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首页> 外文期刊>World Journal of Gastroenterology >High-density lipoprotein as a potential carrier for delivery of a lipophilic antitumoral drug into hepatoma cells.
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High-density lipoprotein as a potential carrier for delivery of a lipophilic antitumoral drug into hepatoma cells.

机译:高密度脂蛋白作为潜在的载体,可将亲脂性抗肿瘤药物传递到肝癌细胞中。

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AIM: To investigate the possibility of recombinant high-density lipoprotein (rHDL) being a carrier for delivering antitumoral drug to hepatoma cells. METHODS: Recombinant complex of HDL and aclacinomycin (rHDL-ACM) was prepared by cosonication of apoproteins from HDL (Apo HDL) and ACM as well as phosphatidylcholine. Characteristics of the rHDL-ACM were elucidated by electrophoretic mobility, including the size of particles, morphology and entrapment efficiency. Binding activity of rHDL-ACM to human hepatoma cells was determined by competition assay in the presence of excess native HDL. The cytotoxicity of rHDL-ACM was assessed by MTT method. RESULTS: The density range of rHDL-ACM was 1.063-1.210 g/mL, and the same as that of native HDL. The purity of all rHDL-ACM preparations was more than 92%. Encapsulated efficiencies of rHDL-ACM were more than 90%. rHDL-ACM particles were typical sphere model of lipoproteins and heterogeneous in particle size. The average diameter was 31.26+/-5.62 nm by measure of 110 rHDL-ACM particles in the range of diameter of lipoproteins. rHDL-ACM could bind on SMMC-7721 cells, and such binding could be competed against in the presence of excess native HDL. rHDL-ACM had same binding capacity as native HDL. The cellular uptake of rHDL-ACM by SMMC-7721 hepatoma cells was significantly higher than that of free ACM at the concentration range of 0.5-10 microg/mL (P<0.01). Cytotoxicity of rHDL-ACM to SMMC-7721 cells was significantly higher than that of free ACM at concentration range of less than 5 microg/mL (P<0.01) and IC50 of rHDL-ACM was lower than IC50 of free ACM (1.68 nmol/L vs 3 nmol/L). Compared to L02 hepatocytes, a normal liver cell line, the cellular uptake of rHDL-ACM by SMMC-7721 cells was significantly higher (P<0.01) and in a dose-dependent manner at the concentration range of 0.5-10 microg/mL. Cytotoxicity of the rHDL-ACM to SMMC-7721 cells was significantly higher than that to L02 cells at concentration range of 1-7.5 microg/mL (P<0.01). IC50 for SMMC-7721 cells (1.68 nmol/L) was lower than that for L02 cells (5.68 nmol/L), showing a preferential cytotoxicity of rHDL-ACM for SMMC-7721 cells. CONCLUSION: rHDL-ACM complex keeps the basic physical and biological binding properties of native HDL and shows a preferential cytotoxicity for SMMC-7721 hepatoma to normal L02 hepatocytes. HDL is a potential carrier for delivering lipophilic antitumoral drug to hepatoma cells.
机译:目的:探讨重组高密度脂蛋白(rHDL)作为向肝癌细胞传递抗肿瘤药物的载体的可能性。方法:通过超声处理高密度脂蛋白(Apo HDL)和ACM以及磷脂酰胆碱中载脂蛋白,制备高密度脂蛋白和阿克拉霉素(rHDL-ACM)重组复合物。通过电泳迁移率阐明了rHDL-ACM的特征,包括颗粒大小,形态和包封效率。在过量天然HDL存在下,通过竞争测定法测定rHDL-ACM与人肝癌细胞的结合活性。通过MTT法评估rHDL-ACM的细胞毒性。结果:rHDL-ACM的密度范围为1.063-1.210 g / mL,与天然HDL相同。所有rHDL-ACM制剂的纯度均超过92%。 rHDL-ACM的封装效率超过90%。 rHDL-ACM颗粒是脂蛋白的典型球形模型,粒径不均一。通过测量脂蛋白直径范围内的110个rHDL-ACM颗粒,平均直径为31.26 +/- 5.62 nm。 rHDL-ACM可以结合SMMC-7721细胞,并且在存在过量的天然HDL的情况下,这种结合可以竞争。 rHDL-ACM具有与天然HDL相同的结合能力。在0.5-10μg/ mL的浓度范围内,SMMC-7721肝癌细胞对rHDL-ACM的细胞摄取显着高于对游离ACM的摄取(P <0.01)。在浓度范围小于5 microg / mL时,rHDL-ACM对SMMC-7721细胞的细胞毒性显着高于游离ACM(P <0.01),rHDL-ACM的IC50低于游离ACM的IC50(1.68nmol / ml)。 L vs 3 nmol / L)。与正常肝细胞系L02肝细胞相比,SMMC-7721细胞对rHDL-ACM的细胞摄取显着更高(P <0.01),并且在0.5-10 microg / mL的浓度范围内呈剂量依赖性。在1-7.5 microg / mL的浓度范围内,rHDL-ACM对SMMC-7721细胞的细胞毒性显着高于对L02细胞的细胞毒性(P <0.01)。 SMMC-7721细胞(1.68 nmol / L)的IC50低于L02细胞(5.68 nmol / L),显示rHDL-ACM对SMMC-7721细胞具有优先的细胞毒性。结论:rHDL-ACM复合物保留了天然HDL的基本物理和生物学结合特性,并显示SMMC-7721肝癌对正常L02肝细胞具有优先的细胞毒性。 HDL是将亲脂性抗肿瘤药物传递给肝癌细胞的潜在载体。

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