Author/Authors :
Arnab K. Chatterjee، نويسنده , , Hong Liu، نويسنده , , David C. Tully، نويسنده , , Jianhua Guo، نويسنده , , Robert Epple، نويسنده , , Ross Russo، نويسنده , , Jennifer Williams، نويسنده , , Michael Roberts، نويسنده , , Tove Tuntland، نويسنده , , Jonathan Chang، نويسنده , , Perry Gordon، نويسنده , , Thomas Hollenbeck، نويسنده , , Christine Tumanut، نويسنده , , Jun Li، نويسنده , , Jennifer L. Harris، نويسنده ,
Abstract :
Peptidic, non-covalent inhibitors of lysosomal cysteine protease cathepsin S (1 and 2) were investigated due to low oral bioavailability, leading to an improved series of peptidomimetic inhibitors. Utilizing phenyl succinamides as the P2 residue increased the oral exposure of this lead series of compounds, while retaining selective inhibition of the cathepsin S isoform. Concurrent investigation of the P1 and P2 subsites resulted in the discovery of several potent and selective inhibitors of cathepsin S with good pharmacokinetic properties due to the elimination of saturated aliphatic P2 residues.
