Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt

[Image: see text] The inhibition of the nuclear receptor retinoic-acid-receptor-related orphan receptor γt (RORγt) is a promising strategy in the treatment of autoimmune diseases. RORγt features an allosteric binding site within its ligand-binding domain that provides an opportunity to overcome draw...

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Autores principales: Meijer, Femke A., Saris, Annet O.W.M., Doveston, Richard G., Oerlemans, Guido J.M., de Vries, Rens M.J.M., Somsen, Bente A., Unger, Anke, Klebl, Bert, Ottmann, Christian, Cossar, Peter J., Brunsveld, Luc
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2021
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8273893/
https://www.ncbi.nlm.nih.gov/pubmed/34008974
http://dx.doi.org/10.1021/acs.jmedchem.1c00475
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author Meijer, Femke A.
Saris, Annet O.W.M.
Doveston, Richard G.
Oerlemans, Guido J.M.
de Vries, Rens M.J.M.
Somsen, Bente A.
Unger, Anke
Klebl, Bert
Ottmann, Christian
Cossar, Peter J.
Brunsveld, Luc
author_facet Meijer, Femke A.
Saris, Annet O.W.M.
Doveston, Richard G.
Oerlemans, Guido J.M.
de Vries, Rens M.J.M.
Somsen, Bente A.
Unger, Anke
Klebl, Bert
Ottmann, Christian
Cossar, Peter J.
Brunsveld, Luc
author_sort Meijer, Femke A.
collection PubMed
description [Image: see text] The inhibition of the nuclear receptor retinoic-acid-receptor-related orphan receptor γt (RORγt) is a promising strategy in the treatment of autoimmune diseases. RORγt features an allosteric binding site within its ligand-binding domain that provides an opportunity to overcome drawbacks associated with orthosteric modulators. Recently, trisubstituted isoxazoles were identified as a novel class of allosteric RORγt inverse agonists. This chemotype offers new opportunities for optimization into selective and efficacious allosteric drug-like molecules. Here, we explore the structure–activity relationship profile of the isoxazole series utilizing a combination of structure-based design, X-ray crystallography, and biochemical assays. The initial lead isoxazole (FM26) was optimized, resulting in compounds with a ∼10-fold increase in potency (low nM), significant cellular activity, promising pharmacokinetic properties, and a good selectivity profile over the peroxisome-proliferated-activated receptor γ and the farnesoid X receptor. We envisage that this work will serve as a platform for the accelerated development of isoxazoles and other novel chemotypes for the effective allosteric targeting of RORγt.
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spelling pubmed-82738932021-07-13 Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt Meijer, Femke A. Saris, Annet O.W.M. Doveston, Richard G. Oerlemans, Guido J.M. de Vries, Rens M.J.M. Somsen, Bente A. Unger, Anke Klebl, Bert Ottmann, Christian Cossar, Peter J. Brunsveld, Luc J Med Chem [Image: see text] The inhibition of the nuclear receptor retinoic-acid-receptor-related orphan receptor γt (RORγt) is a promising strategy in the treatment of autoimmune diseases. RORγt features an allosteric binding site within its ligand-binding domain that provides an opportunity to overcome drawbacks associated with orthosteric modulators. Recently, trisubstituted isoxazoles were identified as a novel class of allosteric RORγt inverse agonists. This chemotype offers new opportunities for optimization into selective and efficacious allosteric drug-like molecules. Here, we explore the structure–activity relationship profile of the isoxazole series utilizing a combination of structure-based design, X-ray crystallography, and biochemical assays. The initial lead isoxazole (FM26) was optimized, resulting in compounds with a ∼10-fold increase in potency (low nM), significant cellular activity, promising pharmacokinetic properties, and a good selectivity profile over the peroxisome-proliferated-activated receptor γ and the farnesoid X receptor. We envisage that this work will serve as a platform for the accelerated development of isoxazoles and other novel chemotypes for the effective allosteric targeting of RORγt. American Chemical Society 2021-05-19 2021-07-08 /pmc/articles/PMC8273893/ /pubmed/34008974 http://dx.doi.org/10.1021/acs.jmedchem.1c00475 Text en © 2021 The Authors. Published by American Chemical Society Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Meijer, Femke A.
Saris, Annet O.W.M.
Doveston, Richard G.
Oerlemans, Guido J.M.
de Vries, Rens M.J.M.
Somsen, Bente A.
Unger, Anke
Klebl, Bert
Ottmann, Christian
Cossar, Peter J.
Brunsveld, Luc
Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt
title Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt
title_full Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt
title_fullStr Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt
title_full_unstemmed Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt
title_short Structure–Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt
title_sort structure–activity relationship studies of trisubstituted isoxazoles as selective allosteric ligands for the retinoic-acid-receptor-related orphan receptor γt
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8273893/
https://www.ncbi.nlm.nih.gov/pubmed/34008974
http://dx.doi.org/10.1021/acs.jmedchem.1c00475
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