首页> 外文期刊>Journal of cell biology >Cadherin-6 Mediates the Heterotypic Interactions between the Hemopoietic Osteoclast Cell Lineage and Stromal Cells in a Murine Model of Osteoclast Differentiation
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Cadherin-6 Mediates the Heterotypic Interactions between the Hemopoietic Osteoclast Cell Lineage and Stromal Cells in a Murine Model of Osteoclast Differentiation

机译:Cadherin-6介导破骨细胞分化的小鼠模型中造血性破骨细胞细胞谱系和基质细胞之间的异型相互作用。

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Osteoclasts are multinucleated cells of hemopoietic origin that are responsible for bone resorption during physiological bone remodeling and in a variety of bone diseases. Osteoclast development requires direct heterotypic cell–cell interactions of the hemopoietic osteoclast precursors with the neighboring osteoblast/stromal cells. However, the molecular mechanisms underlying these heterotypic interactions are poorly understood. We isolated cadherin-6 isoform, denoted cadherin-6/2 from a cDNA library of human osteoclast-like cells. The isolated cadherin-6/2 is 3,423 bp in size consisting of an open reading frame of 2,115 bp, which encodes 705 amino acids. This isoform lacks 85 amino acids between positions 333 and 418 and contains 9 different amino acids in the extracellular domain compared with the previously described cadherin-6. The human osteoclast-like cells also expressed another isoform denoted cadherin-6/1 together with the cadherin-6. Introduction of cadherin-6/2 into L-cells that showed no cell–cell contact caused evident morphological changes accompanied with tight cell–cell association, indicating the cadherin-6/2 we isolated here is functional. Moreover, expression of dominant-negative or antisense cadherin-6/2 construct in bone marrow–derived mouse stromal ST2 cells, which express only cadherin-6/2, markedly impaired their ability to support osteoclast formation in a mouse coculture model of osteoclastogenesis. Our results suggest that cadherin-6 may be a contributory molecule to the heterotypic interactions between the hemopoietic osteoclast cell lineage and osteoblast/bone marrow stromal cells required for the osteoclast differentiation. Since both osteoclasts and osteoblasts/bone marrow stromal cells are the primary cells controlling physiological bone remodeling, expression of cadherin-6 isoforms in these two cell types of different origin suggests a critical role of these molecules in the relationship of osteoclast precursors and cells of osteoblastic lineage within the bone microenvironment.
机译:破骨细胞是造血来源的多核细胞,负责在生理性骨重塑过程中和各种骨骼疾病中的骨吸收。破骨细胞的发育需要造血性破骨细胞前体与邻近的成骨细胞/基质细胞直接发生异型细胞相互作用。然而,对这些异型相互作用的分子机制了解甚少。我们从人破骨细胞样细胞的cDNA文库中分离出cadherin-6亚型,表示为cadherin-6 / 2。分离的钙粘着蛋白-6/2大小为3,423 bp,由2,115 bp的开放阅读框组成,其编码705个氨基酸。与先前描述的钙粘着蛋白6相比,该同工型在位置333和418之间缺少85个氨基酸,并且在细胞外结构域中包含9个不同的氨基酸。人破骨细胞样细胞还表达了另一种同工型,称为钙粘蛋白-6/1和钙粘蛋白6。在没有细胞间接触的L细胞中导入钙黏着蛋白6/2不会引起明显的形态变化,同时伴随着紧密的细胞间结合,这说明我们在这里分离出的钙黏着蛋白6/2是有功能的。此外,在骨髓衍生的小鼠基质ST2细胞中仅表达钙粘着蛋白6/2的显性阴性或反义钙粘着蛋白6/2构建体的表达显着削弱了它们在破骨细胞生成的小鼠共培养模型中支持破骨细胞形成的能力。我们的结果表明,钙粘着蛋白6可能是造血细胞破骨细胞谱系与破骨细胞分化所需的成骨细胞/骨髓基质细胞之间异型相互作用的一个贡献分子。由于破骨细胞和成骨细胞/骨髓基质细胞都是控制生理性骨重塑的主要细胞,因此钙钙粘蛋白-6同工型在这两种不同来源的细胞中的表达表明这些分子在破骨细胞前体与成骨细胞之间的关系中起着至关重要的作用。骨骼微环境内的血统。

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