Genetic Ablation of MiR-22 Fosters Diet-Induced Obesity and NAFLD Development

Monika Gjorgjieva; Cyril Sobolewski; Anne-Sophie Ay; Daniel Abegg; Marta Correia de Sousa; Dorothea Portius; Flavien Berthou; Margot Fournier; Christine Maeder; Pia Rantakari; Fu-Ping Zhang; Matti Poutanen; Didier Picard; Xavier Montet; Serge Nef; Alexander Adibekian; Michelangelo Foti

doi:10.3390/jpm10040170

Genetic Ablation of MiR-22 Fosters Diet-Induced Obesity and NAFLD Development

J Pers Med. 2020 Oct 14;10(4):170. doi: 10.3390/jpm10040170.

Authors

Monika Gjorgjieva¹, Cyril Sobolewski¹, Anne-Sophie Ay¹, Daniel Abegg², Marta Correia de Sousa¹, Dorothea Portius¹, Flavien Berthou¹, Margot Fournier¹, Christine Maeder¹, Pia Rantakari³, Fu-Ping Zhang³, Matti Poutanen³, Didier Picard⁴, Xavier Montet⁵, Serge Nef⁶, Alexander Adibekian², Michelangelo Foti^{1

7}

Affiliations

¹ Department of Cell Physiology and Metabolism, Faculty of Medicine, University of Geneva, 1206 Geneva, Switzerland.
² Department of Chemistry, The Scripps Research Institute, 130 Scripps Way, Jupiter, FL 33458, USA.
³ Institute of Biomedicine, Research Centre for Integrative Physiology and Pharmacology, and Turku Center for Disease Modeling, University of Turku, FI-20014 Turku, Finland.
⁴ Department of Cell Biology, Faculty of Science, University of Geneva, 1205 Geneva, Switzerland.
⁵ Department of Radiology, Faculty of Medicine, University of Geneva, 1206 Geneva, Switzerland.
⁶ Department of Genetic Medicine and Development, Faculty of Medicine, University of Geneva, 1206 Geneva, Switzerland.
⁷ Diabetes Center, Faculty of Medicine, University of Geneva, 1206 Geneva, Switzerland.

Abstract

miR-22 is one of the most abundant miRNAs in the liver and alterations of its hepatic expression have been associated with the development of hepatic steatosis and insulin resistance, as well as cancer. However, the pathophysiological roles of miR-22-3p in the deregulated hepatic metabolism with obesity and cancer remains poorly characterized. Herein, we observed that alterations of hepatic miR-22-3p expression with non-alcoholic fatty liver disease (NAFLD) in the context of obesity are not consistent in various human cohorts and animal models in contrast to the well-characterized miR-22-3p downregulation observed in hepatic cancers. To unravel the role of miR-22 in obesity-associated NAFLD, we generated constitutive Mir22 knockout (miR-22KO) mice, which were subsequently rendered obese by feeding with fat-enriched diet. Functional NAFLD- and obesity-associated metabolic parameters were then analyzed. Insights about the role of miR-22 in NAFLD associated with obesity were further obtained through an unbiased proteomic analysis of miR-22KO livers from obese mice. Metabolic processes governed by miR-22 were finally investigated in hepatic transformed cancer cells. Deletion of Mir22 was asymptomatic when mice were bred under standard conditions, except for an onset of glucose intolerance. However, when challenged with a high fat-containing diet, Mir22 deficiency dramatically exacerbated fat mass gain, hepatomegaly, and liver steatosis in mice. Analyses of explanted white adipose tissue revealed increased lipid synthesis, whereas mass spectrometry analysis of the liver proteome indicated that Mir22 deletion promotes hepatic upregulation of key enzymes in glycolysis and lipid uptake. Surprisingly, expression of miR-22-3p in Huh7 hepatic cancer cells triggers, in contrast to our in vivo observations, a clear induction of a Warburg effect with an increased glycolysis and an inhibited mitochondrial respiration. Together, our study indicates that miR-22-3p is a master regulator of the lipid and glucose metabolism with differential effects in specific organs and in transformed hepatic cancer cells, as compared to non-tumoral tissue.

Keywords: fatty liver disease; glycolysis; lipid metabolism; microRNAs; obesity.

Abstract

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