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软组织中纤维胶原蛋白的周转率及其在腹主动脉瘤扩张中的应用。

Turnover of fibrillar collagen in soft biological tissue with application to the expansion of abdominal aortic aneurysms.

机构信息

Department of Solid Mechanics, School of Engineering Sciences, Royal Institute of Technology (KTH), Osquars Backe 1, 100 44 Stockholm, Sweden.

出版信息

J R Soc Interface. 2012 Dec 7;9(77):3366-77. doi: 10.1098/rsif.2012.0416. Epub 2012 Aug 15.

Abstract

A better understanding of the inherent properties of vascular tissue to adapt to its mechanical environment is crucial to improve the predictability of biomechanical simulations. Fibrillar collagen in the vascular wall plays a central role in tissue adaptation owing to its relatively short lifetime. Pathological alterations of collagen turnover may fail to result in homeostasis and could be responsible for abdominal aortic aneurysm (AAA) growth at later stages of the disease. For this reason our previously reported multiscale constitutive framework (Martufi, G. & Gasser, T. C. 2011 J. Biomech. 44, 2544-2550 (doi:10.1016/j.jbiomech.2011.07.015)) has been enriched by a collagen turnover model. Specifically, the framework's collagen fibril level allowed a sound integration of vascular wall biology, and the impact of collagen turnover on the macroscopic properties of AAAs was studied. To this end, model parameters were taken from the literature and/or estimated from clinical follow-up data of AAAs (on average 50.7 mm-large). Likewise, the in vivo stretch of the AAA wall was set, such that 10 per cent of collagen fibres were engaged. Results showed that the stretch spectrum, at which collagen fibrils are deposed, is the most influential parameter, i.e. it determines whether the vascular geometry grows, shrinks or remains stable over time. Most importantly, collagen turnover also had a remarkable impact on the macroscopic stress field. It avoided high stress gradients across the vessel wall, thus predicted a physiologically reasonable stress field. Although the constitutive model could be successfully calibrated to match the growth of small AAAs, a rigorous validation against experimental data is crucial to further explore the model's descriptive and predictive capabilities.

摘要

更好地了解血管组织适应其力学环境的固有特性对于提高生物力学模拟的可预测性至关重要。血管壁中的纤维状胶原蛋白由于其相对较短的寿命,在组织适应中起着核心作用。胶原蛋白周转率的病理性改变可能无法导致体内平衡,并且可能是疾病后期腹主动脉瘤(AAA)生长的原因。出于这个原因,我们之前报告的多尺度本构框架(Martufi,G. 和 Gasser,T. C. 2011 J. Biomech. 44,2544-2550(doi:10.1016/j.jbiomech.2011.07.015))已经通过胶原蛋白周转率模型得到了丰富。具体来说,该框架的胶原蛋白纤维水平允许对血管壁生物学进行合理的整合,并研究了胶原蛋白周转率对 AAA 宏观特性的影响。为此,模型参数取自文献和/或从 AAA 的临床随访数据中估计(平均直径为 50.7mm)。同样,设定了 AAA 壁的体内拉伸,使得 10%的胶原蛋白纤维参与。结果表明,胶原蛋白纤维沉积的拉伸谱是最具影响力的参数,即它决定了血管几何形状是随着时间的推移而生长、收缩还是保持稳定。最重要的是,胶原蛋白周转率对宏观应力场也有显著影响。它避免了血管壁上的高应力梯度,从而预测了一个生理上合理的应力场。尽管本构模型可以成功地校准以匹配小 AAA 的生长,但对实验数据的严格验证对于进一步探索模型的描述和预测能力至关重要。

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