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使用基于显微CT的有限元分析对体内小鼠胫骨加载模型中的松质骨和皮质骨应变进行表征。

Characterization of cancellous and cortical bone strain in the in vivo mouse tibial loading model using microCT-based finite element analysis.

作者信息

Yang Haisheng, Butz Kent D, Duffy Daniel, Niebur Glen L, Nauman Eric A, Main Russell P

机构信息

Musculoskeletal Biology and Mechanics Lab, Department of Basic Medical Sciences, Purdue University, IN, USA.

School of Mechanical Engineering, Purdue University, IN, USA.

出版信息

Bone. 2014 Sep;66:131-9. doi: 10.1016/j.bone.2014.05.019. Epub 2014 Jun 9.

Abstract

The in vivo mouse tibial loading model has been increasingly used to understand the mechanisms governing the mechanobiological responses of cancellous and cortical bone tissues to physical stimuli. Accurate characterization of the strain environment throughout the tibia is fundamental in relating localized mechanobiological processes to specific strain stimuli in the skeleton. MicroCT-based finite element analysis, together with diaphyseal strain gauge measures, was conducted to quantify the strain field in the tibiae of 16-wk-old female C57Bl/6 mice during in vivo dynamic compressive loading. Despite a strong correlation between the experimentally-measured and computationally-modeled strains at the gauge site, no correlations existed between the strain at the gauge site and the peak strains in the proximal cancellous and midshaft cortical bone, indicating the limitations of using a single diaphyseal strain gauge to estimate strain in the entire tibia. The peak compressive and tensile principal strain magnitudes in the proximal cancellous bone were 10% and 34% lower than those in the midshaft cortical bone. Sensitivity analyses showed that modeling bone tissue as a heterogeneous material had a strong effect on cancellous strain characterization while cortical strain and whole-bone stiffness were primarily affected by the presence of the fibula and the proximal boundary conditions. These results show that microCT-based finite element analysis combined with strain gauge measures provides detailed resolution of the tissue-level strain in both the cancellous and cortical bones of the mouse tibia during in vivo compression loading, which is necessary for interpreting localized patterns of modeling/remodeling and, potentially, gene and protein expression in skeletal mechanobiology studies.

摘要

体内小鼠胫骨加载模型越来越多地用于了解松质骨和皮质骨组织对物理刺激的力学生物学反应机制。准确表征整个胫骨的应变环境对于将局部力学生物学过程与骨骼中的特定应变刺激联系起来至关重要。进行了基于微计算机断层扫描(MicroCT)的有限元分析,并结合骨干应变片测量,以量化16周龄雌性C57Bl/6小鼠在体内动态压缩加载过程中胫骨的应变场。尽管在应变片位置实验测量应变与计算模型应变之间存在很强的相关性,但应变片位置的应变与近端松质骨和骨干皮质骨中的峰值应变之间不存在相关性,这表明使用单个骨干应变片来估计整个胫骨的应变存在局限性。近端松质骨中的峰值压缩和拉伸主应变大小分别比骨干皮质骨中的低10%和34%。敏感性分析表明,将骨组织建模为非均质材料对松质骨应变表征有很大影响,而皮质骨应变和全骨刚度主要受腓骨的存在和近端边界条件的影响。这些结果表明,基于MicroCT的有限元分析与应变片测量相结合,可在体内压缩加载过程中为小鼠胫骨的松质骨和皮质骨提供组织水平应变的详细分辨率,这对于解释建模/重塑的局部模式以及骨骼力学生物学研究中潜在的基因和蛋白质表达是必要的。

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