Enhancement of Inhibitory Activity by Combining Allosteric Inhibitors Putatively Binding to Different Allosteric Sites on Cathepsin K

Shun Sato; Kana Yamamoto; Moeno Ito; Katsutoshi Nishino; Takanao Otsuka; Kazuhiro Irie; Masaya Nagao

doi:10.3390/molecules28104197

Enhancement of Inhibitory Activity by Combining Allosteric Inhibitors Putatively Binding to Different Allosteric Sites on Cathepsin K

Molecules. 2023 May 19;28(10):4197. doi: 10.3390/molecules28104197.

Authors

Shun Sato¹, Kana Yamamoto¹, Moeno Ito¹, Katsutoshi Nishino¹, Takanao Otsuka², Kazuhiro Irie³, Masaya Nagao¹

Affiliations

¹ Graduate School of Biostudies, Kyoto University, Kyoto 606-8502, Japan.
² Department of Applied Chemistry and Biotechnology, Okayama University of Science, Okayama 700-0005, Japan.
³ Graduate School of Agriculture, Kyoto University, Kyoto 606-8502, Japan.

Abstract

Background: Cathepsin K, which is involved in bone resorption, is a good target for treating osteoporosis, but no clinically approved medicine has been developed. Recently, allosteric inhibitors with high specificity and few side effects have been attracting attention for use in new medicines.

Methods: Cathepsin K inhibitors were isolated from the methanol extract of Chamaecrista nomame (Leguminosae) using cathepsin K inhibition activity-assisted multi-step chromatography. Standard kinetic analysis was employed to examine the mechanism of cathepsin K inhibition when an isolated inhibitor and its derivative were used. The allosteric binding of these cathepsin K inhibitors was supported by a docking study using AutoDock vina. Combinations of allosteric cathepsin K inhibitors expected to bind to different allosteric sites were examined by means of cathepsin K inhibition assay.

Results: Two types of cathepsin K inhibitors were identified in the methanol extract of Chamaecrista nomame. One type consisted of cassiaoccidentalin B and torachrysone 8-β-gentiobioside, and inhibited both cathepsin K and B with similar inhibitory potential, while the other type of inhibitor consisted of pheophytin a, and inhibited cathepsin K but not cathepsin B, suggesting that pheophytin a binds to an allosteric site of cathepsin K. Kinetic analysis of inhibitory activity suggested that pheophytin a and its derivative, pheophorbide b, bind allosterically to cathepsin K. This possibility was supported by a docking study on cathepsin K. The cathepsin K inhibitory activity of pheophytin a and pheophorbide b was enhanced by combining them with the allosteric inhibitors NSC 13345 and NSC94914, which bind to other allosteric sites on cathepsin K.

Conclusions: Different allosteric inhibitors that bind to different sites in combination, as shown in this study, may be useful for designing new allosteric inhibitory drugs with high specificity and few side effects.

Keywords: Chamaecrista nomame; allosteric; cathepsin K; inhibitor; pheophorbide b; pheophytin a.

MeSH terms

Allosteric Site
Bone Resorption*
Cathepsin K / metabolism
Cathepsins / metabolism
Humans
Kinetics
Methanol*

Substances

Cathepsin K
Methanol
Cathepsins

Grants and funding

JPMJSA1506/Japan Science and Technology Agency