The discovery of a potent Nav1.3 inhibitor with good oral pharmacokinetics

D C Pryde; N A Swain; P A Stupple; C W West; B Marron; C J Markworth; D Printzenhoff; Z Lin; P J Cox; R Suzuki; S McMurray; G J Waldron; C E Payne; J S Warmus; M L Chapman

doi:10.1039/c7md00131b

The discovery of a potent Na_v1.3 inhibitor with good oral pharmacokinetics

Medchemcomm. 2017 Apr 28;8(6):1255-1267. doi: 10.1039/c7md00131b. eCollection 2017 Jun 1.

Authors

D C Pryde¹, N A Swain¹, P A Stupple¹, C W West², B Marron², C J Markworth², D Printzenhoff², Z Lin², P J Cox³, R Suzuki³, S McMurray³, G J Waldron³, C E Payne³, J S Warmus⁴, M L Chapman²

Affiliations

¹ Worldwide Medicinal Chemistry , Pfizer Neuroscience and Pain Research Unit , Portway Building, Granta Park , Cambridge , CB21 6GS , UK . Email: david@curadev.co.uk.
² Pfizer Neuroscience and Pain Research Unit , 4222 Emperor Boulevard, Suite 350 , Durham , North Carolina NC27703 , USA.
³ Pfizer Neuroscience and Pain Research Unit , Portway Building, Granta Park , Cambridge , CB21 6GS , UK.
⁴ Worldwide Medicinal Chemistry , Pfizer Neuroscience and Pain Research Unit , Groton , CT , USA.

Abstract

In this article, we describe the discovery of an aryl ether series of potent and selective Na_v1.3 inhibitors. Based on structural analogy to a similar series of compounds we have previously shown bind to the domain IV voltage sensor region of Na_v channels, we propose this series binds in the same location. We describe the development of this series from a published starting point, highlighting key selectivity and potency data, and several studies designed to validate Na_v1.3 as a target for pain.