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Simulation-assisted design of microfluidic sample traps for optimal trapping and culture of non-adherent single cells tissues and spheroids

机译:模拟辅助设计的微流控样品阱可最佳捕获和培养非粘附性单细胞组织和球体

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摘要

This work focuses on modelling design and operation of “microfluidic sample traps” (MSTs). MSTs regroup a widely used class of microdevices that incorporate wells, recesses or chambers adjacent to a channel to individually trap, culture and/or release submicroliter 3D tissue samples ranging from simple cell aggregates and spheroids, to ex vivo tissue samples and other submillimetre-scale tissue models. Numerous MST designs employing various trapping mechanisms have been proposed in the literature, spurring the development of 3D tissue models for drug discovery and personalized medicine. Yet, there lacks a general framework to optimize trapping stability, trapping time, shear stress, and sample metabolism. Herein, the effects of hydrodynamics and diffusion-reaction on tissue viability and device operation are investigated using analytical and finite element methods with systematic parametric sweeps over independent design variables chosen to correspond to the four design degrees of freedom. Combining different results, we show that, for a spherical tissue of diameter d < 500 μm, the simplest, closest to optimal trap shape is a cube of dimensions w equal to twice the tissue diameter: w = 2d. Furthermore, to sustain tissues without perfusion, available medium volume per trap needs to be 100× the tissue volume to ensure optimal metabolism for at least 24 hours.
机译:这项工作的重点是“微流体样品阱”(MST)的建模设计和操作。 MST重新组合了广泛使用的微设备类别,该设备合并了与通道相邻的孔,凹口或腔室,以分别捕获,培养和/或释放亚微升3D组织样本,范围从简单的细胞聚集体和椭球体,到离体组织样本和其他亚毫米级组织模型。在文献中已经提出了采用各种诱集机制的许多MST设计,从而刺激了3D组织模型的开发,以用于药物发现和个性化医学。但是,目前缺乏优化捕集稳定性,捕集时间,剪切应力和样品代谢的通用框架。在本文中,使用解析和有限元方法研究流体动力学和扩散反应对组织生存力和设备操作的影响,方法是对与四个设计自由度相对应的独立设计变量进行系统的参数化扫描。结合不同的结果,我们发现,对于直径为d <500μm的球形组织,最简单,最接近最佳陷阱形状的立方体是尺寸w等于组织直径的两倍的立方体:w = 2d。此外,为了维持组织而不进行灌注,每个陷阱的可用培养基体积必须是组织体积的100倍,以确保至少24小时的最佳代谢。

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