ER network heterogeneity guides diffusive transport and kinetics

Zubenelgenubi C. Scott, Katherine Koning, Molly Vanderwerp, Lorna Cohen, Laura M. Westrate, Elena F. Koslover
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Abstract

The endoplasmic reticulum (ER) is a dynamic network of interconnected sheets and tubules that orchestrates the distribution of lipids, ions, and proteins throughout the cell. The impact of its complex, dynamic morphology on its function as an intracellular transport hub remains poorly understood. To elucidate the functional consequences of ER network structure and dynamics, we quantify how the heterogeneity of the peripheral ER in COS7 cells affects diffusive protein transport. In vivo imaging of photoactivated ER membrane proteins demonstrates their non-uniform spreading to adjacent regions, in a manner consistent with simulations of diffusing particles on extracted network structures. Using a minimal network model to represent tubule rearrangements, we demonstrate that ER network dynamics are sufficiently slow to have little effect on diffusive protein transport. Furthermore, stochastic simulations reveal a novel consequence of ER network heterogeneity: the existence of 'hot spots' where sparse diffusive reactants are more likely to find one another. Intriguingly, ER exit sites are disproportionately found in these highly accessible regions. Combining in vivo experiments with analytic calculations, quantitative image analysis, and computational modeling, we demonstrate how structure guides diffusive protein transport and reactions in the ER.
内质网的异质性指导扩散传输和动力学
内质网(ER)是一个由相互连接的薄片和小管组成的动态网络,它协调着脂质、离子和蛋白质在整个细胞中的分布。其复杂的动态形态对其作为细胞内运输枢纽的功能的影响仍然知之甚少。为了阐明内质网网络结构和动力学的功能后果,我们量化了COS7细胞外周内质网的异质性如何影响弥漫性蛋白质运输。光激活内质网膜蛋白的体内成像显示它们不均匀地扩散到邻近区域,这与在提取的网络结构上扩散颗粒的模拟方式一致。使用最小网络模型来表示小管重排,我们证明内质网动力学足够慢,对弥漫性蛋白质运输几乎没有影响。此外,随机模拟揭示了ER网络异质性的一个新结果:“热点”的存在,在这些热点中,稀疏的扩散反应物更容易找到彼此。有趣的是,急诊室的出口地点不成比例地出现在这些交通便利的地区。结合体内实验、分析计算、定量图像分析和计算建模,我们展示了结构如何引导内质网中的弥散蛋白运输和反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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