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In vitro activity of propyl gallate-azole drug combination against fluconazole- and itraconazole-resistant Candida albicans strains

机译:没食子酸丙酯-唑类药物组合对耐氟康唑和伊曲康唑的白色念珠菌菌株的体外活性

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摘要

Aims: The influence of an antioxidant, propyl gallate (PG), on the In vitro antifungal activity of itraconazole and fluconazole, was investigated to determine whether PG could increase the antifungal activity and reduce strain resistance. Methods and Results: Susceptibility tests were performed against azole-resistant isolates of Candida albicans by the microbroth dilution method in the presence of PG at 400 mug ml(-1). PG-triazole combination brought about a marked reduction of inhibitory azole concentration. In particular, the MIC90 for itraconazole and fluconazole dropped from 1 mug ml(-1) to 0.125 mug ml(-1) and from >64 mug ml(-1)-8 mug ml(-1), respectively. Conclusions: It is likely that more than one mechanism is involved in the above synergistic interaction, including effects of PG on ATP synthesis, thus reducing the ABC transporters activity, or an effect on the target of azole, i.e. the P-450 cytochrome. Significance and Impact of the Study: The PG-triazole combination may have a role in future topical antifungal strategies but other studies are warranted.
机译:目的:研究抗氧化剂没食子酸丙酯(PG)对伊曲康唑和氟康唑的体外抗真菌活性的影响,以确定PG是否可以增加抗真菌活性并降低菌株的抗性。方法与结果:在400毫升/ ml PG浓度下,通过微肉汤稀释法对白色念珠菌的抗唑类菌株进行了药敏试验。 PG-三唑组合物显着降低了抑制唑的浓度。特别是,伊曲康唑和氟康唑的MIC90分别从1毫升ml(-1)降至0.125毫升ml(-1)和> 64毫升ml(-1)-8毫升ml(-1)。结论:以上协同相互作用可能涉及一种以上的机制,包括PG对ATP合成的影响,从而降低了ABC转运蛋白的活性,或对吡咯靶标(即P-450细胞色素)的影响。研究的意义和影响:PG-三唑组合可能在未来的局部抗真菌策略中起作用,但有必要进行其他研究。

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