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Simulations of (An)Isotropic Diffusion on Curved Biological Surfaces

机译:弯曲生物表面上(各向同性)扩散的模拟

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摘要

We present a computational particle method for the simulation of isotropic and anisotropic diffusion on curved biological surfaces that have been reconstructed from image data. The method is capable of handling surfaces of high curvature and complex shape, which are often encountered in biology. The method is validated on simple benchmark problems and is shown to be second-order accurate in space and time and of high parallel efficiency. It is applied to simulations of diffusion on the membrane of endoplasmic reticula (ER) in live cells. Diffusion simulations are conducted on geometries reconstructed from real ER samples and are compared to fluorescence recovery after photobleaching experiments in the same ER samples using the transmembrane protein tsO45-VSV-G, C-terminally tagged with green fluorescent protein. Such comparisons allow derivation of geometry-corrected molecular diffusion constants for membrane components from fluorescence recovery after photobleaching data. The results of the simulations indicate that the diffusion behavior of molecules in the ER membrane differs significantly from the volumetric diffusion of soluble molecules in the lumen of the same ER. The apparent speed of recovery differs by a factor of ∼4, even when the molecular diffusion constants of the two molecules are identical. In addition, the specific shape of the membrane affects the recovery half-time, which is found to vary by a factor of ∼2 in different ER samples.
机译:我们提出了一种计算粒子方法,用于模拟从图像数据重建的弯曲生物表面上的各向同性和各向异性扩散。该方法能够处理生物学中经常遇到的高曲率和复杂形状的表面。该方法在简单的基准问题上得到了验证,并且在空间和时间上具有二阶精度,并且并行效率很高。它用于模拟活细胞内质网(ER)膜上的扩散。使用从真实ER样品重建的几何形状进行扩散模拟,并将其与使用跨膜蛋白tsO45-VSV-G(在C端标记有绿色荧光蛋白)的相同ER样品进行光漂白实验后,与荧光回收率进行比较。这样的比较允许从光漂白数据后的荧光回收率导出膜组分的几何校正的分子扩散常数。仿真结果表明,分子在ER膜中的扩散行为与可溶分子在同一ER腔中的体积扩散有显着差异。表观的恢复速度相差约4倍,即使两个分子的分子扩散常数相同。此外,膜的特定形状会影响半衰期,在不同的ER样品中,半衰期的变化约为2倍。

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