Autophagy regulates lipid metabolism through selective turnover of NCoR1

Selective autophagy ensures the removal of specific soluble proteins, protein aggregates, damaged mitochondria, and invasive bacteria from cells. Defective autophagy has been directly linked to metabolic disorders. However how selective autophagy regulates metabolism remains largely uncharacterized. Here we show that a deficiency in selective autophagy is associated with suppression of lipid oxidation. Hepatic loss of Atg7 or Atg5 significantly impairs the production of ketone bodies upon fasting, due to decreased expression of enzymes involved in beta-oxidation following suppression of transactivation by PPAR alpha. Mechanistically, nuclear receptor co-repressor 1 (NCoR1), which interacts with PPAR alpha to suppress its transactivation, binds to the autophagosomal GABARAP family proteins and is degraded by autophagy. Consequently, loss of autophagy causes accumulation of NCoR1, suppressing PPAR alpha activity and resulting in impaired lipid oxidation. These results suggest that autophagy contributes to PPAR alpha activation upon fasting by promoting degradation of NCoR1 and thus regulates beta-oxidation and ketone bodies production.

Autophagy regulates lipid metabolism through selective turnover of NCoR1

Drug Screening in C. elegans to identify new pharmacological mitochondrial stress inducers

Cold stress-induced autophagy and apoptosis disorders are mainly mediated by AMPK/PPAR/PI3K/AKT/mTOR pathways

Grape polyphenols decrease circulating branched chain amino acids in overfed adults

Drug Screening in C. elegans to identify new pharmacological mitochondrial stress inducers

Cold stress-induced autophagy and apoptosis disorders are mainly mediated by AMPK/PPAR/PI3K/AKT/mTOR pathways

Grape polyphenols decrease circulating branched chain amino acids in overfed adults