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开发用于理解动脉粥样硬化和钙化位置的患者特异性多尺度模型:与主动脉夹层的体内数据比较

Development of a Patient-Specific Multi-Scale Model to Understand Atherosclerosis and Calcification Locations: Comparison with In vivo Data in an Aortic Dissection.

作者信息

Alimohammadi Mona, Pichardo-Almarza Cesar, Agu Obiekezie, Díaz-Zuccarini Vanessa

机构信息

Mechanical Engineering, University College London London UK.

Vascular Unit, University College Hospital London, UK.

出版信息

Front Physiol. 2016 Jun 21;7:238. doi: 10.3389/fphys.2016.00238. eCollection 2016.

DOI:10.3389/fphys.2016.00238
PMID:27445834
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4914588/
Abstract

Vascular calcification results in stiffening of the aorta and is associated with hypertension and atherosclerosis. Atherogenesis is a complex, multifactorial, and systemic process; the result of a number of factors, each operating simultaneously at several spatial and temporal scales. The ability to predict sites of atherogenesis would be of great use to clinicians in order to improve diagnostic and treatment planning. In this paper, we present a mathematical model as a tool to understand why atherosclerotic plaque and calcifications occur in specific locations. This model is then used to analyze vascular calcification and atherosclerotic areas in an aortic dissection patient using a mechanistic, multi-scale modeling approach, coupling patient-specific, fluid-structure interaction simulations with a model of endothelial mechanotransduction. A number of hemodynamic factors based on state-of-the-art literature are used as inputs to the endothelial permeability model, in order to investigate plaque and calcification distributions, which are compared with clinical imaging data. A significantly improved correlation between elevated hydraulic conductivity or volume flux and the presence of calcification and plaques was achieved by using a shear index comprising both mean and oscillatory shear components (HOLMES) and a non-Newtonian viscosity model as inputs, as compared to widely used hemodynamic indicators. The proposed approach shows promise as a predictive tool. The improvements obtained using the combined biomechanical/biochemical modeling approach highlight the benefits of mechanistic modeling as a powerful tool to understand complex phenomena and provides insight into the relative importance of key hemodynamic parameters.

摘要

血管钙化会导致主动脉僵硬,并与高血压和动脉粥样硬化相关。动脉粥样硬化的形成是一个复杂、多因素且全身性的过程,是多种因素共同作用的结果,这些因素在多个空间和时间尺度上同时发挥作用。预测动脉粥样硬化形成部位的能力对临床医生制定诊断和治疗计划非常有用。在本文中,我们提出了一个数学模型,作为理解动脉粥样硬化斑块和钙化为何出现在特定位置的工具。然后,使用一种机械多尺度建模方法,将患者特异性的流固耦合模拟与内皮机械转导模型相结合,利用该模型分析一名主动脉夹层患者的血管钙化和动脉粥样硬化区域。基于最新文献的一些血流动力学因素被用作内皮通透性模型的输入,以研究斑块和钙化分布,并与临床影像数据进行比较。与广泛使用的血流动力学指标相比,通过使用包含平均和振荡剪切分量的剪切指数(HOLMES)和非牛顿粘度模型作为输入,在升高的水力传导率或体积通量与钙化和斑块的存在之间实现了显著改善的相关性。所提出的方法有望成为一种预测工具。使用联合生物力学/生物化学建模方法所取得的改进突出了机械建模作为理解复杂现象的有力工具的优势,并深入了解了关键血流动力学参数的相对重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7484/4914588/be342d4a0d95/fphys-07-00238-g0010.jpg
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