Discovery of a Series of Indazole TRPA1 Antagonists

David C Pryde; Brian E Marron; Christopher W West; Steven Reister; George Amato; Katrina Yoger; Brett Antonio; Karen Padilla; Peter J Cox; Jamie Turner; Joseph S Warmus; Nigel A Swain; Kiyoyuki Omoto; John H Mahoney; Aaron C Gerlach

doi:10.1021/acsmedchemlett.7b00140

Discovery of a Series of Indazole TRPA1 Antagonists

ACS Med Chem Lett. 2017 May 18;8(6):666-671. doi: 10.1021/acsmedchemlett.7b00140. eCollection 2017 Jun 8.

Authors

Affiliations

¹ Pfizer Worldwide Medicinal Chemistry, Neuroscience and Pain Research Unit, Portway Building, Granta Park, Great Abington, Cambridgeshire CB21 6GS, U.K.
² Pfizer Neuroscience and Pain Research Unit, 4222 Emperor Boulevard, Suite 350, Durham, North Carolina NC27703, United States.
³ Pfizer Worldwide Medicinal Chemistry, Neuroscience and Pain Research Unit, Groton, Connecticut 06340, United States.

Abstract

A series of TRPA1 antagonists is described which has as its core structure an indazole moiety. The physical properties and in vitro DMPK profiles are discussed. Good in vivo exposure was obtained with several analogs, allowing efficacy to be assessed in rodent models of inflammatory pain. Two compounds showed significant activity in these models when administered either systemically or topically. Protein chimeras were constructed to indicate compounds from the series bound in the S5 region of the channel, and a computational docking model was used to propose a binding mode for example compounds.

Keywords: AITC; Cinnamaldehyde flare; Indazole; Ion channel; Pain; TRPA1; Topical administration; Transient receptor potential.