首页> 外文会议>ASME Global Congress on Nanoengineering for Medicine and Biology >MONITORING CELLULAR TRAFFICKING OF NANOPARTICLE CARGO IN MURINE MACROPHAGES THROUGH PLASMON COUPLING MICROSCOPY
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MONITORING CELLULAR TRAFFICKING OF NANOPARTICLE CARGO IN MURINE MACROPHAGES THROUGH PLASMON COUPLING MICROSCOPY

机译:通过等离子体偶联显微镜监测米胺巨噬细胞纳米粒子货物的细胞贩运

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摘要

A detailed analysis of silver nanoparticle (NP) uptake and trafficking in the murine macrophage cell line J774A.1 through spectral analysis of the resonance wavelength of the metal NP cargo is presented. The NP spectra reveal a strong phenotypic variability in the NP uptake and processing on the single cell level. Cells containing non- or low-agglomerated NPs are found to coexist with cells containing NPs of varying degrees of NP agglomeration, clearly indicated by a spectral red-shift in the resonance wavelength. Pharmacological inhibition studies indicate that the observed differences in the intracellular NP organization result from coexisting actin- and clathrin-dependent endocytosis mechanisms. Correlation with fluorescence macrophage maturity markers shows that differentiated J774A.1 macrophages preferentially contain compact NP agglomerates, whereas monocyte-like macrophages contain non-agglomerated NPs.
机译:介绍了对银纳米粒子(NP)摄取和鼠巨噬细胞系J774A.1通过光谱分析金属NP货物的谐振波长的光谱分析。 NP光谱揭示了在单细胞水平上的NP吸收和加工中强的表型变异性。发现含有非聚集NPS的细胞与含有不同程度的NP附聚的NPS的细胞共存,通过谐振波长的光谱红移清楚地表明。药理抑制研究表明,观察到细胞内NP组织的差异是共存的诱因和克拉族蛋白依赖性内吞作用机制。与荧光巨噬细胞成熟度标记的相关性表明,分化的J774A.1巨噬细胞优先含有紧凑的NP附聚物,而单核细胞样巨噬细胞含有非聚集的NPS。

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