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Magnetically triggered drug release from nanoparticles and its applications in anti-tumor treatment

机译:纳米颗粒磁触发药物释放及其在抗肿瘤治疗中的应用

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摘要

The objective of this study was to describe the magnetic nanoparticle–drug conjugates for improved control of drug delivery and drug release. The widely used anticancer agent Doxorubicin (DOX) was successfully conjugated via amine groups to the carboxylic functional groups coating magnetic nanoparticles (fluidMAG-CMX). Following purification of the nanoparticles, the conjugation of DOX on fluidMAG-CMX was confirmed using FTIR spectroscopy and confocal microscopy. The observed drug loading capacity of DOX was 22.3%. Studies of magnetically triggered release were performed under an oscillating magnetic field (OMF). DOX exhibited a significant release percentage of 70% under an OMF, as compared with the release in enzyme. A magnetic field turn-on and turn-off experiment was also conducted to confirm the control of drug release using this triggered system. In vivo experiments indicated that the tumor-inhibitory rate of CMX–DOX NPs under a magnetic field was higher than the other control groups. According to the toxicity assessments, CMX–DOX NPs were not noticeably toxic to mice at our tested dose.
机译:本研究的目的是描述磁性纳米颗粒 - 药物缀合物,用于改善药物递送和药物释放的控制。广泛使用的抗癌剂Doxorubicin(DOX)通过胺基成功缀合到羧基官能团涂覆磁性纳米颗粒(Flualmag-CMX)。在纳米颗粒纯化后,使用FTIR光谱和共聚焦显微镜确认DOX对流体-CMX的缀合。观察到的DOX的药物负载能力为22.3%。在振荡磁场(OMF)下进行磁触发释放的研究。与酶释放相比,DOX在OMF下显示出70%的显着释放百分比。还进行了磁场开启和关闭实验,以确认使用该触发系统对药物释放的控制。体内实验表明,磁场下CMX-DOX NP的肿瘤抑制率高于其他对照组。根据毒性评估,在我们测试剂量的小鼠中,CMX-DOX NPS对小鼠没有明显毒性。

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