Department of Virology, Nagoya University Graduate School of Medicine, Nagoya, Aichi, Japan.
Laboratory of Proteome Research, National Institutes of Biomedical Innovation, Health and Nutrition, Ibaraki, Osaka, Japan.
J Virol. 2019 Apr 3;93(8). doi: 10.1128/JVI.01707-18. Print 2019 Apr 15.
Temporally controlled gene expression is necessary for the propagation of herpesviruses. To achieve this, herpesviruses encode several transcriptional regulators. In Epstein-Barr virus, BcRF1 associates with five viral proteins (BDLF4, BGLF3, BFRF2, BVLF1, and BDLF3.5) to form the viral late (L) gene regulatory complex, which is called the viral preinitiation complex (vPIC), on TATT-containing promoters. However, regulation of the vPIC has been largely unexplored. In this study, we performed two screens using a kinase inhibitor library and identified a series of cyclin-dependent kinase (CDK) inhibitors that downregulated the expression of L genes without any impact on viral DNA replication through destabilization of the BDLF4 protein. Knockdown of CDK2 by short hairpin RNA (shRNA) and proteasome inhibitor treatment showed that phosphorylation of the BDLF4 protein prevented ubiquitin-mediated degradation. Moreover, we demonstrated that cyclin A- and E-associated CDK2 complexes phosphorylated BDLF4 , and we identified several serine/threonine phosphorylation sites in BDLF4. Phosphoinactive and phosphomimic mutants revealed that phosphorylation at threonine 91 plays a role in stabilizing BDLF4. Therefore, our findings indicate that S-like-phase CDKs mediate the regulation of L gene expression through stabilization of the BDLF4 protein, which makes the temporal L gene expression system more robust. Late (L) genes represent more than one-third of the herpesvirus genome, suggesting that many of these genes are indispensable for the life cycle of the virus. With the exception of BCRF1, BDLF2, and BDLF3, Epstein-Barr virus L genes are transcribed by viral regulators, which are known as the viral preinitiation complex (vPIC) and the host RNA polymerase II complex. Because the vPIC is conserved in beta- and gammaherpesviruses, studying the control of viral L gene expression by the vPIC contributes to the development of drugs that specifically inhibit these processes in beta- and gammaherpesvirus infections/diseases. In this study, we demonstrated that CDK inhibitors induced destabilization of the vPIC component BDLF4, leading to a reduction in L gene expression and subsequent progeny production. Our findings suggest that CDK inhibitors may be a therapeutic option against beta- and gammaherpesviruses in combination with existing inhibitors of herpesvirus lytic replication, such as ganciclovir.
瞬时控制基因表达是疱疹病毒复制所必需的。为此,疱疹病毒编码了几种转录调节因子。在 EBV 中,BcRF1 与五种病毒蛋白(BDLF4、BGLF3、BFRF2、BVLF1 和 BDLF3.5)结合形成病毒晚期(L)基因调节复合物,称为病毒起始复合物(vPIC),在 TATT 含有启动子上。然而,vPIC 的调控在很大程度上尚未得到探索。在这项研究中,我们使用激酶抑制剂文库进行了两次筛选,发现了一系列细胞周期蛋白依赖性激酶(CDK)抑制剂,这些抑制剂通过破坏 BDLF4 蛋白的稳定性,在不影响病毒 DNA 复制的情况下下调 L 基因的表达。短发夹 RNA(shRNA)和蛋白酶体抑制剂处理敲低 CDK2 后,BDLF4 蛋白的磷酸化阻止了泛素介导的降解。此外,我们证明了细胞周期蛋白 A 和 E 相关的 CDK2 复合物磷酸化 BDLF4,并在 BDLF4 中鉴定了几个丝氨酸/苏氨酸磷酸化位点。磷酸化和模拟磷酸化突变体表明,苏氨酸 91 的磷酸化在稳定 BDLF4 中起作用。因此,我们的研究结果表明,S 期 CDKs 通过稳定 BDLF4 蛋白来调节 L 基因的表达,这使得时间 L 基因表达系统更加稳健。晚期(L)基因代表疱疹病毒基因组的三分之一以上,这表明这些基因中的许多对于病毒的生命周期是不可或缺的。除了 BCRF1、BDLF2 和 BDLF3 之外,Epstein-Barr 病毒的 L 基因是由病毒调节因子转录的,这些调节因子被称为病毒起始复合物(vPIC)和宿主 RNA 聚合酶 II 复合物。由于 vPIC 在β和γ疱疹病毒中是保守的,因此研究 vPIC 对病毒 L 基因表达的控制有助于开发专门针对β和γ疱疹病毒感染/疾病中这些过程的药物。在这项研究中,我们证明 CDK 抑制剂诱导 vPIC 成分 BDLF4 的不稳定,导致 L 基因表达减少和随后的子代产生减少。我们的研究结果表明,CDK 抑制剂可能是与现有的疱疹病毒裂解复制抑制剂(如更昔洛韦)联合治疗β和γ疱疹病毒的一种治疗选择。
