衰老
生物
细胞生物学
水泡性口炎病毒
DNA损伤
细胞
表型
细胞周期
病毒
免疫学
遗传学
DNA
基因
作者
Maite Baz-Martínez,Sabela Da Silva‐Álvarez,Estefanía Rodríguez,Jorge Guerra‐Varela,Ahmed El Motiam,Anxo Vidal,Tomás García‐Caballero,Miguel González‐Barcia,Laura Sánchez,César Muñoz‐Fontela,Manuel Collado,Carmen Rivas
摘要
Cellular senescence is often considered a protection mechanism triggered by conditions that impose cellular stress. Continuous proliferation, DNA damaging agents or activated oncogenes are well-known activators of cell senescence. Apart from a characteristic stable cell cycle arrest, this response also involves a proinflammatory phenotype known as senescence-associated secretory phenotype (SASP). This, together with the widely known interference with senescence pathways by some oncoviruses, had led to the hypothesis that senescence may also be part of the host cell response to fight virus. Here, we evaluate this hypothesis using vesicular stomatitis virus (VSV) as a model. Our results show that VSV replication is significantly impaired in both primary and tumor senescent cells in comparison with non-senescent cells, and independently of the stimulus used to trigger senescence. Importantly, we also demonstrate a protective effect of senescence against VSV in vivo. Finally, our results identify the SASP as the major contributor to the antiviral defense exerted by cell senescence in vitro, and points to a role activating and recruiting the immune system to clear out the infection. Thus, our study indicates that cell senescence has also a role as a natural antiviral defense mechanism.
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