Discovery of VTP-27999, an Alkyl Amine Renin Inhibitor with Potential for Clinical Utility

Lanqi Jia; Robert D Simpson; Jing Yuan; Zhenrong Xu; Wei Zhao; Salvacion Cacatian; Colin M Tice; Joan Guo; Alexey Ishchenko; Suresh B Singh; Zhongren Wu; Brian M McKeever; Yuri Bukhtiyarov; Judith A Johnson; Christopher P Doe; Richard K Harrison; Gerard M McGeehan; Lawrence W Dillard; John J Baldwin; David A Claremon

doi:10.1021/ml200137x

Discovery of VTP-27999, an Alkyl Amine Renin Inhibitor with Potential for Clinical Utility

ACS Med Chem Lett. 2011 Aug 9;2(10):747-51. doi: 10.1021/ml200137x. eCollection 2011 Oct 13.

Authors

Lanqi Jia¹, Robert D Simpson¹, Jing Yuan¹, Zhenrong Xu¹, Wei Zhao¹, Salvacion Cacatian¹, Colin M Tice¹, Joan Guo¹, Alexey Ishchenko¹, Suresh B Singh¹, Zhongren Wu¹, Brian M McKeever¹, Yuri Bukhtiyarov¹, Judith A Johnson¹, Christopher P Doe², Richard K Harrison¹, Gerard M McGeehan¹, Lawrence W Dillard¹, John J Baldwin¹, David A Claremon¹

Affiliations

¹ Vitae Pharmaceuticals, 502 West Office Center Drive, Fort Washington, Pennsylvania 19034, United States.
² GlaxoSmithKline, 709 Swedeland Road, King of Prussia, Pennsylvania 19406, United States.

Abstract

Structure guided optimization of a series of nonpeptidic alkyl amine renin inhibitors allowed the rational incorporation of additional polar functionality. Replacement of the cyclohexylmethyl group occupying the S1 pocket with a (R)-(tetrahydropyran-3-yl)methyl group and utilization of a different attachment point led to the identification of clinical candidate 9. This compound demonstrated excellent selectivity over related and unrelated off-targets, >15% oral bioavailability in three species, oral efficacy in a double transgenic rat model of hypertension, and good exposure in humans.

Keywords: Renin; aspartyl protease; hypertension; structure-based drug design.