This study revealed that mild mitochondrial ribosomal stress in hypothalamic POMC neurons triggers mitohormesis, mediating the metabolic benefits of regular exercise. MOTS-c was identified as a circulating signal elevated during this process, contributing to exercise-induced high-turnover metabolism and improved energy balance.
Abstract
Low-grade mitochondrial stress can promote health and longevity, a phenomenon termed mitohormesis. Here, we demonstrate the opposing metabolic effects of low-level and high-level mitochondrial ribosomal (mitoribosomal) stress in hypothalamic proopiomelanocortin (POMC) neurons. POMC neuron-specific severe mitoribosomal stress due to Crif1 homodeficiency causes obesity in mice. By contrast, mild mitoribosomal stress caused by Crif1 heterodeficiency in POMC neurons leads to high-turnover metabolism and resistance to obesity. These metabolic benefits are mediated by enhanced thermogenesis and mitochondrial unfolded protein responses (UPR) in distal adipose tissues. In POMC neurons, partial Crif1 deficiency increases the expression of β-endorphin (β-END) and mitochondrial DNA-encoded peptide MOTS-c. Central administration of MOTS-c or β-END recapitulates the adipose phenotype of Crif1 heterodeficient mice, suggesting these factors as potential mediators. Consistently, regular running exercise at moderate intensity stimulates hypothalamic MOTS-c/β-END expression and induces adipose tissue UPRand thermogenesis. Our findings indicate that POMC neuronal mitohormesis may underlie exercise-induced high-turnover metabolism.
Authors
Kang, Gil Myoung; Min, Se Hee; Lee, Chan Hee; Kim, Ji Ye; Lim, Hyo Sun; Choi, Min Jeong; Jung, Saet-Byel; Park, Jae Woo; Kim, Seongjun; Park, Chae Beom; Dugu, Hong; Choi, Jong Han; Jang, Won Hee; Park, Se Eun; Cho, Young Min; Kim, Jae Geun; Kim, Kyung-Gon; Choi, Cheol Soo; Kim, Young-Bum; Lee, Changhan; Shong, Minho; Kim, Min-Seon