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  • Design, synthesis, and structure-activity relationship of podocarpic acid amides as liver X receptor agonists for potential treatment of atherosclerosis.

Design, synthesis, and structure-activity relationship of podocarpic acid amides as liver X receptor agonists for potential treatment of atherosclerosis.

Bioorganic & medicinal chemistry letters (2005-08-30)
Weiguo Liu, Steve Chen, James Dropinski, Lawrence Colwell, Michael Robins, Michael Szymonifka, Nancy Hayes, Neelam Sharma, Karen MacNaul, Melba Hernandez, Charlotte Burton, Carl P Sparrow, John G Menke, Sheo B Singh
RÉSUMÉ

A series of podocarpic acid amides were identified as potent agonists for Liver X receptor alpha and beta subtypes, which are members of a nuclear hormone receptor superfamily that are involved in the regulation of a variety of metabolic pathways including cholesterol metabolism. We recently reported podocarpic acid anhydride and imide dimers as potent LXR agonists. Through parallel organic synthesis, we rapidly identified a series of new podocarpate leads with stable structures exemplified by adamantyl- and phenylcyclohexylmethyl-podocarpic acid amides (14 and 18). Compound 18 exhibited LXRalpha/beta 50/20 nM (binding affinity) and 33.7/35.3-fold receptor inductions. Synthesis, SAR, and biological activities of new podocarpate analogs are discussed.

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Podocarpic acid, 98%