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米替福新在体外对白色念珠菌和尖孢镰刀菌指甲生物膜有效。

Miltefosine is effective against Candida albicans and Fusarium oxysporum nail biofilms in vitro.

作者信息

Machado Vila Taissa Vieira, Sousa Quintanilha Natália, Rozental Sonia

机构信息

Laboratório de Biologia Celular de Fungos, Instituto de Biofísica Carlos Chagas Filho, Universidade Federal do Rio de Janeiro, Rio de Janeiro, RJ, Brazil.

出版信息

J Med Microbiol. 2015 Nov;64(11):1436-1449. doi: 10.1099/jmm.0.000175. Epub 2015 Sep 23.

Abstract

Onychomycosis is a fungal nail infection that represents ∼50 % of all nail disease cases worldwide. Clinical treatment with standard antifungals frequently requires long-term systemic therapy to avoid chronic disease. Onychomycosis caused by non-dermatophyte moulds, such as Fusarium spp., and yeasts, such as Candida spp., is particularly difficult to treat, possibly due to the formation of drug-resistant fungal biofilms on affected areas. Here, we show that the alkylphospholipid miltefosine, used clinically against leishmaniasis and cutaneous breast metastases, has potent activity against biofilms of Fusarium oxysporum and Candida albicans formed on human nail fragments in vitro. Miltefosine activity was compared with that of commercially available antifungals in the treatment of biofilms at two distinct developmental phases: formation and maturation (pre-formed biofilms). Drug activity towards biofilms formed on nail fragments and on microplate surfaces (microdilution assays) was evaluated using XTT [2,3-bis(2-methoxy-4-nitro-5-sulfophenyl)-2H-tetrazolium-5-carboxanilide] assays, and drug effects on fingernail biofilms were analysed by scanning electron microscopy (SEM). For F. oxysporum, miltefosine at 8 μg ml- 1 inhibited biofilm formation by 93%, whilst 256 μg ml- 1 reduced the metabolic activity of pre-formed nail biofilms by 93%. Treatment with miltefosine at 1000 μg ml- 1 inhibited biofilm formation by 89% and reduced the metabolic activity of pre-formed C. albicans biofilms by 99%. SEM analyses of biofilms formed on fingernail fragments showed a clear reduction in biofilm biomass after miltefosine treatment, in agreement with XTT results. Our results show that miltefosine has potential as a therapeutic agent against onychomycosis and should be considered for in vivo efficacy studies, especially in topical formulations for refractory disease treatment.

摘要

甲癣是一种指甲真菌感染,约占全球所有指甲疾病病例的50%。使用标准抗真菌药物进行临床治疗通常需要长期的全身治疗以避免疾病慢性化。由非皮肤癣菌霉菌(如镰刀菌属)和酵母菌(如念珠菌属)引起的甲癣尤其难以治疗,这可能是由于在受影响区域形成了耐药真菌生物膜。在此,我们表明临床上用于治疗利什曼病和皮肤乳腺转移瘤的烷基磷脂米替福新,在体外对在人指甲碎片上形成的尖孢镰刀菌和白色念珠菌生物膜具有强大活性。在两个不同的发育阶段(形成阶段和成熟阶段(预先形成的生物膜))将米替福新的活性与市售抗真菌药物在生物膜治疗中的活性进行了比较。使用XTT [2,3-双(2-甲氧基-4-硝基-5-磺基苯基)-2H-四唑-5-羧基苯胺] 测定法评估药物对在指甲碎片和微孔板表面形成的生物膜(微量稀释测定法)的活性,并通过扫描电子显微镜 (SEM) 分析药物对指甲生物膜的影响。对于尖孢镰刀菌,8 μg/ml的米替福新可抑制93%的生物膜形成,而256 μg/ml可使预先形成的指甲生物膜的代谢活性降低93%。用1000 μg/ml的米替福新处理可抑制89%的生物膜形成,并使预先形成的白色念珠菌生物膜的代谢活性降低99%。对在指甲碎片上形成的生物膜的SEM分析表明,米替福新处理后生物膜生物量明显减少,这与XTT结果一致。我们的结果表明,米替福新有潜力作为治疗甲癣的药物,应考虑进行体内疗效研究,特别是用于难治性疾病治疗的局部制剂。

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