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Cellular Delivery of Nanoparticles Revealed with Combined Optical and Isotopic Nanoscopy

机译:结合光学和同位素纳米技术揭示的纳米粒子的细胞传递。

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Direct polymerization of an oxaliplatin analogue was used to reproducibly generate amphiphiles in one pot, which consistently and spontaneously self-assemble into well-defined nanoparticles (NPs). Despite inefficient drug leakage in cell-free assays, the NPs were observed to be as cytotoxic as free oxaliplatin in cell culture experiments. We investigated this phenomenon by super-resolution fluorescence structured illumination microscopy (SIM) and nanoscale secondary ion mass spectrometry (NanoSIMS). In combination, these techniques revealed NPs are taken up via endocytic pathways before intracellular release of their cytotoxic cargo. As with other drug-carrying nanomaterials, these systems have potential as cellular delivery vehicles. However, high-resolution methods to track nanocarriers and their cargo at the micro- and nanoscale have been underutilized in general, limiting our understanding of their interactions with cells and tissues. We contend this type of combined optical and isotopic imaging strategy represents a powerful and potentially generalizable methodology for cellular tracking of nanocarriers and their cargo.
机译:奥沙利铂类似物的直接聚合反应可用于在一个罐中可重复生成两亲物,该两亲物始终如一地自发地自组装成定义明确的纳米粒子(NP)。尽管在无细胞试验中药物泄漏效率很低,但在细胞培养实验中仍观察到NP与游离奥沙利铂一样具有细胞毒性。我们通过超分辨率荧光结构照明显微镜(SIM)和纳米级二次离子质谱(NanoSIMS)研究了这一现象。结合起来,这些技术揭示了NP在细胞内释放其细胞毒性货物之前是通过内吞途径吸收的。与其他载药纳米材料一样,这些系统具有作为细胞递送载体的潜力。但是,在微米和纳米规模上跟踪纳米载体及其货物的高分辨率方法通常没有得到充分利用,这限制了我们对它们与细胞和组织相互作用的理解。我们认为这种类型的光学和同位素成像相结合的策略代表了一种对纳米载体及其货物进行细胞跟踪的强大且可能具有通用性的方法。

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