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Hypericin-bearing magnetic iron oxide nanoparticles for selective drug delivery in photodynamic therapy.

机译:含有金丝桃素的磁性氧化铁纳米粒子,用于光动力疗法中的选择性药物递送。

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摘要

© 2015 Unterweger et al.Combining the concept of magnetic drug targeting and photodynamic therapy is a promising approach for the treatment of cancer. A high selectivity as well as significant fewer side effects can be achieved by this method, since the therapeutic treatment only takes place in the area where accumulation of the particles by an external electromagnet and radiation by a laser system overlap. In this article, a novel hypericin-bearing drug delivery system has been developed by synthesis of superparamagnetic iron oxide nanoparticles (SPIONs) with a hypericin-linked functionalized dextran coating. For that, sterically stabilized dextran-coated SPIONs were produced by coprecipitation and crosslinking with epichlorohydrin to enhance stability. Carboxymethylation of the dextran shell provided a functionalized platform for linking hypericin via glutaraldehyde. Particle sizes obtained by dynamic light scattering were in a range of 55-85 nm, whereas investigation of single magnetite or maghemite particle diameter was performed by transmission electron microscopy and X-ray diffraction and resulted in approximately 4.5-5.0 nm. Surface chemistry of those particles was evaluated by Fourier transform infrared spectroscopy and ζ potential measurements, indicating successful functionalization and dispersal stabilization due to a mixture of steric and electrostatic repulsion. Flow cytometry revealed no toxicity of pure nanoparticles as well as hypericin without exposure to light on Jurkat T-cells, whereas the combination of hypericin, alone or loaded on particles, with light-induced cell death in a concentration and exposure time-dependent manner due to the generation of reactive oxygen species. In conclusion, the combination of SPIONs’ targeting abilities with hypericin’s phototoxic properties represents a promising approach for merging magnetic drug targeting with photodynamic therapy for the treatment of cancer.
机译:©2015 Unterweger等人,将磁性药物靶向和光动力疗法的概念相结合是一种有前途的癌症治疗方法。通过该方法可以实现高选择性以及显着较少的副作用,因为治疗仅在外部电磁体聚集的粒子和激光系统产生的辐射重叠的区域进行。在本文中,已经开发了一种新型的带有金丝桃素的药物递送系统,该系统通过与金丝桃素连接的功能化右旋糖酐涂层的超顺磁性氧化铁纳米粒子(SPIONs)合成。为此,通过共沉淀并与表氯醇交联以增强稳定性,制得了空间稳定的葡聚糖包被的SPION。葡聚糖壳的羧甲基化提供了通过戊二醛连接金丝桃素的功能化平台。通过动态光散射获得的粒径在55-85nm的范围内,而通过透射电子显微镜和X射线衍射进行的单个磁铁矿或磁赤铁矿粒径的研究结果为约4.5-5.0nm。通过傅立叶变换红外光谱和ζ电位测量评估了这些颗粒的表面化学性质,表明由于空间和静电排斥的混合,成功实现了功能化和分散稳定。流式细胞仪显示,未暴露于Jurkat T细胞的光下,纯纳米颗粒和金丝桃素没有毒性,而单独或装载在颗粒上的金丝桃素的组合则以浓度和曝光时间依赖的方式导致光诱导的细胞死亡产生活性氧。总之,将SPIONs的靶向能力与金丝桃素的光毒性相结合,代表了将磁性药物靶向与光动力疗法相结合以治疗癌症的一种有前途的方法。

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