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用其水痘-带状疱疹病毒对应物替换单纯疱疹病毒1型Vmw175 DNA结合结构域,会产生一种具有新型调节特性且能支持病毒生长的蛋白质。

Replacement of the herpes simplex virus type 1 Vmw175 DNA binding domain with its varicella-zoster virus counterpart results in a protein with novel regulatory properties that can support virus growth.

作者信息

Tyler J K, Orr A, Everett R D

机构信息

MRC Virology Unit, Glasgow, UK.

出版信息

J Gen Virol. 1997 Jan;78 ( Pt 1):179-88. doi: 10.1099/0022-1317-78-1-179.

Abstract

The alphaherpesviruses encode major immediate early transactivator proteins that are essential for the expression of later classes of viral genes. We have previously shown that the extensive sequence similarity between the herpes simplex virus type 1 (HSV-1) and varicella-zoster virus (VZV) members of the family (proteins Vmw175 and VZV140k) extends to function, since a virus which expresses VZV140k in place of Vmw175 is able to grow, albeit at reduced efficiency. We have also shown that the DNA binding characteristics of the isolated DNA binding domains of Vmw175 and VZV140k are related but distinct. In order to assess whether the different DNA binding properties of the two proteins are responsible for the differences in their individual transcriptional regulatory functions, we constructed a plasmid and an HSV-1 virus in which the VZV140k DNA binding domain coding sequences replace those of Vmw175. The characteristics of the resultant hybrid protein in transfection assays and during virus infection suggest that the nature of the DNA binding domain plays a significant role in the transactivation and repression properties of the Vmw1 75 family of proteins.

摘要

α疱疹病毒编码主要立即早期反式激活蛋白,这些蛋白对于后期各类病毒基因的表达至关重要。我们先前已经表明,该病毒家族中单纯疱疹病毒1型(HSV-1)和水痘带状疱疹病毒(VZV)成员(蛋白Vmw175和VZV140k)之间广泛的序列相似性延伸到了功能方面,因为一种表达VZV140k来替代Vmw175的病毒能够生长,尽管效率有所降低。我们还表明,Vmw175和VZV140k分离的DNA结合结构域的DNA结合特性相关但不同。为了评估这两种蛋白不同的DNA结合特性是否导致其各自转录调控功能的差异,我们构建了一个质粒和一种HSV-1病毒,其中VZV140k DNA结合结构域的编码序列取代了Vmw175的编码序列。转染试验和病毒感染期间所得杂交蛋白的特性表明,DNA结合结构域的性质在Vmw175蛋白家族的反式激活和抑制特性中起重要作用。

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