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用于脂质体的新型半乳糖基化聚乙二醇 - 胆固醇作为肝细胞靶向药物载体

Novel Galactosylated Poly(ethylene glycol)-Cholesterol for Liposomes as a Drug Carrier for Hepatocyte-Targeting.

作者信息

Zhang Huafang, Xiao Yan, Cui Shengmiao, Zhou Yuefang, Zeng Ke, Yan Mina, Zhao Chunshun

出版信息

J Nanosci Nanotechnol. 2015 Jun;15(6):4058-69. doi: 10.1166/jnn.2015.9707.

Abstract

In this study, three types of galactosylated cholesterol (i.e., gal-PEG194-chol, gal-PEG1000-chol and gal-PEG2000-chol) were synthesized with one terminal of polyethylene glycol of various chain lengths conjugated to the galactoside moiety, and the other terminal conjugated to the cholesterol. The galactose-modified liposomes were prepared by thin film-hydration method and doxorubicin (DOX) was loaded to the liposomes by using a ammonium sulfate gradient procedure. The liposomal formulations with galactosylated cholesterol were characterized. Flow cytometry and laser confocal scanning microscopy analyses showed that the galactose-modified liposomes facilitated the intracellular uptake of liposomes into HepG2 via asialoglycoprotein receptor (ASGP-R) mediated endocytosis. Cytotoxicity assay showed that the cell proliferation inhibition effect of galactose-modified liposomes was higher than that of the unmodified liposomes. Additionally, the study on frozen section of liver showed that the galactose-modified liposomes enhanced the intracellular uptake of liposomes into hepatocytes. Taken together, these results suggested that liposomes containing such galactosylated cholesterol (i.e., gal-PEG-chol), had a great potential as drug delivery carriers for hepatocyte-selective targeting.

摘要

在本研究中,合成了三种类型的半乳糖基化胆固醇(即gal-PEG194-chol、gal-PEG1000-chol和gal-PEG2000-chol),其中不同链长的聚乙二醇一端与半乳糖苷部分共轭,另一端与胆固醇共轭。通过薄膜水化法制备半乳糖修饰的脂质体,并采用硫酸铵梯度法将阿霉素(DOX)载入脂质体。对含半乳糖基化胆固醇的脂质体制剂进行了表征。流式细胞术和激光共聚焦扫描显微镜分析表明,半乳糖修饰的脂质体通过去唾液酸糖蛋白受体(ASGP-R)介导的内吞作用促进了脂质体对HepG2细胞的摄取。细胞毒性试验表明,半乳糖修饰的脂质体对细胞增殖的抑制作用高于未修饰的脂质体。此外,肝脏冰冻切片研究表明,半乳糖修饰的脂质体增强了脂质体对肝细胞的摄取。综上所述,这些结果表明,含有此类半乳糖基化胆固醇(即gal-PEG-chol)的脂质体作为肝细胞选择性靶向的药物递送载体具有巨大潜力。

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