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红细胞变形性和聚集性对微观血流中无细胞层及表观黏度的影响。

Effects of erythrocyte deformability and aggregation on the cell free layer and apparent viscosity of microscopic blood flows.

作者信息

Zhang Junfeng, Johnson Paul C, Popel Aleksander S

机构信息

School of Engineering, Laurentian University, Sudbury, Canada.

出版信息

Microvasc Res. 2009 May;77(3):265-72. doi: 10.1016/j.mvr.2009.01.010. Epub 2009 Feb 4.

Abstract

Concentrated erythrocyte (i.e., red blood cell) suspensions flowing in microchannels have been simulated with an immersed-boundary lattice Boltzmann algorithm, to examine the cell layer development process and the effects of cell deformability and aggregation on hemodynamic and hemorheological behaviors. The cells are modeled as two-dimensional deformable biconcave capsules and experimentally measured cell properties have been utilized. The aggregation among cells is modeled by a Morse potential. The flow development process demonstrates how red blood cells migrate away from the boundary toward the channel center, while the suspending plasma fluid is displaced to the cell free layer regions left by the migrating cells. Several important characteristics of microscopic blood flows observed experimentally have been well reproduced in our model, including the cell free layer, blunt velocity profile, changes in apparent viscosity, and the Fahraeus effect. We found that the cell free layer thickness increases with both cell deformability and aggregation strength. Due to the opposing effects of the cell free layer lubrication and the high viscosity of cell-concentrated core, the influence of aggregation is complex but the lubrication effect appears to dominate, causing the relative apparent viscosity to decrease with aggregation. It appears therefore that the immersed-boundary lattice Boltzmann numerical model may be useful in providing valuable information on microscopic blood flows in various microcirculation situations.

摘要

已采用浸入边界格子玻尔兹曼算法模拟了在微通道中流动的浓缩红细胞(即红细胞)悬浮液,以研究细胞层的形成过程以及细胞变形性和聚集对血液动力学和血液流变学行为的影响。细胞被建模为二维可变形双凹胶囊,并利用了实验测量的细胞特性。细胞间的聚集通过莫尔斯势进行建模。流动发展过程展示了红细胞如何从边界向通道中心迁移,而悬浮的血浆则被排到迁移细胞留下的无细胞层区域。实验观察到的微观血流的几个重要特征在我们的模型中得到了很好的再现,包括无细胞层、钝性速度分布、表观粘度变化和法厄效应。我们发现无细胞层厚度随细胞变形性和聚集强度的增加而增加。由于无细胞层润滑和细胞浓缩核心高粘度的相反作用,聚集的影响很复杂,但润滑效应似乎占主导,导致相对表观粘度随聚集而降低。因此,浸入边界格子玻尔兹曼数值模型似乎可用于提供各种微循环情况下微观血流的有价值信息。

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