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环孢素A可降低白色念珠菌临床分离株的氟康唑最低抑菌浓度,但不影响生物膜形成和细胞生长。

Cyclosporine A decreases the fluconazole minimum inhibitory concentration of Candida albicans clinical isolates but not biofilm formation and cell growth.

作者信息

Wibawa T, Baly I, Daeli P R, Kartasasmita G, Wijayanti N

机构信息

Department of Microbiology, Faculty of Medicine; Universitas Gadjah Mada, Yogyakarta 55281, Indonesia.

Research Center for Biotechnology; Universitas Gadjah Mada, Yogyakarta 55281, Indonesia.

出版信息

Trop Biomed. 2015 Mar;32(1):176-82.

Abstract

Among the genus Candida, Candida albicans is the most abundant species in humans. One of the virulent factors of C. albicans is its ability to develop biofilm. Biofilm forming microbes are characterized by decreasing of its susceptibility to antibiotics and antifungal. The fungicidal effect of fluconazole may be enhanced by cyclosporine A in laboratory engineered C. albicans strains. The aim of this work is to analyze the synergistic effect of cyclosporine A with fluconazole in C. albicans clinical isolates and the effect of cycolsporine A alone in the biofilm formation. Six fluconazole resistant and six sensitive C. albicans clinical isolates were analyzed for its minimum inhibitory concentration (MICs), biofilm formation, and cell growths. A semi-quantitative XTT [2,3-bis(2-methoxy-4-nitro-5- sulfo-phenyl)-2H-tetrazolium-5-carboxanilide] reduction assay was conducted to measure the biofilm formation. Cyclosporine A has synergistic effect with fluconazole that was shown by decreasing MICs of both fluconazole resistant and sensitive C. albicans clinical isolates. However, cyclosporine A alone did not influence the biofilm formation and cell growth of both fluconazole resistant and sensitive C. albicans clinical isolates. These results indicated that cyclosporine A might be a promising candidate of adjuvant therapy for fluconazole against both fluconazole resistant and sensitive C. albicans clinical isolates.

摘要

在念珠菌属中,白色念珠菌是人类体内最为常见的菌种。白色念珠菌的致病因素之一是其形成生物膜的能力。形成生物膜的微生物对抗生素和抗真菌药物的敏感性会降低。在实验室构建的白色念珠菌菌株中,环孢素A可能会增强氟康唑的杀菌效果。本研究的目的是分析环孢素A与氟康唑对白色念珠菌临床分离株的协同作用,以及环孢素A单独对生物膜形成的影响。对6株耐氟康唑和6株敏感的白色念珠菌临床分离株进行了最小抑菌浓度(MIC)、生物膜形成和细胞生长分析。采用半定量XTT[2,3-双(2-甲氧基-4-硝基-5-磺基苯基)-2H-四唑-5-羧基苯胺]还原试验来检测生物膜的形成。环孢素A与氟康唑具有协同作用,这表现为耐氟康唑和敏感的白色念珠菌临床分离株的MIC均降低。然而,单独使用环孢素A对耐氟康唑和敏感的白色念珠菌临床分离株的生物膜形成和细胞生长均无影响。这些结果表明,环孢素A可能是氟康唑治疗耐氟康唑和敏感白色念珠菌临床分离株的一种有前景的辅助治疗候选药物。

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