Author/Authors :
David J. Witter، نويسنده , , Paul Harrington، نويسنده , , Kevin J. Wilson، نويسنده , , Melissa Chenard، نويسنده , , Judith C. Fleming، نويسنده , , Brian Haines، نويسنده , , Astrid M. Kral، نويسنده , , J. Paul Secrist، نويسنده , , Thomas A. Miller، نويسنده ,
Abstract :
A class of biaryl benzamides was identified and optimized as selective HDAC1&2 inhibitors (SHI-1:2). These agents exhibit selectivity over class II HDACs 4–7, as well as class I HDACs 3 and 8; providing examples of selective HDAC inhibitors for the HDAC isoforms most closely associated with cancer. The hypothesis for the increased selectivity is the binding of a pendant aromatic group in the internal cavity of the HDAC1&2 enzymes. SAR development based on an initial lead led to a series of potent and selective inhibitors with reduced off-target activity and tumor growth inhibition activity in a HCT-116 xenograft model.
Keywords :
Histone deacetylase , Aminobenzamides , biaryl , HDAC
