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Rta表达的调控对于γ疱疹病毒感染后病毒和细胞基因的转录起着关键的决定作用。

Control of Rta expression critically determines transcription of viral and cellular genes following gammaherpesvirus infection.

作者信息

Hair James R, Lyons Paul A, Smith Kenneth G C, Efstathiou Stacey

机构信息

Division of Virology, Department of Pathology, University of Cambridge, Tennis Court Road, Cambridge CB2 1QP, UK.

Cambridge Institute for Medical Research and the Department of Medicine, Wellcome Trust/MRC Building, University of Cambridge, Addenbrooke's Hospital, Cambridge CB2 2XY, UK.

出版信息

J Gen Virol. 2007 Jun;88(Pt 6):1689-1697. doi: 10.1099/vir.0.82548-0.

Abstract

The replication and transcriptional activator (Rta), encoded by ORF50 of gammaherpesviruses, initiates the lytic cycle of gene expression; therefore understanding the impact of Rta on viral and cellular gene expression is key to elucidating the transcriptional events governing productive infection and reactivation from latency. To this end, the impact of altering Rta transcription on viral and cellular gene expression was studied in the context of a whole virus infection. Recombinant murine gammaherpesvirus (MHV)-68 engineered to overexpress Rta greatly accelerated expression of specific lytic cycle ORFs, but repressed transcription of the major latency gene, ORF73. Increased expression of Rta accelerated the dysregulation in transcription of specific cellular genes when compared with cells infected with wild-type and revertant viruses. A subset of cellular genes was dysregulated only in cells infected with Rta-overexpressing virus, and never in those infected with non-overexpressing viruses. These data highlight the critical role of Rta abundance in governing viral and cellular gene transcription, and demonstrate the importance of understanding how the relative expression of ORF50 during the virus life cycle impacts on these processes.

摘要

γ疱疹病毒的开放阅读框50(ORF50)编码的复制和转录激活因子(Rta)启动基因表达的裂解周期;因此,了解Rta对病毒和细胞基因表达的影响是阐明控制 productive感染和从潜伏期 reactivation 的转录事件的关键。为此,在全病毒感染的背景下研究了改变Rta转录对病毒和细胞基因表达的影响。经基因工程改造以过表达Rta的重组鼠γ疱疹病毒(MHV)-68极大地加速了特定裂解周期开放阅读框的表达,但抑制了主要潜伏期基因ORF73的转录。与感染野生型和回复病毒的细胞相比,Rta表达的增加加速了特定细胞基因转录的失调。一部分细胞基因仅在感染过表达Rta病毒的细胞中失调,而在感染非过表达病毒的细胞中从未失调。这些数据突出了Rta丰度在控制病毒和细胞基因转录中的关键作用,并证明了了解病毒生命周期中ORF50的相对表达如何影响这些过程的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4212/2884955/c1d1763ac81b/1689fig1.jpg

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