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Core-shell structured Fe3O4@TiO2-doxorubicin nanoparticles for targeted chemo-sonodynamic therapy of cancer

机译:核心壳结构Fe3O4 @ TiO2-Doxorubicin纳米粒子用于靶向化疗的癌症

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摘要

To facilitate targeting drug delivery and combined therapy, we develop titanium dioxide-encapsulated Fe3O4 nanoparticles (Fe3O4@TiO2 NPs). Titanium dioxide (TiO2), which is employed as a sonosensitizer for sonodynamic therapy (SDT), can also be used for the loading of doxorubicin (DOX). The fabricated Fe3O4@TiO2 NPs exhibit pH-dependent loading and release of doxorubicin (DOX) in vitro. After incubation with cancer cells, reactive oxygen species (ROS) are generated efficiently upon the irradiation of ultrasound. In the biodistribution experiments, extremely high in vivo tumor accumulation of Fe3O4@TiO2 NPs and long-time retention effect are observed. Compared with chemotherapy or sonodynamic treatment alone, the combined therapy demonstrated a synergistic effect, resulting in stronger cytotoxicity and higher therapeutic efficacy. Thus, the constructed NPs are endowed with multifunctions which allow them to selectively deliver combinatorial therapeutic payload to tumor with enhanced therapeutic effectiveness and minimal side effects. (C) 2015 Elsevier B.V. All rights reserved.
机译:为了促进靶向药物递送和组合治疗,我们开发二氧化钛包封的Fe3O4纳米颗粒(Fe3O4 @ TiO2 NPS)。二氧化钛(TiO 2),其作为超声动力治疗(SDT)的超声溶胶剂,也可用于加载多柔比星(DOX)。制造的Fe3O4 @ TiO2 NPS在体外表现出pH依赖性加载和释放多柔比星(DOX)。与癌细胞孵育后,在超声波照射时有效地产生反应性氧物质(ROS)。在生物分布试验中,观察到Fe3O4 @ TiO2 NPS和长期保留效果的体内肿瘤积累。与单独的化疗或超声动力学治疗相比,联合疗法表现出一种协同效应,导致细胞毒性更强,治疗效果更高。因此,构造的NPS具有多隙,其允许它们选择性地将组合治疗性有效载荷与增强的治疗效果和最小副作用的肿瘤一起递送至肿瘤。 (c)2015 Elsevier B.v.保留所有权利。

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