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是否应该忽略无法测量的因素?非均匀拉伸、非均匀壁厚和小分支如何影响小鼠主动脉生物力学的计算。

Should We Ignore What We Cannot Measure? How Non-Uniform Stretch, Non-Uniform Wall Thickness and Minor Side Branches Affect Computational Aortic Biomechanics in Mice.

机构信息

Institute of Bioengineering, Ecole Polytechnique Fédérale de Lausanne, LHTC STI IBI EPFL, MED 32924 Station 9, 1015, Lausanne, Switzerland.

IBiTech - bioMMeda, Ghent University, Ghent, Belgium.

出版信息

Ann Biomed Eng. 2018 Jan;46(1):159-170. doi: 10.1007/s10439-017-1945-y. Epub 2017 Oct 25.

DOI:10.1007/s10439-017-1945-y
PMID:29071528
Abstract

In order to advance the state-of-the-art in computational aortic biomechanics, we investigated the influence of (i) a non-uniform wall thickness, (ii) minor aortic side branches and (iii) a non-uniform axial stretch distribution on the location of predicted hotspots of principal strain in a mouse model for dissecting aneurysms. After 3 days of angiotensin II infusion, a murine abdominal aorta was scanned in vivo with contrast-enhanced micro-CT. The animal was subsequently sacrificed and its aorta was scanned ex vivo with phase-contrast X-ray tomographic microscopy (PCXTM). An automatic morphing framework was developed to map the non-pressurized, non-stretched PCXTM geometry onto the pressurized, stretched micro-CT geometry. The output of the morphing model was a structural FEM simulation where the output strain distribution represents an estimation of the wall deformation, not only due to the pressurization, but also due to the local axial stretch field. The morphing model also included minor branches and a mouse-specific wall thickness. A sensitivity study was then performed to assess the influence of each of these novel features on the outcome of the simulations. The results were supported by comparing the computed hotspots of principal strain to hotspots of early vascular damage as detected on PCXTM. Non-uniform axial stretch, non-uniform wall thickness and minor subcostal arteries significantly alter the locations of calculated hotspots of maximal principal strain. Even if experimental data on these features are often not available in clinical practice, one should be aware of the important implications that simplifications in the model might have on the final simulated result.

摘要

为了推动计算主动脉生物力学的最新进展,我们研究了(i)非均匀壁厚、(ii)小主动脉侧支和(iii)非均匀轴向拉伸分布对预测夹层动脉瘤小鼠模型中主应变热点位置的影响。在血管紧张素 II 输注 3 天后,用对比增强微 CT 对小鼠腹主动脉进行体内扫描。随后处死动物,用相衬 X 射线断层显微镜(PCXTM)对其主动脉进行离体扫描。开发了一种自动变形框架,将无压力、无拉伸的 PCXTM 几何形状映射到加压、拉伸的微 CT 几何形状上。变形模型的输出是一个结构有限元模拟,其输出应变分布不仅代表了由于加压,而且还代表了局部轴向拉伸场引起的壁变形的估计。变形模型还包括小分支和特定于小鼠的壁厚。然后进行了敏感性研究,以评估这些新特征中的每一个对模拟结果的影响。通过将计算出的主应变热点与 PCXTM 上检测到的早期血管损伤的热点进行比较,验证了结果。非均匀轴向拉伸、非均匀壁厚和小肋下动脉会显著改变计算出的最大主应变热点的位置。即使在临床实践中通常无法获得这些特征的实验数据,也应该意识到模型中的简化可能对最终模拟结果产生的重要影响。

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