| Autor: |
Doroshenko, Natalya, Tseng, Boo Shan, Howlin, Robert P., Deacon, Jill, Wharton, Julian A., Thurner, Philipp J., Gilmore, Brendan F., Parsek, Matthew R., Stoodley, Paul |
| Zdroj: |
Antimicrobial Agents and Chemotherapy; September 2014, Vol. 58 Issue: 12 p7273-7282, 10p |
| Abstrakt: |
ABSTRACTStaphylococcus epidermidisbiofilm formation is responsible for the persistence of orthopedic implant infections. Previous studies have shown that exposure of S. epidermidisbiofilms to sub-MICs of antibiotics induced an increased level of biofilm persistence. BODIPY FL-vancomycin (a fluorescent vancomycin conjugate) and confocal microscopy were used to show that the penetration of vancomycin through sub-MIC-vancomycin-treated S. epidermidisbiofilms was impeded compared to that of control, untreated biofilms. Further experiments showed an increase in the extracellular DNA (eDNA) concentration in biofilms preexposed to sub-MIC vancomycin, suggesting a potential role for eDNA in the hindrance of vancomycin activity. Exogenously added, S. epidermidisDNA increased the planktonic vancomycin MIC and protected biofilm cells from lethal vancomycin concentrations. Finally, isothermal titration calorimetry (ITC) revealed that the binding constant of DNA and vancomycin was 100-fold higher than the previously reported binding constant of vancomycin and its intended cellular d-Ala-d-Ala peptide target. This study provides an explanation of the eDNA-based mechanism of antibiotic tolerance in sub-MIC-vancomycin-treated S. epidermidisbiofilms, which might be an important factor for the persistence of biofilm infections. |
| Databáze: |
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