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巨细胞病毒主要立即早期增强子在急性感染和潜伏激活中的作用。

Role of the cytomegalovirus major immediate early enhancer in acute infection and reactivation from latency.

作者信息

Stinski Mark F, Isomura Hiroki

机构信息

Department of Microbiology, Carver College of Medicine, University of Iowa, Iowa City, IA 52242, USA.

出版信息

Med Microbiol Immunol. 2008 Jun;197(2):223-31. doi: 10.1007/s00430-007-0069-7. Epub 2007 Dec 19.

Abstract

The cytomegalovirus (CMV) major immediate early (MIE) enhancer-containing promoter regulates the expression of the downstream MIE genes, which have critical roles in reactivation from latency and acute infection. The enhancer consists of binding sites for cellular transcription factors that are repeated multiple times. The primate and nonprimate CMV enhancers can substitute for one another. The enhancers are not functionally equivalent, but they do have overlapping activities. The CMV MIE enhancers are located between divergent promoters where the leftward genes are critical and essential for reactivation from latency and acute infection and the rightward gene is nonessential. The rightward transcription unit is controlled by an enhancer for murine CMV. In contrast, human CMV has a set of repressor elements that prevents enhancer effects on the rightward viral promoter. The human CMV enhancer that controls the leftward transcription unit has a distal component that is nonessential at high multiplicity of infection (MOI), but has a significant impact on the MIE gene expression at low MOI. The proximal enhancer influences directly the level of transcription of the MIE genes and contains an essential Sp-1 site. The MIE promoter has a site adjacent to the transcription start site that is essential at the earliest stage of infection. The MIE enhancer-containing promoter responds to signal transduction events and to cellular differentiation. The role of the CMV MIE enhancer-containing promoter in acute infection and reactivation from latency are reviewed.

摘要

巨细胞病毒(CMV)主要即刻早期(MIE)含增强子的启动子调控下游MIE基因的表达,这些基因在潜伏激活和急性感染中起关键作用。增强子由多次重复的细胞转录因子结合位点组成。灵长类和非灵长类CMV增强子可相互替代。这些增强子在功能上并非完全等同,但确实具有重叠活性。CMV MIE增强子位于两个不同启动子之间,其中向左的基因对潜伏激活和急性感染至关重要且必不可少,而向右的基因则并非必需。向右的转录单元由鼠CMV的一个增强子控制。相比之下,人CMV有一组阻遏元件,可防止增强子对向右的病毒启动子产生影响。控制向左转录单元的人CMV增强子有一个远端元件,在高感染复数(MOI)时并非必需,但在低MOI时对MIE基因表达有显著影响。近端增强子直接影响MIE基因的转录水平,并包含一个必需的Sp-1位点。MIE启动子在转录起始位点附近有一个位点,在感染的最早阶段是必需的。含CMV MIE增强子的启动子对信号转导事件和细胞分化有反应。本文综述了含CMV MIE增强子的启动子在急性感染和潜伏激活中的作用。

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