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Fast Metabolic Response to Drug Intervention Through Analysis on a Miniaturized, Highly Integrated Molecular Imaging System

机译:通过微型化,高度集成的分子成像系统分析对药物干预的快速代谢反应

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摘要

We report on a radiopharmaceutical imaging platform designed to capture the kinetics of cellular responses to drugs. Methods: A portable in vitro molecular imaging system comprising a microchip and a β-particle imaging camera permitted routine cell-based radioassays of small numbers of either suspended or adherent cells. We investigated the kinetics of responses of model lymphoma and glioblastoma cancer cell lines to ^(18)F-FDG uptake after drug exposure. Those responses were correlated with kinetic changes in the cell cycle or with changes in receptor tyrosine kinase signaling. Results: The platform enabled direct radioassays of multiple cell types and yielded results comparable to those from conventional approaches; however, the platform used smaller sample sizes, permitted a higher level of quantitation, and did not require cell lysis. Conclusion: The kinetic analysis enabled by the platform provided a rapid (∼1 h) drug screening assay.
机译:我们报告了一个旨在捕获细胞对药物反应动力学的放射性药物成像平台。方法:便携式体外分子成像系统,包括微芯片和β粒子成像相机,可对少量悬浮细胞或粘附细胞进行常规的基于细胞的放射分析。我们研究了暴露于药物后模型淋巴瘤和胶质母细胞瘤癌细胞系对^(18)F-FDG摄取的反应动力学。这些反应与细胞周期的动力学变化或受体酪氨酸激酶信号传导的变化相关。结果:该平台可直接进行多种细胞类型的放射测定,并产生与传统方法相当的结果;但是,该平台使用的样本量较小,允许更高的定量水平,并且不需要细胞裂解。结论:该平台支持的动力学分析提供了快速(约1小时)的药物筛选测定。

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