Minor Structural Change to Tertiary Sulfonamide RORc Ligands Led to Opposite Mechanisms of Action

Olivier René; Benjamin P Fauber; Gladys de Leon Boenig; Brenda Burton; Céline Eidenschenk; Christine Everett; Alberto Gobbi; Sarah G Hymowitz; Adam R Johnson; James R Kiefer; Marya Liimatta; Peter Lockey; Maxine Norman; Wenjun Ouyang; Heidi A Wallweber; Harvey Wong

doi:10.1021/ml500420y

Minor Structural Change to Tertiary Sulfonamide RORc Ligands Led to Opposite Mechanisms of Action

ACS Med Chem Lett. 2014 Dec 4;6(3):276-81. doi: 10.1021/ml500420y. eCollection 2015 Mar 12.

Authors

Olivier René¹, Benjamin P Fauber¹, Gladys de Leon Boenig¹, Brenda Burton², Céline Eidenschenk¹, Christine Everett¹, Alberto Gobbi¹, Sarah G Hymowitz¹, Adam R Johnson¹, James R Kiefer¹, Marya Liimatta¹, Peter Lockey², Maxine Norman², Wenjun Ouyang¹, Heidi A Wallweber¹, Harvey Wong¹

Affiliations

¹ Genentech, Inc., 1 DNA Way, South San Francisco, California 94080, United States.
² Argenta, Early Discovery, Charles River, 7-9 Spire Green Centre, Flex Meadow, Harlow, Essex CM19 5TR, U.K.

Abstract

A minor structural change to tertiary sulfonamide RORc ligands led to distinct mechanisms of action. Co-crystal structures of two compounds revealed mechanistically consistent protein conformational changes. Optimized phenylsulfonamides were identified as RORc agonists while benzylsulfonamides exhibited potent inverse agonist activity. Compounds behaving as agonists in our biochemical assay also gave rise to an increased production of IL-17 in human PBMCs whereas inverse agonists led to significant suppression of IL-17 under the same assay conditions. The most potent inverse agonist compound showed >180-fold selectivity over the ROR isoforms as well as all other nuclear receptors that were profiled.

Keywords: IL-17; PBMC; RORc; RORγ; TH17; agonist; inverse agonist.

Grants and funding

National Institutes of Health, United States