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Inducing chemotactic and haptotactic cues in microfluidic devices for three-dimensional in vitro assays

机译:在微流体装置中诱导趋化和触觉暗示以进行三维体外测定

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摘要

Microfluidic devices allow for the production of physiologically relevant cellular microenvironments by including biomimetic hydrogels and generating controlled chemical gradients. During transport, the biomolecules interact in distinct ways with the fibrillar networks: as purely diffusive factors in the soluble fluid or bound to the matrix proteins. These two main mechanisms may regulate distinct cell responses in order to guide their directional migration: caused by the substrate-bound chemoattractant gradient (haptotaxis) or by the gradient established within the soluble fluid (chemotaxis). In this work 3D diffusion experiments, in combination with ELISA assays, are performed using microfluidic platforms in order to quantify the distribution of PDGF-BB and TGF-β1 across collagen and fibrin gels. Furthermore, to gain a deeper understanding of the fundamental processes, the experiments are reproduced by computer simulations based on a reaction-diffusion transport model. This model yields an accurate prediction of the experimental results, confirming that diffusion and binding phenomena are established within the microdevice.
机译:微流体装置通过包括仿生水凝胶并产生受控的化学梯度来允许产生生理上相关的细胞微环境。在运输过程中,生物分子以不同的方式与原纤维网络相互作用:作为可溶性流体中的纯扩散因子或与基质蛋白结合。这两种主要机制可能调节不同的细胞反应,以指导其方向迁移:由底物结合的趋化因子梯度(趋同性)或可溶流体内建立的梯度(趋化性)引起。在这项工作中,使用微流体平台与ELISA分析相结合进行3D扩散实验,以定量PDGF-BB和TGF-β1在胶原蛋白和纤维蛋白凝胶上的分布。此外,为了更深入地了解基本过程,通过基于反应扩散传输模型的计算机模拟来重现实验。该模型可准确预测实验结果,从而确认在微器件内已建立了扩散和结合现象。

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