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Stereoscopic Particle Image Velocimetry Analysis of Healthy and Emphysemic Alveolar Sac Models

机译:健康的肺气肿囊模型的立体粒子图像测速分析

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Emphysema is a progressive lung disease that involves permanent destruction of the alveolar walls. Fluid mechanics in the pulmonary region and how they are altered with the presence of emphysema are not well understood. Much of our understanding of the flow fields occurring in the healthy pulmonary region is based on idealized geometries, and little attention has been paid to emphysemic geometries. The goal of this research was to utilize actual replica lung geometries to gain a better understanding of the mechanisms that govern fluid motion and particle transport in the most distal regions of the lung and to compare the differences that exist between healthy and emphysematous lungs. Excised human healthy and emphysemic lungs were cast, scanned, graphically reconstructed, and used to fabricate clear, hollow, compliant models. Three dimensional flow fields were obtained experimentally using stereoscopic particle image velocimetry techniques for healthy and emphysematic breathing conditions. Measured alveolar velocities ranged over two orders of magnitude from the duct entrance to the wall in both models. Recirculating flow was not found in either the healthy or the emphysematic model, while the average flow rate was three times larger in emphysema as compared to healthy. Diffusion dominated particle flow, which is characteristic in the pulmonary region of the healthy lung, was not seen for emphysema, except for very small particle sizes. Flow speeds dissipated quickly in the healthy lung (60% reduction in 0.25 mm) but not in the emphysematic lung (only 8% reduction 0.25 mm). Alveolar ventilation per unit volume was 30% smaller in emphysema compared to healthy. Destruction of the alveolar walls in emphysema leads to significant differences in flow fields between the healthy and emphysemic lung. Models based on replica geometry provide a useful means to quantify these differences and could ultimately improve our understanding of disease progression.
机译:肺气肿是一种进行性肺部疾病,涉及肺泡壁的永久性破坏。肺部区域的流体力学及其在存在肺气肿时的变化方式尚不十分清楚。我们对健康肺区域中发生的流场的大多数了解是基于理想化的几何形状,而对肺气肿的几何形状却很少关注。这项研究的目的是利用实际的复制肺部几何形状更好地了解控制肺部最远端区域的流体运动和颗粒运输的机制,并比较健康肺与气肿性肺之间存在的差异。摘除人体健康和肺气肿的肺,进行扫描,图形重建,并用于制造清晰,空心,顺应性的模型。使用立体粒子图像测速技术,针对健康和气喘的呼吸条件,通过实验获得了三维流场。在两种模型中,从管道入口到壁的测量肺泡速度范围都超过两个数量级。在健康模型或肺气肿模型中均未发现回流,而在肺气肿中,平均流速是健康模型的三倍。肺气肿未见以扩散为主的颗粒流,这是健康肺的肺区域的特征,除了非常小的颗粒大小。流速在健康的肺中迅速消散(0.25 mm减少了60%),但在肺气肿的肺中没有消散(0.25 mm仅减少了8%)。与健康相比,肺气肿每单位体积的肺泡通气量减少了30%。肺气肿中肺泡壁的破坏导致健康肺与肺气肿之间的流场显着不同。基于复制品几何的模型为量化这些差异提供了一种有用的手段,最终可以改善我们对疾病进展的了解。

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