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Contrast-enhanced micro-computed tomography of fatigue microdamage accumulation in human cortical bone.

机译:人体皮质骨疲劳微损伤累积的对比增强微计算机断层扫描。

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摘要

Conventional methods used to image and quantify microdamage accumulation in bone are limited to histological sections, which are inherently invasive, destructive, two-dimensional, and tedious. These limitations inhibit investigation of microdamage accumulation with respect to volumetric spatial variation in mechanical loading, bone mineral density, and microarchitecture. Therefore, the objective of this study was to investigate non-destructive, three-dimensional (3-D) detection of microdamage accumulation in human cortical bone using contrast-enhanced micro-computed tomography (micro-CT), and to validate micro-CT measurements against conventional histological methods. Unloaded controls and specimens loaded in cyclic uniaxial tension to a 5% and 10% reduction in secant modulus were labeled with a precipitated BaSO stain for micro-CT and basic fuchsin for histomorphometry. Linear microcracks were similarly labeled by BaSO and basic fuchsin as shown by backscattered electron microscopy and light microscopy, respectively. The higher X-ray attenuation of BaSO relative to the bone extracellular matrix provided enhanced contrast for the detection of damage that was otherwise not able to be detected by micro-CT prior to staining. Therefore, contrast-enhanced micro-CT was able to nondestructively detect the presence, 3-D spatial location, and accumulation of fatigue microdamage in human cortical bone specimens in vitro. Microdamage accumulation was quantified on segmented micro-CT reconstructions as the ratio of BaSO stain volume (SV) to total bone volume (BV). The amount of microdamage measured by both micro-CT (SV/BV) and histomorphometry (Cr.N, Cr.Dn, Cr.S.Dn) progressively increased from unloaded controls to specimens loaded to a 5% and 10% reduction in secant modulus (p < 0.001). Group means for micro-CT measurements of damage accumulation were strongly correlated to those using histomorphometry (p < 0.05), validating the new methods. Limitations of the new methods in the present study included that the precipitated BaSO stain was non-specific and non-biocompatible, and that micro-CT measurements exhibited greater variability compared to conventional histology. Nonetheless, contrast-enhanced micro-CT enabled non-destructive imaging and 3-D spatial information, which are not possible using conventional histological methods.
机译:用于对骨骼中的微损伤累积进行成像和量化的常规方法仅限于组织切片,这些切片固有地具有侵入性,破坏性,二维性和乏味性。这些局限性阻碍了有关机械载荷,骨矿物质密度和微结构的体积空间变化方面的微损伤累积的研究。因此,本研究的目的是研究使用造影剂增强型计算机断层扫描技术(micro-CT)对人皮质骨中微损伤累积的无损三维(3-D)检测,并验证micro-CT常规组织学方法进行测量。将未加载的对照和样品以循环单轴张力加载至割线模量分别降低5%和10%的位置,用沉淀的BaSO染色剂进行micro-CT染色,并用碱性品红蛋白进行组织形态测定。线性微裂纹分别由BaSO和碱性品红标记,分别由反向散射电子显微镜和光学显微镜显示。相对于骨细胞外基质,BaSO 3的更高的X射线衰减为检测损伤提供了增强的对比度,否则在染色前用micro-CT无法检测到损伤。因此,对比增强的微型CT能够在体外无损检测人类皮质骨标本中疲劳微损伤的存在,3-D空间位置和积累。在分段式微CT重建上量化微损伤的累积量,以BaSO染色体积(SV)与总骨体积(BV)的比率表示。通过微型CT(SV / BV)和组织形态测量法(Cr.N,Cr.Dn,Cr.S.Dn)测得的微损伤量从未加样的对照到加样的割线逐渐减少了5%和10%模量(p <0.001)。微型CT测量损伤累积的组均值与使用组织形态计量学的均值高度相关(p <0.05),验证了新方法。本研究中新方法的局限性包括沉淀的BaSO染色是非特异性和非生物相容性的,并且与常规组织学相比,微CT测量显示出更大的可变性。尽管如此,对比增强的微型CT可以实现无损成像和3-D空间信息,而这是使用常规组织学方法无法实现的。

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