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Analysis of the mechanical behavior of chondrocytes in unconfined compression tests for cyclic loading.

机译:在无限制压缩测试中循环载荷下软骨细胞的力学行为分析。

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Experimental evidence indicates that the biosynthetic activity of chondrocytes is associated with the mechanical environment. For example, excessive, repetitive loading has been found to induce cell death, morphological and cellular damage, as seen in degenerative joint disease, while cyclic, physiological-like loading has been found to trigger a partial recovery of morphological and ultrastructural aspects in osteoarthritic human articular chondrocytes. Mechanical stimuli are believed to influence the biosynthetic activity via the deformation of cells. However, the in situ deformation of chondrocytes for cyclic loading conditions has not been investigated experimentally or theoretically. The purpose of the present study was to simulate the mechanical response of chondrocytes to cyclic loading in unconfined compression tests using a finite element model. The material properties of chondrocytes and extracellular matrix were considered to be biphasic. The time-histories of the shape and volume variationsof chondrocytes at three locations (i.e., surface, center, and bottom) within the cartilage were predicted for static and cyclic loading conditions at two frequencies (0.02 and 0.1 Hz) and two amplitudes (0.1 and 0.2 MPa). Our results show that cells at different depths within the cartilage deform differently during cyclic loading, and that the depth dependence of cell deformation is influenced by the amplitude of the cyclic loading. Cell deformations under cyclic loading of 0.02 Hz were found to be similar to those at 0.1 Hz. We conclude from the simulation results that, in homogeneous cartilage layers, cell deformations are location-dependent, and further are affected by load magnitude. In physiological conditions, the mechanical environment of cells are even more complex due to the anisotropy, depth-dependent inhomogeneity, and tension-compression non-linearity of the cartilage matrix. Therefore, it is feasible to speculate that biosynthetic responses of chondrocytes to cyclic loading depend on cell location and load magnitude.
机译:实验证据表明,软骨细胞的生物合成活性与机械环境有关。例如,如在退行性关节疾病中所见,发现过度的重复负荷可导致细胞死亡,形态学和细胞损伤,而周期性的类似生理的负荷可触发骨关节炎人类形态和超微结构方面的部分恢复关节软骨细胞。认为机械刺激通过细胞变形影响生物合成活性。但是,对于软骨细胞在循环载荷条件下的原位变形尚未进行实验或理论研究。本研究的目的是使用有限元模型在无侧限压缩测试中模拟软骨细胞对循环负荷的机械反应。软骨细胞和细胞外基质的材料特性被认为是双相的。针对两个频率(0.02和0.1 Hz)和两个振幅(0.1和0.1)的静态和循环载荷条件,预测了软骨内三个位置(即表面,中心和底部)软骨细胞的形状和体积变化的时程0.2 MPa)。我们的研究结果表明,在周期性加载过程中,软骨内不同深度的细胞变形不同,并且细胞变形的深度依赖性受周期性加载幅度的影响。发现在0.02Hz的循环载荷下的单元变形与在0.1Hz下的单元变形相似。从仿真结果可以得出结论,在同质软骨层中,细胞变形与位置有关,并且还受载荷量的影响。在生理条件下,由于软骨基质的各向异性,深度相关的不均匀性和张力-压缩非线性,细胞的机械环境甚至更加复杂。因此,可以推测软骨细胞对循环负荷的生物合成反应取决于细胞的位置和负荷大小。

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