Author/Authors :
Percy H. Carter، نويسنده , , Gregory D. Brown، نويسنده , , Sarah R. Friedrich، نويسنده , , Robert J. Cherney، نويسنده , , Andrew J. Tebben، نويسنده , , Yvonne C. Lo، نويسنده , , Gengjie Yang، نويسنده , , Heather Jezak، نويسنده , , Kimberly A. Solomon، نويسنده , , Peggy A. Scherle، نويسنده , , Carl P. Decicco، نويسنده ,
Abstract :
A new series of CCR2 antagonists has been discovered that incorporates intramolecular hydrogen bonding as a strategy for rigidifying the scaffold. The structure–activity relationship was established through initial systematic modification of substitution pattern and chain length, followed by independent optimization of three different substituents (benzylamine, carboxamide, and benzamide). Several of the acyclic compounds display 10–30 nM binding affinity for CCR2. Moreover, these antagonists are able to block both MCP-1-induced Ca2+ flux and monocyte chemotaxis, and are selective for binding to CCR2 over CCR1 and CCR3.
Keywords :
CCR2 , Small molecule , Antagonist , G-protein coupled receptor , chemokine , inflammation
