Scully A L, Sommer M H, Schwartz R, Spector D H
Department of Biology, University of California, San Diego, La Jolla 92093-0357, USA.
J Virol. 1995 Oct;69(10):6533-40. doi: 10.1128/JVI.69.10.6533-6540.1995.
The 86-kDa immediate-early 2 protein (IE2 86) of human cytomegalovirus is a powerful transactivator of homologous and heterologous promoters, including the human cytomegalovirus 1.2-kb RNA early promoter. Two potential mechanisms for gene activation by IE2 86 include interaction with cellular proteins and direct DNA binding. In this report, we show that the 1.2-kb RNA promoter contains a cis-acting AP-1 site, critical for its activation by IE2 86 in vivo, and that IE2 86, purified as a glutathione S-transferase-IE86 fusion protein, can interact with c-Jun and JunB. Additionally, by coimmunoprecipitation, we document that JunB and IE2 86 do associate in vivo. Further in vitro analysis reveals that Fos proteins are able to associate with glutathione S-transferase-IE86 only when present as a Jun-Fos heterodimer. With a set of IE2 86 mutants, we demonstrate that three independent regions of the IE2 86 interact in vitro with c-Jun, two of which are essential for activation of the 1.2-kb RNA promoter in vivo. We also show that IE2 86 can bind directly to this promoter through a sequence located just upstream of the AP-1 site between nucleotides -125 and -97. This discrete domain shares sequence homology with the cis-repression signal on the IE gene.
人巨细胞病毒的86-kDa立即早期2蛋白(IE2 86)是同源和异源启动子的强大反式激活因子,包括人巨细胞病毒1.2-kb RNA早期启动子。IE2 86激活基因的两种潜在机制包括与细胞蛋白相互作用和直接结合DNA。在本报告中,我们表明1.2-kb RNA启动子含有一个顺式作用的AP-1位点,该位点对其在体内被IE2 86激活至关重要,并且作为谷胱甘肽S-转移酶-IE86融合蛋白纯化的IE2 86可以与c-Jun和JunB相互作用。此外,通过共免疫沉淀,我们证明JunB和IE2 86在体内确实存在关联。进一步的体外分析表明,Fos蛋白只有以Jun-Fos异二聚体形式存在时才能与谷胱甘肽S-转移酶-IE86结合。利用一组IE2 86突变体,我们证明IE2 86的三个独立区域在体外与c-Jun相互作用,其中两个区域对体内1.2-kb RNA启动子的激活至关重要。我们还表明,IE2 86可以通过位于AP-1位点上游核苷酸-125和-97之间的序列直接结合该启动子。这个离散结构域与IE基因上的顺式抑制信号具有序列同源性。
