Structure-Activity Relationship of Novel and Selective Biaryl-Chroman GPR40 AgoPAMs

Helen Y Chen; Christopher W Plummer; Dong Xiao; Harry R Chobanian; Duane DeMong; Michael Miller; Maria E Trujillo; Melissa Kirkland; Daniel Kosinski; Joel Mane; Michele Pachanski; Boonlert Cheewatrakoolpong; Jerry Di Salvo; Brande Thomas-Fowlkes; Sarah Souza; Daniel A Tatosian; Qing Chen; Michael J Hafey; Robert Houle; Andrew F Nolting; Robert Orr; Juliann Ehrhart; Adam B Weinglass; Richard Tschirret-Guth; Andrew D Howard; Steven L Colletti

doi:10.1021/acsmedchemlett.8b00149

Structure-Activity Relationship of Novel and Selective Biaryl-Chroman GPR40 AgoPAMs

ACS Med Chem Lett. 2018 Jun 14;9(7):685-690. doi: 10.1021/acsmedchemlett.8b00149. eCollection 2018 Jul 12.

Authors

Helen Y Chen¹, Christopher W Plummer¹, Dong Xiao¹, Harry R Chobanian¹, Duane DeMong¹, Michael Miller¹, Maria E Trujillo¹, Melissa Kirkland¹, Daniel Kosinski¹, Joel Mane¹, Michele Pachanski¹, Boonlert Cheewatrakoolpong¹, Jerry Di Salvo¹, Brande Thomas-Fowlkes¹, Sarah Souza¹, Daniel A Tatosian¹, Qing Chen¹, Michael J Hafey¹, Robert Houle¹, Andrew F Nolting¹, Robert Orr¹, Juliann Ehrhart¹, Adam B Weinglass¹, Richard Tschirret-Guth¹, Andrew D Howard¹, Steven L Colletti¹

Affiliation

¹ Departments of Discovery Chemistry, Process Chemistry, Pharmacokinetics, Pharmacodynamics and Drug Metabolism, In Vivo Pharmacology, and In Vitro Pharmacology, Merck & Co., Inc., Kenilworth, New Jersey 07033, United States.

Abstract

A series of biaryl chromans exhibiting potent and selective agonism for the GPR40 receptor with positive allosteric modulation of endogenous ligands (AgoPAM) were discovered as potential therapeutics for the treatment of type II diabetes. Optimization of physicochemical properties through modification of the pendant aryl rings resulted in the identification of compound AP5, which possesses an improved metabolic profile while demonstrating sustained glucose lowering.