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Pharmacological and physiological activation of TGR5 in the NTS lowers food intake by enhancing leptin-STAT3 signaling

Author

Listed:
  • Kyla Bruce

    (UHN
    University of Toronto)

  • Song-Yang Zhang

    (UHN)

  • Ameth N. Garrido

    (UHN
    University of Toronto)

  • Melissa T. Wang

    (UHN
    University of Toronto)

  • Tomás P. Bachor

    (University of California)

  • Pengcheng Wang

    (Ministry of Education)

  • Allison W. Xu

    (University of California)

  • Zeyu Yang

    (UHN)

  • Tony K. T. Lam

    (UHN
    University of Toronto
    University of Toronto
    University of Toronto)

Abstract

Feeding increases plasma bile acid levels while the nucleus of the solitary tract (NTS) and area postrema (AP) of the brain detect changes in hormones to regulate feeding. However, whether an increase in bile acids activates Takeda G protein-coupled receptor 5 (TGR5) in the NTS and/or AP to lower feeding through a negative feedback pathway is unknown. Here, we discover that infusion of TGR5 agonist CCDC in the NTS of male rats lowered food intake without causing conditional taste avoidance in short-term high fat (HF) fed male rats in association with HF-induced increase in TGR5 expression in the NTS. In contrast, CCDC infusion into the AP failed to lower food intake in HF rats with a reduction in TGR5 expression in the AP. CCDC infusion in the NTS activates TGR5 to reverse HF-induced leptin resistance by enhancing a leptin-leptin receptor-STAT3 signaling axis selectively in the NTS to lower feeding. Finally, metabolomic analysis indicated that HF impaired a refeeding-induced rise of endogenous TGR5 ligand deoxycholic acid in the plasma and subsequently in the NTS in association with hyperphagia, while direct infusion of deoxycholic acid in the NTS of HF rats activated TGR5 to lower feeding and enhanced leptin-STAT3 signaling, thereby altogether demonstrating physiological and pharmacological activation of TGR5 in the NTS regulates food intake. In summary, we discover that an activation of TGR5 in the NTS enhances leptin-STAT3 signaling to lower food intake. Our findings highlight the potential of targeting TGR5 to reverse leptin resistance in the NTS.

Suggested Citation

  • Kyla Bruce & Song-Yang Zhang & Ameth N. Garrido & Melissa T. Wang & Tomás P. Bachor & Pengcheng Wang & Allison W. Xu & Zeyu Yang & Tony K. T. Lam, 2025. "Pharmacological and physiological activation of TGR5 in the NTS lowers food intake by enhancing leptin-STAT3 signaling," Nature Communications, Nature, vol. 16(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-60331-1
    DOI: 10.1038/s41467-025-60331-1
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