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首页> 外文期刊>RSC Advances >Transferrin-conjugated drug/dye-co-encapsulated magnetic nanocarriers for active-targeting fluorescent/magnetic resonance imaging and anti-tumor effects in human brain tumor cells
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Transferrin-conjugated drug/dye-co-encapsulated magnetic nanocarriers for active-targeting fluorescent/magnetic resonance imaging and anti-tumor effects in human brain tumor cells

机译:转铁蛋白偶联的药物/染料共包裹的磁性纳米载体,用于人脑肿瘤细胞中的主动靶向荧光/磁共振成像和抗肿瘤作用

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A combinatorial nanosystem with the advantages of superparamagnetic iron oxide nanoparticles (SPIO NPs) and targeting polymer carriers is expected to improve the therapeutic effects in developing multifunctional delivery systems. Here we developed an innovative tumor-specific multi-functional SPIO NPs nanoplatform containing the antitumor drug doxorubicin (DOX) and fluorescent dye rhodamine B isothiocyanate (RBITC) for theranostic analysis and anti-tumor therapy in human brain tumor U251 MG cells. The core nanocarrier SPIO NPs (gamma-Fe2O3) were synthesized and decorated with chitosan (CS), subsequently followed with conjugation with tumor-specific ligand transferrin (Tf) to fabricate tumor-targeted Tf-CS/SPIO NPs. The anti-tumor drug DOX was then loaded onto Tf-CS/SPIO NPs, and transferred into U251 MG cells for assaying their biological effects. Besides, the produced Tf-CS/SPIO NPs were fluorescently labeled with RBITC for simultaneously intracellular fluorescent/magnetic resonance imaging in targeted U251 MG cells. The results showed that the fabricated Tf-CS/SPIO NPs nanocarriers demonstrated some favorable properties, including immediate responses under magnetic fields, stable behavior in different media, efficient encapsulation for drug loading, undetectable cytotoxicity, and effective intracellular visualization. Moreover, the fluorescent Tf-CS/SPIO NPs could be successfully applied for concurrent fluorescent/magnetic resonance imaging, and the finalized drug-loading Tf-CS/SPIO NPs displayed an improved cellular uptake, and thus effectively killed tumor cells through inducing a concurrence of cell apoptosis and autophagy in the treated tumor U251 cells. Therefore, the fabricated Tf-CS/SPIO NPs should be of great significance in developing multi-purpose nanocarriers for anti-tumor drug delivery and fluorescent/magnetic resonance imaging in human brain tumor treatments.
机译:具有超顺磁性氧化铁纳米颗粒(SPIO NPs)和靶向聚合物载体优势的组合纳米系统有望改善开发多功能递送系统的治疗效果。在这里,我们开发了一种创新的肿瘤特异性多功能SPIO NPs纳米平台,该平台包含抗肿瘤药阿霉素(DOX)和荧光染料若丹明B异硫氰酸盐(RBITC),用于人脑肿瘤U251 MG细胞的组织学分析和抗肿瘤治疗。合成了核心纳米载体SPIO NP(γ-Fe2O3),并用壳聚糖(CS)修饰,随后与肿瘤特异性配体转铁蛋白(Tf)结合,制备了靶向肿瘤的Tf-CS / SPIO NP。然后将抗肿瘤药物DOX加载到Tf-CS / SPIO NP上,并转移到U251 MG细胞中以分析其生物学效应。此外,用RBITC对产生的Tf-CS / SPIO NP进行荧光标记,以同时在靶向的U251 MG细胞中进行细胞内荧光/磁共振成像。结果表明,所制备的Tf-CS / SPIO NPs纳米载体表现出一些良好的性能,包括在磁场下的即时响应,在不同介质中的稳定行为,有效的载药封装,不可检测的细胞毒性以及有效的细胞内可视化。此外,荧光Tf-CS / SPIO NPs可成功用于同步荧光/磁共振成像,最终的载药Tf-CS / SPIO NPs显示出改善的细胞摄取,并因此通过诱导并发而有效杀死肿瘤细胞。处理的肿瘤U251细胞中细胞凋亡和自噬的作用因此,制备的Tf-CS / SPIO NPs在开发用于人类脑肿瘤治疗中的抗肿瘤药物递送和荧光/磁共振成像的多功能纳米载体方面将具有重要意义。

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