Identification of Potent and Selective Cathepsin S Inhibitors Containing Different Central Cyclic Scaffolds

Starting from the weakly active dual CatS/K inhibitor 5, structure-based design supported by X-ray analysis led to the discovery of the potent and selective (>50 000-fold vs CatK) cyclopentane derivative 22 by exploiting specific ligand–receptor interactions in the S2 pocket of CatS. Changing the...

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Bibliographic Details
Published in:Journal of medicinal chemistry 2013-12, Vol.56 (23), p.9789-9801
Main Authors: Hilpert, Hans, Mauser, Harald, Humm, Roland, Anselm, Lilli, Kuehne, Holger, Hartmann, Guido, Gruener, Sabine, Banner, David W, Benz, Joerg, Gsell, Bernard, Kuglstatter, Andreas, Stihle, Martine, Thoma, Ralf, Sanchez, Rubén Alvarez, Iding, Hans, Wirz, Beat, Haap, Wolfgang
Format: Article
Language:English
Subjects:
Animals
Cathepsins - antagonists & inhibitors
Cyclopentanes - chemistry
Cysteine Proteinase Inhibitors - chemical synthesis
Cysteine Proteinase Inhibitors - pharmacokinetics
Humans
Mice
Proline - analogs & derivatives
Structure-Activity Relationship
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Summary:Starting from the weakly active dual CatS/K inhibitor 5, structure-based design supported by X-ray analysis led to the discovery of the potent and selective (>50 000-fold vs CatK) cyclopentane derivative 22 by exploiting specific ligand–receptor interactions in the S2 pocket of CatS. Changing the central cyclopentane scaffold to the analogous pyrrolidine derivative 57 decreased the enzyme as well as the cell-based activity significantly by 24- and 69-fold, respectively. The most promising scaffold identified was the readily accessible proline derivative (e.g., 79). This compound, with an appealing ligand efficiency (LE) of 0.47, included additional structural modifications binding in the S1 and S3 pockets of CatS, leading to favorable in vitro and in vivo properties. Compound 79 reduced IL-2 production in a transgenic DO10.11 mouse model of antigen presentation in a dose-dependent manner with an ED50 of 5 mg/kg.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm401528k