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首页> 外文期刊>RSC Advances >Novel cathepsin K inhibitors block osteoclasts in vitro and increase spinal bone density in zebrafish
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Novel cathepsin K inhibitors block osteoclasts in vitro and increase spinal bone density in zebrafish

机译:新型组织蛋白酶K抑制剂在体外阻断破骨细胞并增加斑马鱼的脊骨密度

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Cathepsin K (Cat K) is a predominant cysteine protease and highly potent collagenase expressed in osteoclasts. Cat K inhibitors are anti-resorptive agents to treat osteoporosis. A novel scaffold of cathepsin K inhibitors, exemplified by lead compound 1x , was used as the template for designing and synthesizing a total of 61 derivatives that have not been reported before. An exploratory structure–activity relationship analysis identified the potent Cat K inhibitor A22 , which displayed an IC _(50) value of 0.44 μM against Cat K. A22 was very specific for Cat K and caused a significantly higher in vitro inhibition of the enzyme as compared to that of lead compound 1x . A surface plasmon resonance analysis confirmed in vitro binding of A22 to Cat K. Molecular docking studies indicated several favourable interaction sites for A22 within the active pocket of Cat K. Furthermore, A22 also blocked active osteoclasts in vitro and increased spinal bone density in zebrafish, in which it showed an activity that was higher than that of the marketed therapeutic bone metabolizer etidronate disodium. A22 represents a very promising lead compound for the development of novel antiresorptive agents functioning as orthosteric inhibitors of Cat K.
机译:组织蛋白酶K(Cat K)是破骨细胞中主要的半胱氨酸蛋白酶和高效胶原酶。 Cat K抑制剂是用于治疗骨质疏松症的抗吸收剂。一种新型的组织蛋白酶K抑制剂支架,以铅化合物1x为例,被用作模板来设计和合成总共61种以前未报道的衍生物。探索性的结构-活性关系分析确定了有效的Cat K抑制剂A22,其对Cat K的IC _(50)值为0.44μM。A22对Cat K具有非常高的特异性,并且在体外对酶的抑制作用显着高于与铅化合物1x相比。表面等离振子共振分析证实了A22在体外与Cat K结合。分子对接研究表明,A22在Cat K的活性囊内有几个有利的相互作用位点。此外,A22在体外还阻断了活性破骨细胞并增加了斑马鱼的脊骨密度,其中显示出的活性高于市售的治疗性骨代谢剂依替膦酸钠二钠。 A22代表一种非常有前途的先导化合物,可用于开发新型抗吸收剂,用作Cat K的正构抑制剂。

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