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首页> 外文期刊>Nanoscale >Doxorubicin-loaded polypyrrole nanovesicles for suppressing tumor metastasis through combining photothermotherapy and lymphatic system-targeted chemotherapy
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Doxorubicin-loaded polypyrrole nanovesicles for suppressing tumor metastasis through combining photothermotherapy and lymphatic system-targeted chemotherapy

机译:Doxorubicin-loaded聚吡咯nanovesicles为通过结合抑制肿瘤转移photothermotherapy和淋巴system-targeted化疗

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摘要

The lymphatic system provides a main route for the dissemination of most malignancies, which was related to high mortality in cancer patients. Traditional intravenous chemotherapy is of limited effectiveness on lymphatic metastasis due to the difficulty in accessing the lymphatic system. Herein, a novel lymphatic-targeting nanoplatform is prepared by loading doxorubicin (DOX) into sub-50 nm polypyrrole nanovesicles (PPy NVs). The PPy NVs possessed hollow spherical morphologies and a negative surface charge, leading to high drug loading capacity. These vesicles can also convert near-infrared (NIR) light into heat and thus can be used for tumor thermal ablation. DOX loaded PPy NVs (PPy@DOX NVs) along with NIR illumination are highly effective against 4T1 breast cancer cells in vitro. More importantly, following subcutaneous (SC) injection, a direct lymphatic migration of PPy@DOX NVs is confirmed through fluorescence observation of the isolated draining nodes. The acidic conditions in metastatic nodes might subsequently trigger the release of the encapsulated DOX NVs based on their pH-sensitive release profile. In a mouse model bearing 4T1 breast cancer, lymphatic metastases, as well as lung metastases, are significantly inhibited by nanocarrier-mediated trans-lymphatic drug delivery in combination with photothermal ablation. In conclusion, this platform holds great potential in impeding tumor growth and metastasis.
机译:淋巴系统提供了一个主要途径大多数恶性肿瘤的传播,这是在癌症患者高死亡率有关。传统静脉化疗的对淋巴转移的效果有限访问淋巴的困难系统。nanoplatform是由负载阿霉素(阿霉素)在这纳米聚吡咯nanovesicles(PPy NVs)。形态和消极的表面电荷,导致高药物装载能力。囊泡也可以把近红外(NIR)光成热,因此可用于肿瘤热烧蚀。随着近红外照明高度NVs)有效对抗4 t1乳腺癌细胞体外。(SC)注入,直接淋巴转移通过荧光PPy@DOX NVs确认观察的孤立节点。在转移性淋巴结可能酸性条件随后引发的释放根据pH-sensitive封装阿霉素NVs发布概要文件。乳腺癌淋巴转移,以及肺转移,明显抑制nanocarrier-mediated trans-lymphatic药物交付与光热光谱分析相结合消融。在阻碍肿瘤的生长,也有着巨大的潜力转移。

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