| Literature DB >> 33915088 |
Yeonghyeon Lee1, Jaejin Kim1, Mi-Sung Kim1, Yoojin Kwon1, Sanghee Shin2, Hyerim Yi2, Hyeonkyeong Kim2, Moon Jong Chang3, Chong Bum Chang4, Seung-Baik Kang3, V Narry Kim2, Jin-Hong Kim2, Jong-Seo Kim2, Stephen J Elledge5, Chanhee Kang6.
Abstract
Cellular senescence is a complex stress response implicated in aging. Autophagy can suppress senescence but is counterintuitively necessary for full senescence. Although its anti-senescence role is well described, to what extent autophagy contributes to senescence establishment and the underlying mechanisms is poorly understood. Here, we show that selective autophagy of multiple regulatory components coordinates the homeostatic state of senescence. We combined a proteomic analysis of autophagy components with protein stability profiling, identifying autophagy substrate proteins involved in several senescence-related processes. Selective autophagy of KEAP1 promoted redox homeostasis during senescence. Furthermore, selective autophagy limited translational machinery components to ameliorate senescence-associated proteotoxic stress. Lastly, selective autophagy of TNIP1 enhanced senescence-associated inflammation. These selective autophagy networks appear to operate in vivo senescence during human osteoarthritis. Our data highlight a caretaker role of autophagy in the stress support network of senescence through regulated protein stability and unravel the intertwined relationship between two important age-related processes.Entities:
Keywords: aging; autophagy; cellular senescence; inflammation; oxidative stress; proteostasis; regulated protein stability; selective autophagy; stress response
Year: 2021 PMID: 33915088 DOI: 10.1016/j.devcel.2021.04.008
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270