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Osteocyte-derived HB-GAM (pleiotrophin) is associated with bone formation and mechanical loading.

机译:骨细胞衍生的HB-GAM(促卵磷脂)与骨形成和机械负荷有关。

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摘要

HB-GAM (also known as pleiotrophin) is a cell matrix-associated protein that is highly expressed in bone. It affects osteoblast function, and might therefore play a role in bone development and remodeling. We aimed to investigate the role of HB-GAM in bone in vivo and in vitro. The bones of HB-GAM deficient mice with an inbred mouse background were studied by histological, histomorphometrical, radiological, biomechanical and mu-CT analyses and the effect of immobilization was evaluated. HB-GAM localization in vivo was studied. MLO-Y4 osteocytes were subjected to fluid shear stress in vitro, and gene and protein expression were studied by subtractive hybridization, quantitative PCR and Western blot. Human osteoclasts were cultured in the presence of rhHB-GAM and their formation and resorption activities were assayed. In agreement with previous reports, the skeletal structure of the HB-GAM knockout mice developed normally. However, a growth retardation of the weight-bearing bones was observed by 2 months of age, suggesting a link to physical activity. Adult HB-GAM deficient mice were characterized by low bone formation and osteopenia, as well as resistance to immobilization-dependent bone remodeling. HB-GAM was localized around osteocytes and their processes in vivo and furthermore, osteocytic HB-GAM expression was upregulated by mechanical loading in vitro. HB-GAM did not affect on human osteoclast formation or resorption in vitro. Taken together, our results suggest that HB-GAM is an osteocyte-derived factor that could participate in mediating the osteogenic effects of mechanical loading on bone.
机译:HB-GAM(也称为多营养蛋白)是一种与细胞基质相关的蛋白质,在骨骼中高度表达。它会影响成骨细胞的功能,因此可能在骨骼发育和重塑中发挥作用。我们旨在研究HB-GAM在体内和体外在骨骼中的作用。通过组织学,组织形态学,放射学,生物力学和mu-CT分析研究了具有近交小鼠背景的HB-GAM缺陷小鼠的骨骼,并评估了固定效果。研究了HB-GAM在体内的定位。 MLO-Y4骨细胞在体外受到流体剪切应力作用,并通过消减杂交,定量PCR和Western印迹研究了基因和蛋白质表达。在rhHB-GAM存在下培养人破骨细胞,并测定其形成和吸收活性。与先前的报道一致,HB-GAM基因敲除小鼠的骨骼结构正常发育。但是,到2个月大时,观察到了负重骨骼的生长发育迟缓,表明与体育锻炼有关。成年HB-GAM缺陷小鼠的特征是低骨形成和骨量减少,以及对固定化依赖性骨重塑的抗性。 HB-GAM定位于骨细胞及其体内过程,此外,体外机械负荷会上调骨细胞HB-GAM的表达。 HB-GAM不会影响人破骨细胞的形成或体外吸收。综上所述,我们的结果表明HB-GAM是一种骨细胞衍生的因子,可以参与介导机械负荷对骨骼的成骨作用。

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