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Effects of Lysozyme, Proteinase K, and Cephalosporins on Biofilm Formation by Clinical Isolates of Pseudomonas aeruginosa

机译:溶菌酶,蛋白酶K和头孢菌素对铜绿假单胞菌临床分离株生物膜形成的影响

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摘要

Pseudomonas aeruginosa is an opportunistic pathogen that can form biofilms, which confer resistance to immune clearance and antibacterial treatment. Therefore, effective strategies to prevent biofilm formation are warranted. Here, 103 P. aeruginosa clinical isolates were quantitatively screened for biofilm formation ability via the tissue culture plate method. The effects of lysozyme (hydrolytic enzyme) and proteinase K (protease) on biofilm formation were evaluated at different concentrations. Lysozyme (30 μg/mL), but not proteinase K, significantly inhibited biofilm formation (19% inhibition). Treatment of 24-hour-old biofilms of P. aeruginosa isolates with 50 times the minimum inhibitory concentrations (MICs) of ceftazidime and cefepime significantly decreased the biofilm mass by 32.8% and 44%, respectively. Moreover, the exposure of 24-hour-old biofilms of P. aeruginosa isolates to lysozyme (30 μg/mL) and 50 times MICs of ceftazidime or cefepime resulted in a significant reduction in biofilm mass as compared with the exposure to lysozyme or either antibacterial agent alone. The best antibiofilm effect (49.3%) was observed with the combination of lysozyme (30 μg/mL) and 50 times MIC of cefepime. The promising antibiofilm activity observed after treatment with 50 times MIC of ceftazidime or cefepime alone or in combination with lysozyme (30 μg/mL) is indicative of a novel strategy to eradicate pseudomonal biofilms in intravascular devices and contact lenses.
机译:假单胞菌铜绿假单胞菌是一种能够形成生物膜的机会主义病原体,其赋予免疫清除和抗菌治疗的抗性。因此,有必要预防生物膜形成的有效策略。这里,通过组织培养板法定量地筛选103吨铜绿假单胞菌的生物膜形成能力。在不同浓度下评价溶菌酶(水解酶)和蛋白酶K(蛋白酶K(蛋白酶K(蛋白酶)对生物膜形成的影响。溶菌酶(30μg/ ml),但不是蛋白酶K,显着抑制生物膜形成(19%抑制)。治疗铜绿假单胞菌的24小时常见的生物膜与大肠杆菌和头孢噻肟的最小抑制浓度(MIC)和头孢噻肟的50倍显着降低了Biofilm Mass,分别将生物膜质量显着降低32.8%和44%。此外,与溶菌酶的暴露或抗菌暴露相比,将24小时铜绿假单胞菌(30μg/ ml)和50次MIC的暴露于溶菌酶(30μg/ ml)和50次麦芽糖麦芽糖导致生物膜质量的显着降低。单独的代理人。用溶菌酶(30μg/ ml)和50倍MIC的头孢噻肟的组合观察到最佳抗抗膜效应(49.3%)。在用50倍的CeTtazidime或Cefepime或与溶菌酶(30μg/ ml的组合的MIC处理后观察到的有前途的抗生素活性表明在血管内装置和隐形眼镜中消除假致生物膜的新策略。

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