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骨质疏松症羊模型中骨小梁内纳米力学性能和组织成分的变化及治疗。

Variations in nanomechanical properties and tissue composition within trabeculae from an ovine model of osteoporosis and treatment.

机构信息

Sibley School of Mechanical and Aerospace Engineering, Cornell University, Ithaca, NY 14850, USA.

出版信息

Bone. 2013 Jan;52(1):326-36. doi: 10.1016/j.bone.2012.10.018. Epub 2012 Oct 23.

Abstract

Osteoporosis and treatment may affect both composition and nanomechanical properties and their spatial distributions within the individual trabeculae of cancellous bone at length scales that cannot be captured by bulk measurements. This study utilized 25 mature adult ewes divided into 5 treatment groups. Four treatment groups were given a dietary model for human high-turnover osteoporosis, and two of these were treated with antiresorptive drugs, either zoledronate (ZOL) or raloxifene (RAL), to examine their effects on bulk tissue properties and nanoscale tissue composition and mechanical properties within trabeculae. Treatment effects were most pronounced at the nanoscale, where RAL increased indentation modulus and hardness throughout trabeculae by 10% relative to the osteoporosis model. In comparison, ZOL increased these properties exclusively at the surfaces of trabeculae (indentation modulus +12%, hardness +16%). Nanomechanical alterations correlated with changes in tissue mineralization, carbonate substitution, crystallinity, and aligned collagen. Despite only minimal changes in bulk tissue tBMD, the nanomechanical improvements within trabeculae with both treatments greatly improved the predicted theoretical bending stiffness of individual trabeculae when idealized as cylindrical struts. Hence, small tissue-level alterations in critical locations for resisting trabecular failure could account for some of the discrepancy between the large reductions in fracture risk and the only modest changes in BMD with antiresorptive treatments.

摘要

骨质疏松症及其治疗可能会影响松质骨中个体小梁的组成和纳米力学性能及其空间分布,这些在尺度上是无法通过体测量获得的。本研究使用了 25 只成熟的成年母羊,分为 5 个治疗组。四个治疗组给予了人类高转换型骨质疏松症的饮食模型,其中两个治疗组用抗吸收药物唑来膦酸(ZOL)或雷洛昔芬(RAL)进行治疗,以研究它们对体组织特性和小梁内纳米级组织成分和力学性能的影响。在纳米尺度上,RAL 对骨密度模型的小梁内的压痕模量和硬度的相对增加了 10%,治疗效果最为显著。相比之下,ZOL 仅在小梁表面增加了这些特性(压痕模量增加 12%,硬度增加 16%)。纳米力学的改变与组织矿化、碳酸盐取代、结晶度和定向胶原的变化有关。尽管体组织 tBMD 只有很小的变化,但两种治疗方法都能显著改善小梁内纳米力学性能,当将小梁理想化作为圆柱形支柱时,大大提高了个体小梁的预测理论弯曲刚度。因此,在抵抗小梁失效的关键位置上的微小组织水平改变可能是抗吸收治疗导致骨折风险大大降低而骨密度仅适度变化的原因之一。

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