Author/Authors :
Christopher P. Holmes، نويسنده , , Xianfeng Li، نويسنده , , Yijun Pan، نويسنده , , Caiding Xu، نويسنده , , Ashok Bhandari، نويسنده , , Claire M. Moody، نويسنده , , Joy A. Miguel، نويسنده , , Steven W. Ferla، نويسنده , , M. Nuria De Francisco، نويسنده , , Brian T. Frederick، نويسنده , , Siqun Zhou، نويسنده , , Natalie Macher، نويسنده , , Larry Jang، نويسنده , , Jennifer D. Irvine، نويسنده , , J. Russell Grove، نويسنده ,
Abstract :
We have synthesized and evaluated a series of triaryl sulfonamide-based PTP1B inhibitors in which a difluoro-methylenephosphonate group of a potent lead has been replaced by potential bioisosteric replacements. Several mono- or di-charged compounds (8a, 8b, and 15a) were shown exhibit inhibitory activity in the low micromolar range, demonstrating the feasibility of using this approach in identifying non-phosphonate pTyr mimetics in a small molecular scaffold. These results also provide a useful indication of the relative effectiveness of these pTyr mimetics.
Keywords :
PTP1B , phosphatase , Bioisostere , Sulfonamide
