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Magnetic Driven Nanocarriers for pH-Responsive Doxorubicin Release in Cancer Therapy

机译:磁性驱动纳米载体用于pH响应阿霉素在癌症治疗中的释放

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摘要

Doxorubicin is one of the most widely used anti-cancer drugs, but side effects and selectivity problems create a demand for alternative drug delivery systems. Herein we describe a hybrid magnetic nanomaterial as a pH-dependent doxorubicin release carrier. This nanocarrier comprises magnetic iron oxide cores with a diameter of 10 nm, enveloped in a hybrid material made of siliceous shells and ĸ-carrageenan. The hybrid shells possess high drug loading capacity and a favorable drug release profile, while the iron oxide cores allows easy manipulation via an external magnetic field. The pH responsiveness was assessed in phosphate buffers at pH levels equivalent to those of blood (pH 7.4) and tumor microenvironment (pH 4.2 and 5). The nanoparticles have a loading capacity of up to 12.3 wt.% and a release profile of 80% in 5 h at acidic pH versus 25% at blood pH. In vitro drug delivery tests on human breast cancer and non-cancer cellular cultures have shown that, compared to the free drug, the loaded nanocarriers have comparable antiproliferative effect but a less intense cytotoxic effect, especially in the non-cancer cell line. The results show a clear potential for these new hybrid nanomaterials as alternative drug carriers for doxorubicin.
机译:阿霉素是使用最广泛的抗癌药物之一,但是副作用和选择性问题引起了对替代药物递送系统的需求。在本文中,我们将杂化磁性纳米材料描述为pH依赖性阿霉素释放载体。该纳米载体包含直径为10 nm的磁性氧化铁核,包裹在由硅质壳和β-角叉菜胶制成的混合材料中。混合壳具有高载药量和良好的药物释放特性,而氧化铁核则允许通过外部磁场轻松操纵。在与血液(pH 7.4)和肿瘤微环境(pH 4.2和5)相等的pH值的磷酸盐缓冲液中评估pH响应度。纳米颗粒在酸性pH下5小时内具有高达12.3重量%的负载能力和80%的释放曲线,而在血液pH下具有25%的释放曲线。对人乳腺癌和非癌细胞培养物的体外药物递送试验表明,与游离药物相比,负载的纳米载体具有相当的抗增殖作用,但细胞毒性作用较弱,特别是在非癌细胞系中。结果表明,这些新型杂化纳米材料作为阿霉素的替代药物载体具有明显的潜力。

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