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金纳米星的细胞内光学探测。

Intracellular optical probing with gold nanostars.

机构信息

Humboldt-Universität zu Berlin, Department of Chemistry, Brook-Taylor-Str. 2, 12489 Berlin, Germany.

出版信息

Nanoscale. 2021 Jan 14;13(2):968-979. doi: 10.1039/d0nr07031a. Epub 2020 Dec 24.

DOI:10.1039/d0nr07031a
PMID:33367430
Abstract

Gold nanostars are important nanoscopic tools in biophotonics and theranostics. To understand the fate of such nanostructures in the endolysosomal system of living cells as an important processing route in biotechnological approaches, un-labelled, non-targeted gold nanostars synthesized using HEPES buffer were studied in two cell lines. The uptake of the gold nanostructures leads to cell line-dependent intra-endolysosomal agglomeration, which results in a greater enhancement of the local optical fields than those around individual nanostars and near aggregates of spherical gold nanoparticles of the same size. As demonstrated by non-resonant surface-enhanced Raman scattering (SERS) spectra in the presence and absence of aggregation, the spectroscopic signals of molecules are of very similar strength over a wide range of concentrations, which is ideal for label-free vibrational characterization of cells and other complex environments. In 3T3 and HCT-116 cells, SERS data were analyzed together with the properties of the intracellular nanostar agglomerates. Vibrational spectra indicate that the processing of nanostars by cells and their interaction with the surrounding endolysosomal compartment is connected to their morphological properties through differences in the structure and interactions in their intracellular protein corona. Specifically, different intracellular processing was found to result from a different extent of hydrophobic interactions at the pristine gold surface, which varies for nanostars of different spike lengths. The sensitive optical monitoring of surroundings of nanostars and their intracellular processing makes them a very useful tool for optical bionanosensing and therapy.

摘要

金纳米星是生物光子学和治疗学中的重要纳米工具。为了了解这些纳米结构在活细胞的内溶酶体系统中的命运,作为生物技术方法中的重要处理途径,我们研究了使用 HEPES 缓冲液合成的未标记、非靶向的金纳米星在两种细胞系中的情况。金纳米结构的摄取导致细胞系依赖性的内溶酶体聚集,这导致局部光场的增强大于单个纳米星周围和相同尺寸的球形金纳米粒子聚集体附近的光场增强。正如存在和不存在聚集时的非共振表面增强拉曼散射 (SERS) 光谱所证明的那样,分子的光谱信号在很宽的浓度范围内具有非常相似的强度,这非常适合用于无标记的细胞和其他复杂环境的振动特征化。在 3T3 和 HCT-116 细胞中,与细胞内纳米星聚集体的特性一起分析了 SERS 数据。振动光谱表明,细胞对纳米星的处理及其与周围内溶酶体隔室的相互作用与其形态特性有关,这与细胞内蛋白质冠中的结构和相互作用的差异有关。具体而言,发现不同的细胞内处理是由于不同程度的原始金表面的疏水性相互作用,对于不同刺长的纳米星,这种相互作用的程度不同。对纳米星周围环境和其细胞内处理的敏感光学监测使它们成为光学生物传感和治疗的非常有用的工具。

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