首页> 外文期刊>Journal of Biosciences and Medicines >Mutant Selection Windows of Azalomycin F5a in Combination with Vitamin K3 against Methicillin-Resistant Staphylococcus aureus
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Mutant Selection Windows of Azalomycin F5a in Combination with Vitamin K3 against Methicillin-Resistant Staphylococcus aureus

机译:阿扎霉素F5a与维生素K3结合抗甲氧西林金黄色葡萄球菌的突变体选择窗口

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Azalomycin F5a, a 36-membered macrocyclic lactone isolated from several streptomyces strains, presented remarkable anti-methicillin-resistant Staphylococcus aureus (MRSA) activities. To improve its anti-MRSA potential and to evaluate the probability of MRSA resistant to it before development, the anti-MRSA activities of azalomycin F5a in combination with vitamin K3 were first evaluated using checkerboard assay. Then the minimal concentration inhibiting colony formation by 99% (MIC99) and mutant prevention concentration (MPC) of azalomycin F5a alone and in combination with vitamin K3 against MRSA were determined using agar plates with linear antimicrobial concentration decrease. The fractional inhibitory concentration indexes (FICIs) of 0.25 - 0.50 showed the synergistic activity of azalomycin F5a in combination with vitamin K3. The mutant selection windows (MSWs, MIC99-MPC) of azalomycin F5a alone against MRSA tested were 2.07 - 6.40 μg/mL, and the MPCs of azalomycin F5a in combination with vitamin K3 against MRSA tested were 1.60 - 3.20 μg/mL. These indicated that the MPCs of azalomycin F5a in combination could drop down to below its MIC99 alone. According to the hypothesis of MSW, the narrower MSWs of azalomycin F5a alone, even closed MSWs in combination with vitamin K3, together with their synergistic anti-MRSA activities, indicated that azalomycin F5a had a good potential to develop as a new antimicrobial agent.
机译:从几个链霉菌菌株中分离出的具有36个成员的大环内酯阿扎霉素F5a具有显着的抗甲氧西林抗性金黄色葡萄球菌(MRSA)活性。为了提高其抗MRSA的潜力并评估MRSA对其产生抗药性的可能性,首先使用棋盘分析法评估了阿扎霉素F5a与维生素K3的抗MRSA活性。然后,使用线性抗菌剂浓度降低的琼脂平板,确定单独的阿扎霉素F5a和与维生素K3结合使用的抗MRSA的最低99%抑制菌落形成(MIC99)和突变预防浓度(MPC)。分数抑制浓度指数(FICI)为0.25-0.50,显示了阿扎霉素F5a与维生素K3的协同活性。单独的阿扎霉素F5a对抗MRSA的突变选择窗口(MSWs,MIC99-MPC)为2.07-6.40μg/ mL,而阿扎霉素F5a结合维生素K3对抗MRSA的MPC为1.60-3.20μg/ mL。这些表明,结合的阿扎霉素F5a的MPC可降至单独的MIC99以下。根据MSW的假说,单独使用阿扎霉素F5a的较窄MSW,甚至与维生素K3结合的封闭MSW,以及它们的协同抗MRSA活性,都表明阿扎霉素F5a具有作为新的抗菌剂发展的良好潜力。

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