作者
Kenneth Down,Augustin Amour,Ian T. Baldwin,Anthony W. J. Cooper,Angela M. Deakin,Leigh Felton,Stephen B. Guntrip,C.J. Hardy,Z.A. Harrison,Katherine L. Jones,Paul S. Jones,Suzanne E. Keeling,Joelle Le,Stefano Livia,Fiona Lucas,Christopher J. Lunniss,Nigel J. Parr,Ed Robinson,Paul Rowland,Sarah E. Smith,Daniel A. Thomas,Giovanni Vitulli,Yoshiaki Washio,J. Hamblin
摘要
Optimization of lead compound 1, through extensive use of structure-based design and a focus on PI3Kδ potency, isoform selectivity, and inhaled PK properties, led to the discovery of clinical candidates 2 (GSK2269557) and 3 (GSK2292767) for the treatment of respiratory indications via inhalation. Compounds 2 and 3 are both highly selective for PI3Kδ over the closely related isoforms and are active in a disease relevant brown Norway rat acute OVA model of Th2-driven lung inflammation.