Novel orally active growth hormone secretagogues.

Journal of medicinal chemistry1998PMID: 9733496

Plain Language Summary

Describes a novel class of smaller (500–650 Da) orally bioavailable GH secretagogues developed rationally from ipamorelin by reducing molecular size while retaining in vivo potency in swine. Demonstrates that oral GH secretagogues can be derived from peptide leads through systematic medicinal chemistry strategies.

Abstract

A novel class of growth hormone-releasing compounds with a molecular weight in the range from 500 to 650 has been discovered. The aim of this study was to obtain growth hormone secretagogues with oral bioavailability. By a rational approach we were able to reduce the size of the lead compound ipamorelin (4) and simultaneously to reduce hydrogen-bonding potential by incorporation of backbone isosters while retaining in vivo potency in swine. A rat pituitary assay was used for screening of all compounds and to evaluate which compounds should be tested further for in vivo potency in swine and oral bioavailability, fpo, in dogs. Most of the tested compounds had fpo in the range of 10-55%. In vivo potency in swine after iv dosing is reported, and ED50 was found to be 30 nmol/kg of body weight for the most potent compound.

Authors

Hansen, T K; Ankersen, M; Hansen, B S; Raun, K; Nielsen, K K; Lau, J; Peschke, B; Lundt, B F; Thøgersen, H; Johansen, N L; Madsen, K; Andersen, P H