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Enhanced gene delivery using Bubble liposomes and ultrasound for folate-PEG liposomes

机译:叶酸-PEG脂质体使用Bubble脂质体和超声增强基因传递

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We have previously reported that the transfection efficiency of laminin-derived AG73-peptide labeled polyethyleneglycol-modified liposomes (AG73-PEG liposomes) was enhanced by echo-contrast gas entrapping PEG liposomes (Bubble liposomes, BLs) and ultrasound (US) exposure by improving endosomal escape. However, it has not been well understood whether BLs and US exposure can enhance the transfection efficiency of other carriers except AG73-PEG liposomes. In this study, to evaluate whether BLs and US exposure can be generally applied to gene delivery carriers, we focused on folate as a model ligand and examined whether BLs and US exposure could enhance the transfection efficiency of folate-PEG liposomes. Folate-PEG liposomes could internalize into cells efficiently, whereas they could not deliver genes into cytosol from endosomes sufficiently. BLs and US exposure could enhance the transfection efficiency of folate-PEG liposomes compared with folate-PEG liposomes alone without their direct induction into cells. These results suggested that BLs and US exposure could enhance the transfection efficiency of folate-PEG liposomes in the same manner as AG73-PEG liposomes. Thus, BLs and US exposure may be a promising tool to achieve efficient gene transfection into various gene carriers in general.
机译:我们以前曾报道过,回声造影剂截留PEG脂质体(气泡脂质体,BLs)和超声(US)暴露可以改善层粘连蛋白衍生的AG73肽标记的聚乙二醇修饰的脂质体(AG73-PEG脂质体)的转染效率。内体逃逸。但是,尚不清楚BL和US暴露是否可以增强AG73-PEG脂质体以外的其他载体的转染效率。在这项研究中,为了评估BLs和US暴露是否可以普遍应用于基因传递载体,我们集中研究叶酸作为模型配体,并研究了BLs和US暴露是否可以提高叶酸-PEG脂质体的转染效率。叶酸-PEG脂质体可以有效地内化到细胞中,但是它们不能充分地将基因从内体传递到胞质溶胶中。与单独的叶酸-PEG脂质体相比,BLs和US暴露可提高叶酸-PEG脂质体的转染效率,而无需直接诱导它们进入细胞。这些结果表明BLs和US暴露可以以与AG73-PEG脂质体相同的方式提高叶酸-PEG脂质体的转染效率。因此,一般而言,BL和US暴露可能是实现有效基因转染到各种基因载体中的有前途的工具。

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