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首页> 外文期刊>The Journal of Antimicrobial Chemotherapy >Induction of multiple antibiotic resistance in Bacteroides fragilis by benzene and benzene-derived active compounds of commonly used analgesics, antiseptics and cleaning agents.
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Induction of multiple antibiotic resistance in Bacteroides fragilis by benzene and benzene-derived active compounds of commonly used analgesics, antiseptics and cleaning agents.

机译:苯和常用镇痛药,防腐剂和清洁剂的苯衍生活性化合物在脆弱类杆菌中诱导多种抗生素耐药性。

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摘要

OBJECTIVES: To determine the potential of active compounds (ACs) present in commonly used analgesics/antiseptics and cleaning agents (detergents and disinfectants) to induce multiple antibiotic resistance (MAR) in Bacteroides fragilis. METHODS: B. fragilis ATCC 25285 untreated or pretreated with sublethal concentrations of ACs (n = 25) was grown for 12 h. Susceptibility of cells pre-treated with various ACs to antibiotics and expression of resistance nodulation division family (bmeB) efflux pumps and putative marA-like global activators (PGAs) were measured. RESULTS: Twelve aromatic ACs containing benzene or its activated derivatives (salicylate, acetaminophen, gingerol, benzoate, phenol, chlorhexidine gluconate, capsaicin, juglone, cinnamaldehyde, benzene, ibuprofen and Triton X-100) induced MAR, which was reduced by carbonyl cyanide m-chlorophenylhydrazone. There was a positive correlation between the predicted degree of benzene activation and the level of induction. Deactivated benzene or non-aromatic ACs were either poor inducers or non-inducers. Efflux pumps bmeB1, 3, 4, 7 and two PGAs bfrA1 and bfrA2 were overexpressed. Expression of bfrA1 or bfrA2 in Escherichia coli caused a >2-fold increase in the MAR and overexpression of acrB, suggesting that they were putative marA orthologues. CONCLUSIONS: These data demonstrate (i) the presence of an MarA-like system(s) in B. fragilis and (ii) the propensity of benzene or its activated derivatives present in pharmaceutical products to induce MAR.
机译:目的:确定常用镇痛药/防腐剂和清洁剂(洗涤剂和消毒剂)中存在的活性化合物(ACs)在脆弱类拟杆菌中引起多重抗药性(MAR)的潜力。方法:未经处理或用亚致死浓度的AC(n = 25)预处理的脆弱脆弱芽孢杆菌ATCC 25285生长12小时。测量了用各种AC预处理的细胞对抗生素的敏感性以及耐药性结节分裂家族(bmeB)外排泵和假定的marA样全局激活剂(PGA)的表达。结果:十二种含有苯或其活化衍生物(水杨酸酯,对乙酰氨基酚,姜醇,苯甲酸酯,苯酚,葡萄糖酸洗必泰,辣椒素,朱龙,肉桂醛,苯,布洛芬和Triton X-100)的芳香族AC诱导的MAR被羰基氰化物m还原-氯苯基hydr。预测的苯活化程度与诱导水平之间呈正相关。失活的苯或非芳香族ACs是不良诱导剂或非诱导剂。外排泵bmeB1、3、4、7和两个PGA bfrA1和bfrA2过表达。大肠杆菌中bfrA1或bfrA2的表达引起MAR的> 2倍增加和acrB的过度表达,表明它们是推定的marA直向同源物。结论:这些数据证明(i)脆弱类芽孢杆菌中存在MarA样系统,以及(ii)药物产品中存在的苯或其活化衍生物诱导MAR的倾向。

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