Carboxylic acid based quinolines as liver X receptor modulators that have LXRβ receptor binding selectivity

Baihua Hu,Elaine Quinet,Rayomand J. Unwalla,Mike Collini,James W. Jetter,Rebecca Dooley,Diane Andraka,Lisa M. Nogle,Dawn Savio,Anita R Halpern,Annika Goos-Nilsson,Anna Wilhelmsson,Ponnal Nambi,Jay E. Wrobel

Carboxylic acid based quinolines as liver X receptor modulators that have LXRβ receptor binding selectivity

2008

Baihua Hu
Elaine Quinet
Rayomand J. Unwalla
Mike Collini
James W. Jetter
Rebecca Dooley
Diane Andraka
Lisa M. Nogle
Dawn Savio
Anita R Halpern
Annika Goos-Nilsson
Anna Wilhelmsson
Ponnal Nambi
Jay E. Wrobel

A series of potent and binding selective LXRβ agonists was developed using the previously reported non-selective LXR ligand WAY-254011 as a structural template. With the aid of molecular modeling, it was found that 2,3-diMe-Ph, 2,5-diMe-Ph, and naphthalene substituted quinoline acetic acids (such as quinoline 33, 37, and 38) showed selectivity for LXRβ over LXRα in binding assays.

Keywords:

Selectivity
Organic chemistry
Nuclear receptor
Carboxylic acid
Quinoline
Stereochemistry
Biochemistry
Molecular model
Liver X receptor
Ligand (biochemistry)
Ligand
Chemistry

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