DPP-IV-resistant, long-acting oxyntomodulin derivatives

Alessia Santoprete; Elena Capitò; Paul E Carrington; Alessandro Pocai; Marco Finotto; Annunziata Langella; Paolo Ingallinella; Karolina Zytko; Simone Bufali; Simona Cianetti; Maria Veneziano; Fabio Bonelli; Lan Zhu; Edith Monteagudo; Donald J Marsh; Ranabir Sinharoy; Elisabetta Bianchi; Antonello Pessi

doi:10.1002/psc.1328

DPP-IV-resistant, long-acting oxyntomodulin derivatives

J Pept Sci. 2011 Apr;17(4):270-80. doi: 10.1002/psc.1328. Epub 2011 Feb 3.

Authors

Alessia Santoprete¹, Elena Capitò, Paul E Carrington, Alessandro Pocai, Marco Finotto, Annunziata Langella, Paolo Ingallinella, Karolina Zytko, Simone Bufali, Simona Cianetti, Maria Veneziano, Fabio Bonelli, Lan Zhu, Edith Monteagudo, Donald J Marsh, Ranabir Sinharoy, Elisabetta Bianchi, Antonello Pessi

Affiliation

¹ Istituto di Ricerche di Biologia Molecolare P. Angeletti, 00040 Pomezia, Rome, Italy.

PMID: 21294225
DOI: 10.1002/psc.1328

Abstract

Obesity is one of the major risk factors for type 2 diabetes, and the development of agents, that can simultaneously achieve glucose control and weight loss, is being actively pursued. Therapies based on peptide mimetics of the gut hormone glucagon-like peptide 1 (GLP-1) are rapidly gaining favor, due to their ability to increase insulin secretion in a strictly glucose-dependent manner, with little or no risk of hypoglycemia, and to their additional benefit of causing a modest, but durable weight loss. Oxyntomodulin (OXM), a 37-amino acid peptide hormone of the glucagon (GCG) family with dual agonistic activity on both the GLP-1 (GLP1R) and the GCG (GCGR) receptors, has been shown to reduce food intake and body weight in humans, with a lower incidence of treatment-associated nausea than GLP-1 mimetics. As for other peptide hormones, its clinical application is limited by the short circulatory half-life, a major component of which is cleavage by the enzyme dipeptidyl peptidase IV (DPP-IV). SAR studies on OXM, described herein, led to the identification of molecules resistant to DPP-IV degradation, with increased potency as compared to the natural hormone. Analogs derivatized with a cholesterol moiety display increased duration of action in vivo. Moreover, we identified a single substitution which can change the OXM pharmacological profile from a dual GLP1R/GCGR agonist to a selective GLP1R agonist. The latter finding enabled studies, described in detail in a separate study (Pocai A, Carrington PE, Adams JR, Wright M, Eiermann G, Zhu L, Du X, Petrov A, Lassman ME, Jiang G, Liu F, Miller C, Tota LM, Zhou G, Zhang X, Sountis MM, Santoprete A, Capitò E, Chicchi GG, Thornberry N, Bianchi E, Pessi A, Marsh DJ, SinhaRoy R. Glucagon-like peptide 1/glucagon receptor dual agonism reverses obesity in mice. Diabetes 2009; 58: 2258-2266), which highlight the potential of GLP1R/GCGR dual agonists as a potentially superior class of therapeutics over the pure GLP1R agonists currently in clinical use.

MeSH terms

Amino Acid Sequence
Animals
Blood Glucose / drug effects
Body Weight / drug effects
Dipeptidyl Peptidase 4 / metabolism*
Eating / drug effects
Humans
Mice
Molecular Sequence Data
Molecular Structure
Obesity / drug therapy
Oxyntomodulin / chemistry*
Oxyntomodulin / metabolism*
Oxyntomodulin / pharmacology
Oxyntomodulin / therapeutic use
Peptides / chemical synthesis
Peptides / chemistry
Peptides / genetics
Weight Loss / drug effects

Substances

Blood Glucose
Oxyntomodulin
Peptides
Dipeptidyl Peptidase 4