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首页> 外文期刊>Advanced drug delivery reviews >Fluorescence microscopy to follow the targeting of liposomes and micelles to cells and their intracellular fate.
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Fluorescence microscopy to follow the targeting of liposomes and micelles to cells and their intracellular fate.

机译:荧光显微镜观察脂质体和胶束对细胞及其细胞内命运的靶向作用。

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Fluorescence microscopy may provide important information regarding interactions between nanoparticulate drugs carriers, such as liposomes and micelles, with target cells as well as their intracellular fate. Current paper describes various applications of fluorescence microscopy to investigate specific targeting of antibody-modified drug carriers to cancer cells. The enhanced antibody-mediated targeting of drug-loaded immunomicelles confirmed by fluorescence microscopy resulted in enhanced cancer cell killing compared to free drug or drug-loaded nontargeted micelles. Fluorescence microscopy was also used to prove the endosomal escape of properly assembled polymeric micelles (based on polyethylene glycol-phosphatidylethanolamine conjugate, PEG-PE) containing various additives destabilizing the endosomal membrane. When loaded with the anticancer drug (paclitaxel or vitamin K3), such micelles demonstrate increased cytotoxicity. Fluorescence microscopy was also applied to investigate the capture of cell-penetrating TAT peptide-modified liposomes by various cells and stability and intracellular trafficking of captured TAT-liposomes inside cells. It was also used to confirm the successful transfection of cells with TAT-liposomes bearing the plasmid encoding for the Green Fluorescent Protein (GFP).
机译:荧光显微镜可以提供有关纳米颗粒药物载体(如脂质体和胶束)与靶细胞及其细胞内命运之间相互作用的重要信息。当前论文描述了荧光显微镜的各种应用,以研究抗体修饰的药物载体对癌细胞的特异性靶向。与游离药物或载药的非靶向胶束相比,荧光显微镜证实,增强的抗体介导的载药免疫胶束的靶向作用导致癌细胞杀伤力的增强。荧光显微镜还用于证明适当组装的聚合物胶束(基于聚乙二醇-磷脂酰乙醇胺共轭物,PEG-PE)的内体逸出,该胶束含有各种破坏内体膜的添加剂。当装载抗癌药(紫杉醇或维生素K3)时,此类胶束表现出增加的细胞毒性。荧光显微镜还用于研究各种细胞对细胞穿透TAT肽修饰的脂质体的捕获以及细胞内捕获的TAT脂质体的稳定性和细胞内运输。它也被用于确认带有编码绿色荧光蛋白(GFP)质粒的TAT-脂质体成功转染细胞。

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