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Enhanced Tumor Delivery and Antitumor Activity in Vivo of Liposomal Doxorubicin Modified with MCF-7-Specific Phage Fusion Protein

机译:MCF-7特异性噬菌体融合蛋白修饰的脂质体阿霉素增强的肿瘤传递和体内抗肿瘤活性。

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摘要

A novel strategy to improve the therapeutic index of chemotherapy has been developed by the integration of nanotechnology with phage technique. The objective of this study was to combine phage display, identifying tumor-targeting ligands, with a liposomal nanocarrier for targeted delivery of doxorubicin. Following the proof of concept in cell-based experiments, this study focused on in vivo assessment of antitumor activity and potential side-effects of phage fusion protein-modified liposomal doxorubicin. MCF-7-targeted phage-Doxil treatments led to greater tumor remission and faster onset of antitumor activity than the treatments with non-targeted formulations. The enhanced anticancer effect induced by the targeted phage-Doxil correlated with an improved tumor accumulation of doxorubicin. Tumor sections consistently revealed enhanced apoptosis, reduced proliferation activity and extensive necrosis. Phage-Doxil-treated mice did not show any sign of hepatotoxicity and maintained overall health. Therefore, MCF-7-targeted phage-Doxil seems to be an active and tolerable chemotherapy for breast cancer treatment.
机译:通过将纳米技术与噬菌体技术相结合,已经开发出一种提高化学疗法治疗指数的新策略。这项研究的目的是将噬菌体展示,识别肿瘤靶向配体与脂质体纳米载体相结合,以靶向性递送阿霉素。继在基于细胞的实验中验证概念后,该研究集中在体内评估抗噬菌体活性和噬菌体融合蛋白修饰的脂质体阿霉素的潜在副作用。与非靶向制剂相比,以MCF-7为靶标的噬菌体-多西尔治疗可导致更大的肿瘤缓解和更快的抗肿瘤活性发作。靶向噬菌体-多西尔诱导的增强的抗癌作用与阿霉素的肿瘤积累改善有关。肿瘤切片始终显示出增强的细胞凋亡,降低的增殖活性和广泛的坏死。经噬菌体多西尔治疗的小鼠未显示任何肝毒性迹象,并保持了整体健康。因此,靶向MCF-7的噬菌体-Doxil似乎是一种有效且可耐受的乳腺癌化疗药物。

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