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首页> 外文期刊>Acta biomaterialia >Sensitizing bacterial cells to antibiotics by shape recovery triggered biofilm dispersion
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Sensitizing bacterial cells to antibiotics by shape recovery triggered biofilm dispersion

机译:通过形状恢复使细菌细胞敏感到抗生素触发的生物膜分散体

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Microbial biofilms are a leading cause of chronic infections in humans and persistent biofouling in industries due to extremely high-level tolerance of biofilm cells to antimicrobial agents. Eradicating mature biofilms is especially challenging because of the protection of the extracellular matrix and slow growth of biofilm cells. Recently, we reported that established biofilms can be effectively removed (e.g. 99.9% dispersion of 48 h Pseudomonas aeruginosa PAO1 biofilms) by shape memory polymer-based dynamic changes in surface topography. Here, we demonstrate that such biofilm dispersion also sensitizes biofilm cells to conventional antibiotics. For example, shape recovery in the presence of 50 mu g/mL tobramycin reduced biofilm cell counts by more than 3 logs (2,479-fold) compared to the static flat control. The observed effects were attributed to the disruption of biofilm structure and increase in cellular activities as evidenced by an 11.8-fold increase in intracellular level of adenosine triphosphate (ATP), and 4.1-fold increase in expression of the rrnB gene in detached cells. These results can help guide the design of new control methods to better combat biofilm associated antibiotic-resistant infections.
机译:微生物生物膜是由于生物膜细胞极高耐受性抗微生物剂的行业中的人类和持续生物污染的慢性感染的主要原因。由于保护细胞外基质和生物膜细胞缓慢的缓慢,消除成熟生物膜尤其具有挑战性。最近,我们报道了通过形状的基于记忆聚合物的表面形貌的动态变化,可以有效地除去已建立的生物膜(例如,48h假单胞菌Aeruginosa Pao1 Biofilms的分散体积99.9%。在这里,我们证明这种生物膜分散体也使生物膜细胞敏化至常规抗生素。例如,与静态平面控制相比,在50μg/ ml筛选中,在50μmg/ ml霉霉蛋白的存在下,将生物膜细胞减少超过3个原木(2,479倍)。观察到的效果归因于生物膜结构的破坏,并且细胞活性的增加,如脱磷酸三磷酸腺苷(ATP)的细胞内水平的11.8倍的增加,和4.1倍的拆开细胞中的RRNB基因表达的增加。这些结果可以帮助指导新的控制方法设计,以更好地打击生物膜相关的抗生素抗性感染。

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