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Cell-based high content screening using an integrated microfluidic device

机译:使用集成的微流控设备进行基于细胞的高含量筛选

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摘要

High content screening (HCS) has quickly established itself as a core technique in the early stage of drug discovery for secondary compound screening. It allows several independent cellular parameters to be measured in a single cell or populations of cells in a single assay. In this work, we describe high content screening for the multiparametric measurement of cellular responses in human liver carcinoma (HepG2) cells using an integrated microfluidic device. This device consists of multiple drug gradient generators and parallel cell culture chambers, in which the processes of liquid dilution and diffusion, micro-scale cell culture, cell stimulation and cell labeling can be integrated into a single device. The simple assay provides multiparametric measurements of plasma membrane permeability, nuclear size, mitochondrial transmembrane potential and intracellular redox states in anti-cancer drug-induced apoptosis of HepG2 cells. The established platform is able to rapidly extract the maximum of information from tumor cells in response to several drugs varying in concentration, with minimal sample and less time, which is very useful for basic biomedical research and cancer treatment.
机译:高含量筛选(HCS)在药物研发的早期阶段已迅速确立其核心技术,用于二级化合物筛选。它允许在单个测定或单个测定的细胞群中测量多个独立的细胞参数。在这项工作中,我们描述了使用集成的微流控设备对人肝癌(HepG2)细胞中细胞反应进行多参数测量的高内涵筛选。该设备由多个药物梯度发生器和平行的细胞培养室组成,其中液体稀释和扩散,微型细胞培养,细胞刺激和细胞标记过程可以集成到单个设备中。这种简单的测定方法可在抗癌药物诱导的HepG2细胞凋亡中提供质膜通透性,核大小,线粒体跨膜电位和细胞内氧化还原状态的多参数测量。建立的平台能够响应几种浓度不同的药物,以最少的样品和更少的时间快速从肿瘤细胞中提取最大的信息,这对于基础生物医学研究和癌症治疗非常有用。

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