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Arsenic trioxide encapsulated liposomes prepared via copper acetate gradient loading method and its antitumor efficiency

机译:醋酸铜梯度负载法制备三氧化二砷包裹的脂质体及其抗肿瘤作用

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In this study, arsenic trioxide(ATO) was encapsulated in liposomes via copper acetate(Cu(OAc)2) gradients and high entrapment efficiency of over 80% was obtained. The average particle size and the zeta-potential of the liposomes were detected to be 115.1 ± 29.1 nm and-21.97 ± 0.6 m V, respectively. The TEM images showed rod-like precipitates in the inner aqueous phase, which was supposed be due to the formation of insoluble ATO–Cu complex.The in vitro drug release of ATO–Cu liposomes exhibited a sustained release over 72 h, and the release rates decreased with the increase of the p H of release media. Pharmacokinetic and tissue distribution studies of ATO liposomes showed significantly reduced plasma clearance rate, increased AUC0–12h and T1/2, and improved tumor distribution of As compared to iv administration of ATO solution. The anti-tumor effect of ATO loaded liposomes to S180 tumor-bearing mice was significantly improved with a tumor inhibition rate of 61.2%,meanwhile the toxicity of encapsulated ATO was greatly decreased. In conclusion, ATO can be effectively encapsulated into liposomes by remote loading method via Cu(OAc)2 gradients;the co-administration of ATO and Cu(Ⅱ) via liposomal formulation may find wide applications in the treatment of various tumors.
机译:在该研究中,通过醋酸铜(Cu(OAC)2)梯度在脂质体中包封砷(ATO),得到超过80%的高夹带效率。检测脂质体的平均粒度和ζ电位分别为115.1±29.1nm和-21.97±0.6mV。 TEM图像显示在内水相中的抗杆状沉淀物,其假定是由于不溶性ATO-Cu复合物的形成。ATO-Cu脂质体的体外药物释放表现出72小时的持续释放,并释放随着释放介质的P H增加,率下降。 ATO脂质体的药代动力学和组织分布研究表现出显着降低的血浆间隙率,增加的AUC0-12H和T1 / 2,以及与ATO溶液施用相比的肿瘤分布。用肿瘤抑制率为61.2%的肿瘤抑制率,ATO加载脂质体对S180肿瘤小鼠的抗肿瘤作用显着提高,同时封装ATO的毒性大大降低。总之,通过Cu(OAC)2梯度远程加载方法可以有效地将ATO与脂质体封装在脂质体中;通过脂质体制剂的ATO和Cu(Ⅱ)的共同施用可以在治疗各种肿瘤中找到广泛的应用。

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