Author/Authors :
Raji Sundaramoorthi، نويسنده , , William C. Shakespeare، نويسنده , , Terence P. Keenan، نويسنده , , Chester A. Metcalf III، نويسنده , , Yihan Wang، نويسنده , , Ukti Mani، نويسنده , , Merry Taylor، نويسنده , , Shuangying Liu، نويسنده , , Regine S. Bohacek، نويسنده , , Surinder S. Narula، نويسنده , , David C. Dalgarno، نويسنده , , Marie Rose Van Schravandijk، نويسنده , , Sheila M. Violette، نويسنده , , Shuenn Liou، نويسنده , , Susan Adams، نويسنده , , Mary K. Ram، نويسنده , , Jeffrey A. Keats، نويسنده , , Manfred Weigele، نويسنده , , Tomi K. Sawyer، نويسنده ,
Abstract :
Src tyrosine kinase is a therapeutic target for bone diseases that has been validated by gene knockout studies. Furthermore, in vitro cellular studies implicate that Src has a positive regulatory role in osteoclasts and a negative regulatory role in osteoblasts. The potential use of Src inhibitors for osteoporosis therapy has been previously shown by novel bone-targeted ligands of the Src SH2 (e.g., AP22408) and non-bone-targeted, ATP-based inhibitors of Src kinase. Significant to this study, compounds 2–12 exemplify novel analogues of known pyrrolopyrimidine and pyrazolopyrimidine template-based Src kinase inhibitors that incorporate bone-targeting group modifications designed to provide tissue (bone) selectivity and diminished side effects. Accordingly, we report here the structure-based design, synthetic chemistry and biological testing of these compounds and proof-of-concept studies thereof.
