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水痘带状疱疹病毒gE逃逸突变体VZV-MSP在感染的细胞培养物和SCID-hu小鼠中均表现出加速的细胞间传播表型。

Varicella-zoster virus gE escape mutant VZV-MSP exhibits an accelerated cell-to-cell spread phenotype in both infected cell cultures and SCID-hu mice.

作者信息

Santos R A, Hatfield C C, Cole N L, Padilla J A, Moffat J F, Arvin A M, Ruyechan W T, Hay J, Grose C

机构信息

Department of Microbiology, University of Iowa, Iowa City, Iowa 52242, USA.

出版信息

Virology. 2000 Sep 30;275(2):306-17. doi: 10.1006/viro.2000.0507.

Abstract

Varicella-zoster virus is considered to have one of the most stable genomes of all human herpesviruses. In 1998, we reported the unanticipated discovery of a wild-type virus that had lost an immunodominant B-cell epitope on the gE ectodomain (VZV-MSP); the gE escape mutant virus exhibited an unusual pattern of egress. Further studies have now documented a markedly enhanced cell-to-cell spread by the mutant virus in cell culture. This property was investigated by laser scanning confocal microscopy combined with a software program that allows the measurement of pixel intensity of the fluorescent signal. For this new application of imaging technology, the VZV immediate early protein 62 (IE 62) was selected as the fluoresceinated marker. By 48 h postinfection, the number of IE 62-positive pixels in the VZV-MSP-infected culture was nearly fourfold greater than the number of pixels in a culture infected with a low-passage laboratory strain. Titrations by infectious center assays supported the above image analysis data. Confirmatory studies in the SCID-hu mouse documented that VZV-MSP spread more rapidly than other VZV strains in human fetal skin implants. Generally, the cytopathology and vesicle formation produced by other strains at 21 days postinfection were demonstrable with VZV-MSP at 14 days. To assess whether additional genes were contributing to the unusual VZV-MSP phenotype, approximately 20 kb of the VZV-MSP genome was sequenced, including ORFs 31 (gB), 37 (gH), 47, 60 (gL), 61, 62 (IE 62), 66, 67 (gI), and 68 (gE). Except for a few polymorphisms, as well as the previously discovered mutation within gE, the nucleotide sequences within most open reading frames were identical to the prototype VZV-Dumas strain. In short, VZV-MSP represents a novel variant virus with a distinguishable phenotype demonstrable in both infected cell cultures and SCID-hu mice.

摘要

水痘带状疱疹病毒被认为是所有人类疱疹病毒中基因组最稳定的病毒之一。1998年,我们报告了一个意外发现,即一种野生型病毒在糖蛋白E(gE)胞外域上失去了一个免疫显性B细胞表位(VZV-MSP);这种gE逃逸突变病毒表现出一种不寻常的释放模式。进一步的研究现已证明,该突变病毒在细胞培养中细胞间传播明显增强。通过激光扫描共聚焦显微镜结合一个允许测量荧光信号像素强度的软件程序对这一特性进行了研究。对于成像技术的这一新应用,选择水痘带状疱疹病毒立即早期蛋白62(IE 62)作为荧光标记物。感染后48小时,VZV-MSP感染培养物中IE 62阳性像素的数量几乎是低传代实验室毒株感染培养物中像素数量的四倍。通过感染中心试验进行的滴定支持了上述图像分析数据。在SCID-hu小鼠中的验证性研究表明,VZV-MSP在人胎儿皮肤植入物中的传播比其他水痘带状疱疹病毒株更快。一般来说,其他毒株在感染后21天产生的细胞病理学和水疱形成在VZV-MSP感染14天时就可显现。为了评估是否有其他基因导致了VZV-MSP的异常表型,对VZV-MSP基因组约20 kb进行了测序,包括开放阅读框31(gB)、37(gH)、47、60(gL)、61、62(IE 62)、66、67(gI)和68(gE)。除了一些多态性以及先前在gE中发现的突变外,大多数开放阅读框内的核苷酸序列与原型VZV-Dumas毒株相同。简而言之,VZV-MSP代表了一种新型变异病毒,其具有在感染细胞培养物和SCID-hu小鼠中均可表现出的可区分表型。

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