A novel phospholipid mimetic targeting LRH-1 ameliorates colitis

Author:

Mays Suzanne G.ORCID,D’Agostino Emma H.ORCID,Flynn Autumn R.ORCID,Huang Xiangsheng,Wang Guohui,Liu Xu,Millings Elizabeth J.,Okafor C. Denise,Patel Anamika,Cato Michael L.,Cornelison Jeffery L.,Melchers Dianna,Houtman René,Moore David D.,Calvert John W.,Jui Nathan T.,Ortlund Eric A.ORCID

Abstract

AbstractPhospholipids are ligands for nuclear hormone receptors (NRs) and regulate transcriptional programs relevant to normal physiology and disease. Here, we demonstrate that mimicking phospholipid-NR interactions greatly improves agonists of liver receptor homolog-1 (LRH-1), a promising therapeutic target for diabetes and colitis. Conventional LRH-1 modulators partially occupy the binding pocket, leaving vacant a region important for phospholipid binding and allostery. Therefore, we constructed a set of hybrid molecules with elements of natural phospholipids appended to a synthetic LRH-1 agonist. The phospholipid-mimicking group improves binding affinity, increases LRH-1 transcriptional activity, promotes coregulator recruitment, and interacts with the targeted LRH-1 residues in crystal structures. The best new agonist markedly improves colonic histopathology and disease-related weight loss in a humanized LRH-1 murine T-cell transfer model of colitis. This is the first evidence of in vivo efficacy for an LRH-1 modulator in colitis, a leap forward in agonist development.

Publisher

Cold Spring Harbor Laboratory

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