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A systematic High-Content Screening microscopy approach reveals key roles for Rab33b, OATL1 and Myo6 in nanoparticle trafficking in HeLa cells

机译:一个系统的高内涵筛选显微镜方法揭示了Rab33b,OATL1和Myo6纳米颗粒贩运HeLa细胞中的关键作用

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Synthetic nanoparticles are promising tools for imaging and drug delivery; however the molecular details of cellular internalization and trafficking await full characterization. Current knowledge suggests that following endocytosis most nanoparticles pass from endosomes to lysosomes. In order to design effective drug delivery strategies that can use the endocytic pathway, or by-pass lysosomal accumulation, a comprehensive understanding of nanoparticle uptake and trafficking mechanisms is therefore fundamental. Here we describe and apply an RNA interference-based high-content screening microscopy strategy to assess the intracellular trafficking of fluorescently-labeled polystyrene nanoparticles in HeLa cells. We screened a total of 408 genes involved in cytoskeleton and membrane function, revealing roles for myosin VI, Rab33b and OATL1 in this process. This work provides the first systematic large-scale quantitative assessment of the proteins responsible for nanoparticle trafficking in cells, paving the way for subsequent genome-wide studies.
机译:合成纳米粒子是用于成像和药物递送的有希望的工具;然而,蜂窝内化和贩运的分子细节等待全部表征。目前的知识表明,在内吞作用之后,大多数纳米颗粒通过内体的溶酶体。为了设计可以使用内吞径的有效药物递送策略,或通过通过溶酶体积累,因此对纳米粒子摄取和贩运机制的全面了解是至关重要的。在这里,我们描述并应用基于RNA干扰的高含量筛选显微镜策略,以评估HeLa细胞中荧光标记的聚苯乙烯纳米颗粒的细胞内运输。我们筛选了总共408个基因,参与了细胞骨架和膜功能,揭示了肌蛋白VI,RAB33B和OATL1在该过程中的作用。这项工作提供了负责纳米粒子贩运群体的蛋白质的第一种系统大规模定量评估,为随后的基因组研究铺平了途径。

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