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Ultrastructural elastic deformation of cortical bone tissue probed by NIR Raman spectroscopy

机译:NIR拉曼光谱法探测皮质骨组织的超微结构弹性变形

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Raman spectroscopy is used as a probe of ultrastructural (molecular) changes in both the mineral and matrix (protein and glycoprotein, predominantly type I collagen) components of murine cortical bone as it responds to loading in the elastic regime. At the ultrastructural level, crystal structure and protein secondary structure distort as the tissue is loaded. These structural changes are followed as perturbations to tissue spectra. We load tissue in a custom-made dynamic mechanical tester that fits on the stage of a Raman microprobe and can accept hydrated tissue specimens. As the specimen is loaded in tension and/or compression, the shifts in mineral P-O_4 v_1 and relative band heights in the Amide III band envelope are followed with the microprobe. Average load is measured using a load cell while the tissue is loaded under displacement control. Changes occur in both the mineral and matrix components of bone as a response to elastic deformation. We propose that the mineral apatitic crystal lattice is deformed by movement of calcium and other ions. The matrix is proposed to respond by deformation of the collagen backbone. Raman microspectroscopy shows that bone mineral is not a passive contributor to tissue strength. The mineral active response to loading may function as a local energy storage and dissipation mechanism, thus helping to protect tissue from catastrophic damage.
机译:拉曼光谱被用作鼠的超微结构(分子)改变了矿物和矩阵两者(蛋白质和糖蛋白,主要是I型胶原)的部件它响应在弹性状态装载骨皮质的探针。在超微结构水平,晶体结构和蛋白质二级结构扭曲随着组织被加载。这些结构上的改变遵循作为扰动组织光谱。我们在一个特制的动态力学测试仪加载组织是在拉曼微舞台配合和可以接受的水合组织标本。作为试件在张力和/或压缩加载,在移位矿物P-O_4 V_1和在酰胺III带包络相对带高度被随后用微探针。平均负载是利用测力传感器,而所述组织位移控制下加载测定。变化发生在骨的两个矿物和基质组分如弹性变形的响应。我们建议,矿物磷灰石晶格是由钙和其他离子的移动而变形。该矩阵是由胶原蛋白骨架的变形提议作出回应。显微拉曼光谱表明,骨矿物质是不是一个被动的贡献者组织的力量。装载矿物活性响应可以用作本地能量存储和耗散机理,从而有助于从灾难性的破坏保护组织。

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