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Overcoming Chemoresistance in Cancer via Combined MicroRNA Therapeutics with Anticancer Drugs Using Multifunctional Magnetic Core-Shell Nanoparticles

机译:通过使用多功能磁芯 - 壳纳米粒子将Microrna治疗剂克服MicroRNA治疗剂克服癌症中的化学抑制剂

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In this study, we report the use of a multifunctional magnetic core shell nanoparticle (MCNP), composed of a highly magnetic zinc-doped iron oxide (ZnFe2O4) core nanoparticle and a biocompatible mesoporous silica (mSi) shell, for the simultaneous delivery of let-7a microRNA (miRNA) and anticancer drugs (e.g., doxorubicin) to overcome chemoresistance in breast cancer. Owing to the ability of let-7a to repress DNA repair mechanisms (e.g., BRCA1 and BRCA2) and downregulate drug efflux pumps (e.g., ABCG2), delivery of let-7a could sensitize chemoresistant breast cancer cells (MDA-MB-231) to subsequent doxorubicin chemotherapy both in vitro and in vivo. Moreover, the multifunctionality of our MCNPs allows for the monitoring of in vivo delivery via magnetic resonance imaging. In short, we have developed a multifunctional MCNP-based therapeutic approach to provide an attractive method with which to enhance our ability not only to deliver combined miRNA therapeutics with small-molecule drugs in both selective and effective manner but also to sensitize cancer cells for the enhanced treatment via the combination of miRNA replacement therapy using a single nanoplatform.
机译:在本研究中,我们报告了使用多官能磁芯壳纳米粒子(MCNP),由高磁性锌掺杂的氧化铁(ZnFe2O4)核纳米颗粒和生物相容性介孔二氧化硅(MSI)壳组成,用于同时递送让-7a microRNA(miRNA)和抗癌药物(例如,多柔比星)克服乳腺癌中的化学化。由于Let-7a抑制DNA修复机制(例如,BRCA1和BRCA2)和下调药物流出泵(例如,ABCG2),Let-7a的递送可以敏化化学抑制乳腺癌细胞(MDA-MB-231)随后的多柔比星化疗在体外和体内。此外,我们的MCNP的多功能性允许通过磁共振成像监测体内输送。简而言之,我们开发了一种基于多功能MCNP的治疗方法,提供了一种吸引力的方法,可以提高我们的能力,不仅可以在选择性和有效的方式中以小分子药物与小分子药物递送组合的miRNA治疗方法,而且还要敏感癌细胞通过使用单个纳米纳米甲型形成的MiRNA替代疗法的组合增强治疗。

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