- Zhang, Cai;
- Seo, Joonbae;
- Murakami, Kazutoshi;
- Salem, Esam SB;
- Bernhard, Elise;
- Borra, Vishnupriya J;
- Choi, Kwangmin;
- Yuan, Celvie L;
- Chan, Calvin C;
- Chen, Xiaoting;
- Huang, Taosheng;
- Weirauch, Matthew T;
- Divanovic, Senad;
- Qi, Nathan R;
- Thomas, Hala Einakat;
- Mercer, Carol A;
- Siomi, Haruhiko;
- Nakamura, Takahisa
RNA silencing inhibits mRNA translation. While mRNA translation accounts for the majority of cellular energy expenditure, it is unclear if RNA silencing regulates energy homeostasis. Here, we report that hepatic Argonaute 2 (Ago2)-mediated RNA silencing regulates both intrinsic energy production and consumption and disturbs energy metabolism in the pathogenesis of obesity. Ago2 regulates expression of specific miRNAs including miR-802, miR-103/107, and miR-148a/152, causing metabolic disruption, while simultaneously suppressing the expression of genes regulating glucose and lipid metabolism, including Hnf1β, Cav1, and Ampka1. Liver-specific Ago2-deletion enhances mitochondrial oxidation and ATP consumption associated with mRNA translation, which results in AMPK activation, and improves obesity-associated pathophysiology. Notably, hepatic Ago2-deficiency improves glucose metabolism in conditions of insulin receptor antagonist treatment, high-fat diet challenge, and hepatic AMPKα1-deletion. The regulation of energy metabolism by Ago2 provides a novel paradigm in which RNA silencing plays an integral role in determining basal metabolic activity in obesity-associated sequelae.