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首页> 外文期刊>FEMS Microbiology Letters >Antimicrobial activities of YycG histidine kinase inhibitors against Staphylococcus epidermidis biofilms
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Antimicrobial activities of YycG histidine kinase inhibitors against Staphylococcus epidermidis biofilms

机译:YycG组氨酸激酶抑制剂对表皮葡萄球菌生物膜的抗菌活性

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Staphylococcus epidermidis has become a significant pathogen causing infections due to biofilm formation on surfaces of indwelling medical devices. Biofilm-associated bacteria exhibit enhanced resistance to many conventional antibiotics. It is therefore, important to design novel antimicrobial reagents targeting S. epidermidis biofilms. In a static chamber system, the bactericidal effect of two leading compounds active as YycG inhibitors was assessed on biofilm cells by confocal laser scanning microscopy combined with viability staining. In young biofilms (6-h-old), the two compounds killed the majority ofthe embedded cells at concentrations of 100 mu M and 25 mu M, respectively. In mature biofilms (24-h-old), one compound was still effectively killing biofilm cells, whereas the other compound mainly killed cells located at the bottom of the biofilm. In contrast, vancomycin was found to stimulate biofilm development at the M13C (8 mu g mL(-1)). Even at a high concentration (128 mu g mL(-1)), vancomycin exhibited poor killing on cells embedded in biofilms. The two compounds exhibited faster and more effective killing of S. epidermidis planktonic cells than vancomycin at the early stage of exposure (6 h). The data suggest that the new inhibitors can serve as potential agents against S. epidermidis biofilms when added alone or in concert with other antimicrobial agents.
机译:表皮葡萄球菌已成为重要的病原体,由于留置医疗设备表面的生物膜形成而引起感染。生物膜相关细菌对许多常规抗生素表现出增强的抗性。因此,重要的是设计针对表皮葡萄球菌生物膜的新型抗菌剂。在静态室系统中,通过共聚焦激光扫描显微镜结合活力染色评估了两种作为YycG抑制剂活跃的主要化合物对生物膜细胞的杀菌作用。在年轻的生物膜(6小时大)中,这两种化合物分别以100μM和25μM的浓度杀死了大部分嵌入的细胞。在成熟的生物膜(24小时龄)中,一种化合物仍可有效杀死生物膜细胞,而另一种化合物主要杀死位于生物膜底部的细胞。相反,发现万古霉素可刺激M13C(8μg mL(-1))的生物膜发育。即使在高浓度(128μg mL(-1))下,万古霉素对嵌入生物膜的细胞也显示出不良的杀伤力。在暴露的早期阶段(6小时),这两种化合物显示出比万古霉素更快,更有效地杀死表皮葡萄球菌浮游细胞。数据表明,当单独或与其他抗微生物剂一起添加时,新抑制剂可作为对抗表皮葡萄球菌生物膜的潜在药物。

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