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对参与转录激活和抑制的单纯疱疹病毒1型立即早期蛋白Vmw175进行突变分析。

Mutational dissection of the HSV-1 immediate-early protein Vmw175 involved in transcriptional transactivation and repression.

作者信息

Paterson T, Everett R D

机构信息

Institute of Virology, Glasgow, Scotland.

出版信息

Virology. 1988 Sep;166(1):186-96. doi: 10.1016/0042-6822(88)90160-2.

Abstract

Vmw175 is one of five immediate-early (IE) proteins encoded by herpes simplex virus type-1 (HSV-1). It is required for the transcription of later classes of genes and for the accompanying repression of IE expression. Vmw175 has been shown to be a transactivator of transcription and also to autoregulate its own synthesis. We have made a large number of small, in-frame, insertion and deletion mutants of a plasmid-borne copy of the gene encoding Vmw175. Study of the activity of the resultant mutant polypeptides in transient transfection assays has defined the regions of the protein important for the repression of its own promoter, and for the transactivation of an HSV early promoter in synergy with another HSV IE protein, Vmw110. Large stretches of the protein are relatively unimportant for either function, while the regions most sensitive to disruption correlate to sequences conserved between Vmw175 and VZV 140K, the corresponding transactivating protein of Varicella-Zoster virus. The region from amino acids 275 to 490 is particularly important for both repression and transactivation, whereas that from around 840 to 1100 seems to be more important for transactivation than repression. The nuclear localization signal has been mapped to within residues 682-774.

摘要

Vmw175是由单纯疱疹病毒1型(HSV-1)编码的五种立即早期(IE)蛋白之一。它是后续基因类转录以及随之而来的IE表达抑制所必需的。Vmw175已被证明是一种转录反式激活因子,并且还能自我调节其自身的合成。我们构建了大量编码Vmw175的基因的质粒携带拷贝的小的、框内插入和缺失突变体。在瞬时转染实验中对所得突变多肽活性的研究确定了该蛋白中对于抑制其自身启动子以及与另一种HSV IE蛋白Vmw110协同反式激活HSV早期启动子重要的区域。该蛋白的大片段对这两种功能相对不重要,而对破坏最敏感的区域与Vmw175和水痘带状疱疹病毒(VZV)的相应反式激活蛋白VZV 140K之间保守的序列相关。从氨基酸275到490的区域对抑制和反式激活都特别重要,而从大约840到1100的区域似乎对反式激活比对抑制更重要。核定位信号已定位到682 - 774位残基内。

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