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首页> 外文期刊>ACS Omega >Redox-Responsive Dipeptide Nanostructures toward Targeted Cancer Therapy
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Redox-Responsive Dipeptide Nanostructures toward Targeted Cancer Therapy

机译:氧化还原响应二肽纳米结构朝向靶向癌症疗法

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Materials that exhibit responsiveness toward biological signals are currently subjected to intense research in the field of drug delivery. In our study, we tried to develop cancer-targeted and redox-responsive nanoparticles (NPs) from disulfide-linked oxidized cysteine-phenylalanine (CFO). The NPs were conjugated with folic acid (FA) to specifically target cancer cells, and the presence of disulfide bonds would enabled the disintegration of the particles in the presence of elevated levels of glutathione (GSH) in cancer cells. Anticancer drug doxorubicin (Dox) was successfully loaded inside the disulfide-linked nanoparticles (CFO-Dox-NPs), which further demonstrated stimuli-responsive drug release in the presence of GSH. We have also demonstrated enhanced uptake of FA-derivatized NPs (FA-CFO-NPs) in cancerous cells (C6 glioma and B16F10 melanoma cells) than in normal cells (HEK293T cells) due to the overexpression of FA receptors on the surface of cancer cells. Cytotoxicity studies in C6 cells and B16F10 cells further revealed enhanced efficacy of Dox loaded (FA-CFO-Dox-NPs) as compared to the native drug. The findings of this study clearly demonstrated that the disulfide-linked nanoparticle system may provide a promising selective drug delivery platform in cancer cells.
机译:表现出对生物信号响应性的材料目前在药物递送领域进行激烈的研究。在我们的研究中,我们试图从二硫化物连接的氧化半胱氨酸 - 苯丙氨酸(CFO)中形成癌症靶向和氧化还原响应纳米颗粒(NPS)。将NPS与叶酸(Fa)缀合至特异性靶癌细胞,并且二硫键的存在将使颗粒在癌细胞中含有谷胱甘肽(GSH)的升高水平存在下崩解。在二硫键连接的纳米粒子(CFO-DOX-NPS)内成功地装载了抗癌药物(DOX),其进一步证明了GSH存在下的刺激反应药物释放。我们还表明,由于癌细胞表面上的FA受体的过度表达,在癌细胞(C6胶质瘤和B16F10黑色素瘤细胞中)中,在癌细胞(C6胶质瘤和B16F10黑色素瘤细胞)中提高了对癌细胞(C6胶质瘤和B16F10细胞)的产生增强。与天然药物相比,C6细胞和B16F10细胞中的细胞毒性研究进一步揭示了DOX(FA-CFO-DOX-NPS)的增强效果。该研究的发现清楚地证明了二硫键连接的纳米颗粒系统可以在癌细胞中提供有希望的选择性药物递送平台。

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