首页> 外文期刊>The Journal of Antimicrobial Chemotherapy >Influence of multidrug efflux systems on methylene blue-mediated photodynamic inactivation of Candida albicans.
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Influence of multidrug efflux systems on methylene blue-mediated photodynamic inactivation of Candida albicans.

机译:多药外排系统对白色假丝酵母亚甲基蓝介导的光动力学失活的影响。

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OBJECTIVES: To investigate whether the major fungal multidrug efflux systems (MESs) affect the efficiency of methylene blue (MB)-mediated antimicrobial photodynamic inactivation (APDI) in pathogenic fungi and test specific inhibitors of these efflux systems to potentiate APDI. METHODS: Candida albicans wild-type and mutants that overexpressed two classes of MESs [ATP-binding cassette (ABC) and major facilitator superfamily (MFS)] were tested for APDI using MB as the photosensitizer with and without addition of MES inhibitors. The uptake and cytoplasm localization of photosensitizer were achieved using laser confocal microscopy. RESULTS: ABC MES overexpression reduced MB accumulation and APDI killing more than MFS MES overexpression. Furthermore, by combining MB APDI with the ABC inhibitor verapamil, fungal killing and MB uptake were potentiated, while by combining MB APDI with the MFS inhibitor INF(271), fungal killing and MB uptake were inhibited. This latter surprising finding may be explained by the hypothesis that the MFS channel can also serve as an uptake mechanism for MB. CONCLUSIONS: The ABC pumps are directly implicated in MB efflux from the cell cytoplasm. Both the influx and efflux of MB may be regulated by MFS systems, and blocking this gate before incubation with MB can decrease the uptake and APDI effects. An ABC inhibitor could be usefully combined with MB APDI for treating C. albicans infections.
机译:目的:调查主要的真菌多药外排系统(MESs)是否影响亚甲基蓝(MB)介导的病原性真菌的抗菌光动力失活(APDI)的效率,并测试这些外排系统的特异性抑制剂来增强APDI。方法:使用MB作为光敏剂,添加和不添加MES抑制剂,对过表达两类MES [ATP结合盒(ABC)和主要促进子超家族(MFS)]的白色念珠菌野生型和突变体进行APDI测试。使用激光共聚焦显微镜可以实现光敏剂的吸收和细胞质定位。结果:ABC MES过表达减少了MB积累,APDI杀死比MFS MES过表达更多。此外,通过将MB APDI与ABC抑制剂维拉帕米联合使用,可增强真菌杀伤和MB摄取,而通过将MB APDI与MFS抑制剂INF(271)结合,可抑制真菌杀伤和MB摄取。后一个令人惊讶的发现可能由以下假设解释:MFS通道也可以充当MB的吸收机制。结论:ABC泵直接参与细胞质的MB外排。 MB的流入和流出都可以通过MFS系统进行调节,在与MB一起孵育之前阻断该门可以降低摄取和APDI效应。 ABC抑制剂可以有效地与MB APDI结合用于治疗白色念珠菌感染。

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