Synthesis and evaluation of arylaminoethyl amides as noncovalent inhibitors of cathepsin S. Part 3: Heterocyclic P3.

David C. Tully,Hong Liu,Phil B. Alper,Arnab K. Chatterjee,Robert Epple,Michael J. Roberts,Jennifer A. Williams,KhanhLinh T. Nguyen,David H. Woodmansee,Christine Tumanut,Jun Li,Glen Spraggon,Jonathan Chang,Tove Tuntland,Jennifer L. Harris,Donald S. Karanewsky

Synthesis and evaluation of arylaminoethyl amides as noncovalent inhibitors of cathepsin S. Part 3: Heterocyclic P3.

2006

David C. Tully
Hong Liu
Phil B. Alper
Arnab K. Chatterjee
Robert Epple
Michael J. Roberts
Jennifer A. Williams
KhanhLinh T. Nguyen
David H. Woodmansee
Christine Tumanut
Jun Li
Glen Spraggon
Jonathan Chang
Tove Tuntland
Jennifer L. Harris
Donald S. Karanewsky

Abstract A series of N α -2-benzoxazolyl-α-amino acid-(arylaminoethyl)amides were identified as potent, selective, and noncovalent inhibitors of cathepsin S. Structure–activity relationships including strategies for modulating the selectivities among cathepsins S, K, and L, and in vivo pharmacokinetics are discussed. A X-ray structure of compound 3 bound to the active site of cathepsin S is also reported.

Keywords:

Peptidomimetic
Chemical synthesis
Organic chemistry
Cathepsin
Biochemistry
Stereochemistry
Structure–activity relationship
Cathepsin S
Amide
Active site
Chemistry
Enzyme inhibitor
Hydrolase

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