Discovery of Novel Quinoline-Based Proteasome Inhibitors for Human African Trypanosomiasis (HAT).
Dennis C KoesterVanessa M MarxSarah WilliamsJan JiricekMaxime DauphinaisOlivier RenéSarah L MillerLei ZhangDebjani PatraYen-Liang ChenHarry CheungJonathan GableSuresh B LakshminarayanaColin OsborneJean-Rene GalarneauUpendra KulkarniWendy RichmondAngela BretzLinda XiaoFrantisek SupekChristian WiesmannSrinivas HonnappaCeline BePascal MäserMarcel KaiserRyan RitchieMichael P BarrettThierry T DiaganaChristopher SarkoSrinivasa P S RaoPublished in: Journal of medicinal chemistry (2022)
Human African Trypanosomiasis (HAT) is a vector-borne disease caused by kinetoplastid parasites of the Trypanosoma genus. The disease proceeds in two stages, with a hemolymphatic blood stage and a meningo-encephalic brain stage. In the latter stage, the parasite causes irreversible damage to the brain leading to sleep cycle disruption and is fatal if untreated. An orally bioavailable treatment is highly desirable. In this study, we present a brain-penetrant, parasite-selective 20S proteasome inhibitor that was rapidly optimized from an HTS singleton hit to drug candidate compound 7 that showed cure in a stage II mouse efficacy model. Here, we describe hit expansion and lead optimization campaign guided by cryo-electron microscopy and an in silico model to predict the brain-to-plasma partition coefficient K p as an important parameter to prioritize compounds for synthesis. The model combined with in vitro and in vivo experiments allowed us to advance compounds with favorable unbound brain-to-plasma ratios ( K p,uu ) to cure a CNS disease such as HAT.
Keyphrases
- resting state
- white matter
- endothelial cells
- functional connectivity
- cerebral ischemia
- physical activity
- multiple sclerosis
- oxidative stress
- magnetic resonance imaging
- depressive symptoms
- magnetic resonance
- body mass index
- induced pluripotent stem cells
- subarachnoid hemorrhage
- computed tomography
- brain injury
- diffusion weighted imaging
- life cycle