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Expanding the Available Assays: Adapting and Validating In-Cell Westerns in Microfluidic Devices for Cell-Based Assays

机译:扩展可用的检测方法:调整和验证微流控设备中的细胞内Westerns进行基于细胞的检测

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摘要

Microfluidic methods for cellular studies can significantly reduce costs due to reduced reagent and biological specimen requirements compared with many traditional culture techniques. However, current types of readouts are limited and this lack of suitable readouts for microfluidic cultures has significantly hindered the application of microfluidics for cell-based assays. The In-Cell Western (ICW) technique uses quantitative immunocytochemistry and a laser scanner to provide an in situ measure of protein quantities in cells grown in microfluidic channels of arbitrary geometries. The use of ICWs in microfluidic channels was validated by a detailed comparison with current macroscale methods and shown to have excellent correlation. Transforming growth factor-β–induced epithelial-to-mesenchymal transition of an epithelial cell line was used as an example for further validation of the technique as a readout for soluble-factor-based assays performed in high-throughput microfluidic channels. The use of passive pumping for sample delivery and laser scanning for analysis opens the door to high-throughput quantitative microfluidic cell-based assays that integrate seamlessly with existing high-throughput infrastructure.
机译:与许多传统培养技术相比,用于细胞研究的微流体方法可减少试剂和生物标本的需求,从而可以大大降低成本。然而,当前的读数类型是有限的,并且对于微流体培养物缺乏合适的读数已经显着阻碍了微流体在基于细胞的测定中的应用。 In-Cell Western(ICW)技术使用定量免疫细胞化学和激光扫描仪来提供在任意几何形状的微流体通道中生长的细胞中蛋白质数量的原位测量。通过与当前的宏观方法进行详细比较,验证了ICW在微流体通道中的使用,并显示出极好的相关性。转化生长因子-β诱导的上皮细胞系上皮-间充质转化为例,进一步验证了该技术,作为在高通量微流体通道中进行的基于可溶性因子的测定的读数。使用被动泵进行样品输送和使用激光扫描进行分析,为基于高通量定量微流体细胞的测定法打开了大门,该测定法与现有的高通量基础设施无缝集成。

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