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在无约束和约束压缩下,聚己内酯-胶原蛋白杂化支架中载荷传递的细观力学研究。

Micromechanical study of the load transfer in a polycaprolactone-collagen hybrid scaffold when subjected to unconfined and confined compression.

机构信息

Department of Mechanical Engineering, INSIGNEO Institute for in Silico Medicine, University of Sheffield, Pam Liversidge Building, Mappin Street, Sheffield, S1 3JD, UK.

出版信息

Biomech Model Mechanobiol. 2018 Apr;17(2):531-541. doi: 10.1007/s10237-017-0976-5. Epub 2017 Nov 11.

Abstract

Scaffolds are used in diverse tissue engineering applications as hosts for cell proliferation and extracellular matrix formation. One of the most used tissue engineering materials is collagen, which is well known to be a natural biomaterial, also frequently used as cell substrate, given its natural abundance and intrinsic biocompatibility. This study aims to evaluate how the macroscopic biomechanical stimuli applied on a construct made of polycaprolactone scaffold embedded in a collagen substrate translate into microscopic stimuli at the cell level. Eight poro-hyperelastic finite element models of 3D printed hybrid scaffolds from the same batch were created, along with an equivalent model of the idealized geometry of that scaffold. When applying an 8% confined compression at the macroscopic level, local fluid flow of up to 20 [Formula: see text]m/s and octahedral strain levels mostly under 20% were calculated in the collagen substrate. Conversely unconfined compression induced fluid flow of up to 10 [Formula: see text]m/s and octahedral strain from 10 to 35%. No relevant differences were found amongst the scaffold-specific models. Following the mechanoregulation theory based on Prendergast et al. (J Biomech 30:539-548, 1997. https://doi.org/10.1016/S0021-9290(96)00140-6 ), those results suggest that mainly cartilage or fibrous tissue formation would be expected to occur under unconfined or confined compression, respectively. This in silico study helps to quantify the microscopic stimuli that are present within the collagen substrate and that will affect cell response under in vitro bioreactor mechanical stimulation or even after implantation.

摘要

支架在各种组织工程应用中被用作细胞增殖和细胞外基质形成的宿主。最常用的组织工程材料之一是胶原蛋白,它是众所周知的天然生物材料,也经常被用作细胞基质,因为它的天然丰富度和内在的生物相容性。本研究旨在评估应用于聚己内酯支架嵌入胶原蛋白基质的构建体的宏观生物力学刺激如何转化为细胞水平的微观刺激。从同一批次创建了 8 个 3D 打印混合支架的多孔超弹性有限元模型,以及该支架理想化几何形状的等效模型。在宏观水平上施加 8%的受限压缩时,计算出胶原蛋白基质中的局部流体流速高达 20 [Formula: see text]m/s,八面体应变水平大多低于 20%。相反,非受限压缩引起的流体流速高达 10 [Formula: see text]m/s,八面体应变从 10 到 35%。在支架特定模型之间没有发现相关差异。根据基于 Prendergast 等人的机械调节理论(J Biomech 30:539-548, 1997. https://doi.org/10.1016/S0021-9290(96)00140-6),这些结果表明,在无约束或约束压缩下,分别预期主要会发生软骨或纤维组织形成。这项计算机模拟研究有助于量化胶原蛋白基质内存在的微观刺激,这些刺激将影响体外生物反应器机械刺激下或甚至植入后的细胞反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3127/5845056/b9be0cc8088d/10237_2017_976_Fig1_HTML.jpg

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