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Microfluidic Enhancement of Intramedullary Pressure Increases Interstitial Fluid Flow and Inhibits Bone Loss in Hindlimb Suspended Mice

机译:微流体增强髓内压可增加间质悬浮小鼠的间质液流量并抑制骨丢失

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摘要

Interstitial fluid flow (IFF) has been widely hypothesized to mediate skeletal adaptation to mechanical loading. Although a large body of in vitro evidence has demonstrated that fluid flow stimulates osteogenic and antiresorptive responses in bone cells, there is much less in vivo evidence that IFF mediates loading-induced skeletal adaptation. This is due in large part to the challenges associated with decoupling IFF from matrix strain. In this study we describe a novel microfluidic system for generating dynamic intramedullary pressure (ImP) and IFF within the femurs of alert mice. By quantifying fluorescence recovery after photobleaching (FRAP) within individual lacunae, we show that microfluidic generation of dynamic ImP significantly increases IFF within the lacunocanalicular system. In addition, we demonstrate that dynamic pressure loading of the intramedullary compartment for 3 minutes per day significantly eliminates losses in trabecular and cortical bone mineral density in hindlimb suspended mice, enhances trabecular and cortical structural integrity, and increases endosteal bone formation rate. Unlike previously developed modalities for enhancing IFF in vivo, this is the first model that allows direct and dynamic modulation of ImP and skeletal IFF within mice. Given the large number of genetic tools for manipulating the mouse genome, this model is expected to serve as a powerful investigative tool in elucidating the role of IFF in skeletal adaptation to mechanical loading and molecular mechanisms mediating this process. © 2010 American Society for Bone and Mineral Research.
机译:间隙流体流(IFF)已被广泛假设为介导骨骼对机械负荷的适应。尽管大量体外证据显示流体流动会刺激骨细胞中的成骨和抗吸收反应,但体内证据表明,IFF介导负荷诱导的骨骼适应。这在很大程度上归因于与IFF与基质应变解耦相关的挑战。在这项研究中,我们描述了一种新型的微流控系统,用于在警觉小鼠股骨内产生动态髓内压(ImP)和IFF。通过量化单个腔内光漂白(FRAP)后的荧光恢复,我们显示了动态ImP的微流产生显着增加了鼻腔系统内的IFF。此外,我们证明了每天3分钟的髓腔隔室动压加载可显着消除后肢悬吊小鼠的小梁和皮质骨矿物质密度损失,增强小梁和皮质结构完整性,并增加骨内膜骨形成率。与先前开发的增强体内IFF的方式不同,这是第一个允许在小鼠中直接和动态调节ImP和骨骼IFF的模型。考虑到操纵小鼠基因组的大量遗传工具,该模型有望成为阐明IFF在骨骼适应机械负荷和介导该过程的分子机制中的作用的有力研究工具。 ©2010美国骨骼和矿物质研究学会。

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