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米替福新在隐球菌性脑膜脑炎和播散性隐球菌病的鼠模型中活性有限。

Limited activity of miltefosine in murine models of cryptococcal meningoencephalitis and disseminated cryptococcosis.

机构信息

University of Texas Health Science Center at San Antonio, San Antonio, Texas, USA.

出版信息

Antimicrob Agents Chemother. 2013 Feb;57(2):745-50. doi: 10.1128/AAC.01624-12. Epub 2012 Nov 19.

Abstract

Miltefosine is an alkyl phosphocholine with good oral bioavailability and in vitro activity against Cryptococcus species that has gained interest as an additional agent for cryptococcal infections. Our objective was to further evaluate the in vivo efficacy of miltefosine in experimental in vivo models of cryptococcal meningoencephalitis and disseminated cryptococcosis. Mice were infected intracranially or intravenously with either C. neoformans USC1597 or H99. Miltefosine treatment (1.8 to 45 mg/kg of body weight orally once daily) began at either 1 h or 1 day postinoculation. Fluconazole (10 mg/kg orally twice daily) or amphotericin B deoxycholate (3 mg/kg intraperitoneally once daily) served as positive controls. In our standard models, miltefosine did not result in significant improvements in survival or reductions in fungal burden against either C. neoformans isolate. There was a trend toward improved survival with miltefosine at 7.2 mg/kg against disseminated cryptococcosis with the H99 strain but only at a low infecting inoculum. In contrast, both fluconazole and amphotericin B significantly improved survival in mice with cryptococcal meningoencephalitis and disseminated cryptococcosis due to USC1597. Amphotericin B also improved survival against both cryptococcal infections caused by H99. Combination therapy with miltefosine demonstrated neither synergy nor antagonism in both models. These results demonstrate limited efficacy of miltefosine and suggest caution with the potential use of this agent for the treatment of C. neoformans infections.

摘要

米替福新是一种烷基磷胆碱,具有良好的口服生物利用度和体外抗隐球菌活性,作为隐球菌感染的附加治疗药物引起了人们的兴趣。我们的目的是进一步评估米替福新在隐球菌性脑膜脑炎和播散性隐球菌病的体内实验模型中的体内疗效。小鼠经颅或静脉感染新型隐球菌 USC1597 或 H99。米替福新治疗(1.8 至 45 毫克/千克体重,每日口服一次)于接种后 1 小时或 1 天开始。氟康唑(10 毫克/千克,每日口服两次)或两性霉素 B 脱氧胆酸盐(3 毫克/千克,每日腹腔内注射一次)作为阳性对照。在我们的标准模型中,米替福新对两种新型隐球菌分离株的存活或真菌负荷均无显著改善。米替福新在 7.2 毫克/千克时对 H99 株播散性隐球菌病有改善存活的趋势,但仅在低感染接种量时有效。相比之下,氟康唑和两性霉素 B 均显著提高了新型隐球菌脑膜脑炎和播散性隐球菌病小鼠的存活率。两性霉素 B 还改善了由 H99 引起的两种隐球菌感染的存活率。米替福新联合治疗在两种模型中均未表现出协同作用或拮抗作用。这些结果表明米替福新疗效有限,提示在治疗新型隐球菌感染时应谨慎使用该药物。

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