Reduction in lipophilicity improved the solubility, plasma-protein binding, and permeability of tertiary sulfonamide RORc inverse agonists

Article ID	Journal	Published Year	Pages	File Type
10591644	Bioorganic & Medicinal Chemistry Letters	2014	7 Pages	PDF

Abstract

Using structure-based drug design principles, we identified opportunities to reduce the lipophilicity of our tertiary sulfonamide RORc inverse agonists. The new analogs possessed improved RORc cellular potencies with >77-fold selectivity for RORc over other nuclear receptors in our cell assay suite. The reduction in lipophilicity also led to an increased plasma-protein unbound fraction and improvements in cellular permeability and aqueous solubility.

Keywords

IL-17 RORγ RORC Solubility X-ray structure Permeability

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Reduction in lipophilicity improved the solubility, plasma-protein binding, and permeability of tertiary sulfonamide RORc inverse agonists

Authors

Benjamin P. Fauber, Olivier René, Gladys de Leon Boenig, Brenda Burton, Yuzhong Deng, Céline Eidenschenk, Christine Everett, Alberto Gobbi, Sarah G. Hymowitz, Adam R. Johnson, Hank La, Marya Liimatta, Peter Lockey, Maxine Norman, Wenjun Ouyang,