腺病毒取代有丝分裂检查点控制。
Adenovirus replaces mitotic checkpoint controls.
作者信息
Turner Roberta L, Groitl Peter, Dobner Thomas, Ornelles David A
机构信息
Department of Microbiology and Immunology, Wake Forest School of Medicine, Winston-Salem, North Carolina, USA.
Heinrich Pette Institute, Leibniz Institute for Experimental Virology, Hamburg, Germany.
出版信息
J Virol. 2015 May;89(9):5083-96. doi: 10.1128/JVI.00213-15. Epub 2015 Feb 18.
UNLABELLED
Infection with adenovirus triggers the cellular DNA damage response, elements of which include cell death and cell cycle arrest. Early adenoviral proteins, including the E1B-55K and E4orf3 proteins, inhibit signaling in response to DNA damage. A fraction of cells infected with an adenovirus mutant unable to express the E1B-55K and E4orf3 genes appeared to arrest in a mitotic-like state. Cells infected early in G1 of the cell cycle were predisposed to arrest in this state at late times of infection. This arrested state, which displays hallmarks of mitotic catastrophe, was prevented by expression of either the E1B-55K or the E4orf3 genes. However, E1B-55K mutant virus-infected cells became trapped in a mitotic-like state in the presence of the microtubule poison colcemid, suggesting that the two viral proteins restrict entry into mitosis or facilitate exit from mitosis in order to prevent infected cells from arresting in mitosis. The E1B-55K protein appeared to prevent inappropriate entry into mitosis through its interaction with the cellular tumor suppressor protein p53. The E4orf3 protein facilitated exit from mitosis by possibly mislocalizing and functionally inactivating cyclin B1. When expressed in noninfected cells, E4orf3 overcame the mitotic arrest caused by the degradation-resistant R42A cyclin B1 variant.
IMPORTANCE
Cells that are infected with adenovirus type 5 early in G1 of the cell cycle are predisposed to arrest in a mitotic-like state in a p53-dependent manner. The adenoviral E1B-55K protein prevents entry into mitosis. This newly described activity for the E1B-55K protein appears to depend on the interaction between the E1B-55K protein and the tumor suppressor p53. The adenoviral E4orf3 protein facilitates exit from mitosis, possibly by altering the intracellular distribution of cyclin B1. By preventing entry into mitosis and by promoting exit from mitosis, these adenoviral proteins act to prevent the infected cell from arresting in a mitotic-like state.
未标记
腺病毒感染会触发细胞DNA损伤反应,其中包括细胞死亡和细胞周期停滞。早期腺病毒蛋白,包括E1B - 55K和E4orf3蛋白,会抑制对DNA损伤的信号传导。感染了无法表达E1B - 55K和E4orf3基因的腺病毒突变体的一部分细胞似乎停滞在类似有丝分裂的状态。在细胞周期G1期早期被感染的细胞在感染后期易倾向于停滞在这种状态。这种表现出有丝分裂灾难特征的停滞状态可通过表达E1B - 55K或E4orf3基因来预防。然而,在存在微管毒物秋水仙酰胺的情况下,E1B - 55K突变病毒感染的细胞会被困在类似有丝分裂的状态,这表明这两种病毒蛋白限制进入有丝分裂或促进从有丝分裂中退出,以防止感染细胞停滞在有丝分裂状态。E1B - 55K蛋白似乎通过与细胞肿瘤抑制蛋白p53相互作用来防止不适当进入有丝分裂。E4orf3蛋白可能通过使细胞周期蛋白B1错误定位并在功能上使其失活来促进从有丝分裂中退出。当在未感染细胞中表达时,E4orf3克服了由抗降解的R42A细胞周期蛋白B1变体引起的有丝分裂停滞。
重要性
在细胞周期G1期早期感染5型腺病毒的细胞易倾向于以p53依赖的方式停滞在类似有丝分裂的状态。腺病毒E1B - 55K蛋白可防止进入有丝分裂。E1B - 55K蛋白这种新描述的活性似乎取决于E1B - 55K蛋白与肿瘤抑制因子p53之间的相互作用。腺病毒E4orf3蛋白促进从有丝分裂中退出,可能是通过改变细胞周期蛋白B1的细胞内分布。通过防止进入有丝分裂和促进从有丝分裂中退出,这些腺病毒蛋白起到防止感染细胞停滞在类似有丝分裂状态的作用。
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