PLoS ONE (Jan 2017)

Pharmacological inhibition of RORγt suppresses the Th17 pathway and alleviates arthritis in vivo.

  • Ulf Guendisch,
  • Jessica Weiss,
  • Florence Ecoeur,
  • Julia Christina Riker,
  • Klemens Kaupmann,
  • Joerg Kallen,
  • Samuel Hintermann,
  • David Orain,
  • Janet Dawson,
  • Andreas Billich,
  • Christine Guntermann

DOI
https://doi.org/10.1371/journal.pone.0188391
Journal volume & issue
Vol. 12, no. 11
p. e0188391

Abstract

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Retinoic acid receptor-related-orphan-receptor-C (RORγt) is the key transcription factor that is driving the differentiation of IL-17 producing T-helper 17 (Th17) cells that are implicated in the pathology of various autoimmune and inflammatory diseases. Based on the importance of RORγt in promoting Th17-driven pathology, there is considerable interest to develop low-molecular-weight compounds with the aim of inhibiting the transcriptional activity of this nuclear hormone receptor. In this article, we describe the in vitro and in vivo pharmacology of a potent and selective small-molecular-weight RORγt inverse agonist. The compound binds to the ligand binding domain (LBD) of RORγt leading to displacement of a co-activator peptide. We show for the first time that a RORγt inverse agonist down-regulates permissive histone H3 acetylation and methylation at the IL17A and IL23R promoter regions, thereby providing insight into the transcriptional inhibition of RORγt-dependent genes. Consistent with this, the compound effectively reduced IL-17A production by polarized human T-cells and γδT-cells and attenuated transcription of RORγt target genes. The inhibitor showed good in vivo efficacy in an antigen-induced arthritis model in rats and reduced the frequencies of IL-17A producing cells in ex vivo recall assays. In summary, we demonstrate that inhibiting RORγt by a low-molecular-weight inhibitor results in efficient and selective blockade of the pro-inflammatory Th17/IL-17A pathway making it an attractive target for Th17-mediated disorders.