人巨细胞病毒主要立即早期近端增强子中的两个Sp1/Sp3结合位点在病毒复制中起重要作用。
Two Sp1/Sp3 binding sites in the major immediate-early proximal enhancer of human cytomegalovirus have a significant role in viral replication.
作者信息
Isomura Hiroki, Stinski Mark F, Kudoh Ayumi, Daikoku Tohru, Shirata Noriko, Tsurumi Tatsuya
机构信息
Division of Virology, Aichi Cancer Center Research Institute, Chikusa-ku, Nagoya, Japan.
出版信息
J Virol. 2005 Aug;79(15):9597-607. doi: 10.1128/JVI.79.15.9597-9607.2005.
Abstract
We previously demonstrated that the major immediate early (MIE) proximal enhancer containing one GC box and the TATA box containing promoter are minimal elements required for transcription and viral replication in human fibroblast cells (H. Isomura, T. Tsurumi, M. F. Stinski, J. Virol. 78:12788-12799, 2004). After infection, the level of Sp1 increased while Sp3 remained constant. Here we report that either Sp1 or Sp3 transcription factors bind to the GC boxes located at approximately positions -55 and -75 relative to the transcription start site (+1). Both the Sp1 and Sp3 binding sites have a positive and synergistic effect on the human cytomegalovirus (HCMV) major immediate-early (MIE) promoter. There was little to no change in MIE transcription or viral replication for recombinant viruses with one or the other Sp1 or Sp3 binding site mutated. In contrast, mutation of both the Sp1 and Sp3 binding sites caused inefficient MIE transcription and viral replication. These data indicate that the Sp1 and Sp3 binding sites have a significant role in HCMV replication in human fibroblast cells.
摘要
我们先前证明,包含一个GC盒的主要立即早期(MIE)近端增强子和包含TATA盒的启动子是人类成纤维细胞中转录和病毒复制所需的最小元件(H. Isomura、T. Tsurumi、M. F. Stinski,《病毒学杂志》78:12788 - 12799,2004年)。感染后,Sp1水平升高而Sp3保持恒定。在此我们报告,Sp1或Sp3转录因子均结合至相对于转录起始位点(+1)大约位于 -55和 -75位置的GC盒。Sp1和Sp3结合位点对人巨细胞病毒(HCMV)主要立即早期(MIE)启动子均具有正向协同效应。对于具有一个或另一个Sp1或Sp3结合位点发生突变的重组病毒,MIE转录或病毒复制几乎没有变化。相比之下,Sp1和Sp3结合位点均发生突变导致MIE转录和病毒复制效率低下。这些数据表明,Sp1和Sp3结合位点在人成纤维细胞的HCMV复制中具有重要作用。
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