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首页> 外文期刊>Nanomedicine >iRGD-conjugated DSPE-PEG2000 nanomicelles for targeted delivery of salinomycin for treatment of both liver cancer cells and cancer stem cells
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iRGD-conjugated DSPE-PEG2000 nanomicelles for targeted delivery of salinomycin for treatment of both liver cancer cells and cancer stem cells

机译:iRGD缀合的DSPE-PEG2000纳米胶束用于靶向递送沙利霉素,以治疗肝癌细胞和癌症干细胞

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Aims: To develop novel iRGD (internalizing Arg-Gly-Asp peptide)-conjugated DSPE-PEG2000 nanomicelles (M-SAL-iRGD) for delivery of salinomycin to both liver cancer cells and cancer stem cells (CSCs). Materials & methods: The characterization, antitumor activity and mechanism of action of M-SAL-iRGD were evaluated. Results & conclusion: M-SAL-iRGD possessed a small size of around 10 nm, and drug encapsulation efficacy higher than 90%. M-SAL-iRGD showed significantly increased cytotoxic effect toward both nontargeted M-SAL (salinomycin-loaded DSPE-PEG2000 nanomicelles) and salinomycin in both liver cancer cells and CSCs. The tissue distribution and antitumor assays in mice bearing liver cancer xenograft confirmed the superior penetration tumor efficacy and antitumor activity of M-SAL-iRGD. M-SAL-iRGD represent a potential effective nanomedicine against liver cancer.
机译:目的:开发新型iRGD(内化Arg-Gly-Asp肽)缀合的DSPE-PEG2000纳米胶束(M-SAL-iRGD),用于将沙利霉素递送至肝癌细胞和癌干细胞(CSC)。材料与方法:评价了M-SAL-iRGD的​​表征,抗肿瘤活性和作用机理。结果与结论:M-SAL-iRGD具有约10 nm的小尺寸,药物包封率高于90%。 M-SAL-iRGD对肝癌细胞和CSC中的非靶向M-SAL(载有盐霉素的DSPE-PEG2000纳米胶束)和盐霉素均具有明显的细胞毒性作用。携带肝癌异种移植物的小鼠的组织分布和抗肿瘤分析证实了M-SAL-iRGD具有优异的穿透肿瘤功效和抗肿瘤活性。 M-SAL-iRGD代表一种潜在的有效的抗肝癌纳米药物。

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