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首页> 外文期刊>Scientific reports. >Co-delivery of docetaxel and palmitoyl ascorbate by liposome for enhanced synergistic antitumor efficacy
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Co-delivery of docetaxel and palmitoyl ascorbate by liposome for enhanced synergistic antitumor efficacy

机译:通过脂质体共同交付多西紫杉醇和棕榈酰抗坏血酸,用于增强协同抗肿瘤功效

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Palmitoyl ascorbate (PA) as an antioxidant has the potential for the treatment of cancer. In the present study, a nanocarrier system was developed for co-delivery of docetaxel (DOC) with palmitoyl ascorbate and the therapeutic efficacy of a combination drug regimen was investigated. For this purpose, different ratios of docetaxel and palmitoyl ascorbate were co-encapsulated in a liposome and they all showed high encapsulation efficiency. The average diameters of the liposomes ranged from 140 to 170?nm. Negative zeta potential values were observed for all systems, ranged from -40?mV to -56?mV. Studies on drug release and cellular uptake of the co-delivery system demonstrated that both drugs were effectively taken up by the cells and released slowly. Moreover, the liposome loading drugs with DOC/PA concentration ratio of 1:200 showed the highest anti-tumor activity to three different types of tumor cells. The higher in vivo therapeutic efficacy with lower systemic toxicity of the DOC-PA200-LPs was also verified by the H22 tumor bearing mice model. Our results showed that such co-loaded delivery systems could serve as a promising therapeutic approach to improve clinical outcomes against hepatic carcinoma.
机译:棕榈酰抗坏血酸(PA)作为抗氧化剂具有治疗癌症的可能性。在本研究中,开发了一种纳米载波系统,用于使用棕榈酰基抗坏血酸和抗坏血酸的多西紫杉醇(DOC),并研究了组合药物方案的治疗效果。为此目的,多西紫杉醇和棕榈酰抗坏血酸的不同比例在脂质体中共封装,它们都显示出高封装效率。脂质体的平均直径范围为140至170℃。对于所有系统,观察到负Zeta电位值,范围为-40?mV至-56?mv。对共递送系统的药物释放和细胞摄取的研究表明,两种药物被细胞有效占用并缓慢释放。此外,具有1:200的DOC / PA浓度比的脂质体加载药物显示出三种不同类型的肿瘤细胞的最高抗肿瘤活性。通过H22肿瘤轴承小鼠模型还验证了DOC-PA200-LPS的较低系统毒性的体内治疗效果较高。我们的研究结果表明,这种共同装载的递送系统可以作为改善肝癌临床结果的有希望的治疗方法。

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