Department of Microbiology and Immunology and Emory Vaccine Center, Emory University School of Medicine, Atlanta, Georgia, USA.
J Virol. 2013 Aug;87(15):8651-64. doi: 10.1128/JVI.01052-13. Epub 2013 May 29.
Human cytomegalovirus-encoded UL91 is a betagamma gene that is essential for viral replication. Here we show that the 111-amino-acid (aa) UL91 protein controls accumulation of true-late (γ2) viral transcripts. The primate betaherpesvirus conserved N-terminal region from aa 1 to 71 is sufficient to fully reconstitute function. Evaluation of viral DNA, RNA, and antigen revealed that UL91 protein is expressed with leaky-late (γ1) kinetics, localizes in the nucleus without influencing viral DNA synthesis, and must be present from 48 h postinfection to support full expression of late viral transcripts and proteins. In the absence of UL91, viral capsid assembly in the nucleus of infected cells is significantly reduced, and mature, cytoplasmic virions fail to form. Taken together, the evidence shows that UL91 regulates late viral gene expression by a mechanism that is apparently conserved in betaherpesviruses and gammaherpesviruses.
人巨细胞病毒编码的 UL91 是一个βγ基因,对病毒复制至关重要。在这里,我们发现 111 个氨基酸(aa)的 UL91 蛋白控制真正晚期(γ2)病毒转录物的积累。从 aa1 到 71 的灵长类疱疹病毒保守的 N 端区域足以完全重建功能。对病毒 DNA、RNA 和抗原的评估表明,UL91 蛋白以渗漏晚期(γ1)动力学表达,定位于核内而不影响病毒 DNA 合成,并且必须从感染后 48 小时开始存在,以支持晚期病毒转录物和蛋白质的充分表达。在没有 UL91 的情况下,感染细胞核内的病毒衣壳组装显著减少,成熟的细胞质病毒颗粒无法形成。总之,这些证据表明,UL91 通过一种在β疱疹病毒和γ疱疹病毒中明显保守的机制来调节晚期病毒基因表达。
