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Reaction Diffusion Modeling of Calcium Dynamics with Realistic ER Geometry

机译:具有实际ER几何的钙动力学反应扩散建模

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摘要

We describe a finite-element model of mast cell calcium dynamics that incorporates the endoplasmic reticulum's complex geometry. The model is built upon a three-dimensional reconstruction of the endoplasmic reticulum (ER) from an electron tomographic tilt series. Tetrahedral meshes provide volumetric representations of the ER lumen, ER membrane, cytoplasm, and plasma membrane. The reaction-diffusion model simultaneously tracks changes in cytoplasmic and ER intraluminal calcium concentrations and includes luminal and cytoplasmic protein buffers. Transport fluxes via PMCA, SERCA, ER leakage, and Type II IP3 receptors are also represented. Unique features of the model include stochastic behavior of IP3 receptor calcium channels and comparisons of channel open times when diffusely distributed or aggregated in clusters on the ER surface. Simulations show that IP3R channels in close proximity modulate activity of their neighbors through local Ca2+ feedback effects. Cytoplasmic calcium levels rise higher, and ER luminal calcium concentrations drop lower, after IP3-mediated release from receptors in the diffuse configuration. Simulation results also suggest that the buffering capacity of the ER, and not restricted diffusion, is the predominant factor influencing average luminal calcium concentrations.
机译:我们描述了结合内质网的复杂几何形状的肥大细胞钙动力学的有限元模型。该模型建立在根据电子断层扫描倾斜序列对内质网(ER)进行三维重建的基础上。四面体网格提供了ER内腔,ER膜,细胞质和质膜的体积表示。反应扩散模型可同时跟踪细胞质和内质网腔内钙浓度的变化,并包括管腔和细胞质蛋白缓冲液。还显示了通过PMCA,SERCA,ER泄漏和II型IP3受体的传输通量。该模型的独特功能包括IP3受体钙通道的随机行为以及当ER表面上的簇中分散分布或聚集时通道开放时间的比较。仿真表明,IP3R通道通过局部Ca 2 + 反馈效应来调节其邻居的活动。 IP3介导的受体从弥散结构释放后,细胞质钙水平升高,而ER内腔钙浓度降低。模拟结果还表明,ER的缓冲能力而不是受限的扩散是影响平均腔内钙浓度的主要因素。

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