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盐酸青藤碱纳米脂质体的制备与评价。

Preparation and Evaluation of Nano-Liposomal Form of Febrifugine Hydrochloride.

机构信息

Institute of Chinese Materia Medica, China Academy of Chinese Medical Sciences, Beijing 100020, P. R. China.

College of Pharmacy, Liaoning University, Shenyang 110036, P. R. China.

出版信息

J Nanosci Nanotechnol. 2020 Apr 1;20(4):2558-2566. doi: 10.1166/jnn.2020.17186.

Abstract

Febrifugine hydrochloride (FFH) has strong pharmacological antimalarial effect. However, compared with oral administration, the efficacy of intravenous administration is significantly reduced. In this study, we prepared conventional liposomes and PEGylated liposomes to improve the efficacy of its intravenous injection. Both liposome formulations were prepared using a modified ethanol injection method. Their mean particle sizes were 126.23 and 114.93 nm, mean zeta potentials were -6.25 and -26.33 mV, and entrapment efficiencies (EE) were 89.43 and 96.42%, respectively. The release profile indicated that the release of FFH from PEGylated liposomes and conventional liposomes was slower than free FFH, with sustained-release effect of PEGylated liposomes being more significant. PEGylated liposomes demonstrated excellent antimalarial activities superior to free FFH and conventional FFH-loaded liposomes. In addition, the PEGylated liposomes resulted in enhanced antimalarial effect in infected mice with delayed recrudescence and prolonged survival time, compared with free FFH and conventional FFH-loaded liposomes administration. Based on these exciting experimental results, PEGylated liposomes could be a potential drug delivery system for FFH, with enhanced pharmacodynamics of intravenous injection.

摘要

盐酸退热净(FFH)具有很强的药理学抗疟作用。然而,与口服给药相比,静脉注射的疗效明显降低。在本研究中,我们制备了常规脂质体和聚乙二醇化脂质体,以提高其静脉注射的疗效。两种脂质体制剂均采用改良的乙醇注入法制备。它们的平均粒径分别为 126.23nm 和 114.93nm,平均 zeta 电位分别为-6.25mV 和-26.33mV,包封率(EE)分别为 89.43%和 96.42%。释放曲线表明,PEG 化脂质体和普通脂质体中 FFH 的释放速度比游离 FFH 慢,PEG 化脂质体具有更显著的缓释效果。PEG 化脂质体表现出优异的抗疟活性,优于游离 FFH 和载有普通 FFH 的脂质体。此外,与游离 FFH 和载有普通 FFH 的脂质体给药相比,PEG 化脂质体在感染小鼠中表现出增强的抗疟作用,潜伏期延长,生存时间延长。基于这些令人兴奋的实验结果,PEG 化脂质体可能是 FFH 的一种有前途的药物传递系统,具有增强的静脉注射药效学。

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