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卡波西肉瘤相关疱疹病毒ori-Lyt依赖性DNA复制:复制与转录激活因子的双重作用

Kaposi's sarcoma-associated herpesvirus ori-Lyt-dependent DNA replication: dual role of replication and transcription activator.

作者信息

Wang Yan, Tang Qiyi, Maul Gerd G, Yuan Yan

机构信息

Department of Microbiology, School of Dental Medicine, University of Pennsylvania, 240 S. 40th Street, Philadelphia, PA 19104, USA.

出版信息

J Virol. 2006 Dec;80(24):12171-86. doi: 10.1128/JVI.00990-06. Epub 2006 Oct 4.

Abstract

Lytic replication of Kaposi's sarcoma-associated herpesvirus (KSHV) is essential for viral propagation and pathogenicity. In Kaposi's sarcoma lesions, constant lytic replication plays a role in sustaining the population of latently infected cells that otherwise are quickly lost by segregation of latent viral episomes as spindle cells divide. Lytic DNA replication initiates from an origin (ori-Lyt) and requires trans-acting elements. Two functional ori-Lyts have been identified in the KSHV genome. Some cis-acting and trans-acting elements for ori-Lyt-dependent DNA replication have been found. Among these, K8 binding sites, a cluster of C/EBP binding motifs, and a replication and transcription activator (RTA) responsive element (RRE) are crucial cis-acting elements. Binding of K8 and RTA proteins to these motifs in ori-Lyt DNA was demonstrated to be absolutely essential for DNA replication. In the present study, functional roles of RTA in ori-Lyt-dependent DNA replication have been investigated. Two distinct functions of RTA were revealed. First, RTA activates an ori-Lyt promoter and initiates transcription across GC-rich tandem repeats. This RTA-mediated transcription is indispensable for DNA replication. Second, RTA is a component of the replication compartment, where RTA interacts with prereplication complexes composed of at least six core machinery proteins and K8. The prereplication complexes are recruited to ori-Lyt DNA through RTA, which interacts with the RRE, as well as K8, which binds to a cluster of C/EBP binding motifs with the aid of C/EBP alpha. The revelation of these two functions of RTA, together with its role in initiation of a transcriptional cascade that leads to transcription of all viral lytic genes, shows that RTA is a critical initiator and regulator of KSHV lytic DNA replication and viral propagation.

摘要

卡波西肉瘤相关疱疹病毒(KSHV)的裂解性复制对于病毒的传播和致病性至关重要。在卡波西肉瘤病变中,持续的裂解性复制在维持潜伏感染细胞群体方面发挥作用,否则这些细胞会因潜伏病毒附加体在纺锤体细胞分裂时的分离而迅速丢失。裂解性DNA复制从一个起始点(ori-Lyt)开始,并需要反式作用元件。在KSHV基因组中已鉴定出两个功能性ori-Lyt。已经发现了一些ori-Lyt依赖性DNA复制的顺式作用和反式作用元件。其中,K8结合位点、一组C/EBP结合基序以及一个复制和转录激活因子(RTA)反应元件(RRE)是关键的顺式作用元件。已证明K8和RTA蛋白与ori-Lyt DNA中的这些基序结合对于DNA复制绝对必要。在本研究中,对RTA在ori-Lyt依赖性DNA复制中的功能作用进行了研究。揭示了RTA的两种不同功能。首先,RTA激活ori-Lyt启动子并启动跨富含GC的串联重复序列的转录。这种RTA介导的转录对于DNA复制是必不可少的。其次,RTA是复制区室的一个组成部分,在那里RTA与由至少六种核心机制蛋白和K8组成的复制前复合物相互作用。复制前复合物通过RTA被招募到ori-Lyt DNA,RTA与RRE相互作用,以及K8在C/EBPα的帮助下与一组C/EBP结合基序结合。RTA这两种功能的揭示,连同其在引发导致所有病毒裂解基因转录的转录级联反应中的作用,表明RTA是KSHV裂解性DNA复制和病毒传播的关键启动子和调节因子。

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