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首页> 外文期刊>Journal of bone and mineral metabolism >Osteoclast differentiation in ectopic bone formation induced by recombinant human bone morphogenetic protein 2 (rhBMP-2).
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Osteoclast differentiation in ectopic bone formation induced by recombinant human bone morphogenetic protein 2 (rhBMP-2).

机译:重组人骨形态发生蛋白2(rhBMP-2)诱导异位骨形成中的破骨细胞分化。

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Osteoclast differentiation in the process of ectopic bone formation induced by recombinant human bone morphogenetic protein 2 (rhBMP-2) was examined to clarify the relationship between osteoclast development and rhBMP-2-induced bone formation. A combination of rhBMP-2 with a porous microsphere (PMS) and blood clot was implanted subcutaneously on the bilateral chest muscles of rats. Tartrate-resistant acid phosphatase (TRAPase) activity, cathepsin K (cath K), and calcitonin receptor (CTR), as markers of osteoclasts and their precursors, were examined using enzyme and immunohistochemical analysis up to 7 days after implantation. Mononuclear cells positive for TRAPase, cath K, and CTR first appeared on day 3 in connective tissue surrounding the PMS after implantation of rhBMP-2. Simultaneously, alkaline phosphatase activity became detectable in mesenchymal cells in the connective tissue. Electron microscopy demonstrated some mononuclear cells with abundant mitochondria and poorly developed rough endoplasmic reticulum in the proximity of mesenchymal cells. However, there was no evidence of cartilage or bone matrix formation on day 3. Osteoclasts in various stages of development, classified by the pattern of immunoreactivity for cath K, were observed by day 7. The polarized intracellular distribution of cath K was found only in osteoclasts attached to bone matrix. In conclusion, we have demonstrated for the first time the appearance of osteoclast precursors before bone matrix formation induced by rhBMP-2, suggesting that bone matrix is not a prerequisite for osteoclast precursor recruitment. Furthermore, we suggest that differentiation into polarized functional osteoclasts is accomplished when the osteoclasts attach to the bone matrix.
机译:检查了重组人骨形态发生蛋白2(rhBMP-2)诱导的异位骨形成过程中的破骨细胞分化,以阐明破骨细胞发育与rhBMP-2诱导的骨形成之间的关系。将rhBMP-2与多孔微球(PMS)和血凝块的组合皮下植入大鼠的双侧胸肌。在植入后长达7天,使用酶和免疫组化分析法检查了抗酒石酸酸性磷酸酶(TRAPase)的活性,组织蛋白酶K(cath K)和降钙素受体(CTR)作为破骨细胞及其前体的标志物。植入rhBMP-2后,第3天,TRAPase,cath K和CTR阳性的单核细胞首先出现在PMS周围的结缔组织中。同时,在结缔组织的间充质细胞中可检测到碱性磷酸酶活性。电子显微镜检查显示,一些单核细胞具有丰富的线粒体,在间充质细胞附近发育较差的粗糙内质网。但是,在第3天没有软骨或骨基质形成的迹象。在第7天,观察到了处于不同发育阶段的破骨细胞(按对Cat K的免疫反应性模式进行分类)。破骨细胞附着在骨基质上。总之,我们首次证明了由rhBMP-2诱导的骨基质形成之前破骨细胞前体的出现,表明骨基质不是破骨细胞前体募集的先决条件。此外,我们建议当破骨细胞附着在骨基质上时,分化为极化功能的破骨细胞就可以完成。

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