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载姜黄素和多柔比星的抗 GLUT1 抗体靶向聚合物胶束的抗癌活性。

Anti-cancer activity of anti-GLUT1 antibody-targeted polymeric micelles co-loaded with curcumin and doxorubicin.

机构信息

Department of Pharmaceutical Sciences, Center for Pharmaceutical Biotechnology and Nanomedicine, Northeastern University , Boston, MA , USA and.

出版信息

J Drug Target. 2013 Dec;21(10):994-1000. doi: 10.3109/1061186X.2013.840639. Epub 2013 Oct 7.

DOI:10.3109/1061186X.2013.840639
PMID:24098980
Abstract

BACKGROUND

Treatment of late stage cancers has proven to be a very difficult task. Targeted therapy and combinatory drug administration may be the solution.

PURPOSE

The study was performed to evaluate the therapeutic efficacy of PEG-PE micelles, co-loaded with curcumin (CUR) and doxorubicin (DOX), and targeted with anti-GLUT1 antibody (GLUT1) against HCT-116 human colorectal adenocarcinoma cells both in vitro and in vivo.

METHODS

HCT-116 cells were treated with non-targeted and GLUT1-targeted CUR and DOX micelles as a single agent or in combination. Cells were inoculated in female nude mice. Established tumors were treated with the micellar formulations at a dose of 4 mg/kg CUR and 0.4 mg/kg DOX every 2 d for a total of 7 injections.

RESULTS

CUR + DOX-loaded micelles decorated with GLUT1 had a robust killing effect even at low doses of DOX in vitro. At the doses chosen, non-targeted CUR and CUR + DOX micelles did not exhibit any significant tumor inhibition versus control. However, GLUT1-CUR and GLUT1-CUR + DOX micelles showed a significant tumor inhibition effect with an improvement in survival.

CONCLUSION

We showed a dramatic improvement in efficacy between the non-targeted and GLUT1-targeted formulations both in vitro and in vivo. Hence, we confirmed that GLUT1-CUR + DOX micelles are effective and deserve further investigation.

摘要

背景

晚期癌症的治疗已被证明是一项非常艰巨的任务。靶向治疗和联合药物给药可能是解决问题的方法。

目的

本研究旨在评估共载姜黄素(CUR)和阿霉素(DOX)的聚乙二醇-聚醚嵌段共聚物胶束(PEG-PE micelles)联合抗 GLUT1 抗体(GLUT1)靶向治疗对 HCT-116 人结直肠腺癌细胞的体内外治疗效果。

方法

用非靶向和 GLUT1 靶向 CUR 和 DOX 胶束单独或联合处理 HCT-116 细胞。将细胞接种于雌性裸鼠。用胶束制剂以 4 mg/kg CUR 和 0.4 mg/kg DOX 的剂量治疗,每 2 天一次,共 7 次,建立肿瘤。

结果

即使在低剂量 DOX 下,GLUT1 修饰的 CUR + DOX 载药胶束在体外也具有很强的杀伤作用。在所选择的剂量下,非靶向 CUR 和 CUR + DOX 胶束与对照组相比没有表现出任何显著的肿瘤抑制作用。然而,GLUT1-CUR 和 GLUT1-CUR + DOX 胶束表现出显著的肿瘤抑制作用,并提高了存活率。

结论

我们在体外和体内均证实了非靶向和 GLUT1 靶向制剂之间疗效的显著改善。因此,我们证实 GLUT1-CUR + DOX 胶束是有效的,值得进一步研究。

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