Discovery of IWP-051, a Novel Orally Bioavailable sGC Stimulator with Once-Daily Dosing Potential in Humans

Takashi Nakai; Nicholas R Perl; Timothy C Barden; Andrew Carvalho; Angelika Fretzen; Peter Germano; G-Yoon J Im; Hong Jin; Charles Kim; Thomas W-H Lee; Kimberly Long; Joel Moore; Jason M Rohde; Renee Sarno; Chrissie Segal; Erik O Solberg; Jenny Tobin; Daniel P Zimmer; Mark G Currie

doi:10.1021/acsmedchemlett.5b00479

Discovery of IWP-051, a Novel Orally Bioavailable sGC Stimulator with Once-Daily Dosing Potential in Humans

ACS Med Chem Lett. 2016 Feb 24;7(5):465-9. doi: 10.1021/acsmedchemlett.5b00479. eCollection 2016 May 12.

Authors

Takashi Nakai¹, Nicholas R Perl¹, Timothy C Barden¹, Andrew Carvalho¹, Angelika Fretzen¹, Peter Germano¹, G-Yoon J Im¹, Hong Jin¹, Charles Kim¹, Thomas W-H Lee¹, Kimberly Long¹, Joel Moore¹, Jason M Rohde¹, Renee Sarno¹, Chrissie Segal¹, Erik O Solberg¹, Jenny Tobin¹, Daniel P Zimmer¹, Mark G Currie¹

Affiliation

¹ Ironwood Pharmaceuticals, Inc. 301 Binney Street Cambridge, Massachusetts 02142 United States.

Abstract

In recent years, soluble guanylate cyclase (sGC, EC 4.6.1.2) has emerged as an attractive therapeutic target for treating cardiovascular diseases and diseases associated with fibrosis and end-organ failure. Herein, we describe our design and synthesis of a series of 4-hydroxypyrimidine sGC stimulators starting with an internally discovered lead. Our efforts have led to the discovery of IWP-051, a molecule that achieves good alignment of potency, stability, selectivity, and pharmacodynamic effects while maintaining favorable pharmacokinetic properties with once-daily dosing potential in humans.

Keywords: IWP-051; NO-independent stimulators; Soluble guanylate cyclase; heme-dependent sGC stimulators; nitric oxide; sGC.