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脑细胞外空间三维扩散的随机游走模型:与微光纤光漂白测量结果的比较

Random-walk model of diffusion in three dimensions in brain extracellular space: comparison with microfiberoptic photobleaching measurements.

作者信息

Jin Songwan, Zador Zsolt, Verkman A S

机构信息

Departments of Medicine and Physiology, University of California, San Francisco, California, USA.

出版信息

Biophys J. 2008 Aug;95(4):1785-94. doi: 10.1529/biophysj.108.131466. Epub 2008 May 9.

Abstract

Diffusion through the extracellular space (ECS) in brain is important in drug delivery, intercellular communication, and extracellular ionic buffering. The ECS comprises approximately 20% of brain parenchymal volume and contains cell-cell gaps approximately 50 nm. We developed a random-walk model to simulate macromolecule diffusion in brain ECS in three dimensions using realistic ECS dimensions. Model inputs included ECS volume fraction (alpha), cell size, cell-cell gap geometry, intercellular lake (expanded regions of brain ECS) dimensions, and molecular size of the diffusing solute. Model output was relative solute diffusion in water versus brain ECS (D(o)/D). Experimental D(o)/D for comparison with model predictions was measured using a microfiberoptic fluorescence photobleaching method involving stereotaxic insertion of a micron-size optical fiber into mouse brain. D(o)/D for the small solute calcein in different regions of brain was in the range 3.0-4.1, and increased with brain cell swelling after water intoxication. D(o)/D also increased with increasing size of the diffusing solute, particularly in deep brain nuclei. Simulations of measured D(o)/D using realistic alpha, cell size and cell-cell gap required the presence of intercellular lakes at multicell contact points, and the contact length of cell-cell gaps to be least 50-fold smaller than cell size. The model accurately predicted D(o)/D for different solute sizes. Also, the modeling showed unanticipated effects on D(o)/D of changing ECS and cell dimensions that implicated solute trapping by lakes. Our model establishes the geometric constraints to account quantitatively for the relatively modest slowing of solute and macromolecule diffusion in brain ECS.

摘要

在大脑中,通过细胞外间隙(ECS)的扩散在药物递送、细胞间通讯和细胞外离子缓冲方面具有重要意义。ECS约占脑实质体积的20%,包含约50纳米的细胞间间隙。我们开发了一种随机游走模型,利用实际的ECS尺寸在三维空间中模拟大分子在脑ECS中的扩散。模型输入包括ECS体积分数(α)、细胞大小、细胞间间隙几何形状、细胞间湖(脑ECS的扩展区域)尺寸以及扩散溶质的分子大小。模型输出是溶质在水中与脑ECS中的相对扩散率(Dₒ/D)。使用微光纤荧光光漂白法测量用于与模型预测进行比较的实验性Dₒ/D,该方法涉及将微米尺寸的光纤立体定位插入小鼠大脑。脑不同区域中小溶质钙黄绿素的Dₒ/D在3.0 - 4.1范围内,且在水中毒后脑细胞肿胀时会增加。Dₒ/D也随着扩散溶质尺寸的增加而增加,特别是在脑深部核团中。使用实际的α、细胞大小和细胞间间隙对测量的Dₒ/D进行模拟时,需要在多细胞接触点存在细胞间湖,且细胞间间隙的接触长度至少比细胞大小小50倍。该模型准确预测了不同溶质尺寸的Dₒ/D。此外,建模显示了改变ECS和细胞尺寸对Dₒ/D的意外影响,这涉及到溶质被湖捕获。我们的模型建立了几何约束,以定量解释溶质和大分子在脑ECS中扩散相对适度减慢的现象。

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