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

Femke A. Meijer; Annet O.W.M. Saris; Richard G. Doveston; Guido J.M. Oerlemans; Rens M.J.M. de Vries; Bente A. Somsen; Anke Unger; Bert Klebl; Christian Ottmann; Peter J. Cossar; Luc Brunsveld

doi:10.1021/acs.jmedchem.1c00475

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

Femke A. Meijer
, Annet O.W.M. Saris
, Richard G. Doveston
, Guido J.M. Oerlemans
, Rens M.J.M. de Vries
, Bente A. Somsen
, Anke Unger
, Bert Klebl
, Christian Ottmann
, Peter J. Cossar
, Luc Brunsveld (Corresponding author)

Onderzoeksoutput: Bijdrage aan tijdschrift › Tijdschriftartikel › Academic › peer review

14 Citaten (Scopus)

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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.

Originele taal-2	Engels
Pagina's (van-tot)	9238–9258
Aantal pagina's	21
Tijdschrift	Journal of Medicinal Chemistry
Volume	64
Nummer van het tijdschrift	13
Vroegere onlinedatum	19 mei 2021
DOI's	https://doi.org/10.1021/acs.jmedchem.1c00475
Status	Gepubliceerd - 8 jul. 2021

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Financiers	Financiernummer
European Union’s Horizon Europe research and innovation programme
H2020 Marie Skłodowska-Curie Actions	705188, H2020-MSCA-IEF-2016, 754462
European Commission
Nederlandse Organisatie voor Wetenschappelijk Onderzoek	711.017.014, 711.018.003, 016.150.366, 024.001.035

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10.1021/acs.jmedchem.1c00475Licentie: CC BY

published versionDefinitieve gepubliceerde versie, 3,53 MBLicentie: CC BY

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Meijer, F. A., Saris, A. O. W. M., Doveston, R. G., Oerlemans, G. J. M., de Vries, R. M. J. M., Somsen, B. A., Unger, A., Klebl, B., Ottmann, C., Cossar, P. J., & Brunsveld, L. (2021). Structure-Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt. Journal of Medicinal Chemistry, 64(13), 9238–9258. https://doi.org/10.1021/acs.jmedchem.1c00475

@article{326926a36f744f599ac04a224a05dd0a,

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

abstract = "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.",

author = "Meijer, \{Femke A.\} and Saris, \{Annet O.W.M.\} and Doveston, \{Richard G.\} and Oerlemans, \{Guido J.M.\} and \{de Vries\}, \{Rens M.J.M.\} and Somsen, \{Bente A.\} and Anke Unger and Bert Klebl and Christian Ottmann and Cossar, \{Peter J.\} and Luc Brunsveld",

year = "2021",

month = jul,

day = "8",

doi = "10.1021/acs.jmedchem.1c00475",

language = "English",

volume = "64",

pages = "9238–9258",

journal = "Journal of Medicinal Chemistry",

issn = "0022-2623",

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Meijer, FA, Saris, AOWM, Doveston, RG, Oerlemans, GJM , de Vries, RMJM, Somsen, BA, Unger, A, Klebl, B, Ottmann, C, Cossar, PJ & Brunsveld, L 2021, 'Structure-Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt', Journal of Medicinal Chemistry, vol. 64, nr. 13, blz. 9238–9258. https://doi.org/10.1021/acs.jmedchem.1c00475

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. et al.
In: Journal of Medicinal Chemistry, Vol. 64, Nr. 13, 08.07.2021, blz. 9238–9258.

Onderzoeksoutput: Bijdrage aan tijdschrift › Tijdschriftartikel › Academic › peer review

TY - JOUR

T1 - Structure-Activity Relationship Studies of Trisubstituted Isoxazoles as Selective Allosteric Ligands for the Retinoic-Acid-Receptor-Related Orphan Receptor γt

AU - Meijer, Femke A.

AU - Saris, Annet O.W.M.

AU - Doveston, Richard G.

AU - Oerlemans, Guido J.M.

AU - de Vries, Rens M.J.M.

AU - Somsen, Bente A.

AU - Unger, Anke

AU - Klebl, Bert

AU - Ottmann, Christian

AU - Cossar, Peter J.

AU - Brunsveld, Luc

PY - 2021/7/8

Y1 - 2021/7/8

N2 - 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.

AB - 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.

UR - https://www.scopus.com/pages/publications/85108288291

U2 - 10.1021/acs.jmedchem.1c00475

DO - 10.1021/acs.jmedchem.1c00475

M3 - Article

C2 - 34008974

SN - 0022-2623

VL - 64

SP - 9238

EP - 9258

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 13

ER -

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

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