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A multiscale mechanobiological modelling framework using agent-based models and finite element analysis: Application to vascular tissue engineering

机译:基于代理的模型和有限元分析的多尺度力学模型框架:应用于血管组织工程

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摘要

Computational models of mechanobiological systems have been widely used to provide insight into these systems and also to predict their behaviour. In this context, vascular tissue engineering benefits from further attention given the challenges involved in developing functional low calibre vascular grafts with long-term patency. In this study, a novel multiscale mechanobiological modelling framework is presented, which takes advantage of lattice-free agentbased models coupled with the finite element method to investigate the dynamics of VSMC growth in vascular tissue engineering scaffolds. The results illustrate the ability of the mechanobiological modelling approach to capture complex multiscalemechanobiological phenomena. Specifically, the framework enabled the study of the influence of scaffold compliance and loading regime in regulating the growth of VSMCs in vascular scaffolds and their role in development of intimal hyperplasia (IH). The model demonstrates that low scaffold compliance compared to host arteries leads to increased luminal ingrowth and IH development. In addition, culture of a tissue-engineered blood vessel under a pulsatile luminal pressure reduced luminal ingrowth and enhanced collagen synthesis within the scaffold compared to non-pulsatile culture. The mechanobiological framework presented provides a robust platform for testing hypotheses in vascular tissue engineering and lends itself to use as an optimisation design tool.
机译:力学系统的计算模型已被广泛用于提供对这些系统的洞察力,并预测其行为。在这种情况下,鉴于开发具有长期通畅的挑战,血管组织工程从进一步关注中受益。在该研究中,提出了一种新型多尺度机械模型建模框架,其利用与有限元方法相结合的晶格代理模型,以研究血管组织工程支架中VSMC生长的动态。结果说明了机械模拟方法捕获复杂的多学用机组能生物现象的能力。具体地,该框架使支架依从性和装载制度在调节血管支架中的VSMC的生长以及它们在内膜增生(IH)的发育中的作用的影响研究。该模型表明,与宿主动脉相比,低支架顺应性导致腔内发光和IH发育增加。此外,与非脉粘型培养相比,在脉动腔压力下减少了脉动腔压力下减少了腔内的腔内腔压缩和增强胶原蛋白合成。提出的机械机械框架提供了一种强大的平台,用于测试血管组织工程中的假设,并利用作为优化设计工具的假设。

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