Departamento de Infectómica y Patogénesis Molecular, Centro de Investigación y de Estudios Avanzados del IPN, México City, Mexico.
Departamento de Infectómica y Patogénesis Molecular, Centro de Investigación y de Estudios Avanzados del IPN, México City, Mexico.
Virology. 2020 Nov;550:78-88. doi: 10.1016/j.virol.2020.08.008. Epub 2020 Aug 27.
p53 is implicated in several cellular pathways such as induction of cell-cycle arrest, differentiation, senescence, and apoptosis. p53 is activated by a broad range of stress signals, including viral infections. While some viruses activate p53, others induce its inactivation, and occasionally p53 is differentially modulated during the replicative cycle. During calicivirus infections, apoptosis is required for virus exit and spread into the host; yet, the role of p53 during infection is unknown. By confocal microscopy, we found that p53 associates with FCV VP1, the protease-polymerase NS6/7, and the dsRNA. This interaction was further confirmed by proximity ligation assays, suggesting that p53 participates in the FCV replication. Knocked-down of p53 expression in CrFK cells before infection, resulted in a strong reduction of the non-structural protein levels and a decrease of the viral progeny production. These results indicate that p53 is associated with the viral replication complex and is required for an efficient FCV replication.
p53 参与多种细胞途径,如细胞周期阻滞、分化、衰老和凋亡的诱导。p53 被广泛的应激信号激活,包括病毒感染。虽然一些病毒激活 p53,但其他病毒诱导其失活,偶尔在复制周期中 p53 被差异化调节。在杯状病毒感染期间,凋亡对于病毒的释放和进入宿主传播是必需的;然而,p53 在感染期间的作用尚不清楚。通过共聚焦显微镜,我们发现 p53 与 FCV VP1、蛋白酶-聚合酶 NS6/7 和 dsRNA 结合。通过邻近连接测定进一步证实了这种相互作用,表明 p53 参与了 FCV 的复制。在感染前敲低 CrFK 细胞中的 p53 表达,导致非结构蛋白水平的强烈降低和病毒后代产量的减少。这些结果表明 p53 与病毒复制复合物相关,并且是 FCV 复制所必需的。
