破骨细胞分化机制的研究进展
The advance in the study of the mechanism of osteoclast differentiation
  
DOI:10.3969/j.issn.1006.7108.2015.12.024
中文关键词:  破骨细胞  骨吸收  巨噬细胞集落刺激因子  核因子k B受体活化因子配体
英文关键词:Osteoclast  Bone resorption  Macrophage colony stimulating factor  Receptor activator for nuclear factor-k B ligand
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作者单位
任莉荣1 徐永清2* 1.昆明医科大学昆明650504 2.成都军区昆明总医院骨科昆明650032 
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中文摘要:
      破骨细胞为人体主要的骨吸收细胞,对骨骼的发育及维持具有重要作用,同时破骨细胞的异常活化对多种溶骨性疾病的发展具有重要作用;明确破骨细胞的分化机制,可为多种骨代谢性疾病提供新的治疗策略及药物靶点。大量的实验对破骨细胞的分化机制进行了研究,并确认有一些基因为破骨细胞分化形成所必需,这些基因的缺失或突变将导致破骨细胞形成障碍,进而引起骨质硬化;并且由巨睡细胞集落刺激因子(macrophage colony stimulating factor,M-CSF)、核因子k B受体活化因子 配体(receptor Activator for Nuclear Factor-k B Ligand, RANKL)及免疫受体酪氨酸激活基序(immunoreceptor tyrosine-based activation motif,ITAM)介导的3条重要的信号通路参与其分化过程,3条信号通路相互作用,共同促进破骨细胞的分化形成,但RANKL如何激活ITAM信号通路,有待进一步研究,本文就破骨细胞分化机制的研究进展作一综述。
英文摘要:
      Osteoclasts are the sole bone resorbing cells. These cells are important for the development and maintenance of the bone,and the abnormal activation of osteoclasts plays an important role in the development of a variety of osteolytic diseases. The clear understanding of the mechanism of osteoclast differentiation may provide new therapeutic strategies and novel drug targets for a variety of bone metabolic diseases. A large number of experiments have been done to study the mechanism of osteoclast differentiation. Some genes are required for the osteoclast differentiation. Three vital signal pathways mediated by M-CSF (macrophage colony stimulating factor, M-CSF),RANKL (receptor activator for nuclear factor-kB ligand, RANKL), and ITAM (immunoreceptor tyrosine-based activation motif, ITAM) , respectively, are involved in the differentiation process. To promote the formation of osteoclast, the three signaling pathways interact with each other, but how RANKL activates the ITAM signaling pathway needs to be further studied. This article reviews the advance in the study of mechanism of osteoclast differentiation.
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