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调控单纯疱疹病毒立即早期基因转录的DNA序列分析

Analysis of DNA sequences which regulate the transcription of a herpes simplex virus immediate early gene.

作者信息

Preston C M, Cordingley M G, Stow N D

出版信息

J Virol. 1984 Jun;50(3):708-16. doi: 10.1128/JVI.50.3.708-716.1984.

Abstract

The locations and functions of DNA sequences involved in transcription of the gene encoding herpes simplex virus type 1 immediate early (IE) mRNAs 4 and 5 were analyzed by use of a transient-expression assay. The region upstream of the genes encoding IE mRNAs 4 and 5 was fused to the thymidine kinase gene coding sequences, and production of enzyme or RNA was measured after transfection of plasmids into BHK cells. The effect of deletions in the upstream region was determined in the absence or presence of a virus structural component which stimulates herpes simplex virus IE transcription. Two distinct units were identified. One of these was a promoter which required not more than 69 base pairs of DNA specific for the genes encoding IE mRNAs 4 and 5 upstream from the mRNA 5' terminus. The other was a far-upstream region which mediated the response to the virion component and had an upstream boundary between nucleotides -347 and -335. An origin of DNA replication was interposed between these two units. The element TAATGAGATAC , which represents a consensus sequence present in the upstream regions of all herpes simplex type 1 IE genes, appeared to be essential for stimulation by the virion component. The activity of this element was modulated by the sequences which flank it, especially by regions having extremely high contents of guanine plus cytosine and which contain a conserved unit CCCGCCC or its complement GGGCGGG .

摘要

利用瞬时表达分析方法,对单纯疱疹病毒1型即刻早期(IE)mRNA 4和5编码基因转录过程中涉及的DNA序列的位置和功能进行了分析。将编码IE mRNA 4和5的基因上游区域与胸苷激酶基因编码序列融合,在将质粒转染到BHK细胞后,检测酶或RNA的产生情况。在不存在或存在刺激单纯疱疹病毒IE转录的病毒结构成分的情况下,确定上游区域缺失的影响。鉴定出两个不同的单元。其中一个是启动子,它在mRNA 5'末端上游编码IE mRNA 4和5的基因中需要不超过69个碱基对的特异性DNA。另一个是远上游区域,它介导对病毒粒子成分的反应,其上游边界在核苷酸-347和-335之间。DNA复制起点介于这两个单元之间。元件TAATGAGATAC代表所有单纯疱疹病毒1型IE基因上游区域中存在的共有序列,似乎对病毒粒子成分的刺激至关重要。该元件的活性受到其侧翼序列的调节,尤其是鸟嘌呤加胞嘧啶含量极高且包含保守单元CCCGCCC或其互补序列GGGCGGG的区域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9d7c/255728/5dfe718e806e/jvirol00135-0049-a.jpg

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