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首页> 外文期刊>Biomechanics and modeling in mechanobiology >Can the diverse elastic properties of trabecular and cortical bone be attributed to only a few tissue-independent phase properties and their interactions? Arguments from a multiscale approach
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Can the diverse elastic properties of trabecular and cortical bone be attributed to only a few tissue-independent phase properties and their interactions? Arguments from a multiscale approach

机译:小梁和皮质骨的各种弹性特性能否仅归因于少数与组织无关的相特性及其相互作用?多尺度方法的论点

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摘要

As candidates for tissue-independent phases of cortical and trabecular bone we consider (i) hydroxyapatite, (ii) collagen, (iii) ultrastructural water and non-collagenous organic matter, and (iv) marrow (water) filling the Haversian canals and the intertrabecular space. From experiments reported in the literature, we assign stiffness properties to these phases (experimental set I). On the basis of these phase definitions, we develop, within the framework of continuum micromechanics, a two-step homogenization procedure: (i) at a length scale of 100–200 nm, hydroxyapatite (HA) crystals build up a crystal foam (polycrystal), and water and non-collagenous organic matter fill the intercrystalline space (homogenization step I); (ii) at the ultrastructural scale of mineralized tissues (5–10 microns), collagen assemblies composed of collagen molecules are embedded into the crystal foam, acting mechanically as cylindrical templates. At an enlarged material scale of 5–10 mm, the second homogenization step also accommodates the micropore space as cylindrical pore inclusions (Haversian and Volkmann canals, inter-trabecular space) that are suitable for both trabecular and cortical bone. The inputs for this micromechanical model are the tissue-specific volume fractions of HA, collagen, and of the micropore space. The outputs are the tissue-specific ultrastructural and microstructural (=macroscopic=apparent) elasticity tensors. A second independent experimental set (composition data and experimental stiffness values) is employed to validate the proposed model. We report a small mean prediction error for the macroscopic stiffness values. The validation suggests that hydroxyapatite, collagen, and water are tissue-independent phases, which define, through their mechanical interaction, the elasticity of all bones, whether cortical or trabecular.
机译:作为皮质和小梁骨的组织独立相的候选者,我们考虑(i)羟基磷灰石,(ii)胶原蛋白,(iii)超微结构水和非胶原有机物,以及(iv)填充哈弗里斯运河和马路的骨髓(水)小梁间空间。从文献报道的实验中,我们将刚度属性分配给这些阶段(实验组I)。根据这些相的定义,我们在连续微力学的框架内开发了两步均化程序:(i)在100-200 nm的长度范围内,羟基磷灰石(HA)晶体形成晶体泡沫(多晶),水和非胶原有机物填充晶间空间(均质化步骤I); (ii)在矿化组织(5-10微米)的超微结构尺度上,由胶原分子组成的胶原组装体被嵌入晶体泡沫中,机械地充当圆柱模板。在5-10 mm的扩大材料尺度下,第二步均质化步骤还将微孔空间容纳为圆柱孔夹杂物(Haversian和Volkmann运河,小梁间空间),适用于小梁和皮质骨。该微力学模型的输入是HA,胶原蛋白和微孔空间的组织特异性体积分数。输出是组织特定的超结构和微结构(=宏观=表观)弹性张量。第二个独立的实验集(成分数据和实验刚度值)用于验证所提出的模型。我们报告宏观刚度值的平均预测误差小。验证表明,羟基磷灰石,胶原蛋白和水是与组织无关的相,它们通过它们的机械相互作用定义了所有骨骼(无论是皮质的还是小梁的)的弹性。

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