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Merck
CN

Chlorhexidine inhibits the activity of dental cysteine cathepsins.

Journal of dental research (2012-01-24)
P M C Scaffa, C M P Vidal, N Barros, T F Gesteira, A K Carmona, L Breschi, D H Pashley, L Tjäderhane, I L S Tersariol, F D Nascimento, M R Carrilho
摘要

The co-expression of MMPs and cysteine cathepsins in the human dentin-pulp complex indicates that both classes of enzymes can contribute to the endogenous proteolytic activity of dentin. Chlorhexidine (CHX) is an efficient inhibitor of MMP activity. This study investigated whether CHX could also inhibit cysteine cathepsins present in dentin. The inhibitory profile of CHX on the activity of dentin-extracted and recombinant cysteine cathepsins (B, K, and L) was monitored in fluorogenic substrates. The rate of substrate hydrolysis was spectrofluorimetrically measured, and inhibitory constants were calculated. Molecular docking was performed to predict the binding affinity between CHX and cysteine cathepsins. The results showed that CHX inhibited the proteolytic activity of dentin-extracted cysteine cathepsins in a dose-dependent manner. The proteolytic activity of human recombinant cathepsins was also inhibited by CHX. Molecular docking analysis suggested that CHX strongly interacts with the subsites S2 to S2' of cysteine cathepsins B, K, and L in a very similar manner. Taken together, these results clearly showed that CHX is a potent inhibitor of the cysteine cathepsins-proteolytic enzymes present in the dentin-pulp complex.

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Sigma-Aldrich
E-64, protease inhibitor
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货号包装规格是否有货价格数量
100 μg
预计发货时间 2025年5月12日
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Sigma-Aldrich
Z-Phe-Arg 7-酰氨基-4-甲基香豆素 盐酸盐, kallikrein substrate
登录查看公司和协议定价
货号包装规格是否有货价格数量
100 μg
预计发货时间 2025年5月12日
详情...
针对您的靶标提供了无防腐剂重组抗体。欢迎选购 ZRB2114
¥7,733.80