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超级延伸复合物介导的单纯疱疹病毒立即早期基因转录延伸驱动裂解性感染和潜伏激活

Transcriptional Elongation of HSV Immediate Early Genes by the Super Elongation Complex Drives Lytic Infection and Reactivation from Latency.

作者信息

Alfonso-Dunn Roberto, Turner Anne-Marie W, Jean Beltran Pierre M, Arbuckle Jesse H, Budayeva Hanna G, Cristea Ileana M, Kristie Thomas M

机构信息

Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, NIH, Bethesda, MD 20814, USA.

Department of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.

出版信息

Cell Host Microbe. 2017 Apr 12;21(4):507-517.e5. doi: 10.1016/j.chom.2017.03.007.

Abstract

The cellular transcriptional coactivator HCF-1 is required for initiation of herpes simplex virus (HSV) lytic infection and for reactivation from latency in sensory neurons. HCF-1 stabilizes the viral Immediate Early (IE) gene enhancer complex and mediates chromatin transitions to promote IE transcription initiation. In infected cells, HCF-1 was also found to be associated with a network of transcription elongation components including the super elongation complex (SEC). IE genes exhibit characteristics of genes controlled by transcriptional elongation, and the SEC-P-TEFb complex is specifically required to drive the levels of productive IE mRNAs. Significantly, compounds that enhance the levels of SEC-P-TEFb also potently stimulated HSV reactivation from latency both in a sensory ganglia model system and in vivo. Thus, transcriptional elongation of HSV IE genes is a key limiting parameter governing both the initiation of HSV infection and reactivation of latent genomes.

摘要

细胞转录共激活因子HCF-1是单纯疱疹病毒(HSV)裂解感染起始以及感觉神经元中潜伏病毒再激活所必需的。HCF-1可稳定病毒立即早期(IE)基因增强子复合物,并介导染色质转变以促进IE转录起始。在感染细胞中,还发现HCF-1与包括超级延伸复合物(SEC)在内的转录延伸成分网络相关联。IE基因表现出受转录延伸控制的基因特征,并且特别需要SEC-P-TEFb复合物来驱动有活性的IE mRNA水平。值得注意的是,提高SEC-P-TEFb水平的化合物在感觉神经节模型系统和体内均能有效刺激HSV从潜伏状态再激活。因此,HSV IE基因的转录延伸是控制HSV感染起始和潜伏基因组再激活的关键限制参数。

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