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首页> 外文期刊>International Journal of Nanomedicine >Doxorubicin-loaded cell-derived nanovesicles: an alternative targeted approach for anti-tumor therapy
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Doxorubicin-loaded cell-derived nanovesicles: an alternative targeted approach for anti-tumor therapy

机译:载有阿霉素的细胞衍生的纳米囊泡:抗肿瘤治疗的另一种靶向方法

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Cell-derived nanovesicles (CDNs) are an emerging class of biological drug delivery systems (DDS) that retain the characteristics of the cells they were derived from, without the need for further surface functionalization. CDNs are also biocompatible, being derived from natural sources and also take advantage of the enhanced permeability and retention effect due to their nanodimensions. Furthermore, CDNs derived from monocytes were shown to have an in vivo targeting effect, accumulating at the tumor site in a previous study conducted in a mouse tumor model. Here, we report a systematic approach pertaining to various loading methods of the chemotherapeutic drug doxorubicin into our CDNs and examine the differential cellular uptake of drug-loaded CDNs in cancerous (HeLa) and healthy (HEK293) cell lines. Lastly, we proved that the addition of doxorubicin-loaded CDNs to the HeLa and HEK293 co-cultures showed a clear discrimination toward cancer cells at the cellular level. Our results further reinforce the intriguing potential of CDNs as an alternative targeted strategy for anticancer therapy.
机译:细胞衍生的纳米囊泡(CDN)是一类新兴的生物药物传递系统(DDS),可保留其来源细胞的特性,而无需进一步的表面功能化。 CDN也具有生物相容性,来源于自然资源,并且由于其纳米尺寸而还具有增强的渗透性和保留效果。此外,在先前在小鼠肿瘤模型中进行的研究中,显示单核细胞来源的CDN具有体内靶向作用,在肿瘤部位蓄积。在这里,我们报告了一种系统化的方法,该方法涉及将化疗药物阿霉素加载到我们的CDN中的各种方法,并检查了癌细胞(HeLa)和健康(HEK293)细胞系中药物加载CDN的不同细胞摄取。最后,我们证明了向HeLa和HEK293共培养物中添加阿霉素的CDNs在细胞水平上显示出对癌细胞的明显区分。我们的结果进一步增强了CDN作为抗癌治疗的替代靶向策略的潜在潜力。

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