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Variation in within-bone stiffness measured by nanoindentation in mice bred for high levels of voluntary wheel running

机译:通过纳米压痕法测量高水平自转轮繁殖的小鼠的骨内刚度变化

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摘要

The hierarchical structure of bone, involving micro-scale organization and interaction of material components, is a critical determinant of macro-scale mechanics. Changes in whole-bone morphology in response to the actions of individual genes, physiological loading during life, or evolutionary processes, may be accompanied by alterations in underlying mineralization or architecture. Here, we used nanoindentation to precisely measure compressive stiffness in the femoral mid-diaphysis of mice that had experienced 37 generations of selective breeding for high levels of voluntary wheel running (HR). Mice (n= 48 total), half from HR lines and half from non-selected control (C) lines, were divided into two experimental groups, one with 13–14 weeks of access to a running wheel and one housed without wheels (n = 12 in each group). At the end of the experiment, gross and micro-computed tomography (μCT)-based morphometric traits were measured, and reduced elastic modulus (Er) was estimated separately for four anatomical quadrants of the femoral cortex: anterior, posterior, lateral, and medial. Two-way, mixed-model analysis of covariance (ancova) showed that body mass was a highly significant predictor of all morphometric traits and that structural change is more apparent at the μCT level than in conventional morphometrics of whole bones. Both linetype (HR vs. C) and presence of the mini-muscle phenotype (caused by a Mendelian recessive allele and characterized by a ∼50% reduction in mass of the gastrocnemius muscle complex) were significant predictors of femoral cortical cross-sectional anatomy. Measurement of reduced modulus obtained by nanoindentation was repeatable within a single quadrant and sensitive enough to detect inter-individual differences. Although we found no significant effects of linetype (HR vs. C) or physical activity (wheel vs. no wheel) on mean stiffness, anterior and posterior quadrants were significantly stiffer (P< 0.0001) than medial and lateral quadrants (32.67 and 33.09 GPa vs. 29.78 and 30.46 GPa, respectively). Our findings of no significant difference in compressive stiffness in the anterior and posterior quadrants agree with previous results for mice, but differ from those for large mammals. Integrating these results with others from ongoing research on these mice, we hypothesize that the skeletons of female HR mice may be less sensitive to the effects of chronic exercise, due to decreased circulating leptin levels and potentially altered endocannabinoid signaling.
机译:骨骼的层次结构涉及微观尺度的组织和材料成分的相互作用,是宏观力学的关键决定因素。响应各个基因的作用,生命中的生理负荷或进化过程,全骨形态的变化可能伴随着潜在矿化或构造的变化。在这里,我们使用纳米压痕技术精确测量了经历了37代选择性繁殖的高水平自动滚轮(HR)小鼠的股骨中骨干的抗压刚度。小鼠(共48只),一半来自HR线,另一半来自非选择的对照(C)线,分为两个实验组,一个组有13–14周的行走轮接触,而一个组则没有轮子(n =每组12个)。在实验结束时,测量了基于总体和微观计算机断层扫描(μCT)的形态特征,并分别评估了股骨皮质的四个解剖象限的弹性模量(Er)的降低:前,后,外侧和内侧。对协方差(ancova)进行的两种混合模型分析表明,体重是所有形态特征的高度重要预测指标,并且在μCT水平上的结构变化比整个骨骼的常规形态学更明显。线型(HR vs. C)和小肌肉表型的存在(由孟德尔隐性等位基因引起,并以腓肠肌复合物质量降低约50%为特征)都是股骨皮质横截面解剖结构的重要预测指标。通过纳米压痕获得的降低模量的测量可在一个象限内重复进行,并且足够灵敏以检测个体之间的差异。尽管我们发现线型(HR vs. C)或体力活动(车轮vs.无车轮)对平均刚度没有显着影响,但前象限和后象限比内侧和外侧象限(32.67和33.09 GPa)强得多(P <0.0001)分别为29.78和30.46 GPa)。我们在前象限和后象限中抗压刚度无显着差异的发现与先前对小鼠的结果一致,但与大型哺乳动物的结果不同。将这些结果与这些小鼠正在进行的研究中的其他结果相结合,我们假设雌性HR小鼠的骨骼可能对慢性运动的影响较不敏感,这是由于循环中的瘦素水平降低以及潜在的内源性大麻素信号改变。

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