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首页> 外文期刊>Scientific reports. >Epirubicin-loaded marine carrageenan oligosaccharide capped gold nanoparticle system for pH-triggered anticancer drug release
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Epirubicin-loaded marine carrageenan oligosaccharide capped gold nanoparticle system for pH-triggered anticancer drug release

机译:装载表柔比星的海洋角叉菜胶低聚糖加盖的金纳米颗粒系统用于pH触发的抗癌药物释放

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Gold nanoparticles (AuNPs) and the pH stimuli-responsive drug delivery system have been extensively applied in cancer treatment. Carrageenan derived from marine red algae shows a promising application prospect for drug delivery as a nanomaterial for its biodegradability, abundance, and non-toxicity. Carrageenan oligosaccharide (CAO) was used as a biocompatible reductant for green synthesis of CAO-AuNPs, and the obtained CAO-AuNPs were further used as a delivery system for pH-triggered delivery of epirubicin (EPI). The EPI-CAO-AuNPs were demonstrated to be spherical and homogeneous with mean diameter of 141?±?6?nm by means of electron microscopy and Malvern particle size analyzer. Results showed that the release of EPI from EPI-CAO-AuNPs was significant under acidic condition that simulated cancer environment, while it was negligible under physiological pH in vitro. Confocal laser scanning microscope and flow cytometry analysis showed that EPI-CAO-AuNPs were localized in cellular nucleus and induced more apoptosis of HCT-116 and HepG2 cells than free EPI. A new pH-triggered anticancer drug release was achieved by EPI-CAO-AuNPs system for the first time. The developed EPI-CAO-AuNPs nanosystem shows a promising prospect for pH-triggered delivery of antitumor drugs, and our work provides a new idea for targeted drug delivery by using biocompatible marine carbohydrates as nanomaterial.
机译:金纳米颗粒(AuNPs)和pH刺激响应药物传递系统已广泛应用于癌症治疗。来源于海洋红藻的角叉菜胶由于其生物可降解性,丰度和无毒性而作为纳米材料在药物递送方面显示出广阔的应用前景。角叉菜胶低聚糖(CAO)被用作绿色合成CAO-AuNPs的生物相容性还原剂,而获得的CAO-AuNPs进一步被用作pH触发的表柔比星(EPI)的传递系统。 EPI-CAO-AuNPs呈球形,均质,电子显微镜和Malvern粒度分析仪测得平均直径为141?±?6?nm。结果表明,在模拟癌症环境的酸性条件下,EPI-CAO-AuNPs的EPI释放显着,而在体外生理pH下则可忽略不计。共聚焦激光扫描显微镜和流式细胞仪分析表明,EPI-CAO-AuNPs定位在细胞核中,比游离EPI诱导更多的HCT-116和HepG2细胞凋亡。通过EPI-CAO-AuNPs系统首次实现了pH触发的新抗癌药物释放。已开发的EPI-CAO-AuNPs纳米系统显示了通过pH触发的抗肿瘤药物前景广阔的前景,并且我们的工作为使用生物相容性海洋碳水化合物作为纳米材料的靶向药物交付提供了新思路。

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