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首页> 外文期刊>Osteoporosis international: a journal established as result of cooperation between the European Foundation for Osteoporosis and the National Osteoporosis Foundation of the USA >Mechanical loading-related changes in osteocyte sclerostin expression in mice are more closely associated with the subsequent osteogenic response than the peak strains engendered.
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Mechanical loading-related changes in osteocyte sclerostin expression in mice are more closely associated with the subsequent osteogenic response than the peak strains engendered.

机译:与产生的峰值菌株相比,小鼠中骨细胞硬化素表达中与机械负荷相关的变化与随后的成骨反应更紧密相关。

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摘要

Osteocyte sclerostin is regulated by loading and disuse in mouse tibiae but is more closely related to subsequent local osteogenesis than the peak strains engendered.The purpose of this study was to assess the relationship between loading-related change in osteocyte sclerostin expression, local strain magnitude, and local bone modeling/remodeling.The right tibiae of 19-week-old female C57BL/6 mice were subjected to non-invasive, dynamic axial loading and/or to sciatic neurectomy-induced disuse. The sclerostin status of osteocytes was evaluated immunohistochemically, changes in bone mass by micro-computed tomography, new bone formation by histomorphometry, and loading-induced strain by strain gauges and finite element analysis.In cortical bone of the tibial shaft, loading engendered strains of similar peak magnitude proximally and distally. Proximally, sclerostin-positive osteocytes decreased and new bone formation increased. Distally, there was neither decrease in sclerostin-positive osteocytes nor increased osteogenesis. In trabecular bone of the proximal secondary spongiosa, loading decreased sclerostin-positive osteocytes and increased bone volume. Neither occurred in the primary spongiosa. Disuse increased sclerostin-positive osteocytes and decreased bone volume at all four sites. Loading reversed this sclerostin upregulation to a level below baseline in the proximal cortex and secondary spongiosa.Loading-related sclerostin downregulation in osteocytes of the mouse tibia is associated preferentially with regions where new bone formation is stimulated rather than where high peak strains are engendered. The mechanisms involved remain unclear, but could relate to peak surface strains not accurately reflecting the strain-related osteogenic stimulus or that sclerostin regulation occurs after sufficient signal processing to distinguish between local osteogenic and non-osteogenic responses.
机译:骨胫骨中的骨细胞硬化素受负荷和不使用的调节,但与随后产生的峰值菌株相比,与随后的局部成骨作用更紧密相关。本研究的目的是评估骨水泥硬化素表达的负荷相关变化与局部应变幅度之间的关系。对19周大的雌性C57BL / 6小鼠的右胫骨进行无创动态轴向负荷和/或坐骨神经切除术所致的废用。通过免疫组织化学方法评估骨细胞的硬化素状态,通过显微计算机断层扫描评估骨量的变化,通过组织形态计量学评估新骨的形成,通过应变仪和有限元分析来评估加载引起的应变。在胫骨干的皮质骨中,加载产生的应变近端和远端的峰值大小相似。近端,硬化素阳性骨细胞减少,新骨形成增加。从远端来看,硬化素阳性骨细胞既没有减少,也没有增加成骨作用。在近端继发性海绵状骨的小梁骨中,负荷减少了硬化素阳性的骨细胞并增加了骨体积。两者均未发生于原发性海绵体内。停用增加硬化蛋白阳性的骨细胞,并减少所有四个部位的骨量。负荷使硬化蛋白的上调逆转至近端皮质和继发性海绵体内的基线以下。与负荷相关的小鼠胫骨骨细胞中的硬化蛋白下调优先与刺激新骨形成的区域相关,而不是与产生高峰值应变的区域相关。所涉及的机制尚不清楚,但可能与峰值表面应变不完全反映应变相关的成骨刺激有关,或硬化信号调节发生在充分信号处理以区分局部成骨和非成骨反应后。

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