Author/Authors :
Gregory S. Bisacchi، نويسنده , , William A. Slusarchyk، نويسنده , , Scott A Bolton، نويسنده , , Karen S. Hartl، نويسنده , , Glenn Jacobs، نويسنده , , Arvind Mathur، نويسنده , , Wei Meng، نويسنده , , Martin L. Ogletree، نويسنده , , Zulan Pi، نويسنده , , James C. Sutton، نويسنده , , Uwe Treuner، نويسنده , , Robert Zahler، نويسنده , , Guohua Zhao، نويسنده , , Steven M. Seiler، نويسنده ,
Abstract :
Azetidinones such as BMS-363131 (2) and BMS-363130 (3), which contain a guanidine group in the C-3 side chain were previously shown to be very potent inhibitors of human tryptase with high selectivity versus other serine proteases, including trypsin. In this letter, we describe the discovery of a number of potent azetidinone tryptase inhibitors in which the guanidine moiety at the ring C-3 position is replaced with primary or secondary amine or aminopyridine functionality. In particular, BMS-354326 (4) is a highly potent tryptase inhibitor (IC50=1.8 nM), which has excellent selectivity against trypsin and most other related serine proteases.
