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Preparation and biological characterization of hollow magnetic Fe_3O_4@C nanoparticles as drug carriers with high drug loading capability, pH-control drug release and MRI properties

机译:中空磁性Fe_3O_4 @ C纳米粒子作为载药能力强,pH控制药物释放和MRI特性的药物载体的制备和生物学表征

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Fe_3O_4@C nanocapsules were synthesized via a sacrificial-template method by coating SiO_2 nanospheres with an Fe_3O_4@C double-shell structure, followed by dissolving SiO_2 nanospheres through ammonia water under hydrothermal conditions. The nanocapsules show a loading capacity as high as 1300 mg g~(-1) for doxorubicin (DOX), and the DOX loaded on the surface of the carbon shells displays pH-sensitive release behavior. Drug release experiments were carried out at pH 7.4, 6.2 and 5.0. It was found that the drug release rate at pH 6.2 was about two times as fast as that at pH 7.4, and even faster at pH 5.0. A MTT assay was used to test the cytotoxicity of the DOX, nanocapsules and DOX-nanocapsules, which indicated the low cytotoxicity of the nanocapsules towards cells. The DOX-nanocapsules can be taken up by cancer cells through endocytosis, releasing DOX into the cytoplasm, which was observed by both transmission electron microscopy and confocal microscopy. In vitro magnetic resonance imaging (MRI) experiments validated the potential use of these nanocapsules as MRI contrast agents.
机译:通过牺牲模板法,用Fe_3O_4 @ C双壳结构包覆SiO_2纳米球,然后在水热条件下通过氨水溶解SiO_2纳米球,通过牺牲模板法合成了Fe_3O_4 @ C纳米胶囊。纳米胶囊对阿霉素(DOX)的负载能力高达1300 mg g(-1),而负载在碳壳表面的DOX表现出pH敏感的释放行为。在pH 7.4、6.2和5.0下进行药物释放实验。发现在pH 6.2时的药物释放速率约为在pH 7.4时的两倍,在pH 5.0时甚至更快。使用MTT测定法测试DOX,纳米胶囊和DOX-纳米胶囊的细胞毒性,这表明纳米胶囊对细胞的低细胞毒性。癌细胞可以通过内吞作用吸收DOX纳米颗粒,将DOX释放到细胞质中,这在透射电子显微镜和共聚焦显微镜下都可以观察到。体外磁共振成像(MRI)实验验证了这些纳米胶囊作为MRI造影剂的潜在用途。

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