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微裂纹的积累和合并导致骨结构性能的退化。

Degradation of bone structural properties by accumulation and coalescence of microcracks.

作者信息

Danova N A, Colopy S A, Radtke C L, Kalscheur V L, Markel M D, Vanderby R, McCabe R P, Escarcega A J, Muir P

机构信息

Comparative Orthopaedic Research Laboratory, Department of Surgical Sciences, School of Veterinary Medicine, University of Wisconsin-Madison, 2015 Linden Drive, Madison, WI 53706, USA.

出版信息

Bone. 2003 Aug;33(2):197-205. doi: 10.1016/s8756-3282(03)00155-8.

Abstract

Failure of bone adaptation to protect the skeleton from fatigue fracture is common, and site-specific accumulation and coalescence of microcracking in regions of high strain during cyclic loading is considered a key factor that decreases the resistance of whole bones to fracture. We investigated the effect of cyclic fatigue loading on the monotonic structural properties of the rat ulna during accumulation and coalescence of microcracks. Cyclic end-loading of the ulna was performed at 4 Hz ex vivo at an initial peak strain of -6000 muepsilon to 20% loss of stiffness (n = 7) or 40% loss of stiffness (n = 7) bilaterally. A 0% loss of stiffness monotonically loaded control group (n = 7) was also included. Volumetric bone mineral density (vBMD), ultimate strength (F(u)), stiffness (S), and energy-to-failure (U) were determined in one ulna and in the contralateral ulna vBMD, cortical bone area (B.Ar), maximum and minimum second moments of inertia (I(MAX) and I(MIN)), microcrack density (Cr.Dn), microcrack mean length (Cr.Le), and microcrack surface density (Cr.S.Dn) were determined. In two additional groups of rats, cyclic end-loading of the ulna was also performed ex vivo unilaterally to 20% loss of stiffness (n = 10) and 40% loss of stiffness (n = 10) and then vBMD, F(u), S, U, B.Ar, I(MAX), and I(MIN) were determined bilaterally. Fatigue loading had incremental degradative effects on ulna structural properties. This decreased resistance to fracture was associated with accumulation and coalescence of branching arrays of microcracks within the cortex of the ulna. Microcracking was most prominent in the middiaphysis and corresponded to the region of the bone that fractured during monotonic structural testing. Fatigue loading influenced the relationship between bone cross-sectional geometry and vBMD and ulna structural properties. At 40% loss of stiffness, F(u), S, and U were all significantly correlated with cross-sectional bone geometry and vBMD, whereas this was not the case at 20% loss of stiffness and with the 0% loss of stiffness monotonic control ulnae. We also found a biologically significant individual animal effect. Larger ulnae required a higher number of load cycles for fatigue to develop, retained higher strength, and accumulated a greater amount of microcracking at the end of the cyclic fatigue testing. Small increases in bone size and density can substantially improve the resistance of whole bones to fracture as microcracking accumulates and coalesces during cyclic fatigue loading.

摘要

骨骼适应性未能保护骨骼免受疲劳骨折的情况很常见,并且在循环加载过程中高应变区域微裂纹的位点特异性积累和合并被认为是降低全骨抗骨折能力的关键因素。我们研究了在微裂纹积累和合并过程中,循环疲劳加载对大鼠尺骨单调结构特性的影响。在体外以4Hz对尺骨进行循环端加载,初始峰值应变为-6000με,直至刚度损失20%(n = 7)或40%(n = 7),双侧进行。还包括一个刚度损失0%的单调加载对照组(n = 7)。在一侧尺骨中测定骨体积密度(vBMD)、极限强度(F(u))、刚度(S)和破坏能量(U),在对侧尺骨中测定vBMD、皮质骨面积(B.Ar)、最大和最小惯性矩(I(MAX)和I(MIN))、微裂纹密度(Cr.Dn)、微裂纹平均长度(Cr.Le)和微裂纹表面密度(Cr.S.Dn)。在另外两组大鼠中,也在体外对尺骨进行单侧循环端加载至刚度损失20%(n = 10)和40%(n = 10),然后双侧测定vBMD、F(u)、S、U、B.Ar、I(MAX)和I(MIN)。疲劳加载对尺骨结构特性有渐进性的降解作用。这种抗骨折能力的降低与尺骨皮质内微裂纹分支阵列的积累和合并有关。微裂纹在骨干中部最为突出,并且与单调结构测试期间骨折的骨区域相对应。疲劳加载影响了骨横截面几何形状与vBMD以及尺骨结构特性之间的关系。在刚度损失40%时,F(u)、S和U均与横截面骨几何形状和vBMD显著相关,而在刚度损失20%时以及刚度损失0%的单调对照尺骨中情况并非如此。我们还发现了具有生物学意义的个体动物效应。较大的尺骨在疲劳发展过程中需要更高的加载循环次数,保留更高的强度,并且在循环疲劳测试结束时积累更多的微裂纹。随着微裂纹在循环疲劳加载过程中积累和合并,骨大小和密度的小幅度增加可以显著提高全骨的抗骨折能力。

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