RRC ID 81966
著者 Martin CK, Samolej J, Olson AT, Bertoli C, Wiebe MS, de Bruin RAM, Mercer J.
タイトル Vaccinia Virus Arrests and Shifts the Cell Cycle.
ジャーナル Viruses
Abstract Modulation of the host cell cycle is a common strategy used by viruses to create a pro-replicative environment. To facilitate viral genome replication, vaccinia virus (VACV) has been reported to alter cell cycle regulation and trigger the host cell DNA damage response. However, the cellular factors and viral effectors that mediate these changes remain unknown. Here, we set out to investigate the effect of VACV infection on cell proliferation and host cell cycle progression. Using a subset of VACV mutants, we characterise the stage of infection required for inhibition of cell proliferation and define the viral effectors required to dysregulate the host cell cycle. Consistent with previous studies, we show that VACV inhibits and subsequently shifts the host cell cycle. We demonstrate that these two phenomena are independent of one another, with viral early genes being responsible for cell cycle inhibition, and post-replicative viral gene(s) responsible for the cell cycle shift. Extending previous findings, we show that the viral kinase F10 is required to activate the DNA damage checkpoint and that the viral B1 kinase and/or B12 pseudokinase mediate degradation of checkpoint effectors p53 and p21 during infection. We conclude that VACV modulates host cell proliferation and host cell cycle progression through temporal expression of multiple VACV effector proteins. (209/200.).
巻・号 14(2)
公開日 2022-2-19
DOI 10.3390/v14020431
PII v14020431
PMID 35216024
PMC PMC8874441
MeSH Cell Cycle / physiology* Cell Proliferation DNA Damage* HCT116 Cells HeLa Cells Host-Pathogen Interactions / genetics* Humans Mutation Tumor Suppressor Protein p53 Vaccinia virus / genetics* Vaccinia virus / physiology Viral Proteins / genetics* Virus Replication
IF 3.816
リソース情報
ヒト・動物細胞 HeLa/Fucci(RCB2812)