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CRGD-functionalized polymeric magnetic nanoparticles as a dual-drug delivery system for safe targeted cancer therapy

机译:CRGD功能化的聚合物磁性纳米颗粒作为用于安全靶向癌症治疗的双重药物输送系统

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In this paper we give a method of integrated treatment for cancer and drug-induced complications in the process of cancer therapy through dual-drug delivery system (DDDS). Two hydrophilic drugs, doxorubicin (an antitumor drug) and verapamil (an antiangiocardiopathy drug) combined preliminarily with chitosan shell coated on magnetic nanoparticles (MNPs), followed by entrapping into the PLGA nanoparticles. Further modification was conducted by conjugating tumor-targeting ligand, cyclo(Arg-Gly-Asp-D-Phe-Lys) (c(RGDfK)) peptide, onto the end carboxyl groups on the PLGA-NPs. The size of the resulting cRGD-DOX/VER-MNP-PLGA NPs was approximately 144 nm under simulate physiological environment. Under present experiment condition, the entrapment efficiencies of DOX and VER were approximately 74.8 and 53.2 wt% for cRGD-DOX/VER-MNP-PLGA NPs. This paper contains interesting pilot data such as NIR-triggered drug release, in vivo drug distribution studies and whole-mouse optical imaging. Histopathological examinations and electrocardiogram comparison demonstrated that the intelligent DDDS could markedly inhibit the growth of tumor and potentially offer an approach for safe cancer therapy. ? 2013 Elsevier B.V. All rights reserved.
机译:在本文中,我们提供了一种通过双药递送系统(DDDS)对癌症和药物引起的并发症进行综合治疗的方法。先将两种亲水性药物阿霉素(一种抗肿瘤药)和维拉帕米(一种抗心血管病药)与包裹在磁性纳米颗粒(MNPs)上的壳聚糖壳结合,然后包埋到PLGA纳米颗粒中。通过将靶向肿瘤的配体环(Arg-Gly-Asp-D-Phe-Lys)(c(RGDfK))肽缀合到PLGA-NP的末端羧基上,进行了进一步修饰。在模拟生理环境下,生成的cRGD-DOX / VER-MNP-PLGA NP的大小约为144 nm。在目前的实验条件下,对于cRGD-DOX / VER-MNP-PLGA NPs,DOX和VER的包封率分别约为74.8和53.2 wt%。本文包含有趣的试验数据,例如NIR触发的药物释放,体内药物分布研究和全小鼠光学成像。组织病理学检查和心电图比较表明,智能DDDS可以显着抑制肿瘤的生长,并可能为安全的癌症治疗提供一种方法。 ? 2013 Elsevier B.V.保留所有权利。

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