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单纯疱疹病毒1型基因组内一段序列被宿主细胞因子扩增。

Amplification by host cell factors of a sequence contained within the herpes simplex virus 1 genome.

作者信息

Sears A E, Roizman B

机构信息

Marjorie B. Kovler Viral Oncology Laboratories, University of Chicago, IL 60637.

出版信息

Proc Natl Acad Sci U S A. 1990 Dec;87(23):9441-4. doi: 10.1073/pnas.87.23.9441.

Abstract

We report that a cloned 1620-base-pair (bp) DNA fragment mapping in the BamHI O fragment of herpes simplex virus 1 DNA is amplified after transfection into uninfected cells. The DNA fragment maps entirely within a portion of the open reading frame encoding the large subunit of the viral ribonucleotide reductase and does not contain any of the known lytic origins of viral DNA synthesis. Amplification of this sequence in transfected cells results in accumulation of full-sized Dpn I-resistant plasmids containing the sequence in Hirt extracts of low molecular weight DNA. Subfragments of the 1620-bp fragment were not amplified, whereas larger fragments containing the intact 1620-bp fragment were amplified. The amplification of the fragment in MCF7 cells, which express steroid receptors, was stimulated by the addition of estrogen to the medium. Addition of progesterone, dexamethasone, or testosterone was ineffective. The viral genome therefore contains at least one origin of DNA synthesis capable of supporting replication of viral DNA by cellular factors. The existence of such a host origin of DNA replication in the viral genome was predicted by the hypothesis that viral DNA is amplified by cellular enzymes in sensory neurons harboring latent virus; the link between these sequences and amplification of viral DNA during latency remains to be proven.

摘要

我们报道,将单纯疱疹病毒1型DNA的BamHI O片段中一个克隆的1620碱基对(bp)DNA片段转染到未感染的细胞后会被扩增。该DNA片段完全位于编码病毒核糖核苷酸还原酶大亚基的开放阅读框的一部分内,并且不包含任何已知的病毒DNA合成裂解起始位点。转染细胞中该序列的扩增导致在低分子量DNA的Hirt提取物中积累含有该序列的全长抗Dpn I质粒。1620-bp片段的亚片段未被扩增,而包含完整1620-bp片段的较大片段被扩增。在表达类固醇受体的MCF7细胞中,向培养基中添加雌激素可刺激该片段的扩增。添加孕酮、地塞米松或睾酮则无效。因此,病毒基因组至少包含一个能够支持病毒DNA通过细胞因子进行复制的DNA合成起始位点。病毒基因组中存在这样一个宿主DNA复制起始位点,这是由病毒DNA在携带潜伏病毒的感觉神经元中被细胞酶扩增这一假说所预测的;这些序列与潜伏期间病毒DNA扩增之间的联系仍有待证实。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7780/55181/7857e4fb7124/pnas01048-0379-a.jpg

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