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高度多孔的胶原蛋白-糖胺聚糖支架中细胞应变的有限元预测。

A finite element prediction of strain on cells in a highly porous collagen-glycosaminoglycan scaffold.

作者信息

Stops A J F, McMahon L A, O'Mahoney D, Prendergast P J, McHugh P E

机构信息

Department of Mechanical and Biomedical Engineering, National University of Ireland, Galway, Ireland.

出版信息

J Biomech Eng. 2008 Dec;130(6):061001. doi: 10.1115/1.2979873.

Abstract

Tissue engineering often involves seeding cells into porous scaffolds and subjecting the scaffold to mechanical stimulation. Current experimental techniques have provided a plethora of data regarding cell responses within scaffolds, but the quantitative understanding of the load transfer process within a cell-seeded scaffold is still relatively unknown. The objective of this work was to develop a finite element representation of the transient and heterogeneous nature of a cell-seeded collagen-GAG-scaffold. By undertaking experimental investigation, characteristics such as scaffold architecture and shrinkage, cellular attachment patterns, and cellular dimensions were used to create a finite element model of a cell-seeded porous scaffold. The results demonstrate that a very wide range of microscopic strains act at the cellular level when a sample value of macroscopic (apparent) strain is applied to the collagen-GAG-scaffold. An external uniaxial strain of 10% generated a cellular strain as high as 49%, although the majority experienced less than approximately 5% strain. The finding that the strain on some cells could be higher than the macroscopic strain was unexpected and proves contrary to previous in vitro investigations. These findings indicate a complex system of biophysical stimuli created within the scaffolds and the difficulty of inducing the desired cellular responses from artificial environments. Future in vitro studies could also corroborate the results from this computational prediction to further explore mechanoregulatory mechanisms in tissue engineering.

摘要

组织工程通常涉及将细胞接种到多孔支架中,并对支架施加机械刺激。目前的实验技术已经提供了大量关于支架内细胞反应的数据,但对于接种细胞的支架内载荷传递过程的定量理解仍然相对较少。这项工作的目的是建立一个有限元模型来描述接种细胞的胶原 - GAG支架的瞬态和异质性。通过进行实验研究,利用支架结构和收缩、细胞附着模式以及细胞尺寸等特征,创建了一个接种细胞的多孔支架的有限元模型。结果表明,当对胶原 - GAG支架施加宏观(表观)应变的样本值时,在细胞水平上会出现非常广泛的微观应变。10%的外部单轴应变会产生高达49%的细胞应变,尽管大多数细胞的应变小于约5%。某些细胞上的应变可能高于宏观应变这一发现出乎意料,并且与之前的体外研究结果相反。这些发现表明支架内产生了一个复杂的生物物理刺激系统,以及从人工环境中诱导所需细胞反应的困难。未来的体外研究也可以证实这一计算预测的结果,以进一步探索组织工程中的机械调节机制。

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