Novel Autotaxin Inhibitors for the Treatment of Osteoarthritis Pain: Lead Optimization via Structure-Based Drug Design

Spencer B Jones; Lance A Pfeifer; Thomas J Bleisch; Thomas J Beauchamp; Jim D Durbin; V Joseph Klimkowski; Norman E Hughes; Christopher J Rito; Yen Dao; Joseph M Gruber; Hai Bui; Mark G Chambers; Srinivasan Chandrasekhar; Chaohua Lin; Denis J McCann; Daniel R Mudra; Jennifer L Oskins; Craig A Swearingen; Kannan Thirunavukkarasu; Bryan H Norman

doi:10.1021/acsmedchemlett.6b00207

Novel Autotaxin Inhibitors for the Treatment of Osteoarthritis Pain: Lead Optimization via Structure-Based Drug Design

ACS Med Chem Lett. 2016 Aug 2;7(9):857-61. doi: 10.1021/acsmedchemlett.6b00207. eCollection 2016 Sep 8.

Authors

Spencer B Jones¹, Lance A Pfeifer¹, Thomas J Bleisch¹, Thomas J Beauchamp¹, Jim D Durbin¹, V Joseph Klimkowski¹, Norman E Hughes¹, Christopher J Rito¹, Yen Dao¹, Joseph M Gruber¹, Hai Bui¹, Mark G Chambers¹, Srinivasan Chandrasekhar¹, Chaohua Lin¹, Denis J McCann¹, Daniel R Mudra¹, Jennifer L Oskins¹, Craig A Swearingen¹, Kannan Thirunavukkarasu¹, Bryan H Norman¹

Affiliation

¹ Lilly Research Laboratories , A Division of Eli Lilly and Company, Indianapolis, Indiana 46285, United States.

Abstract

In an effort to develop a novel therapeutic agent aimed at addressing the unmet need of patients with osteoarthritis pain, we set out to develop an inhibitor for autotaxin with excellent potency and physical properties to allow for the clinical investigation of autotaxin-induced nociceptive and neuropathic pain. An initial hit identification campaign led to an aminopyrimidine series with an autotaxin IC50 of 500 nM. X-ray crystallography enabled the optimization to a lead compound that demonstrated favorable potency (IC50 = 2 nM), PK properties, and a robust PK/PD relationship.

Keywords: Autotaxin; LPA; osteoarthritis; tool molecule.