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Doxorubicin loaded silica nanorattles actively seek tumors with improved anti-tumor effects

机译:阿霉素加载硅nanorattles积极寻求与改善肿瘤的抗肿瘤效应

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摘要

Silica nanorattles (SNs) have proven to be promising vehicles for drug delivery. In order to further enhance efficacy and minimize adverse effects, active targeted delivery to tumors is necessary. In this work, SNs modified with a tumor specific targeting ligand, folic acid (FA), was used as carrier of doxorubicin (DOX) (DOX-FA-SNs). Drug loading, cytotoxicity and cellular uptake of DOX-FA-SNs in vitro in human cervical carcinoma cells (HeLa cells) were evaluated. DOX-FA-SNs showed a higher cytotoxicity in human cervical carcinoma cells (HeLa cells) than DOX loaded carboxyl (-COOH) and polyethylene glycol) (PEG) modified SNs (DOX-COOH-SNs and DOX-PEG-SNs, respectively). However, DOX-FA-SNs showed lower cytotoxicity in folate receptor negative normal mouse fibroblast cells (L929 cells) compared with free DOX. In vivo tumor-targeted fluorescence imaging indicated specific tumor targeting and uptake of FA-SNs in nude mice bearing subcutaneous HeLa cell-derived xenograft tumors. In vivo anti-tumor experiments demonstrated that DOX-FA-SNs (10 mg kg~(-1) of DOX) significantly regressed the tumor growth and reduced toxicity compared with free DOX. These results have great significance in developing and optimizing SNs as effective intracellular delivery and specific tumor targeting vehicles.
机译:硅nanorattles (SNs)已被证明有前途的药物输送的载体。进一步提高疗效和减少不良影响,主动靶向肿瘤必要的。肿瘤特定的靶向配体,叶酸(FA),作为载体的阿霉素(阿霉素)(DOX-FA-SNs)。DOX-FA-SNs体外的细胞吸收人类宫颈癌细胞(海拉细胞)评估。细胞毒性在人宫颈癌细胞(海拉细胞)比阿霉素羧基(羧基)和加载聚乙二醇(PEG) SNs修改(分别DOX-COOH-SNs和DOX-PEG-SNs)。然而,DOX-FA-SNs显示较低的细胞毒性叶酸受体-正常小鼠成纤维细胞细胞(L929细胞)与自由阿霉素。体内tumor-targeted荧光成像技术表示特定的肿瘤靶向和吸收FA-SNs裸小鼠皮下海拉细胞衍生异种移植肿瘤。实验表明,DOX-FA-SNs(10毫克公斤~(1)的强力霉素)肿瘤明显退化增长和降低毒性与自由阿霉素。开发和优化SNs同样有效细胞内交付和特定的肿瘤针对车辆。

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