Author/Authors :
Ho Yin Lo، نويسنده , , J?rg Bentzien، نويسنده , , Roman W. Fleck، نويسنده , , Steven S. Pullen، نويسنده , , Hnin Hnin Khine، نويسنده , , Joseph R. Woska Jr.، نويسنده , , Stanley Z. Kugler، نويسنده , , Mohammed A. Kashem، نويسنده , , Hidenori Takahashi، نويسنده ,
Abstract :
Based on the information from molecular modeling and X-ray crystal structures, the kinase specificity pocket of ITK could be occupied upon extension of the right-hand-side of the 2-benzimidazole core of the inhibitors. 2-Aminobenzimidazoles with a trans-stilbene-like extension were designed and synthesized as novel ITK antagonists. Significant improvement on binding affinity and cellular activity were obtained through the trans-stilbene-like antagonists. Several compounds showed inhibitory activity in an IL-2 functional assay.
Keywords :
ITK , T-cell kinase , Aminobenzimidazoles , inflammation , Kinase specificity pocket
