Discovery of PF-5190457, a Potent, Selective, and Orally Bioavailable Ghrelin Receptor Inverse Agonist Clinical Candidate

发现 PF-5190457,一种强效、选择性、口服生物可利用的生长素释放肽受体反向激动剂临床候选药物

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作者:Samit K Bhattacharya, Kim Andrews, Ramsay Beveridge, Kimberly O Cameron, Chiliu Chen, Matthew Dunn, Dilinie Fernando, Hua Gao, David Hepworth, V Margaret Jackson, Vishal Khot, Jimmy Kong, Rachel E Kosa, Kimberly Lapham, Paula M Loria, Allyn T Londregan, Kim F McClure, Suvi T M Orr, Jigna Patel, Coli

Abstract

The identification of potent, highly selective orally bioavailable ghrelin receptor inverse agonists from a spiro-azetidino-piperidine series is described. Examples from this series have promising in vivo pharmacokinetics and increase glucose-stimulated insulin secretion in human whole and dispersed islets. A physicochemistry-based strategy to increase lipophilic efficiency for ghrelin receptor potency and retain low clearance and satisfactory permeability while reducing off-target pharmacology led to the discovery of 16h. Compound 16h has a superior balance of ghrelin receptor pharmacology and off-target selectivity. On the basis of its promising pharmacological and safety profile, 16h was advanced to human clinical trials.

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