Optimization of Orally Bioavailable PI3Kδ Inhibitors and Identification of Vps34 as a Key Selectivity Target.
Zoë A HenleyAugustin AmourNick BartonMarcus BantscheffGiovanna BergaminiSophie M BertrandMáire ConveryKenneth DownBirgit DümpelfeldChris D EdwardsPaola GrandiPaul M GoreSteve KeelingStefano LiviaDavid MallettAoife MaxwellMark PriceChristina RauFriedrich B M ReinhardJames RowedderPaul RowlandJonathan A TaylorDaniel A ThomasEdith M HesselJ Nicole HamblinPublished in: Journal of medicinal chemistry (2020)
Optimization of a lead series of PI3Kδ inhibitors based on a dihydroisobenzofuran core led to the identification of potent, orally bioavailable compound 19. Selectivity profiling of compound 19 showed similar potency for class III PI3K, Vps34, and PI3Kδ, and compound 19 was not well-tolerated in a 7-day rat toxicity study. Structure-based design led to an improvement in selectivity for PI3Kδ over Vps34 and, a focus on oral phramacokinetics properties resulted in the discovery of compound 41, which showed improved toxicological outcomes at similar exposure levels to compound 19.