Author/Authors :
Kim K. Adkison، نويسنده , , David G. Barrett، نويسنده , , David N. Deaton، نويسنده , , Robert T. Gampe Jr.، نويسنده , , Anne M. Hassell، نويسنده , , Stacey T. Long، نويسنده , , Robert B. McFadyen، نويسنده , , Aaron B. Miller، نويسنده , , Larry R. Miller، نويسنده , , J. Alan Payne، نويسنده , , Lisa M. Shewchuk، نويسنده , , Kevin J. Wells-Knecht، نويسنده , , Derril H. Willard Jr.، نويسنده , , Lois L. Wright، نويسنده ,
Abstract :
Starting from potent aldehyde inhibitors with poor drug properties, derivatization to semicarbazones led to the identification of a series of semicarbazone-based cathepsin K inhibitors with greater solubility and better pharmacokinetic profiles than their parent aldehydes. Furthermore, a representative semicarbazone inhibitor attenuated bone resorption in an ex vivo rat calvarial bone resorption model. However, based on enzyme inhibition comparisons at neutral pH, semicarbazone hydrolysis rates, and 13C NMR experiments, these semicarbazones probably function as prodrugs of aldehydes.
Keywords :
prodrugs , Cathepsin K inhibitors , Cysteine protease inhibitors , Aldehydes , Semicarbazones
