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Simultaneous detection of intracellular target and off-target binding of small molecule cancer drugs at nanomolar concentrations

机译:同时检测纳摩尔浓度的小分子抗癌药物的细胞内靶标和脱靶结合

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摘要

Background and purpose:In vitro assays that determine activities of drug candidates with isolated targets have only limited predictive value for activities in cellular assays. Poor membrane permeability and off-target binding are major reasons for such discrepancies. However, it still difficult to directly analyse off-target binding at the same time as target binding, on a subcellular level. Here, we present a combination of fluorescence correlation spectroscopy (FCS) and fluorescence cross-correlation spectroscopy (FCCS) as a solution to this problem.
机译:背景和目的:确定具有分离靶标的候选药物活性的体外测定对于细胞测定中的活性只有有限的预测价值。膜通透性差和脱靶结合是这种差异的主要原因。然而,仍然难以在亚细胞水平上与靶标结合同时直接分析脱靶结合。在这里,我们提出了荧光相关光谱学(FCS)和荧光互相关光谱学(FCCS)的组合作为解决此问题的方法。

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