首页> 外文期刊>International Journal of Pharmaceutics >Synergistic targeted delivery of payload into tumor cells by dual-ligand liposomes co-modified with cholesterol anchored transferrin and TAT
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Synergistic targeted delivery of payload into tumor cells by dual-ligand liposomes co-modified with cholesterol anchored transferrin and TAT

机译:通过与胆固醇锚定的转铁蛋白和TAT共同修饰的双配体脂质体将靶向负载协同有效地靶向肿瘤细胞

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摘要

This study was mainly focused on developing a dual-ligand liposomal delivery system to enhance both targeting specificity and cellular uptake. The specific ligand transferrin (TF) and the cationic cell-penetrating peptide TAT were connected with cholesterol via a polyethylene glycol (PEG) spacer to prepare the dualligand liposomes (TAT/TF-PEG-LP). Then the in vitro cellular uptake by three kinds of cells that possessed different expressing levels of transferrin receptor (TFR) and the in vivo delivery efficiency were evaluated. Compared to the single-ligand TAT or TF modified liposomes (TAT-PEG-LP or TF-PEG-LP), TAT/TF-PEG-LP exhibited the enhanced cellular uptake and selectivity via the synergistic effect of both ligands in vitro. The ex vivo fluorescence imaging of tumors, the qualitative observation of tumor frozen section and the quantitative determination of cellular uptake in tumor tissues altogether showed the in vivo delivery efficiency of TAT/TF-PEG-LP was higher than that of other liposomes. In conclusion, the dual-ligand liposomes co-modified with TF and TAT possessed a strong capability for synergistic targeted delivery of payload into tumor cells both in vitro and in vivo.
机译:这项研究主要集中在开发双配体脂质体递送系统,以增强靶向特异性和细胞摄取。特定的配体转铁蛋白(TF)和穿透阳离子细胞的肽TAT通过聚乙二醇(PEG)间隔子与胆固醇连接,以制备双配体脂质体(TAT / TF-PEG-LP)。然后评估了具有不同表达水平的转铁蛋白受体(TFR)的三种细胞的体外细胞摄取和体内递送效率。与单配体TAT或TF修饰的脂质体(TAT-PEG-LP或TF-PEG-LP)相比,TAT / TF-PEG-LP通过两种配体的体外协同作用表现出增强的细胞摄取和选择性。肿瘤的离体荧光成像,肿瘤冷冻切片的定性观察以及肿瘤组织中细胞摄取的定量测定表明,TAT / TF-PEG-LP的体内递送效率高于其他脂质体。总之,与TF和TAT共修饰的双配体脂质体具有强大的能力,可以在体内外协同有效地将有效载荷靶向递送至肿瘤细胞。

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