1. Academic Validation
  2. Enantiomer-specific activities of an LRH-1 and SF-1 dual agonist

Enantiomer-specific activities of an LRH-1 and SF-1 dual agonist

  • Sci Rep. 2020 Dec 17;10(1):22279. doi: 10.1038/s41598-020-79251-9.
Suzanne G Mays 1 2 Józef Stec 3 4 Xu Liu 1 Emma H D'Agostino 1 Richard J Whitby 3 Eric A Ortlund 5
Affiliations

Affiliations

  • 1 Department of Biochemistry, Emory University, Atlanta, GA, 30322, USA.
  • 2 Centre for Genomic Regulation, Carrer Dr. Aiguader, 88, 08003, Barcelona, Spain.
  • 3 School of Chemistry, University of Southampton, Southampton, Hants, SO17, United Kingdom.
  • 4 Department of Pharmaceutical Sciences, College of Pharmacy, Marshall B. Ketchum University, 2575 Yorba Linda Blvd, Fullerton, CA, 82831, USA.
  • 5 Department of Biochemistry, Emory University, Atlanta, GA, 30322, USA. eortlun@emory.edu.
Abstract

Chirality is an important consideration in drug development: it can influence recognition of the intended target, pharmacokinetics, and off-target effects. Here, we investigate how chirality affects the activity and mechanism of action of RJW100, a racemic agonist of the nuclear receptors liver receptor homolog-1 (LRH-1) and steroidogenic factor-1 (SF-1). LRH-1 and SF-1 modulators are highly sought as treatments for metabolic and neoplastic diseases, and RJW100 has one of the few scaffolds shown to activate them. However, enantiomer-specific effects on receptor activation are poorly understood. We show that the enantiomers have similar binding affinities, but RR-RJW100 stabilizes both receptors and is 46% more active than SS-RJW100 in LRH-1 luciferase reporter assays. We present an LRH-1 crystal structure that illuminates striking mechanistic differences: SS-RJW100 adopts multiple configurations in the pocket and fails to make an interaction critical for activation by RR-RJW100. In molecular dynamics simulations, SS-RJW100 attenuates intramolecular signalling important for coregulator recruitment, consistent with previous observations that it weakly recruits coregulators in vitro. These studies provide a rationale for pursuing enantiomerically pure RJW100 derivatives: they establish RR-RJW100 as the stronger LRH-1 agonist and identify a potential for optimizing the SS-RJW100 scaffold for antagonist design.

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