首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >Circulating fibronectin affects bone matrix, whereas osteoblast fibronectin modulates osteoblast function.
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Circulating fibronectin affects bone matrix, whereas osteoblast fibronectin modulates osteoblast function.

机译:循环纤连蛋白会影响骨基质,而成骨细胞纤连蛋白会调节成骨细胞功能。

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The bone matrix is composed mostly of collagen, but the initial and continuous presence of fibronectin was found to be crucial for collagen matrix integrity in vitro. It has been assumed that osteoblasts produce the fibronectin required for bone matrix formation. Using transgenic mice, we conditionally deleted fibronectin in the osteoblasts and in the liver using the cre-loxP system. We also used mice with mutated fibronectin and conditionally deleted beta(1)-integrin in osteoblasts to identify the receptor involved in fibronectin effects on osteoblasts. Conditional deletion of fibronectin in the differentiating osteoblasts [using the 2.3 kb collagen-alpha1(I) promoter] failed to show a decrease in fibronectin amount in the bone matrix despite evidence of successful deletion. Using these mice we established that osteoblast-derived fibronectin solely affects osteoblast function. This effect was not mediated by integrins that bind to the RGD motif. Conditional deletion of fibronectin in the liver showed a marked decrease in fibronectin content in the matrix associated with decreased mineral-to-matrix ratio and changed biomechanical properties but had no effect on osteoblasts or osteoclasts. In conclusion, osteoblast fibronectin affects osteoblasts function. This does not seem to be mediated by the RGD motif on fibronectin. In contrast, liver-derived fibronectin affects bone matrix properties without affecting osteoblast or osteoclast function. A novel role for liver-derived circulating fibronectin thus was defined and delineated from that of locally produced fibronectin.
机译:骨基质主要由胶原蛋白组成,但发现纤连蛋白的最初和持续存在对体外胶原蛋白基质的完整性至关重要。已经假定成骨细胞产生骨基质形成所需的纤连蛋白。使用转基因小鼠,我们使用cre-loxP系统有条件地删除了成骨细胞和肝脏中的纤连蛋白。我们还使用了纤连蛋白突变和成骨细胞中有条件删除的beta(1)-整合素的小鼠,以鉴定参与纤连蛋白对成骨细胞作用的受体。尽管有成功删除的证据,但在分化的成骨细胞中有条件地删除纤连蛋白[使用2.3 kb胶原-α1(I)启动子]未能显示出骨基质中纤连蛋白的量减少。使用这些小鼠,我们确定成骨细胞衍生的纤连蛋白仅影响成骨细胞的功能。这种作用不是由结合RGD基序的整联蛋白介导的。肝脏中纤连蛋白的条件性缺失显示基质中纤连蛋白的含量显着降低,与矿物质与基质的比率降低以及生物力学性质改变有关,但对成骨细胞或破骨细胞没有影响。总之,成骨细胞纤连蛋白会影响成骨细胞的功能。这似乎不是由纤连蛋白上的RGD基序介导的。相反,肝源性纤连蛋白会影响骨基质特性,而不会影响成骨细胞或破骨细胞功能。因此定义了肝脏衍生的循环纤连蛋白的新作用,并与局部产生的纤连蛋白的作用进行了描述。

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