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A Liposomal Formulation Able to Incorporate a High Content of Paclitaxel and Exert Promising Anticancer Effect

机译:一种脂质体制剂,能够掺入高含量的紫杉醇并发挥有效的抗癌作用

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A liposome formulation for paclitaxel was developed in this study. The liposomes, composed of naturally unsaturated and hydrogenated phosphatidylcholines, with significant phase transition temperature difference, were prepared and characterized. The liposomes exhibited a high content of paclitaxel, which was incorporated within the segregated microdomains coexisting on phospholipid bilayer of liposomes. As much as 15% paclitaxel to phospholipid molar ratio were attained without precipitates observed during preparation. In addition, the liposomes remained stable in liquid form at 4∘Cfor at least 6 months. The special composition of liposomal membrane which could reduce paclitaxel aggregation could account for such a capacity and stability. The cytotoxicity of prepared paclitaxel liposomes on the colon cancer C-26 cell culture was comparable to Taxol. Acute toxicity test revealed that LD50for intravenous bolus injection in mice exceeded by 40 mg/kg. In antitumor efficacy study, the prepared liposomal paclitaxel demonstrated the increase in the efficacy against human cancer in animal model. Taken together, the novel formulated liposomes can incorporate high content of paclitaxel, remaining stable for long-term storage. These animal data also demonstrate that the liposomal paclitaxel is promising for further clinical use.
机译:在这项研究中开发了紫杉醇的脂质体制剂。制备并表征了由天然不饱和和氢化的磷脂酰胆碱组成的脂质体,它们具有明显的相变温度差。脂质体显示出高含量的紫杉醇,紫杉醇被并入脂质体的磷脂双层上共存的分离的微区中。紫杉醇与磷脂的摩尔比高达15%,在制备过程中未观察到沉淀。此外,脂质体在4°C下以液体形式稳定至少6个月。可以减少紫杉醇聚集的脂质体膜的特殊组成可以解释这种容量和稳定性。制备的紫杉醇脂质体对结肠癌C-26细胞培养的细胞毒性与紫杉醇相当。急性毒性试验表明,静脉推注小鼠的LD50超过40μmg/ kg。在抗肿瘤功效研究中,制备的脂质体紫杉醇在动物模型中证明了抗人类癌症功效的提高。两者合计,新配制的脂质体可以掺入高含量的紫杉醇,保持稳定以长期保存。这些动物数据还表明脂质体紫杉醇有望用于进一步的临床应用。

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