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治疗药物在体外及原发性阿米巴脑膜脑炎小鼠模型中对福氏耐格里阿米巴的活性

Activities of therapeutic agents against Naegleria fowleri in vitro and in a mouse model of primary amebic meningoencephalitis.

作者信息

Goswick Shannon M, Brenner George M

机构信息

Department of Pharmacology and Physiology, Oklahoma State University Center for Health Sciences, Tulsa, Oklahoma 74107-1898, USA.

出版信息

J Parasitol. 2003 Aug;89(4):837-42. doi: 10.1645/GE-87R.

DOI:10.1645/GE-87R
PMID:14533700
Abstract

Inhalation of water contaminated with Naegleria fowleri may lead to a potentially fatal infection of the central nervous system known as primary amebic meningoencephalitis (PAM). Amphotericin B (AMB), an antifungal drug, is the only agent with established clinical efficacy in the treatment of PAM, though therapy with this drug is not always effective and has been associated with adverse effects on the kidneys and other organs. We investigated the activity of various therapeutic agents against N. fowleri in an attempt to identify other useful agents for treating PAM. Several of these agents exhibited in vitro activity against the Lee (M67) strain of N. fowleri. The minimum inhibitory concentrations of these agents were 0.1 microg/ml (ketoconazole), 1 microg/ml (liposomal AMB), and 10 microg/ml (minocycline, quinupristin-dalfopristin, and trifluoperazine). Other agents had a minimum inhibitory concentration > 10 microg/ml (linezolid) or > 100 microg/ml (rifampin). In a mouse model of PAM, none of the untreated control mice survived, whereas the survival of treated animals was 50% (quinupristin-dalfopristin), 30% (ketoconazole and liposomal AMB), 20% (trifluoperazine), and 10% (linezolid and minocycline). Further studies are needed to ascertain whether these agents have synergistic activity with AMB in vitro and in vivo.

摘要

吸入被福氏耐格里阿米巴污染的水可能会导致一种潜在致命的中枢神经系统感染,即原发性阿米巴脑膜脑炎(PAM)。两性霉素B(AMB)是一种抗真菌药物,是唯一在治疗PAM方面具有已确定临床疗效的药物,尽管用这种药物治疗并不总是有效,且与对肾脏和其他器官的不良反应有关。我们研究了各种治疗药物对福氏耐格里阿米巴的活性,试图确定其他治疗PAM的有用药物。其中几种药物在体外对福氏耐格里阿米巴的Lee(M67)菌株表现出活性。这些药物的最低抑菌浓度分别为0.1微克/毫升(酮康唑)、1微克/毫升(脂质体AMB)和10微克/毫升(米诺环素、奎奴普丁-达福普汀和三氟拉嗪)。其他药物的最低抑菌浓度>10微克/毫升(利奈唑胺)或>100微克/毫升(利福平)。在PAM小鼠模型中,未治疗的对照小鼠无一存活,而治疗动物的存活率分别为50%(奎奴普丁-达福普汀)、30%(酮康唑和脂质体AMB)、20%(三氟拉嗪)和10%(利奈唑胺和米诺环素)。需要进一步研究以确定这些药物在体外和体内是否与AMB具有协同活性。

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