Rakotomanga M, Blanc S, Gaudin K, Chaminade P, Loiseau P M
Chimiothérapie Antiparasitaire, UMR 8076 CNRS, Faculté de Pharmacie, Université Paris-Sud XI, F-92290 Châtenay-Malabry, France.
Antimicrob Agents Chemother. 2007 Apr;51(4):1425-30. doi: 10.1128/AAC.01123-06. Epub 2007 Jan 22.
Miltefosine (hexadecylphosphocholine [HePC]) is the first orally active antileishmanial drug. Transient HePC treatment of Leishmania donovani promastigotes at 10 microM significantly reduced the phosphatidylcholine content and enhanced the phosphatidylethanolamine (PE) content in parasite membranes, suggesting a partial inactivation of PE-N-methyltransferase. Phospholipase D activity did not seem to be affected by HePC. In addition, the enhancement of the lysophosphatidylcholine content could be ascribed to phospholipase A2 activation. Moreover, transient HePC treatment had no effect on the fatty acid alkyl chain length or the fatty acid unsaturation rate. Concerning sterols, we found a strong reduction of the C24 alkylated sterol content, and the enhancement of the cholesterol content could be the result of the HePC condensation effect with sterols. Because some of the effects observed after transient HePC treatment were different from those previously observed in HePC-resistant parasites, it could be hypothesized that continuous in vitro drug pressure induces the mechanisms of regulation in Leishmania lipid metabolism.
米替福新(十六烷基磷酸胆碱[HePC])是第一种口服有效的抗利什曼原虫药物。用10微摩尔的HePC对杜氏利什曼原虫前鞭毛体进行短暂处理,可显著降低寄生虫膜中的磷脂酰胆碱含量,并提高磷脂酰乙醇胺(PE)含量,这表明PE-N-甲基转移酶部分失活。磷脂酶D活性似乎不受HePC影响。此外,溶血磷脂酰胆碱含量的增加可归因于磷脂酶A2的激活。此外,短暂的HePC处理对脂肪酸烷基链长度或脂肪酸不饱和度没有影响。关于甾醇,我们发现C24烷基化甾醇含量大幅降低,胆固醇含量的增加可能是HePC与甾醇缩合作用的结果。由于短暂HePC处理后观察到的一些效应与之前在HePC抗性寄生虫中观察到的不同,因此可以推测,持续的体外药物压力会诱导利什曼原虫脂质代谢的调节机制。
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