Optimization of GPR40 Agonists for Type 2 Diabetes

Jiwen Jim Liu; Yingcai Wang; Zhihua Ma; Mike Schmitt; Liusheng Zhu; Sean P Brown; Paul J Dransfield; Ying Sun; Rajiv Sharma; Qi Guo; Run Zhuang; Jane Zhang; Jian Luo; George R Tonn; Simon Wong; Gayathri Swaminath; Julio C Medina; Daniel C-H Lin; Jonathan B Houze

doi:10.1021/ml400501x

Optimization of GPR40 Agonists for Type 2 Diabetes

ACS Med Chem Lett. 2014 Feb 6;5(5):517-21. doi: 10.1021/ml400501x. eCollection 2014 May 8.

Authors

Jiwen Jim Liu¹, Yingcai Wang¹, Zhihua Ma¹, Mike Schmitt¹, Liusheng Zhu¹, Sean P Brown¹, Paul J Dransfield¹, Ying Sun¹, Rajiv Sharma¹, Qi Guo¹, Run Zhuang¹, Jane Zhang¹, Jian Luo¹, George R Tonn¹, Simon Wong¹, Gayathri Swaminath¹, Julio C Medina¹, Daniel C-H Lin¹, Jonathan B Houze¹

Affiliation

¹ Department of Therapeutic Discovery, Metabolic Disorders, Translational Sciences, Amgen Inc. , 1120 Veterans Boulevard, South San Francisco, CA 94080, United States.

Abstract

GPR40 (FFA1 and FFAR1) has gained significant interest as a target for the treatment of type 2 diabetes. TAK-875 (1), a GPR40 agonist, lowered hemoglobin A1c (HbA1c) and lowered both postprandial and fasting blood glucose levels in type 2 diabetic patients in phase II clinical trials. We optimized phenylpropanoic acid derivatives as GPR40 agonists and identified AMG 837 (2) as a clinical candidate. Here we report our efforts in searching for structurally distinct back-ups for AMG 837. These efforts led to the identification of more polar GPR40 agonists, such as AM-4668 (10), that have improved potency, excellent pharmacokinetic properties across species, and minimum central nervous system (CNS) penetration.

Keywords: FFA1; FFAR1; GPCR; GPR40; agonist; insulin secretagogue; type II diabetes.