3,5-Disubstituted-indole-7-carboxamides as IKKβ Inhibitors: Optimization of Oral Activity via the C3 Substituent

Jeffrey K Kerns; Jakob Busch-Petersen; Wei Fu; Jeffrey C Boehm; Hong Nie; Michael Muratore; Ann Bullion; Guoliang Lin; Huijie Li; Roderick Davis; Xichen Lin; Ami S Lakdawala; Rick Cousins; Rita Field; Jeremy Payne; David D Miller; Paul Bamborough; John A Christopher; Ian Baldwin; Ruth R Osborn; John Yonchuk; Edward Webb; William L Rumsey

doi:10.1021/acsmedchemlett.8b00291

3,5-Disubstituted-indole-7-carboxamides as IKKβ Inhibitors: Optimization of Oral Activity via the C3 Substituent

ACS Med Chem Lett. 2018 Oct 30;9(12):1164-1169. doi: 10.1021/acsmedchemlett.8b00291. eCollection 2018 Dec 13.

Authors

Jeffrey K Kerns¹, Jakob Busch-Petersen¹, Wei Fu¹, Jeffrey C Boehm¹, Hong Nie¹, Michael Muratore¹, Ann Bullion¹, Guoliang Lin¹, Huijie Li¹, Roderick Davis¹, Xichen Lin¹, Ami S Lakdawala^{1

2}, Rick Cousins², Rita Field², Jeremy Payne², David D Miller², Paul Bamborough², John A Christopher², Ian Baldwin², Ruth R Osborn¹, John Yonchuk¹, Edward Webb¹, William L Rumsey¹

Affiliations

¹ GlaxoSmithKline Inc., 709 Swedeland Road, King of Prussia Pennsylvania 19406, United States.
² Medicines Research Centre, GlaxoSmithKline R&D, Gunnels Wood Road, Stevenage, Hertfordshire SG1 2NY, U.K.

Abstract

IκB kinase β (IKKβ or IKK2) is a key regulator of nuclear factor kappa B (NF-κB) and has received attention as a therapeutic target. Herein we report on the optimization of a series of 3,5-disubstituted-indole-7-carboxamides for oral activity. In doing so, we focused attention on potency, ligand efficiency (LE), and physicochemical properties and have identified compounds 24 and (R)-28 as having robust in vivo activity.