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Real-time visualization of clustering and intracellular transport of gold nanoparticles by correlative imaging

机译:通过相关成像实时可视化金纳米颗粒的聚集和细胞内运输

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Mechanistic understanding of the endocytosis and intracellular trafficking of nanoparticles is essential for designing smart theranostic carriers. Physico-chemical properties, including size, clustering and surface chemistry of nanoparticles regulate their cellular uptake and transport. Significantly, even single nanoparticles could cluster intracellularly, yet their clustering state and subsequent trafficking are not well understood. Here, we used DNA-decorated gold (fPlas-gold) nanoparticles as a dually emissive fluorescent and plasmonic probe to examine their clustering states and intracellular transport. Evidence from correlative fluorescence and plasmonic imaging shows that endocytosis of fPlas-gold follows multiple pathways. In the early stages of endocytosis, fPlas-gold nanoparticles appear mostly as single particles and they cluster during the vesicular transport and maturation. The speed of encapsulated fPlas-gold transport was critically dependent on the size of clusters but not on the types of organelle such as endosomes and lysosomes. Our results provide key strategies for engineering theranostic nanocarriers for efficient health management.
机译:对纳米颗粒的内吞作用和细胞内运输的机械理解对于设计智能的治疗治疗载体至关重要。纳米粒子的物理化学性质(包括大小,聚集和表面化学性质)调节其细胞摄取和转运。值得注意的是,即使是单个纳米颗粒也可以在细胞内聚集,但是它们的聚集状态和随后的运输尚不清楚。在这里,我们使用了DNA修饰的金(fPlas-gold)纳米颗粒作为双重发射荧光和等离子体探针,以检查它们的聚集状态和细胞内转运。相关荧光和等离子体成像的证据表明,fPlas-gold的内吞作用遵循多种途径。在内吞作用的早期阶段,fPlas-gold纳米颗粒主要以单颗粒形式出现,并在水泡运输和成熟过程中聚集。封装的fPlas-gold转运的速度主要取决于簇的大小,而不取决于细胞器的类型,例如内体和溶酶体。我们的结果提供了工程化纳米治疗载体以进行有效健康管理的关键策略。

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