APOE4, the major genetic risk factor for Alzheimer’s disease (AD), and ABCA1, required for lipidation of APOE are gene products of the liver X receptor (LXR) receptor. LXR agonists have been validated in animal models as therapeutics for AD, atherosclerosis, and many other diseases. Clinical progress has been thwarted by unwanted hepatic lipogenesis. Structurally diverse LXR ligands were profiled in coregulator TR-FRET (CRT) assays analyzing ligand-induced coactivator recruitment, coactivator se
In search of nonlipogenic ABCA1 inducers (NLAI): precision coregulator TR-FRET identifies diverse signatures for LXR ligands
Megan S. Laham·Gregory RJ Thatcher·Fahmida Alam·Sarah Turner·Ganga Reddy Velma·Christopher Penton·Soumya Reddy Musku·Manan Rana·Senthilkumar Thulasingam·Anandhan Annadurai·Maha Ibrahim Sulaiman·Nina Ma·Martha Ackerman-Berrier