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Mass diffusion coefficient measurement for vitreous humor using FEM and MRI

机译:使用FEM和MRI测量玻璃体液的质量扩散系数

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摘要

In early studies, the ‘contour method’ for determining the diffusion coefficient of the vitreous humor was developed. This technique relied on careful injection of an MRI contrast agent (surrogate drug) into the vitreous humor of fresh bovine eyes, and tracking the contours of the contrast agent in time. In addition, an analytical solution was developed for the theoretical contours built on point source model for the injected surrogate drug. The match between theoretical and experimental contours as a least square fit, while floating the diffusion coefficient, led to the value of the diffusion coefficient. This method had its limitation that the initial injection of the surrogate had to be spherical or ellipsoidal because of the analytical result based on the point-source model. With a new finite element model for the analysis in this study, the technique is much less restrictive and handles irregular shapes of the initial bolus. The fresh bovine eyes were used for drug diffusion study in the vitreous and three contrast agents of different molecular masses: gadolinium-diethylenetriaminepentaacetic acid (Gd-DTPA, 938 Da), non-ionic gadoteridol (Prohance, 559 Da), and bovine albumin conjugated with gadolinium (Galbumin, 74 kDa) were used as drug surrogates to visualize the diffusion process by MRI. The 3D finite element model was developed to determine the diffusion coefficients of these surrogates with the images from MRI. This method can be used for other types of bioporous media provided the concentration profile can be visualized (by methods such as MRI or fluorescence).
机译:在早期研究中,开发了用于确定玻璃体液扩散系数的“轮廓法”。该技术依赖于将MRI造影剂(替代药物)小心地注入新鲜牛眼的玻璃体液中,并及时追踪造影剂的轮廓。此外,针对注射替代药物的点源模型建立了理论轮廓的解析解决方案。理论和实验轮廓之间的匹配为最小二乘拟合,同时使扩散系数浮动,从而得出了扩散系数的值。该方法的局限性在于,由于基于点源模型的分析结果,替代物的初始注入必须为球形或椭圆形。在本研究中使用新的有限元模型进行分析时,该技术的限制要少得多,并且可以处理初始弹丸的不规则形状。新鲜的牛眼用于在玻璃体和三种不同分子量的造影剂中进行药物扩散研究:g-二乙烯三胺五乙酸(Gd-DTPA,938 Da),非离子性加多利多(Prohance,559 Da)和结合的牛白蛋白用g(Galbumin,74 kDa)作为药物替代物,通过MRI观察扩散过程。开发了3D有限元模型,用MRI图像确定这些替代物的扩散系数。该方法可用于其他类型的生物多孔介质,条件是浓度分布图可以可视化(通过MRI或荧光法)。

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