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用于癌细胞靶向和可追踪细胞内药物递送的 SERS 编码两亲性金纳米粒子自组装等离子体囊泡。

Self-assembled plasmonic vesicles of SERS-encoded amphiphilic gold nanoparticles for cancer cell targeting and traceable intracellular drug delivery.

机构信息

School of Chemical and Biomedical Engineering, Nanyang Technological University, 70 Nanyang Drive, Singapore 637457.

出版信息

J Am Chem Soc. 2012 Aug 15;134(32):13458-69. doi: 10.1021/ja305154a. Epub 2012 Aug 6.

Abstract

We report the development of bioconjugated plasmonic vesicles assembled from SERS-encoded amphiphilic gold nanoparticles for cancer-targeted drug delivery. This new type of plasmonic assemblies with a hollow cavity can play multifunctional roles as delivery carriers for anticancer drugs and SERS-active plasmonic imaging probes to specifically label targeted cancer cells and monitor intracellular drug delivery. We have shown that the pH-responsive disassembly of the plasmonic vesicle, stimulated by the hydrophobic-to-hydrophilic transition of the hydrophobic brushes in acidic intracellular compartments, allows for triggered intracellular drug release. Because self-assembled plasmonic vesicles exhibit significantly different plasmonic properties and greatly enhanced SERS intensity in comparison with single gold nanoparticles due to strong interparticle plasmonic coupling, disassembly of the vesicles in endocytic compartments leads to dramatic changes in scattering properties and SERS signals, which can serve as independent feedback mechanisms to signal cargo release from the vesicles. The unique structural and optical properties of the plasmonic vesicle have made it a promising platform for targeted combination therapy and theranostic applications by taking advantage of recent advances in gold nanostructure based in vivo bioimaging and photothermal therapy and their loading capacity for both hydrophilic (nucleic acids and proteins) and hydrophobic (small molecules) therapeutic agents.

摘要

我们报告了由表面增强拉曼散射(SERS)编码两亲性金纳米粒子组装而成的生物共轭等离子体囊泡的发展,用于癌症靶向药物输送。这种具有中空腔的新型等离子体组装体可以作为抗癌药物和 SERS 活性等离子体成像探针的多功能载体,特异性标记靶向癌细胞并监测细胞内药物输送。我们已经表明,由于疏水性至亲水性的转变,在酸性细胞内隔室中刺激等离子体囊泡的 pH 响应性解组装,允许触发细胞内药物释放。由于自组装的等离子体囊泡由于颗粒间的强等离子体耦合而表现出与单个金纳米颗粒相比明显不同的等离子体性质和大大增强的 SERS 强度,因此在内涵体中解组装会导致散射性质和 SERS 信号的剧烈变化,这可以作为从囊泡中释放货物的独立反馈机制。由于利用了基于金纳米结构的体内生物成像和光热治疗的最新进展及其对亲水性(核酸和蛋白质)和疏水性(小分子)治疗剂的负载能力,等离子体囊泡的独特结构和光学特性使其成为靶向联合治疗和治疗应用的有前途的平台。

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