Distinct roles of cathepsin K and cathepsin L in osteoclastic bone resorption

The role of cathepsin K (CAK), cloned as a novel collagenolytic cysteine protease (CCP), cathepsin L (CAL) and cathepsin B (CAB) in bone resorption was investigated. In mouse calvarial organ culture medium, GAL, detected in trace amounts in control conditions, and CCP activity were increased by stimulants of bone resorption: 1 alpha,25-(0H)(2)D-3 parathyroid hormone (PTH), IL-1 alpha, IL-6 or TNF-alpha. CAK was the most abundantly detected CCP and was not increased by these stimulants. In the absence of the stimulants, only antisense oligodeoxynucleotide (AS-ODN) for CAK suppressed collagenolysis and CCP activity. On the other hand, in the presence of the stimulants, AS-ODN for both CAK and CAL suppressed collagenolysis and CCP activity, and these activities were additive. AS-ODN for CAB did not suppress collagenolysis. These results suggested CAK was constitutively synthesized as the main CCP, and CAL was synthesized as an inducible CCP in osteoclasts to degrade type-I collagen in combination with CAK.