| Literature DB >> 27268696 |
Olaf Kinzel1, Christoph Steeneck2, Thomas Schlüter2, Andreas Schulz2, Christian Gege2, Ulrike Hahn3, Eva Hambruch2, Martin Hornberger2, Adriana Spalwisz2, Katharina Frick2, Sanja Perović-Ottstadt2, Ulrich Deuschle2, Michael Burnet3, Claus Kremoser2.
Abstract
Several isoxazole-containing series of FXR agonists have been published over the last 15years, subsequent to the prototypical amphiphilic 'hammerhead'-type structure that was originally laid out by GW4064, the first potent synthetic FXR agonist. A set of novel compounds where the hammerhead is connected to the terminal carboxylic acid-bearing aryl or heteroaryl moiety by either a cyclopropyl, a hydroxycyclobutyl or a hydroxyazetidinyl linker was synthesized in order to improve upon the ADME properties of such isoxazoles. The resulting compounds all demonstrated high potencies at the target receptor FXR but with considerable differences in their physicochemical and in vivo profiles. The structure-activity relationships for key chemical features that have a major impact on the in vivo pharmacology of this series are discussed.Entities:
Keywords: C57BL/6J mice; FXR agonist; Farnesoid X receptor; GW4064; High fat diet; NAFLD; NASH
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Year: 2016 PMID: 27268696 DOI: 10.1016/j.bmcl.2016.05.070
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823