized during lytic infection of Vero cells. The results indicate that the intergenic region controlling gene 28 and 29 expression includes overlapping, divergent promoters. The ORF 28 and 29 promoters are active in SVV-infected Vero cells, but not in uninfected cells. The SVV immediate-early gene 62 (IE62) product transactivates ORF 28 and 29 expression, and a cellular upstream stimulatory factor-binding site is important for efficient IE62 induction of genes 28 and 29. DNA sequence analysis of the 185 bp intergenic region identified putative cellular transcription factor-binding sites. Transcriptional analysis mapped ORF 28 and 29 RNA start sites. A recombinant SVV was employed to demonstrate that the ORF 29 promoter can express a heterologous gene (green fluorescent protein) when inserted into a novel site (the ORF 12/13 intergenic region) within the SVV genome. The findings demonstrate similarities between SVV and VZV ORF 28/29 expression and indicate that the simian varicella model may be useful to investigate the differential regulation of viral genes during lytic and latent infection.

摘要

猴水痘病毒(SVV)是一种嗜神经性α疱疹病毒,可在非人灵长类动物中引发自然的水痘样疾病。原发性疾病消退后,SVV与其人类对应病毒水痘-带状疱疹病毒(VZV)一样,在宿主神经节中建立潜伏感染。在本研究中,对分别编码病毒DNA聚合酶和DNA结合蛋白的SVV开放阅读框(ORF)28和29在Vero细胞裂解感染期间的基因表达进行了表征。结果表明,控制基因28和29表达的基因间隔区包括重叠、反向的启动子。ORF 28和29启动子在感染SVV的Vero细胞中具有活性,但在未感染的细胞中无活性。SVV立即早期基因62(IE62)产物可反式激活ORF 28和29的表达,且一个细胞上游刺激因子结合位点对于IE62有效诱导基因28和29很重要。对185 bp基因间隔区的DNA序列分析确定了假定的细胞转录因子结合位点。转录分析绘制了ORF 28和29的RNA起始位点。使用重组SVV证明,当将ORF 29启动子插入SVV基因组内的一个新位点(ORF 12/13基因间隔区)时,它可以表达一个异源基因(绿色荧光蛋白)。这些发现证明了SVV和VZV的ORF 28/29表达之间的相似性,并表明猴水痘模型可能有助于研究裂解感染和潜伏感染期间病毒基因的差异调控。

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1
Simian varicella virus gene 28 and 29 promoters share a common upstream stimulatory factor-binding site and are induced by IE62 transactivation.猿猴水痘病毒基因28和29启动子共享一个共同的上游刺激因子结合位点,并由IE62反式激活诱导。
J Gen Virol. 2006 Jun;87(Pt 6):1501-1508. doi: 10.1099/vir.0.81645-0.
2
Sequence analysis of the leftward end of simian varicella virus (EcoRI-I fragment) reveals the presence of an 8-bp repeat flanking the unique long segment and an 881-bp open-reading frame that is absent in the varicella zoster virus genome.猴水痘病毒左端(EcoRI-I片段)的序列分析显示,在独特的长片段侧翼存在一个8碱基对重复序列,以及一个水痘带状疱疹病毒基因组中不存在的881碱基对开放阅读框。
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The DNA element controlling expression of the varicella-zoster virus open reading frame 28 and 29 genes consists of two divergent unidirectional promoters which have a common USF site.控制水痘带状疱疹病毒开放阅读框28和29基因表达的DNA元件由两个具有共同USF位点的反向单向启动子组成。
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Simian varicella virus gene 61 encodes a viral transactivator but is non-essential for in vitro replication.猿猴水痘病毒基因61编码一种病毒反式激活因子,但对体外复制并非必需。
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Transactivation of the simian varicella virus (SVV) open reading frame (ORF) 21 promoter by SVV ORF 62 is upregulated in neuronal cells but downregulated in non-neuronal cells by SVV ORF 63 protein.猿猴水痘病毒(SVV)开放阅读框(ORF)62对SVV开放阅读框21启动子的反式激活在神经元细胞中上调,但在非神经元细胞中被SVV ORF 63蛋白下调。
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DNA sequence of a simian varicella virus gene that encodes a homologue of varicella zoster virus IE62 and herpes simplex virus ICP4.一种编码水痘带状疱疹病毒IE62和单纯疱疹病毒ICP4同源物的猴水痘病毒基因的DNA序列。
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Varicella-zoster virus gene 21: transcriptional start site and promoter region.水痘带状疱疹病毒基因21:转录起始位点和启动子区域。
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Transcriptional analysis of two simian varicella virus glycoprotein genes which are homologous to varicella-zoster virus gpI (gE) and gpIV (gI).对两个与水痘-带状疱疹病毒gpI(gE)和gpIV(gI)同源的猴水痘病毒糖蛋白基因的转录分析。
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The simian varicella virus ORF A is expressed in infected cells but is non-essential for replication in cell culture.猴痘病毒 ORF A 在受感染的细胞中表达,但对于细胞培养中的复制并非必需。
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Simian Varicella Virus: Molecular Virology and Mechanisms of Pathogenesis.猴痘病毒:分子病毒学与发病机制。
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Arch Virol. 2012 Sep;157(9):1803-6. doi: 10.1007/s00705-012-1367-y. Epub 2012 Jun 8.
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Arch Virol. 2011 May;156(5):739-46. doi: 10.1007/s00705-010-0889-4. Epub 2011 Apr 13.
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