Details

Autor(en) / Beteiligte

• Gabe, Maria Buur Nordskov
• Skov-Jeppesen, Kirsa
• Gasbjerg, Lærke Smidt
• Schiellerup, Sine Pasch
• Martinussen, Christoffer
• Gadgaard, Sarina
• Boer, Geke Aline
• Oeke, Jannika
• Torz, Lola Julia
• Veedfald, Simon
• Svane, Maria Saur
• Bojsen-Møller, Kirstine Nyvold
• Madsbad, Sten
• Holst, Jens Juul
• Hartmann, Bolette
• Rosenkilde, Mette Marie

Titel

GIP and GLP-2 together improve bone turnover in humans supporting GIPR-GLP-2R co-agonists as future osteoporosis treatment

Ist Teil von

• Pharmacological research, 2022-02, Vol.176, p.106058, Article 106058

Ort / Verlag

Netherlands: Elsevier Ltd

Erscheinungsjahr

2022

Link zum Volltext

Quelle

MEDLINE

Beschreibungen/Notizen

• The intestinal hormones glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-2 (GLP-2) are key regulators of postprandial bone turnover in humans. We hypothesized that GIP and GLP-2 co-administration would provide stronger effect on bone turnover than administration of the hormones separately, and tested this using subcutaneous injections of GIP and GLP-2 alone or in combination in humans. Guided by these findings, we designed series of GIPR-GLP-2R co-agonists as template for new osteoporosis treatment. The clinical experiment was a randomized cross-over design including 10 healthy men administered subcutaneous injections of GIP and GLP-2 alone or in combination. The GIPR-GLP-2R co-agonists were characterized in terms of binding and activation profiles on human and rodent GIP and GLP-2 receptors, and their pharmacokinetic (PK) profiles were improved by dipeptidyl peptidase-4 protection and site-directed lipidation. Co-administration of GIP and GLP-2 in humans resulted in an additive reduction in bone resorption superior to each hormone individually. The GIPR-GLP-2R co-agonists, designed by combining regions of importance for cognate receptor activation, obtained similar efficacies as the two native hormones and nanomolar potencies on both human receptors. The PK-improved co-agonists maintained receptor activity along with their prolonged half-lives. Finally, we found that the GIPR-GLP-2R co-agonists optimized toward the human receptors for bone remodeling are not feasible for use in rodent models. The successful development of potent and efficacious GIPR-GLP-2R co-agonists, combined with the improved effect on bone metabolism in humans by co-administration, support these co-agonists as a future osteoporosis treatment. [Display omitted] •GIP and GLP-2 reduce bone resorption and GIP also stimulates bone formation in humans.•Co-administration of GIP and GLP-2 additively reduce bone formation in humans.•We have developed uni-molecular potent and efficacious GIPR-GLP-2R co-agonists.•GIPR-GLP-2R co-agonists may be a potential new future treatment of osteoporosis.