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High-content single-cell drug screening with phosphospecific flow cytometry

机译:磷酸特异性流式细胞仪进行高含量单细胞药物筛选

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摘要

Drug screening is often limited to cell-free assays involving purified enzymes, but it is arguably best applied against systems that represent disease states or complex physiological cellular networks. Here, we describe a high-content, cell-based drug discovery platform based on phosphospecific flow cytometry, or phosphoflow, that enabled screening for inhibitors against multiple endogenous kinase signaling pathways in heterogeneous primary cell populations at the single-cell level. From a library of small-molecule natural products, we identified pathway-selective inhibitors of Jak-Stat and MAP kinase signaling. Dose-response experiments in primary cells confirmed pathway selectivity, but importantly also revealed differential inhibition of cell types and new druggability trends across multiple compounds. Lead compound selectivity was confirmed in vivo in mice. Phosphoflow therefore provides a unique platform that can be applied throughout the drug discovery process, from early compound screening to in vivo testing and clinical monitoring of drug efficacy.
机译:药物筛选通常仅限于涉及纯化酶的无细胞分析,但可以说,它最好用于代表疾病状态或复杂生理细胞网络的系统。在这里,我们描述了一种基于磷酸特异性流式细胞仪或phosphoflow的高含量,基于细胞的药物发现平台,该平台能够在单细胞水平上筛选针对异种原代细胞群中多个内源激酶信号通路的抑制剂。从小分子天然产物库中,我们确定了Jak-Stat和MAP激酶信号传导的途径选择性抑制剂。在原代细胞中进行剂量反应实验证实了途径的选择性,但重要的是还揭示了细胞类型的差异抑制和多种化合物之间新的药物形成趋势。在小鼠体内证实了铅化合物的选择性。因此,Phosphoflow提供了一个独特的平台,可用于整个药物发现过程,从早期化合物筛选到体内测试以及药物疗效的临床监测。

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