单纯疱疹病毒立即早期蛋白 ICP0 被 SIAH-1 靶向进行蛋白酶体降解。
Herpes simplex virus immediate-early protein ICP0 is targeted by SIAH-1 for proteasomal degradation.
机构信息
Heinrich Pette Institute-Leibniz Institute for Experimental Virology, Martinistrasse 52, 20251 Hamburg, Germany.
出版信息
J Virol. 2011 Aug;85(15):7644-57. doi: 10.1128/JVI.02207-10. Epub 2011 Jun 1.
Abstract
Herpes simplex virus (HSV) immediate-early protein ICP0 is a transcriptional activator with E3 ubiquitin ligase activity that induces the degradation of ND10 proteins, including the promyelocytic leukemia protein (PML) and Sp100. Moreover, ICP0 has a role in the derepression of viral genomes and in the modulation of the host interferon response to virus infection. Here, we report that ICP0 interacts with SIAH-1, a cellular E3 ubiquitin ligase that is involved in multiple cellular pathways and is itself capable of mediating PML degradation. This novel virus-host interaction profoundly stabilized SIAH-1 and recruited this cellular E3 ligase into ICP0-containing nuclear bodies. Moreover, SIAH-1 mediated the polyubiquitination of HSV ICP0 in vitro and in vivo. After infection of SIAH-1 knockdown cells with HSV, higher levels of ICP0 were produced, ICP0 was less ubiquitinated, and the half-life of this multifunctional viral regulatory protein was increased. These results indicate an inhibitory role of SIAH-1 during lytic infection by targeting ICP0 for proteasomal degradation.
摘要
单纯疱疹病毒 (HSV) 早期即刻蛋白 ICP0 是一种具有 E3 泛素连接酶活性的转录激活因子,可诱导 ND10 蛋白(包括早幼粒细胞白血病蛋白 (PML) 和 Sp100)的降解。此外,ICP0 在病毒基因组的去阻遏以及宿主干扰素对病毒感染反应的调节中发挥作用。在这里,我们报告 ICP0 与 SIAH-1 相互作用,SIAH-1 是一种细胞 E3 泛素连接酶,参与多种细胞途径,本身能够介导 PML 的降解。这种新型的病毒-宿主相互作用使 SIAH-1 高度稳定,并将这种细胞 E3 连接酶募集到含有 ICP0 的核小体中。此外,SIAH-1 在体外和体内介导了 HSV ICP0 的多泛素化。在 SIAH-1 敲低细胞感染 HSV 后,产生了更高水平的 ICP0,ICP0 的泛素化程度降低,这种多功能病毒调节蛋白的半衰期延长。这些结果表明,SIAH-1 通过将 ICP0 靶向蛋白酶体降解来抑制裂解感染。
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