GIPR:GCGR co-agonism restores normal weight in obese rodents

Apr 17, 2026Molecular metabolism

Combined activation of two hormone receptors helps obese rodents return to normal weight

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Abstract

Obesity was corrected in mice without functional GLP-1 receptors using a novel GIPR:GCGR co-agonist.

  • Selective GIPR agonism combined with GCGR agonism corrected obesity and improved glucose levels in diet-induced obese mice.
  • Retatrutide, a triagonist, normalized body weight in obese mice lacking GLP-1 receptors.
  • BWB3054, a GIPR:GCGR co-agonist, was identified as comparably effective as retatrutide for reducing excess body weight.
  • BWB3054 demonstrated over 100-fold reduced potency at GLP-1 receptors while still effectively lowering weight in obese mice.
  • Three independent methods confirmed obesity and glycemia correction without GLP-1 agonism, suggesting reduced gastrointestinal side effects.

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