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Magnetite nanoparticles as smart carriers to manipulate the cytotoxicity of anticancer drugs: Magnetic control and pH-responsive release

机译:磁铁矿纳米颗粒作为控制抗癌药物细胞毒性的智能载体:磁控制和pH响应释放

摘要

We described the smart and targeted magnetic nanocarriers to control the delivery and release of anticancer drug doxorubicin (DOX) in vitro and demonstrated that they can exhibit much higher cytotoxicity to cancer cells than free DOX. The conjugation of targeted magnetite nanoparticles (鈭?4 nm in diameter) and DOX molecule via acid-labile imine bond endows the nanocarriers with three advanced features: magnetically controllable, specific targeting, and pH-responsive. The cell toxicity assays indicated the pH-sensitive magnetic nanocarriers (IC50 of 0.13 渭g mL-1 to HeLa cells) have much higher anticancer activity than free DOX (IC50 of 1.16 渭g mL-1 to HeLa cells). Moreover, the magnetically guided delivery of nanocarriers can further improve the drug efficacy (IC50 of 鈭?.087 渭g mL-1 to HeLa cells). The arginine-glycine-aspartic acid (RGD)-modified magnetic nanocarriers recognized the specific cells effectively (IC50 of 0.93 渭g mL-1 to U-87 MG cells) and showed the increased cytotoxicity to cancer cells under external magnetic fields. This intelligent (magnetically guided, molecular targeted, and pH-responsive) drug delivery system has the ability to improve the chemotherapeutic efficacy and reduce the side effects, which has a great potential to become a favorable strategy for delivery of drugs to the desired sites in patients. 漏 2012 The Royal Society of Chemistry.
机译:我们描述了智能和有针对性的磁性纳米载体,以在体外控制抗癌药阿霉素(DOX)的传递和释放,并证明了它们比游离DOX对癌细胞具有更高的细胞毒性。通过酸不稳定的亚胺键结合靶向的磁铁矿纳米颗粒(直径约4 nm)和DOX分子,使纳米载体具有三个先进的特性:可磁控制,特异性靶向和pH响应。细胞毒性试验表明,pH敏感的磁性纳米载体(对HeLa细胞的IC50为0.13μgmL-1)比游离DOX(对HeLa细胞的IC50为1.16μgmL-1)具有更高的抗癌活性。此外,纳米载体的磁性引导递送可以进一步改善药物功效(对HeLa细胞的IC 50为0.087μgmL-1)。精氨酸-甘氨酸-天冬氨酸(RGD)修饰的磁性纳米载体可有效识别特异性细胞(对U-87 MG细胞的IC50为0.93μgmL-1),并在外部磁场下显示出对癌细胞的增强的细胞毒性。这种智能的(磁性引导,分子靶向和pH响应)药物递送系统具有提高化学治疗功效和减少副作用的能力,这具有很大的潜力,成为将药物递送到体内所需部位的有利策略。耐心。漏2012年,英国皇家化学会。

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