Progress in research of lipogenesis inhibitors for treatment of nonalcoholic fatty liver disease

“…Inflammation-induced inactivation of mitotic fusion 2 activity may impair mitophagy through related pathways, reduce autophagosome formation, and exacerbate hepatic steatosis, leading to the progression of NASH. Activation of mitochondrial enzymes such as peroxisome proliferatoractivated receptor α (PPARα) by specific agonists can significantly increase lipid metabolism and inhibit hepatic steatosis via the miR-21 pathway [40,41].…”

To explore the pathogenesis and scientific connotation of non‐alcoholic fatty liver based on the theory of turbid toxin of traditional Chinese medicine

“…Inflammation-induced inactivation of mitotic fusion 2 activity may impair mitophagy through related pathways, reduce autophagosome formation, and exacerbate hepatic steatosis, leading to the progression of NASH. Activation of mitochondrial enzymes such as peroxisome proliferatoractivated receptor α (PPARα) by specific agonists can significantly increase lipid metabolism and inhibit hepatic steatosis via the miR-21 pathway [40,41].…”

To explore the pathogenesis and scientific connotation of non‐alcoholic fatty liver based on the theory of turbid toxin of traditional Chinese medicine