Biarylether amide quinolines as liver X receptor agonists.

Ronald C. Bernotas,Robert R. Singhaus,David H. Kaufman,John W. Ullrich,Horace Fletcher,Elaine Quinet,Ponnal Nambi,Rayomand J. Unwalla,Anna Wilhelmsson,Annika Goos-Nilsson,Mathias Färnegårdh,Jay E. Wrobel

Biarylether amide quinolines as liver X receptor agonists.

2009

Ronald C. Bernotas
Robert R. Singhaus
David H. Kaufman
John W. Ullrich
Horace Fletcher
Elaine Quinet
Ponnal Nambi
Rayomand J. Unwalla
Anna Wilhelmsson
Annika Goos-Nilsson
Mathias Färnegårdh
Jay E. Wrobel

Abstract A series of 4-(amido-biarylether)-quinolines was prepared as potential LXR agonists. Appropriate substitution with amide groups provided high affinity LXR ligands, some with excellent potency and efficacy in functional assays of LXR activity. Novel amide 4g had a binding IC 50 = 1.9 nM for LXRβ and EC 50 = 34 nM (96% efficacy relative to T0901317) in an ABCA1 gene expression assay in mouse J774 cells, demonstrating that 4-(biarylether)-quinolines with appropriate amide substitution are potent LXR agonists

Keywords:

Gene expression
Agonist
Potency
ABCA1 Gene
Quinoline
Amide
Biochemistry
Liver X receptor
Chemistry
Ligand
Stereochemistry
ABCA1

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