| Literature DB >> 26687681 |
Chin-Chih Liu1, Yu-Ching Lin1, Yu-Hsuan Chen1, Chun-Ming Chen2, Liang-Yu Pang3, Hsuan-An Chen2, Pei-Rung Wu2, Mei-Yao Lin2, Si-Tse Jiang4, Ting-Fen Tsai5, Ruey-Hwa Chen6.
Abstract
Autophagy, a cellular self-eating mechanism, is important for maintaining cell survival and tissue homeostasis in various stressed conditions. Although the molecular mechanism of autophagy induction has been well studied, how cells terminate autophagy process remains elusive. Here, we show that ULK1, a serine/threonine kinase critical for autophagy initiation, is a substrate of the Cul3-KLHL20 ubiquitin ligase. Upon autophagy induction, ULK1 autophosphorylation facilitates its recruitment to KLHL20 for ubiquitination and proteolysis. This autophagy-stimulated, KLHL20-dependent ULK1 degradation restrains the amplitude and duration of autophagy. Additionally, KLHL20 governs the degradation of ATG13, VPS34, Beclin-1, and ATG14 in prolonged starvation through a direct or indirect mechanism. Impairment of KLHL20-mediated regulation of autophagy dynamics potentiates starvation-induced cell death and aggravates diabetes-associated muscle atrophy. Our study identifies a key role of KLHL20 in autophagy termination by controlling autophagy-dependent turnover of ULK1 and VPS34 complex subunits and reveals the pathophysiological functions of this autophagy termination mechanism.Entities:
Keywords: ULK1; VPS34 complex; autophagy; ubiquitination
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Year: 2015 PMID: 26687681 DOI: 10.1016/j.molcel.2015.11.001
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970