A GIPR antagonist conjugated to GLP-1 analogues promotes weight loss with improved metabolic parameters in preclinical and phase 1 settings

Véniant, Murielle M.; Lu, Shu-Chen; Atangan, Larissa; Komorowski, Renée; Stanislaus, Shanaka; Cheng, Yuan; Wu, Bin; Falsey, James R.; Hager, Todd; Thomas, Veena A.; Ambhaikar, Malhar; Sharpsten, Lucie; Zhu, Yineng; Kurra, Vamsi; Jeswani, Rohini; Oberoi, Rajneet K.; Parnes, Jane R.; Honarpour, Narimon; Neutel, Joel; Strande, Jennifer L.

doi:10.1038/s42255-023-00966-w

articleNature MetabolismFeb 5, 2024HYBRID OA

A GIPR antagonist conjugated to GLP-1 analogues promotes weight loss with improved metabolic parameters in preclinical and phase 1 settings

MMMurielle M. Véniant SLShu-Chen Lu LALarissa Atangan RKRenée Komorowski SSShanaka Stanislaus

Amgen (United States) · Orange County Research Center

PubMed

Indexed incrossrefpubmed

Abstract

Obesity is a major public health crisis. Multi-specific peptides have emerged as promising therapeutic strategies for clinical weight loss. Glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP) are endogenous incretins that regulate weight through their receptors (R). AMG 133 (maridebart cafraglutide) is a bispecific molecule engineered by conjugating a fully human monoclonal anti-human GIPR antagonist antibody to two GLP-1 analogue agonist peptides using amino acid linkers. Here, we confirm the GIPR antagonist and GLP-1R agonist activities in cell-based systems and report the ability of AMG 133 to reduce body weight and improve metabolic markers in male obese mice and…

Citation impact

182

total citations

FWCI: 56.52
Percentile: 100%
References: 42

Citations per year

Authors

20

Topics & keywords

Topics

Keywords

Weight loss
Antagonist
Tolerability
Postprandial
Agonist
Endocrinology
Internal medicine
Receptor

UN Sustainable Development Goals

Good health and well-being

No related works found for this paper.

Funding

A
Amgen