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Self-Assembled Gold Nanoclusters for Bright Fluorescence Imaging and Enhanced Drug Delivery

机译:自组装金纳米簇,用于明亮的荧光成像和增强的药物递送

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Nanoparticles combining enhanced cellular drug delivery with efficient fluorescence detection are important tools for the development of theranostic agents. Here, we demonstrate this concept by a simple, fast, and robust protocol of cationic polymer mediated gold nanocluster (Au NCs) self-assembly into nanoparticles (NPs) of ca. 120 nm diameter. An extensive characterization of the monodisperse and positively charged NPs revealed pH-dependent swelling properties, strong fluorescence enhancement, and excellent colloidal and photostability in water, buffer, and culture medium. The versatility of the preparation is demonstrated by using different Au NC surface ligands and cationic polymers. Steady-state and time-resolved fluorescence measurements give insight into the aggregation-induced emission phenomenon (AIE) by tuning the Au NC interactions in the self-assembled nanoparticles using the pH-dependent swelling. In vitro studies in human monocytic cells indicate strongly enhanced uptake of the NPs compared to free Au NCs in endocytic compartments. The NPs keep their assembly structure with quite low cytotoxicity up to 500 mu g Au/mL. Enhanced drug delivery is demonstrated by loading peptides or antibodies in the NPs using a one-pot synthesis. Fluorescence microscopy and flow cytometry confirmed intracellular colocalization of the biomolecules and the NP carriers with a respective 1.7-fold and 6.5-fold enhanced cellular uptake of peptides and antibodies compared to the free biomolecules.
机译:结合增强的细胞药物递送和有效的荧光检测的纳米颗粒是开发治疗药物的重要工具。在这里,我们通过阳离子聚合物介导的金纳米簇(Au NCs)自组装成ca的纳米颗粒(NPs)的简单,快速和强大的协议来演示此概念。直径为120 nm。单分散和带正电荷的NP的广泛表征揭示了pH依赖性的溶胀特性,强烈的荧光增强以及在水,缓冲液和培养基中的出色的胶体和光稳定性。通过使用不同的Au NC表面配体和阳离子聚合物证明了该制剂的多功能性。稳态和时间分辨荧光测量可通过使用pH依赖性溶胀调节自组装纳米颗粒中的Au NC相互作用,从而深入了解聚集诱导的发射现象(AIE)。在人单核细胞中的体外研究表明,与内吞区室中的游离Au NCs相比,NP的摄取大大增强。 NP保持其组装结构的毒性非常低,最高可达500μg Au / mL。通过使用一锅法合成将肽或抗体加载到NP中,可以证明增强的药物传递。荧光显微镜和流式细胞术证实,与游离生物分子相比,生物分子和NP载体在细胞内共定位,肽和抗体的细胞摄取分别增加了1.7倍和6.5倍。

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