Trifluoroethylamines as amide isosteres in inhibitors of cathepsin K
- 作者:W. Cameron Black ; Christopher I. Bayly ; Dana E. Davis ; Sylvie Desmarais ; Jean-Pierre Falgueyret ; Serge Lé ; ger ; Chun Sing Li ; Fré ; dé ; ric Massé ; Daniel J. McKay ; James T. Palmer et a
- 刊名:Bioorganic and Medicinal Chemistry Letters
- 出版年:2005
- 期刊代码:10_0960894x
- 类别:ch
- 出版时间:2005
- 卷:15
- 期:21
- 页码:4741-4744
- 文件大小:241 K
摘要
The P2-P3 amide of dipeptide cathepsin K inhibitors can be replaced by the metabolically stable trifluoroethylamine group. The non-basic nature of the nitrogen allows the important hydrogen bond to Gly66 to be made. The resulting compounds are 10- to 20-fold more potent than the corresponding amide derivatives. Compound 8 is a 5 pM inhibitor of human cathepsin K with >10,000-fold selectivity over other cathepsins.