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Somatostatin Receptor-Mediated Tumor-Targeting Nanocarriers Based on Octreotide-PEG Conjugated Nanographene Oxide for Combined Chemo and Photothermal Therapy

机译:基于奥曲肽-PEG共轭纳米氧化石墨烯的生长抑素受体介导的肿瘤靶向纳米载体,用于化学和光热疗法的联合

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摘要

Nano-sized in vivo active targeting drug delivery systems have been developed to a high anti-tumor efficacy strategy against certain cancer-cells-specific. Graphene based nanocarriers with unique physical and chemical properties have shown significant potentials in this aspect. Here, octreotide (OCT), an efficient biotarget molecule, is conjugated to PEGylated nanographene oxide (NGO) drug carriers for the first time. The obtained NGO-PEG-OCT complex shows low toxicity and excellent stability in vivo and is able to achieve somatostatin receptor-mediated tumor-specific targeting delivery. Owing to the high loading efficiency and accurate targeting delivery of anticancer drug doxorubicin (DOX), our DOX loaded NGO-PEG-OCT complex offers a remarkably improved cancer-cell-specific cellular uptake, chemo-cytotoxicity, and decreased systemic toxicity compared to free DOX or NGO-PEG. More importantly, due to its strong near-infrared absorption, the NGO-PEG-OCT complex further enhances efficient photothermal ablation of tumors, delivering combined chemo and photothermal therapeutic effect against cancer cells.
机译:纳米尺寸的体内活性靶向药物递送系统已经被开发为针对某些癌细胞特异性的高抗肿瘤功效策略。具有独特的物理和化学性质的基于石墨烯的纳米载体在这方面已显示出巨大的潜力。在这里,奥曲肽(OCT)是一种有效的生物靶分子,首次与PEG化纳米氧化石墨烯(NGO)药物载体缀合。所获得的NGO-PEG-OCT复合物在体内显示出低毒性和优异的稳定性,并且能够实现生长抑素受体介导的肿瘤特异性靶向递送。由于抗癌药阿霉素(DOX)的高加载效率和准确的靶向递送,与游离的相比,我们的DOX加载的NGO-PEG-OCT复合物可显着改善癌细胞特异性细胞的摄取,化学细胞毒性和降低的全身毒性DOX或NGO-PEG。更重要的是,由于其强烈的近红外吸收,NGO-PEG-OCT复合物进一步增强了肿瘤的有效光热消融,从而提供了针对癌细胞的化学和光热联合治疗效果。

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