Self-assembled GLP-1/glucagon peptide nanofibrils prolong inhibition of food intake

Oxyntomodulin (Oxm) hormone peptide has a number of beneficial effects on nutrition and metabolism including increased energy expenditure and reduced body weight gain. Despite its many advantages as a potential therapeutic agent, Oxm is subjected to rapid renal clearance and protease degradation lim...

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Veröffentlicht in:Frontiers in endocrinology (Lausanne) 2023-07, Vol.14, p.1217021-1217021
Hauptverfasser: Ouberai, Myriam M, Gomes Dos Santos, Ana L, Kinna, Sonja, Hornigold, David C, Baker, David, Naylor, Jacqueline, Liang, Lihuan, Corkill, Dominic J, Welland, Mark E
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Sprache:eng
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Zusammenfassung:Oxyntomodulin (Oxm) hormone peptide has a number of beneficial effects on nutrition and metabolism including increased energy expenditure and reduced body weight gain. Despite its many advantages as a potential therapeutic agent, Oxm is subjected to rapid renal clearance and protease degradation limiting its clinical application. Previously, we have shown that subcutaneous administration of a fibrillar Oxm formulation can significantly prolong its bioactivity from a few hours to a few days. We used a protease resistant analogue of Oxm, Aib2-Oxm, to form nanfibrils depot and improve serum stability of released peptide. The nanofibrils and monomeric peptide in solution were characterized by spectroscopic, microscopic techniques, potency assay, QCM-D and studies. We show that in comparison to Oxm, Aib2-Oxm fibrils display a slower elongation rate requiring higher ionic strength solutions, and a higher propensity to dissociate. Upon subcutaneous administration of fibrillar Aib2-Oxm in rodents, a 5-fold increase in bioactivity relative to fibrillar Oxm and a significantly longer bioactivity than free Aib2-Oxm were characterized. Importantly, a decrease in food intake was observed up to 72-hour post-administration, which was not seen for free Aib2-Oxm. Our findings provides compelling evidence for the development of long-lasting peptide fibrillar formulations that yield extended plasma exposure and enhanced pharmacological response.
ISSN:1664-2392
1664-2392
DOI:10.3389/fendo.2023.1217021