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Paradoxical Response to Mechanical Unloading in Bone Loss Microarchitecture and Bone Turnover Markers

机译:在骨丢失微结构和骨翻转标记中对机械卸载的矛盾响应

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摘要

>Background: Sclerostin, encoded by the SOST gene, has been implicated in the response to mechanical loading in bone. Some studies demonstrated that unloading leads to up-regulated SOST expression, which may induce bone loss.>Purpose: Most reported studies regarding the changes caused by mechanical unloading were only based on a single site. Considering that the longitudinal bone growth leads to cells of different age with different sensitivity to unloading, we hypothesized that bone turnover in response to unloading is site specific.>Methods: We established a disuse rat model by sciatic neurectomy in tibia. In various regions at two time-points, we evaluated the bone mass and microarchitecture in surgically-operated rats and control rats by micro-Computed Tomography (micro-CT) and histology, sclerostin/SOST by immunohistochemistry, enzyme-linked immunosorbent assay (ELISA), and quantitative reverse transcription polymerase chain reaction (qPCR), tartrate resistant acid phosphatase 5b (TRAP 5b) by ELISA and TRAP staining, and other bone markers by ELISA. >Results: Micro-CT and histological analysis confirmed bone volume in the disuse rats was significantly decreased compared with those in the time-matched control rats, and microarchitecture also changed 2 and 8 weeks after surgery. Compared with the control groups, SOST mRNA expression in the diaphysis was down-regulated at both week 2 and 8. On the contrary, the percentage of sclerostin-positive osteocytes showed an up-regulated response in the 5 - 6 mm region away from the growth plate, while in the 2.5 - 3.5 mm region, the percentage was no significant difference. Nevertheless, in 0.5 - 1.5 mm region, the percentage of sclerostin-positive osteocytes decreased after 8 weeks, consistent with serum SOST level. Besides, the results of TRAP also suggested that the expression in response to unloading may be opposite in different sites or system.>Conclusion: Our data indicated that unloading-induced changes in bone turnover are probably site specific. This implies a more complex response pattern to unloading and unpredictable therapeutics which target SOST or TRAP 5b.
机译:>背景:由SOST基因编码的硬化蛋白与骨骼机械负荷的反应有关。一些研究表明,卸载会导致SOST表达上调,这可能会导致骨骼丢失。>目的:有关机械卸载引起的变化的大多数报道的研究仅基于单个位置。考虑到骨骼的纵向生长会导致不同年龄的细胞对卸荷的敏感性不同,因此我们假设响应卸荷的骨转换是针对特定部位的。>方法:我们通过坐骨神经切除术建立了一个废弃的大鼠模型。胫骨在两个时间点的各个区域,我们通过显微计算机断层扫描(micro-CT)和组织学,免疫组织化学,硬化素/ SOST,酶联免疫吸附测定(ELISA)对手术大鼠和对照大鼠的骨质量和微结构进行了评估)和定量逆转录聚合酶链反应(qPCR),抗酒石酸酸性磷酸酶5b(TRAP 5b)通过ELISA和TRAP染色以及其他骨标记物通过ELISA。 >结果:显微CT和组织学分析证实,与时间匹配的对照组相比,废用大鼠的骨量明显减少,并且在术后2周和8周,微结构也发生了变化。与对照组相比,在第2周和第8周,骨干中SOST mRNA的表达均被下调。相反,硬化蛋白阳性骨细胞的百分比在距牙周5-6 mm区域显示出上调的反应。生长板,而在2.5-3.5 mm区域,百分比没有显着差异。然而,在0.5-1.5 mm区域,硬化素阳性骨细胞的百分比在8周后下降,与血清SOST水平一致。此外,TRAP的结果还表明,在不同部位或系统中,对卸荷的表达可能是相反的。>结论:我们的数据表明,卸荷引起的骨转换变化可能是特定部位的。这意味着针对以SOST或TRAP 5b为目标的卸载和不可预测的治疗方法的反应更为复杂。

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