Optimization of Pharmacokinetics through Manipulation of Physicochemical Properties in a Series of HCV Inhibitors

Scott E Lazerwith; Gina Bahador; Eda Canales; Guofeng Cheng; Lee Chong; Michael O Clarke; Edward Doerffler; Eugene J Eisenberg; Jaclyn Hayes; Bing Lu; Qi Liu; Mike Matles; Michael Mertzman; Michael L Mitchell; Philip Morganelli; Bernard P Murray; Margaret Robinson; Robert G Strickley; Megan Tessler; Neeraj Tirunagari; Jianhong Wang; Yujin Wang; Jennifer R Zhang; Xubin Zheng; Weidong Zhong; William J Watkins

doi:10.1021/ml200163b

Optimization of Pharmacokinetics through Manipulation of Physicochemical Properties in a Series of HCV Inhibitors

ACS Med Chem Lett. 2011 Aug 8;2(10):715-9. doi: 10.1021/ml200163b. eCollection 2011 Oct 13.

Authors

Scott E Lazerwith¹, Gina Bahador¹, Eda Canales¹, Guofeng Cheng¹, Lee Chong¹, Michael O Clarke¹, Edward Doerffler¹, Eugene J Eisenberg¹, Jaclyn Hayes¹, Bing Lu¹, Qi Liu¹, Mike Matles¹, Michael Mertzman¹, Michael L Mitchell¹, Philip Morganelli¹, Bernard P Murray¹, Margaret Robinson¹, Robert G Strickley¹, Megan Tessler¹, Neeraj Tirunagari¹, Jianhong Wang¹, Yujin Wang¹, Jennifer R Zhang¹, Xubin Zheng¹, Weidong Zhong¹, William J Watkins¹

Affiliation

¹ Medicinal Chemistry, Drug Metabolism, Biology, and Formulation and Process Development, Gilead Sciences, Inc. , 333 Lakeside Drive, Foster City, California 94404, United States.

Abstract

A novel series of HCV replication inhibitors based on a pyrido[3,2-d]pyrimidine core were optimized for pharmacokinetics (PK) in rats. Several associations between physicochemical properties and PK were identified and exploited to guide the design of compounds. In addition, a simple new metric that may aid in the prediction of bioavailability for compounds with higher polar surface area is described (3*HBD-cLogP).

Keywords: 3*HBD-cLogP; HCV inhibitors; Pharmacokinetics; pyrido[3,2-d]pyrimidine core.