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Two cholesterol derivative-based PEGylated liposomes as drug delivery system, study on pharmacokinetics and drug delivery to retina

机译:两种基于胆固醇衍生物的聚乙二醇化脂质体作为药物传递系统,研究药物动力学和药物向视网膜的传递

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摘要

In this study, two cholesterol derivatives, (4-cholesterocarbonyl-4'-(N,N,N-triethylamine butyloxyl bromide) azobenzene (CAB) and 4-cholesterocarbonyl-4'-(N,N-diethylamine butyloxyl) azobenzene (ACB), one of which is positively charged while the other is neutral, were synthesized and incorporated with phospholipids and cholesterol to form doxorubicin (DOX)- loaded liposomes. PEGylation was achieved by including 1,2-distearoyl-sn-glycero-3- phosphatiylethanol-amine-N-[methoxy-(polyethylene glycol)-2000 (DSPE-PEG2000). Our results showed that PEGylated liposomes displayed significantly improved stability and the drug leakage was decreased compared to the non-PEGylated ones in vitro. The in vivo study with rats also revealed that the pharmacokinetics and circulation half-life of DOX were significantly improved when liposomes were PEGylated (p < 0.05). In particular, the neutral cholesterol derivative ACB played some role in improving liposomes' stability in systemic circulation compared to the conventional PC liposome and the positively charged CAB liposome, with or without PEGylation. In addition, in the case of local drug delivery, the positively charged PEGliposome not only delivered much more of the drug into the rats' retinas (p < 0.001), but also maintained much longer drug retention time compared to the neutral PEGylated liposomes.
机译:在这项研究中,两种胆固醇衍生物,(4-胆固醇羰基-4'-(N,N,N-三乙胺丁氧基溴化物)偶氮苯(CAB)和4-胆固醇羰基-4'-(N,N-二乙胺丁氧基)偶氮苯(ACB合成了其中一个带正电而另一个为中性的化合物,并与磷脂和胆固醇结合形成负载阿霉素的脂质体,通过加入1,2-二硬脂酰基-sn-甘油-3磷脂酰乙醇来实现聚乙二醇化-胺-N- [甲氧基-(聚乙二醇)-2000(DSPE-PEG2000)。我们的结果表明,与非聚乙二醇化脂质体外相比,聚乙二醇化脂质体显示出显着改善的稳定性,并且药物泄漏减少了。对大鼠的研究还表明,将脂质体聚乙二醇化后,DOX的药代动力学和循环半衰期得到了显着改善(p <0.05),特别是中性胆固醇衍生物ACB在改善脂质体在系统循环中的稳定性方面起了一定作用。 o具有或不具有PEG化作用的常规PC脂质体和带正电荷的CAB脂质体。另外,在局部药物递送的情况下,与中性PEG化脂质体相比,带正电荷的PEG脂质体不仅将更多的药物递送到大鼠的视网膜中(p <0.001),而且还保持了更长的药物保留时间。

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