单纯疱疹病毒1型反式激活因子ICP0对DNA依赖性蛋白激酶活性及其催化亚基的抑制作用
Attenuation of DNA-dependent protein kinase activity and its catalytic subunit by the herpes simplex virus type 1 transactivator ICP0.
作者信息
Lees-Miller S P, Long M C, Kilvert M A, Lam V, Rice S A, Spencer C A
机构信息
Department of Biological Sciences, University of Calgary, Alberta, Canada.
出版信息
J Virol. 1996 Nov;70(11):7471-7. doi: 10.1128/JVI.70.11.7471-7477.1996.
Abstract
The DNA-dependent protein kinase (DNA-PK) is involved in several fundamental nuclear processes, including DNA double-strand break repair, V(D)J recombination, and transcription by RNA polymerases I and II. In this study, we show that infection of mammalian cells with herpes simplex virus type 1 attenuates DNA-PK activity by specifically depleting the p350/DNA-PKcs catalytic subunit. The half-life of the p350/DNA-PKcs protein decreases from greater than 24 h to less than 4 h following infection. The depletion of DNA-PK activity and p350/DNA-PKcs abundance is dependent on expression of the viral immediate-early protein ICP0. As ICP0 acts as a promoter-independent transactivator of gene expression, these data suggest that ICP0 may function by directly or indirectly targeting the p350/DNA-PKcs subunit of DNA-PK, thereby altering the inhibitory effects of DNA-PK on RNA polymerase II transcription.
摘要
DNA依赖性蛋白激酶(DNA-PK)参与多种基本的核过程,包括DNA双链断裂修复、V(D)J重组以及RNA聚合酶I和II介导的转录。在本研究中,我们发现单纯疱疹病毒1型感染哺乳动物细胞会通过特异性消耗p350/DNA-PKcs催化亚基来减弱DNA-PK活性。感染后,p350/DNA-PKcs蛋白的半衰期从大于24小时降至小于4小时。DNA-PK活性和p350/DNA-PKcs丰度的消耗依赖于病毒立即早期蛋白ICP0的表达。由于ICP0作为基因表达的启动子非依赖性反式激活因子,这些数据表明ICP0可能通过直接或间接靶向DNA-PK的p350/DNA-PKcs亚基发挥作用,从而改变DNA-PK对RNA聚合酶II转录的抑制作用。
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