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  2. Pharmacological inhibitors to identify roles of cathepsin K in cell-based studies: a comparison of available tools

Pharmacological inhibitors to identify roles of cathepsin K in cell-based studies: a comparison of available tools

  • Biol Chem. 2009 Sep;390(9):941-8. doi: 10.1515/BC.2009.092.
Sylvie Desmarais 1 Frédéric Massé M David Percival
Affiliations

Affiliation

  • 1 Department of Discovery Biology, Merck Frosst Center for Therapeutic Research, Kirkland, Quebec, Canada.
Abstract

Cathepsin K (Cat K) degrades bone type I collagen and is a target for the pharmacological treatment of osteoporosis. Further roles for Cat K have been recently described, some of which are supported by the use of purportedly selective Cat K inhibitors in human and rodent cell-based assays. Twelve commercial and non-commercial Cat K inhibitors were profiled against a panel of purified human, rat, and mouse cysteine cathepsins and in two cell-based Enzyme occupancy assays for activity against Cat K, B, and L. Ten inhibitors, including the carbohydrazide Cat K inhibitor II (Boc-Phe-Leu-NHNH-CO-NHNH-Leu-Z), the non-covalent K4b, and the epoxide NC-2300, have either little Cat K selectivity, or appear poorly cell penetrant. The amino-acetonitrile-containing inhibitors L-873724 and odanacatib show greater than 100-fold human Cat K Enzyme selectivity and have similar IC(50) values against each Cathepsin in cell-based and Enzyme assays. The basic inhibitor balicatib has greater cellular potencies than expected on the basis of purified Enzyme assays. The accumulation of [(14)C]-balicatib in fibroblasts is blocked by prior treatment of the cells with NH(4)Cl, consistent with balicatib having lysosomotropic properties. These results support the use of L-873724 and odanacatib as tools to identify novel roles for Cat K using human cell-based systems, but suggest using caution in the interpretation of studies employing the Other compounds.

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