Discovery and SAR of JTE-151: A Novel RORγ Inhibitor for Clinical Development.
Takaki MaebaKazuyuki HirataMasayuki KotokuNoriyoshi SekiKatsuya MaedaShintaro HirashimaHiroshi YamanakaTakayuki SakaiShingo ObikaAkimi HoriYoshinori HaraSatoru NojiYoshihiro SuwaMasahiro YokotaShingo FujiokaTakayuki YamaguchiYoshiaki KatsudaTakahiro HataNaoki MiyagawaKojo AritaYukihiro NomuraToshio TaniguchiKota AsahinaYusuke AratsuYuichi NakaTsuyoshi AdachiAkihiro NomuraShota AkaiShin-Ichi OshidaSudhakar PaiPaul CroweErin BradleyRuo SteensmaHaiyan TaoMorgan FennRobert BabineXiaolin LiScott ThacherTakahiro SoetaYutaka UkajiMakoto ShiozakiPublished in: Journal of medicinal chemistry (2024)
A number of RORγ inhibitors have been reported over the past decade. There were also several examples advancing to human clinical trials, however, none of them has reached the market yet, suggesting that there could be common obstacles for their future development. As was expected from the general homology of nuclear receptor ligands, insufficient selectivity as well as poor physicochemical properties were identified as potential risks for a RORγ program. Based on such considerations, we conducted a SAR investigation by prioritizing drug-like properties to mitigate such potential drawbacks. After an intensive SAR exploration with strong emphasis on "drug-likeness" indices, an orally available RORγ inhibitor, JTE-151, was finally generated and was advanced to a human clinical trial. The compound was confirmed to possess highly selective profiles along with good metabolic stability, and most beneficially, no serious adverse events (SAE) and good PK profiles were observed in the human clinical trial.