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双膦酸盐治疗通过微观结构而非基质特性影响小梁骨表观模量。

Bisphosphonate treatment affects trabecular bone apparent modulus through micro-architecture rather than matrix properties.

作者信息

Day J S, Ding M, Bednarz P, van der Linden J C, Mashiba T, Hirano T, Johnston C C, Burr D B, Hvid I, Sumner D R, Weinans H

机构信息

Erasmus Orthopaedic Research Laboratory, Erasmus MC, University Medical Centre of Rotterdam, EE1614, P.O. Box 1738, DR, Rotterdam 3000, The Netherlands.

出版信息

J Orthop Res. 2004 May;22(3):465-71. doi: 10.1016/j.orthres.2003.05.001.

Abstract

Bisphosphonates are emerging as an important treatment for osteoporosis. But whether the reduced fracture risk associated with bisphosphonate treatment is due to increased bone mass, improved trabecular architecture and/or increased secondary mineralization of the calcified matrix remains unclear. We examined the effects of bisphosphonates on both the trabecular architecture and matrix properties of canine trabecular bone. Thirty-six beagles were divided into a control group and two treatment groups, one receiving risedronate and the other alendronate at 5-6 times the clinical dose for osteoporosis treatment. After one year, the dogs were killed, and samples from the first lumbar vertebrae were examined using a combination of micro-computed tomography, finite element modeling, and mechanical testing. By combining these methods, we examined the treatment effects on the calcified matrix and trabecular architecture independently. Conventional histomorphometry and microdamage data were obtained from the second and third lumbar vertebrae of the same dogs [Bone 28 (2001) 524]. Bisphosphonate treatment resulted in an increased apparent Young's modulus, decreased bone turnover, increased calcified matrix density, and increased microdamage. We could not detect any change in the effective Young's modulus of the calcified matrix in the bisphosphonate treated groups. The observed increase in apparent Young's modulus was due to increased bone mass and altered trabecular architecture rather than changes in the calcified matrix modulus. We hypothesize that the expected increase in the Young's modulus of the calcified matrix due to the increased calcified matrix density was counteracted by the accumulation of microdamage.

摘要

双膦酸盐正逐渐成为治疗骨质疏松症的重要方法。但双膦酸盐治疗所带来的骨折风险降低是由于骨量增加、小梁结构改善和/或钙化基质的继发性矿化增加,目前仍不清楚。我们研究了双膦酸盐对犬小梁骨小梁结构和基质特性的影响。36只比格犬被分为一个对照组和两个治疗组,一组接受利塞膦酸盐,另一组接受阿仑膦酸盐,剂量为骨质疏松症治疗临床剂量的5 - 6倍。一年后,处死这些犬,使用微型计算机断层扫描、有限元建模和力学测试相结合的方法检查第一腰椎的样本。通过结合这些方法,我们分别研究了治疗对钙化基质和小梁结构的影响。常规组织形态计量学和微损伤数据取自同一只犬的第二和第三腰椎[《骨》28 (2001) 524]。双膦酸盐治疗导致表观杨氏模量增加、骨转换降低、钙化基质密度增加和微损伤增加。在双膦酸盐治疗组中,我们未检测到钙化基质的有效杨氏模量有任何变化。观察到的表观杨氏模量增加是由于骨量增加和小梁结构改变,而非钙化基质模量的变化。我们推测,钙化基质密度增加所预期的钙化基质杨氏模量增加被微损伤的积累所抵消。

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