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一种识别富含GA元件的序列特异性DNA结合蛋白在单纯疱疹病毒1型IE3启动子处与Oct-1协同作用。

A sequence-specific DNA-binding protein recognising a GA-rich element cooperates with Oct-1 at the herpes simplex virus type 1 IE3 promoter.

作者信息

Bailey A C, Thompson R

机构信息

Department of Virology, University of Glasgow, UK.

出版信息

Intervirology. 1992;34(2):74-85. doi: 10.1159/000150265.

Abstract

Herpes simplex virus immediate early (IE) gene transcription is regulated via the upstream TAATGARAT motif and involves the recruitment of the ubiquitous octamer-binding protein Oct-1 and a component of the virion Vmw65 into a multiprotein complex termed the immediate early complex (IEC). An upstream GA-rich element (GA-RE) has been postulated to mediate a response to Vmw65 independent of TAATGARAT. We have studied IEC formation in gel shift assays using DNA fragments containing these sequence elements from the HSV-1 IE gene 3 promoter in different combinations. The results show that a factor which footprints to the GA-RE cooperates with Oct-1 to increase IEC levels on a TAATGARAT motif located 5 bp 5' to the GA-RE. The factor alone is unable to promote IEC formation. We were unable to demonstrate any effect of this factor on a TAATGARAT motif located 16 bp from the GA-RE, suggesting that this effect is not universal for all TAATGARAT motifs.

摘要

单纯疱疹病毒立即早期(IE)基因转录通过上游TAATGARAT基序进行调控,涉及将普遍存在的八聚体结合蛋白Oct-1和病毒体Vmw65的一个组分募集到一个称为立即早期复合体(IEC)的多蛋白复合体中。已推测一个上游富含GA的元件(GA-RE)介导对Vmw65的反应,且不依赖于TAATGARAT。我们利用含有来自HSV-1 IE基因3启动子的这些序列元件的不同组合的DNA片段,在凝胶迁移试验中研究了IEC的形成。结果表明,一个足迹位于GA-RE的因子与Oct-1协同作用,以增加位于GA-RE 5'端5 bp处的TAATGARAT基序上的IEC水平。单独该因子无法促进IEC形成。我们未能证明该因子对距离GA-RE 16 bp处的TAATGARAT基序有任何影响,这表明这种作用并非对所有TAATGARAT基序都普遍存在。

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