Autophagy mediates the mitotic senescence transition
Cancer Research UK Cambridge Center · Cancer Research UK · +4 more institutions
Abstract
As a stress response, senescence is a dynamic process involving multiple effector mechanisms whose combination determines the phenotypic quality. Here we identify autophagy as a new effector mechanism of senescence. Autophagy is activated during senescence and its activation is correlated with negative feedback in the PI3K-mammalian target of rapamycin (mTOR) pathway. A subset of autophagy-related genes are up-regulated during senescence: Overexpression of one of those genes, ULK3, induces autophagy and senescence. Furthermore, inhibition of autophagy delays the senescence phenotype, including senescence-associated secretion. Our data suggest that autophagy, and its consequent protein turnover, mediate the…
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Authors
11Topics & keywords
- Autophagy
- Senescence
- Biology
- Cell biology
- Effector
- Phenotype
- PI3K/AKT/mTOR pathway
- Gene