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. 2005 Nov 1;15(21):4741-4.
doi: 10.1016/j.bmcl.2005.07.071.

Trifluoroethylamines as amide isosteres in inhibitors of cathepsin K

W Cameron Black  1 Christopher I BaylyDana E DavisSylvie DesmaraisJean-Pierre FalgueyretSerge LégerChun Sing LiFrédéric MasséDaniel J McKayJames T PalmerM David PercivalJoël RobichaudNancy TsouRobert Zamboni
Affiliations

Trifluoroethylamines as amide isosteres in inhibitors of cathepsin K

W Cameron Black et al. Bioorg Med Chem Lett. .

Abstract

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.

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