Optimized chemical probes for REV-ERBα

Ryan P. Trump,Stefano Bresciani,Anthony William James Cooper,James P. Tellam,Justyna Wojno,John Blaikley,Lisa A. Orband-Miller,Jennifer A. Kashatus,Mohamed Boudjelal,Helen C. Dawson,Andrew Loudon,David Ray,Daniel Grant,Stuart N. Farrow,Timothy M. Willson,Nicholas C. O. Tomkinson

Optimized chemical probes for REV-ERBα

2013

Ryan P. Trump
Stefano Bresciani
Anthony William James Cooper
James P. Tellam
Justyna Wojno
John Blaikley
Lisa A. Orband-Miller
Jennifer A. Kashatus
Mohamed Boudjelal
Helen C. Dawson
Andrew Loudon
David Ray
Daniel Grant
Stuart N. Farrow
Timothy M. Willson
Nicholas C. O. Tomkinson

REV-ERBα has emerged as an important target for regulation of circadian rhythm and its associated physiology. Herein, we report on the optimization of a series of REV-ERBα agonists based on GSK4112 (1) for potency, selectivity, and bioavailability.(1) Potent REV-ERBα agonists 4, 10, 16, and 23 are detailed for their ability to suppress BMAL and IL-6 expression from human cells while also demonstrating excellent selectivity over LXRα. Amine 4 demonstrated in vivo bioavailability after either iv or oral dosing.

Keywords:

Selectivity
Biochemistry
In vivo
Potency
Pharmacology
Bioavailability
Structure–activity relationship
Circadian rhythm
ARNTL
Cell culture
Chemistry
Liver X receptor

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