open access publication

Article, 2024

mTORC1 controls murine postprandial hepatic glycogen synthesis via Ppp1r3b

Journal of Clinical Investigation, ISSN 1558-8238, 0021-9738, Volume 134, 7, Page e173782, 10.1172/jci173782

Contributors

Uehara, Kahealani 0000-0003-1142-3466 [1] Lee, Won Dong 0000-0002-2344-171X [2] Stefkovich, Megan L 0000-0002-8983-5551 [1] Biswas, Dipsikha 0000-0003-0990-9678 [3] Santoleri, Dominic A 0000-0002-4468-6564 [1] Whitlock, Anna E Garcia 0000-0003-2980-9885 [1] Quinn, William J. [1] Coopersmith, Talia N. [1] Creasy, Kate Townsend 0000-0003-1870-4586 [1] Rader, Daniel James 0000-0002-9245-9876 [1] Sakamoto, K Kei 0000-0001-8839-5980 [3] Rabinowitz, Joshua Denison 0000-0002-1247-4727 [2] Titchenell, Paul Michael 0000-0002-9941-5649 (Corresponding author) [1]

Affiliations

  1. [1] University of Pennsylvania
    2. [NORA names: United States; America, North; OECD];
  2. [2] Princeton University
    3. [NORA names: United States; America, North; OECD];
  3. [3] University of Copenhagen
    4. [NORA names: KU University of Copenhagen; University; Denmark; Europe, EU; Nordic; OECD]

Abstract

In response to a meal, insulin drives hepatic glycogen synthesis to help regulate systemic glucose homeostasis. The mechanistic target of rapamycin complex 1 (mTORC1) is a well-established insulin target and contributes to the postprandial control of liver lipid metabolism, autophagy, and protein synthesis. However, its role in hepatic glucose metabolism is less understood. Here, we used metabolomics, isotope tracing, and mouse genetics to define a role for liver mTORC1 signaling in the control of postprandial glycolytic intermediates and glycogen deposition. We show that mTORC1 is required for glycogen synthase activity and glycogenesis. Mechanistically, hepatic mTORC1 activity promotes the feeding-dependent induction of Ppp1r3b, a gene encoding a phosphatase important for glycogen synthase activity whose polymorphisms are linked to human diabetes. Reexpression of Ppp1r3b in livers lacking mTORC1 signaling enhances glycogen synthase activity and restores postprandial glycogen content. mTORC1-dependent transcriptional control of Ppp1r3b is facilitated by FOXO1, a well characterized transcriptional regulator involved in the hepatic response to nutrient intake. Collectively, we identify a role for mTORC1 signaling in the transcriptional regulation of Ppp1r3b and the subsequent induction of postprandial hepatic glycogen synthesis.

Keywords

FOXO1, PPP1R3B, activity, complexes 1, content, control, deposition, diabetes, genes, genetics, glucose homeostasis, glucose metabolism, glycogen, glycogen content, glycogen deposition, glycogen synthase activity, glycogen synthesis, glycogenesis, glycolytic intermediates, hepatic glucose metabolism, hepatic glycogen synthesis, homeostasis, human diabetes, induction, insulin, insulin targets, intake, intermediate, isotope tracing, isotopes, lipid metabolism, liver, liver lipid metabolism, mTORC1, mTORC1 activity, mTORC1 signaling, meal, metabolism, metabolomics, mice, mouse genetics, nutrient intake, phosphatase, polymorphism, postprandial control, protein, protein synthesis, rapamycin complex 1, reexpression, regulating systemic glucose homeostasis, regulation, response, response to nutrient intake, signal, synthase activity, synthesis, systemic glucose homeostasis, target, target of rapamycin complex 1, trace, transcriptional control, transcriptional regulation

Funders

  • National Institute of Diabetes and Digestive and Kidney Diseases
  • Novo Nordisk (Denmark)

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