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Co-Encapsulation of Chlorin e6 and Chemotherapeutic Drugs in a PEGylated Liposome Enhance the Efficacy of Tumor Treatment: Pharmacokinetics and Therapeutic Efficacy

机译:在聚乙二醇化脂质体中共包裹氯霉素e6和化学治疗药物可增强肿瘤治疗的功效:药代动力学和治疗功效

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摘要

Long-circulating PEG-modified liposome has been shown to improve pharmacokinetic properties and reduce systemic toxicity in cancer treatment. However, drug bioavailability from liposome remains a major challenge to the improvement of its therapeutic efficacy. Previously, we designed a PEGylated dual-effect liposome (named as PL-Dox-Ce6) with chlorin e6 incorporated in the lipid bilayer and Doxorubicin encapsulated in the interior. In this study, another dual-effect liposome with cisplatin encapsulated in the interior was further developed. The pharmacokinetics of these two dual-effect liposomes were studied in tumor-bearing mice. Based on the kinetic data of tumor and plasma, light irradiation was applied onto the tumors at different time points after drug administration to compare the therapeutic efficacy. We demonstrated that a single dose of the dual-effect liposomes combined with two doses of light irradiation can completely eradicate over 90% of the tumor in mice alone with significant survival rate and no toxicity. Thus, this study established a platform that utilizes the dual-effect liposome which combines photodynamic therapy and chemotherapy to improve the therapeutic outcomes of tumors.
机译:长循环PEG-修饰的脂质体已显示在癌症治疗中改善药代动力学特性并降低全身毒性。然而,脂质体的药物生物利用度仍然是改善其治疗功效的主要挑战。以前,我们设计了一种聚乙二醇化双效脂质体(命名为PL-Dox-Ce6),其中二氢卟酚e6掺入了脂质双层,而阿霉素包裹在内部。在这项研究中,进一步开发了另一种在内部包裹有顺铂的双效脂质体。在荷瘤小鼠中研究了这两种双重作用脂质体的药代动力学。根据肿瘤和血浆的动力学数据,在给药后的不同时间点将光照射到肿瘤上,以比较疗效。我们证明了单剂量的双效脂质体与两次剂量的光照射相结合可以完全根除仅小鼠中90%以上的肿瘤,且存活率高且无毒性。因此,本研究建立了利用双效脂质体的平台,该脂质体结合了光动力疗法和化学疗法来改善肿瘤的治疗效果。

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