| Literature DB >> 33718833 |
Seul Gi Kang1,2, Min Jeong Choi1,2, Saet-Byel Jung1, Hyo Kyun Chung1, Joon Young Chang1,2, Jung Tae Kim1,2, Yea Eun Kang1,3, Ju Hee Lee1,3, Hyun Jung Hong1,2, Sang Mi Jun4,5, Hyun-Joo Ro4,5, Jae Myoung Suh6, Hail Kim6, Johan Auwerx7, Hyon-Seung Yi1,2,3, Minho Shong1,2,3.
Abstract
Perturbation of mitochondrial proteostasis provokes cell autonomous and cell non-autonomous responses that contribute to homeostatic adaptation. Here, we demonstrate distinct metabolic effects of hepatic metabokines as cell non-autonomous factors in mice with mitochondrial OxPhos dysfunction. Liver-specific mitochondrial stress induced by a loss-of-function mutation in Crif1 (LKO) leads to aberrant oxidative phosphorylation and promotes the mitochondrial unfolded protein response. LKO mice are highly insulin sensitive and resistant to diet-induced obesity. The hepatocytes of LKO mice secrete large quantities of metabokines, including GDF15 and FGF21, which confer metabolic benefits. We evaluated the metabolic phenotypes of LKO mice with global deficiency of GDF15 or FGF21 and show that GDF15 regulates body and fat mass and prevents diet-induced hepatic steatosis, whereas FGF21 upregulates insulin sensitivity, energy expenditure, and thermogenesis in white adipose tissue. This study reveals that the mitochondrial integrated stress response (ISRmt) in liver mediates metabolic adaptation through hepatic metabokines.Entities:
Keywords: Cell Biology; Physiology; Systems Biology
Year: 2021 PMID: 33718833 PMCID: PMC7920832 DOI: 10.1016/j.isci.2021.102181
Source DB: PubMed Journal: iScience ISSN: 2589-0042