Utilization of Metabolite Identification and Structural Data to Guide Design of Low-Dose IDO1 Inhibitors.
Brett HopkinsHongjun ZhangIndu BharathanDerun LiQinglin PuHua ZhouTheodore A MartinotAndreas VerrasAlfred LammensCharles A LesburgRyan D CohenJeanine BallardIan KnemeyerKarin OtteStella VincentJ Richard MillerNicolas SolbanMangeng ChengPrasanthi GedaNadya SmotrovXuelei SongDavid Jonathan BennettYongxin HanPublished in: ACS medicinal chemistry letters (2021)
Herein the discovery of potent IDO1 inhibitors with low predicted human dose is discussed. Metabolite identification (MetID) and structural data were used to strategically incorporate cyclopropane rings into this tetrahydronaphthyridine series of IDO1 inhibitors to improve their metabolic stability and potency. Enabling synthetic chemistry was developed to construct these unique fused cyclopropyl compounds, leading to inhibitors with improved pharmacokinetics and human whole blood potency and a predicted human oral dose as low as 9 mg once daily (QD).