Discovery and hit-to-lead optimization of pyrrolopyrimidines as potent, state-dependent Nav1.7 antagonists

Article ID	Journal	Published Year	Pages	File Type
10593809	Bioorganic & Medicinal Chemistry Letters	2012	11 Pages	PDF

Abstract

Herein we describe the discovery, optimization, and structure-activity relationships of novel potent pyrrolopyrimidine Nav1.7 antagonists. Hit-to-lead SAR studies of the pyrrolopyrimidine core, head, and tail groups of the molecule led to the identification of pyrrolopyrimidine 48 as exceptionally potent Nav1.7 blocker with good selectivity over hERG and improved microsomal stability relative to our hit molecule and pyrazolopyrimidine 8 as a promising starting point for future optimization efforts.

Keywords

Nav1.7 paroxysmal extreme pain disorder NaV channels Sodium channel blockers Pyrrolopyrimidine voltage-gated sodium channels

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

Preview

Discovery and hit-to-lead optimization of pyrrolopyrimidines as potent, state-dependent Nav1.7 antagonists

Authors

Nagasree Chakka, Howie Bregman, Bingfan Du, Hanh Nho Nguyen, John L. Buchanan, Elma Feric, Joseph Ligutti, Dong Liu, Jeff S. McDermott, Anruo Zou, Stefan I. McDonough, Erin F. DiMauro,