Title of article :
Discovery of novel isothiazole inhibitors of the TrkA kinase: Structure–activity relationship, computer modeling, optimization, and identification of highly potent antagonists
Author/Authors :
Blaise Lippa، نويسنده , , Joel Morris، نويسنده , , Matthew Corbett، نويسنده , , Tricia A. Kwan، نويسنده , , Mark C. Noe، نويسنده , , Sheri L. Snow، نويسنده , , Thomas G. Gant، نويسنده , , Melchiorra Mangiaracina، نويسنده , , Heather A. Coffey، نويسنده , , Barbara Foster، نويسنده , , Elisabeth A. Knauth، نويسنده , , Matthew D. Wessel، نويسنده ,
Abstract :
The design, synthesis, and biological evaluation of potent inhibitors of the TrkA kinase is presented. A homology model is created to aid in the enhancement of potency and selectivity of isothiazole inhibitors found during a high-throughput screen. Three different syntheses are utilized to make diverse analogs within this series. Aminoheterocycles are found to be good urea surrogates, whereas bicyclic substituents on the C3 thio group were found to be extremely potent TrkA inhibitors in kinase and cell assays.
Keywords :
Antagonist , homology model , Isothiazole , synthesis , TrkA
