Discovery of Chromane Propionic Acid Analogues as Selective Agonists of GPR120 with in Vivo Activity in Rodents

Gregory L Adams; Francisco Velazquez; Charles Jayne; Unmesh Shah; Shouwu Miao; Eric R Ashley; Maria Madeira; Taro E Akiyama; Jerry Di Salvo; Takao Suzuki; Nengxue Wang; Quang Truong; Eric Gilbert; Dan Zhou; Andreas Verras; Melissa Kirkland; Michele Pachanski; Maryann Powles; Wu Yin; Feroze Ujjainwalla; Srikanth Venkatraman; Scott D Edmondson

doi:10.1021/acsmedchemlett.6b00394

Discovery of Chromane Propionic Acid Analogues as Selective Agonists of GPR120 with in Vivo Activity in Rodents

ACS Med Chem Lett. 2016 Dec 6;8(1):96-101. doi: 10.1021/acsmedchemlett.6b00394. eCollection 2017 Jan 12.

Authors

Gregory L Adams¹, Francisco Velazquez², Charles Jayne², Unmesh Shah², Shouwu Miao², Eric R Ashley², Maria Madeira², Taro E Akiyama², Jerry Di Salvo², Takao Suzuki³, Nengxue Wang³, Quang Truong², Eric Gilbert², Dan Zhou², Andreas Verras², Melissa Kirkland², Michele Pachanski², Maryann Powles², Wu Yin², Feroze Ujjainwalla², Srikanth Venkatraman², Scott D Edmondson²

Affiliations

¹ Merck & Co., Inc. , West Point, Pennsylvania 19486, United States.
² Merck & Co., Inc. , Kenilworth, New Jersey 07033, United States.
³ WuXi AppTec , Shanghai 200131, China.

Abstract

GPR120 (FFAR4) is a fatty acid sensing G protein coupled receptor (GPCR) that has been identified as a target for possible treatment of type 2 diabetes. A selective activator of GPR120 containing a chromane scaffold has been designed, synthesized, and evaluated in vivo. Results of these efforts suggest that chromane propionic acid 18 is a suitable tool molecule for further animal studies. Compound 18 is selective over the closely related target GPR40 (FFAR1), has a clean off-target profile, demonstrates suitable pharmacokinetic properties, and has been evaluated in wild-type/knockout GPR120 mouse oGTT studies.

Keywords: FFAR4; GPR120; chromane; insulin sensitization; type 2 diabetes.