Identification of RIPK3 Type II Inhibitors Using High-Throughput Mechanistic Studies in Hit Triage

Amy C Hart; Lynn Abell; Junqing Guo; Michael E Mertzman; Ramesh Padmanabha; John E Macor; Charu Chaudhry; Hao Lu; Kevin O'Malley; Patrick J Shaw; Carolyn Weigelt; Matthew Pokross; Kevin Kish; Kyoung S Kim; Lyndon Cornelius; Andrew E Douglas; Deepa Calambur; Ping Zhang; Brian Carpenter; William J Pitts

doi:10.1021/acsmedchemlett.9b00065

Identification of RIPK3 Type II Inhibitors Using High-Throughput Mechanistic Studies in Hit Triage

ACS Med Chem Lett. 2019 May 6;11(3):266-271. doi: 10.1021/acsmedchemlett.9b00065. eCollection 2020 Mar 12.

Authors

Amy C Hart¹, Lynn Abell¹, Junqing Guo¹, Michael E Mertzman¹, Ramesh Padmanabha¹, John E Macor¹, Charu Chaudhry¹, Hao Lu¹, Kevin O'Malley¹, Patrick J Shaw¹, Carolyn Weigelt¹, Matthew Pokross¹, Kevin Kish¹, Kyoung S Kim¹, Lyndon Cornelius¹, Andrew E Douglas¹, Deepa Calambur¹, Ping Zhang¹, Brian Carpenter¹, William J Pitts¹

Affiliation

¹ Bristol-Myers Squibb Research & Development, P.O. Box 4000, Princeton, New Jersey 08543, United States.

Abstract

Necroptosis has been implicated in a variety of disease states, and RIPK3 is one of the kinases identified to play a critical role in this signaling pathway. In an effort to identify RIPK3 kinase inhibitors with a novel profile, mechanistic studies were incorporated at the hit triage stage. Utilization of these assays enabled identification of a Type II DFG-out inhibitor for RIPK3, which was confirmed by protein crystallography. Structure-based drug design on the inhibitors targeting this previously unreported conformation enabled an enhancement in selectivity against key off-target kinases.