Author/Authors :
Keith W. Woods، نويسنده , , John P. Fischer، نويسنده , , Akiyo Claiborne، نويسنده , , Tongmei Li، نويسنده , , Sheela A. Thomas، نويسنده , , Gui-Dong Zhu، نويسنده , , Robert B. Diebold، نويسنده , , Xuesong Liu، نويسنده , , Yan Shi، نويسنده , , Vered Klinghofer، نويسنده , , Edward K. Han، نويسنده , , Ran Guan، نويسنده , , Shayna R. Magnone، نويسنده , , Eric F. Johnson، نويسنده , , Jennifer J. Bouska، نويسنده , , Amanda M. Olson، نويسنده , , Ron De Jong، نويسنده , , Tilman Oltersdorf، نويسنده , , Yan Luo، نويسنده , , Saul H. Rosenberg، نويسنده , , et al.، نويسنده ,
Abstract :
A series of heteroaryl-pyridine containing inhibitors of Akt are reported. The synthesis and structure–activity relationships are discussed, leading to the discovery of a indazole-pyridine analogue (Ki = 0.16 nM). These compounds bind in the ATP binding site, are potent, ATP competitive, and reversible inhibitors of Akt activity. No selectivity amongst the Akt isoforms is observed for this analogue, but there is good selectivity against an panel of other kinases. It is least selective for other members of the AGC family of kinases but is nonetheless 40-fold selective for Akt over PKA. The compound shows cellular activity and significantly slows tumor growth in vivo.
Keywords :
Protein kinase B , Akt , Serine/threonine kinase , Indazole
