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水痘-带状疱疹病毒gB和gE共表达而非单独的gB或gE表达,会导致大量融合及形成与gH和gL共表达时相当的多核巨细胞。

Varicella-zoster Virus gB and gE coexpression, but not gB or gE alone, leads to abundant fusion and syncytium formation equivalent to those from gH and gL coexpression.

作者信息

Maresova L, Pasieka T J, Grose C

机构信息

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

出版信息

J Virol. 2001 Oct;75(19):9483-92. doi: 10.1128/JVI.75.19.9483-9492.2001.

Abstract

Varicella-zoster virus (VZV) is distinguished from herpes simplex virus type 1 (HSV-1) by the fact that cell-to-cell fusion and syncytium formation require only gH and gL within a transient-expression system. In the HSV system, four glycoproteins, namely, gH, gL, gB, and gD, are required to induce a similar fusogenic event. VZV lacks a gD homologous protein. In this report, the role of VZV gB as a fusogen was investigated and compared to the gH-gL complex. First of all, the VZV gH-gL experiment was repeated under a different set of conditions; namely, gH and gL were cloned into the same vaccinia virus (VV) genome. Surprisingly, the new expression system demonstrated that a recombinant VV-gH+gL construct was even more fusogenic than seen in the prior experiment with two individual expression plasmids containing gH and gL (K. M. Duus and C. Grose, J. Virol. 70:8961-8971, 1996). Recombinant VV expressing VZV gB by itself, however, effected the formation of only small syncytia. When VZV gE and gB genes were cloned into one recombinant VV genome and another fusion assay was performed, extensive syncytium formation was observed. The degree of fusion with VZV gE-gB coexpression was comparable to that observed with VZV gH-gL: in both cases, >80% of the cells in a monolayer were fused. Thus, these studies established that VZV gE-gB coexpression greatly enhanced the fusogenic properties of gB. Control experiments documented that the fusion assay required a balance between the fusogenic potential of the VZV glycoproteins and the fusion-inhibitory effect of the VV infection itself.

摘要

水痘带状疱疹病毒(VZV)与1型单纯疱疹病毒(HSV-1)的区别在于,在瞬时表达系统中,细胞间融合和多核巨细胞形成仅需糖蛋白gH和gL。在HSV系统中,需要四种糖蛋白,即gH、gL、gB和gD才能诱导类似的融合事件。VZV缺乏gD同源蛋白。在本报告中,研究了VZV gB作为融合原的作用,并与gH-gL复合物进行了比较。首先,在不同的条件下重复VZV gH-gL实验;即,将gH和gL克隆到同一痘苗病毒(VV)基因组中。令人惊讶的是,新的表达系统表明,重组VV-gH+gL构建体比先前用两个分别含有gH和gL的表达质粒进行的实验更具融合性(K.M.Duus和C.Grose,《病毒学杂志》70:8961-8971,1996)。然而,单独表达VZV gB的重组VV仅形成小的多核巨细胞。当将VZV gE和gB基因克隆到一个重组VV基因组中并进行另一项融合试验时,观察到广泛的多核巨细胞形成。VZV gE-gB共表达的融合程度与VZV gH-gL观察到的程度相当:在这两种情况下,单层中>80%的细胞发生融合。因此,这些研究证实VZV gE-gB共表达大大增强了gB的融合特性。对照实验证明,融合试验需要在VZV糖蛋白的融合潜力和VV感染本身的融合抑制作用之间取得平衡。

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