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一种用于肠胃外给药的新型蒿甲醚-本芴醇脂质乳剂增强抗疟活性。

Enhanced antimalarial activity by a novel artemether-lumefantrine lipid emulsion for parenteral administration.

作者信息

Ma Yufan, Lu Tingli, Zhao Wen, Wang Ying, Chen Ting, Mei Qibing, Chen Tao

机构信息

School of Medicine, Xi'an Jiaotong University, Xi'an, People's Republic of China Xi'an Libang Pharmaceutical Co., Ltd., Xi'an, People's Republic of China.

Key Laboratory for Space Bioscience and Biotechnology, Faculty of Life, Northwestern Polytechnical University, Xi'an, People's Republic of China.

出版信息

Antimicrob Agents Chemother. 2014 Oct;58(10):5658-65. doi: 10.1128/AAC.01428-13. Epub 2014 Jun 30.

DOI:10.1128/AAC.01428-13
PMID:24982079
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4187974/
Abstract

Artemether and lumefantrine (also known as benflumetol) are difficult to formulate for parenteral administration because of their low aqueous solubility. Cremophor EL as an emulsion excipient has been shown to cause serious side effects. This study reports a method of preparation and the therapeutic efficacies of novel lipid emulsion (LE) delivery systems with artemether, lumefantrine, or artemether in combination with lumefantrine, for parenteral administration. Their physical and chemical stabilities were also evaluated. Furthermore, the in vivo antimalarial activities of the lipid emulsions developed were tested in Plasmodium berghei-infected mice. Artemether, lumefantrine, or artemether in combination with lumefantrine was encapsulated in an oil phase, and the in vivo performance was assessed by comparison with artesunate for injection. It was found that the lumefantrine lipid emulsion (LUM-LE) and artemether-lumefantrine lipid emulsion (ARM-LUM-LE-3) (1:6) began to decrease the parasitemia levels after only 3 days, and the parasitemia inhibition was 90% at doses of 0.32 and 0.27 mg/kg, respectively, with immediate antimalarial effects greater than those of the positive-control group and constant antimalarial effects over 30 days. LUM-LE and ARM-LUM-LE-3 demonstrated the best performance in terms of chemical and physical stabilities and antiplasmodial efficacy, with a mean particle size of 150 nm, and they have many favorable properties for parenteral administration, such as biocompatibility, physical stability, and ease of preparation.

摘要

蒿甲醚和本芴醇(也称为苯芴醇)由于其低水溶性而难以制成肠胃外给药制剂。聚氧乙烯蓖麻油(Cremophor EL)作为一种乳化辅料已被证明会引起严重的副作用。本研究报告了一种用于肠胃外给药的新型脂质乳剂(LE)递送系统的制备方法及其治疗效果,该系统包含蒿甲醚、本芴醇或蒿甲醚与本芴醇的组合。还评估了它们的物理和化学稳定性。此外,在感染伯氏疟原虫的小鼠中测试了所开发脂质乳剂的体内抗疟活性。蒿甲醚、本芴醇或蒿甲醚与本芴醇的组合被包裹在油相中,并通过与注射用青蒿琥酯比较来评估其体内性能。结果发现,本芴醇脂质乳剂(LUM-LE)和蒿甲醚-本芴醇脂质乳剂(ARM-LUM-LE-3)(1:6)仅在3天后就开始降低疟原虫血症水平,在剂量分别为0.32和0.27 mg/kg时,疟原虫血症抑制率分别为90%,其即时抗疟效果大于阳性对照组,且在30天内具有持续的抗疟效果。LUM-LE和ARM-LUM-LE-3在化学和物理稳定性以及抗疟效果方面表现最佳,平均粒径为150 nm,并且它们具有许多有利于肠胃外给药的特性,如生物相容性、物理稳定性和易于制备。

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