Biologic-like In Vivo Efficacy with Small Molecule Inhibitors of TNFα Identified Using Scaffold Hopping and Structure-Based Drug Design Approaches.
Hai-Yun XiaoNing LiJames J-W DuanBin JiangZhonghui LuKhehyong NguJoseph TinoLisa M KopchoHao LuJing ChenAndrew J TebbenSteven SheriffChiehYing Y ChangJoseph YanchunasDeepa CalamburMian GaoDavid J ShusterVojkan SusulicJenny H XieVictor R GuarinoDauh-Rurng WuKurt R GregorChristine B GoldstineJohn HynesJohn E MacorLuisa Salter-CidJames R BurkePatrick J ShawT G Murali DharPublished in: Journal of medicinal chemistry (2020)
Scaffold hopping and structure-based drug design were employed to identify substituted 4-aminoquinolines and 4-aminonaphthyridines as potent, small molecule inhibitors of tumor necrosis factor alpha (TNFα). Structure-activity relationships in both the quinoline and naphthyridine series leading to the identification of compound 42 with excellent potency and pharmacokinetic profile are discussed. X-ray co-crystal structure analysis and ultracentrifugation experiments clearly demonstrate that these inhibitors distort the TNFα trimer upon binding, leading to aberrant signaling when the trimer binds to TNF receptor 1 (TNFR1). Pharmacokinetic-pharmacodynamic activity of compound 42 in a TNF-induced IL-6 mouse model and in vivo activity in a collagen antibody-induced arthritis model, where it showed biologic-like in vivo efficacy, will be discussed.