Development of a neuromedin U-human serum albumin conjugate as a long-acting candidate for the treatment of obesity and diabetes. Comparison with the PEGylated peptide

Philippe Neuner; Andrea M Peier; Fabio Talamo; Paolo Ingallinella; Armin Lahm; Gaetano Barbato; Annalise Di Marco; Kunal Desai; Karolina Zytko; Ying Qian; Xiaobing Du; Davide Ricci; Edith Monteagudo; Ralph Laufer; Alessandro Pocai; Elisabetta Bianchi; Donald J Marsh; Antonello Pessi

doi:10.1002/psc.2582

Development of a neuromedin U-human serum albumin conjugate as a long-acting candidate for the treatment of obesity and diabetes. Comparison with the PEGylated peptide

J Pept Sci. 2014 Jan;20(1):7-19. doi: 10.1002/psc.2582. Epub 2013 Nov 13.

Authors

Philippe Neuner¹, Andrea M Peier, Fabio Talamo, Paolo Ingallinella, Armin Lahm, Gaetano Barbato, Annalise Di Marco, Kunal Desai, Karolina Zytko, Ying Qian, Xiaobing Du, Davide Ricci, Edith Monteagudo, Ralph Laufer, Alessandro Pocai, Elisabetta Bianchi, Donald J Marsh, Antonello Pessi

Affiliation

¹ IRBM P. Angeletti, 00040, Pomezia, RM, Italy; NIBR WSJ-507.1.02, Novartis Pharma AG, Campus, CH-4056, Basel, Switzerland.

PMID: 24222478
DOI: 10.1002/psc.2582

Abstract

Neuromedin U (NMU) is an endogenous peptide implicated in the regulation of feeding, energy homeostasis, and glycemic control, which is being considered for the therapy of obesity and diabetes. A key liability of NMU as a therapeutic is its very short half-life in vivo. We show here that conjugation of NMU to human serum albumin (HSA) yields a compound with long circulatory half-life, which maintains full potency at both the peripheral and central NMU receptors. Initial attempts to conjugate NMU via the prevalent strategy of reacting a maleimide derivative of the peptide with the free thiol of Cys34 of HSA met with limited success, because the resulting conjugate was unstable in vivo. Use of a haloacetyl derivative of the peptide led instead to the formation of a metabolically stable conjugate. HSA-NMU displayed long-lasting, potent anorectic, and glucose-normalizing activity. When compared side by side with a previously described PEG conjugate, HSA-NMU proved superior on a molar basis. Collectively, our results reinforce the notion that NMU-based therapeutics are promising candidates for the treatment of obesity and diabetes.

Keywords: conjugate; diabetes; human serum albumin; neuromedin U; obesity.

Publication types

Comparative Study

MeSH terms

Animals
Anti-Obesity Agents / chemical synthesis*
Anti-Obesity Agents / pharmacokinetics
Anti-Obesity Agents / pharmacology
Blood Glucose
Cell Line
Drug Evaluation, Preclinical
Humans
Hypoglycemic Agents / chemical synthesis*
Hypoglycemic Agents / pharmacokinetics
Hypoglycemic Agents / pharmacology
Male
Mice
Mice, Inbred C57BL
Neuropeptides / chemical synthesis*
Neuropeptides / pharmacokinetics
Neuropeptides / pharmacology*
Polyethylene Glycols / pharmacokinetics
Polyethylene Glycols / pharmacology*
Receptors, Neurotransmitter / agonists
Serum Albumin / chemical synthesis*
Serum Albumin / pharmacokinetics
Serum Albumin / pharmacology
Serum Albumin, Human
Weight Loss / drug effects

Substances

Anti-Obesity Agents
Blood Glucose
HSA(IAc)-NMU
Hypoglycemic Agents
Neuropeptides
PEG-NMU
Receptors, Neurotransmitter
Serum Albumin
neuromedin U receptor
Polyethylene Glycols
Serum Albumin, Human