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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Comparative studies of irinotecan-loaded polyethylene glycol-modified liposomes prepared using different PEG-modification methods
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Comparative studies of irinotecan-loaded polyethylene glycol-modified liposomes prepared using different PEG-modification methods

机译:使用不同PEG修饰方法制备的伊立替康负载聚乙二醇修饰脂质体的比较研究

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Recently, a polyethylene glycol (PEG)-modification method for liposomes prepared using pH-gradient method has been proposed. The differences in the pharmacokinetics and the impact on the antitumor effect were examined; however the impact of PEG-lipid molar weight has not been investigated yet. The main purpose of this study is to evaluate the impact of PEG-lipid molar weight against the differences in the pharmacokinetics, the drug-release profile, and the antitumor effect between the proposed PEG-modification method, called the post-modification method, and the conventional PEG-modification method, called the pre-modification method. Various comparative studies were performed using irinotecan as a general model drrug, The results showed that PEG-lipid degradation could be markedly inhibited in the post-modification method. Furthermore, prolonged circulation time was observed in the post-modification method. The sustained drug-release was observed in the post-modification method by the results of the drug-releasing test in plasma. Moreover, a higher antitumor effect was observed in the post-modification method. It was also confirmed that the same behaviors were observed in all comparative studies even though the PEG molecular weight was lower. In conclusion, the post-modification method has the potential to be a valuable PEG-modification method that can achieve higher preservation stability of PEG-lipid, prolonged circulation time, and higher antitumor effect with only half the amount of PEG-lipid as compared to the pre-modification method. Furthermore, it was demonstrated that PEG_(5000)-lipid would be more desirable than PEG_(2000)-lipid since it requires mueh smaller amount of PEG-lipid to demonstrate the same performances.
机译:近年来,已经提出了使用pH梯度法制备的脂质体的聚乙二醇(PEG)修饰方法。检查了药代动力学的差异以及对抗肿瘤作用的影响;然而,尚未研究PEG-脂质摩尔重量的影响。这项研究的主要目的是评估PEG-脂质摩尔质量对所提议的PEG修饰方法(称为后修饰方法)与药代动力学,药物释放曲线和抗肿瘤作用之间差异的影响。传统的PEG修饰方法称为预修饰方法。使用伊立替康作为一般模型药进行了各种比较研究,结果表明,在修饰后方法中,PEG-脂质降解可以得到显着抑制。此外,在后改性方法中观察到延长的循环时间。通过血浆中药物释放测试的结果,在后修饰方法中观察到了持续的药物释放。此外,在后修饰方法中观察到更高的抗肿瘤作用。还证实在所有比较研究中观察到相同的行为,即使PEG分子量较低。综上所述,后修饰法可能是有价值的PEG修饰法,与PEG脂质相比,仅PEG脂质量的一半,它可以实现更高的PEG脂质保存稳定性,延长的循环时间和更高的抗肿瘤作用。预修改方法。此外,已证明PEG_(5000)-脂质将比PEG_(2000)-脂质更合乎需要,因为它需要更少量的PEG-脂质以表现出相同的性能。

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