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. 2023 Feb 7;35(2):274-286.e10.
doi: 10.1016/j.cmet.2022.12.011. Epub 2023 Jan 10.

Discovery, development, and clinical proof of mechanism of LY3463251, a long-acting GDF15 receptor agonist

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Discovery, development, and clinical proof of mechanism of LY3463251, a long-acting GDF15 receptor agonist

Olivier Benichou et al. Cell Metab. .
Free article

Abstract

GDF15 and its receptor GFRAL/RET form a non-homeostatic system that regulates food intake and body weight in preclinical species. Here, we describe a GDF15 analog, LY3463251, a potent agonist at the GFRAL/RET receptor with prolonged pharmacokinetics. In rodents and obese non-human primates, LY3463251 decreased food intake and body weight with no signs of malaise or emesis. In a first-in-human study in healthy participants, single subcutaneous LY3463251 injections showed a safety and pharmacokinetic profile supporting further clinical development with dose-dependent nausea and emesis in a subset of individuals. A subsequent 12-week multiple ascending dose study in overweight and obese participants showed that LY3463251 induced significant decreases in food intake and appetite scores associated with modest body weight reduction independent of nausea and emesis (clinicaltrials.gov: NCT03764774). These observations demonstrate that agonism of the GFRAL/RET system can modulate energy balance in humans, though the decrease in body weight is surprisingly modest, suggesting challenges in leveraging the GDF15 system for clinical weight-loss applications.

Keywords: GDF15; GFRAL; LY3463251; growth/differentiation factor-15; obesity; overweight; weight loss.

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Conflict of interest statement

Declaration of interests All authors are employees and stockholders of Eli Lilly and Company. The work herein is related to Intl. Patent application publication no. WO 2019/195091 (published 10 October 2019).

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