| Literature DB >> 18973288 |
Jay Wrobel1, Robert Steffan, S Marc Bowen, Ronald Magolda, Edward Matelan, Rayomand Unwalla, Michael Basso, Valerie Clerin, Stephen J Gardell, Ponnal Nambi, Elaine Quinet, Jason I Reminick, George P Vlasuk, Shuguang Wang, Irene Feingold, Christine Huselton, Tomas Bonn, Mathias Farnegardh, Tomas Hansson, Annika Goos Nilsson, Anna Wilhelmsson, Edouard Zamaratski, Mark J Evans.
Abstract
A series of substituted 2-benzyl-3-aryl-7-trifluoromethylindazoles were prepared as LXR modulators. These compounds were partial agonists in transactivation assays when compared to 1 (T0901317) and were slightly weaker with respect to potency and efficacy on LXRalpha than on LXRbeta. Lead compounds in this series 12 (WAY-252623) and 13 (WAY-214950) showed less lipid accumulation in HepG2 cells than potent full agonists 1 and 3 (WAY-254011) but were comparable in efficacy to 1 and 3 with respect to cholesterol efflux in THP-1 foam cells, albeit weaker in potency. Compound 13 reduced aortic lesion area in LDLR knockout mice equivalently to 3 or positive control 2 (GW3965). In a 7-day hamster model, compound 13 showed a lesser propensity for plasma TG elevation than 3, when the compounds were compared at doses in which they elevated ABCA1 and ABCG1 gene expression in duodenum and liver at equal levels. In contrast to results previously published for 2, the lack of TG effect of 13 correlated with its inability to increase liver fatty acid synthase (FAS) gene expression, which was up-regulated 4-fold by 3. These results suggest indazoles such as 13 may have an improved profile for potential use as a therapeutic agent.Entities:
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Year: 2008 PMID: 18973288 DOI: 10.1021/jm800799q
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446