Department of Microbial and Molecular Pathogenesis, College of Medicine, Texas A&M Health Science Center, College Station, TX 77843-1114, USA.
Virus Res. 2011 Jun;158(1-2):199-208. doi: 10.1016/j.virusres.2011.04.001. Epub 2011 Apr 12.
The human papillomavirus oncogenic protein, E6, interacts with a number of cellular proteins, and for some targets, E6 directs their degradation through the ubiquitin-proteasome pathway. Post-translational modification with ubiquitin-like modifiers, such as SUMO, also influences protein activities, protein-protein interactions, and protein stability. We report that the high risk HPVE6 proteins reduce the intracellular quantity of the sole SUMO conjugation enzyme, Ubc9, concomitant with decreased host sumoylation. E6 did not significantly influence transcription of Ubc9, indicating that the effects were likely at the protein level. Consistent with typical E6-mediated proteasomal degradation, E6 bound to Ubc9 in vitro, and required E6AP for reduction of Ubc9 levels. Under stable E6 expression conditions in differentiating keratinocytes there was a decrease in Ubc9 and a loss of numerous sumoylated targets indicating a significant perturbation of the normal sumoylation profile. While E6 is known to inhibit PIASy, a SUMO ligase, our results suggest that HPV E6 also targets the Ubc9 protein to modulate host cell sumoylation, suggesting that the sumoylation system may be an important target during viral reproduction and possibly the subsequent development of cervical cancer.
人乳头瘤病毒致癌蛋白 E6 与许多细胞蛋白相互作用,对于某些靶标,E6 通过泛素-蛋白酶体途径指导其降解。泛素样修饰物(如 SUMO)的翻译后修饰也会影响蛋白质活性、蛋白质-蛋白质相互作用和蛋白质稳定性。我们报告称,高危型 HPV E6 蛋白降低了唯一的 SUMO 缀合酶 Ubc9 的细胞内数量,同时宿主的 SUMO 化减少。E6 对 Ubc9 的转录没有显著影响,这表明这些影响可能发生在蛋白质水平。与典型的 E6 介导的蛋白酶体降解一致,E6 在体外与 Ubc9 结合,并且需要 E6AP 来降低 Ubc9 水平。在分化的角质形成细胞中稳定表达 E6 的情况下,Ubc9 减少,许多 SUMO 化靶标丢失,表明正常 SUMO 化谱受到显著干扰。虽然已知 E6 抑制 SUMO 连接酶 PIASy,但我们的结果表明 HPV E6 还靶向 Ubc9 蛋白以调节宿主细胞 SUMO 化,这表明 SUMO 化系统可能是病毒复制期间和随后宫颈癌发展的重要靶标。
