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首页> 外文期刊>FEBS Open Bio >A dual PMMA/calcium sulfate carrier of vancomycin is more effective than PMMA‐vancomycin at inhibiting Staphylococcus?aureus growth in?vitro
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A dual PMMA/calcium sulfate carrier of vancomycin is more effective than PMMA‐vancomycin at inhibiting Staphylococcus?aureus growth in?vitro

机译:在抑制葡萄球菌的葡萄球菌上的PMMA-VANCOMCIN更有效的双PMMA /硫酸钙载体更有效?

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Both antibiotic‐impregnated poly(methyl acrylate, methyl methacrylate) (PMMA) and antibiotic‐impregnated calcium sulfate have been successfully used as local antibiotic delivery vehicles for the management of chronic osteomyelitis. Here, we examined the antibiotic elution characteristics and antibacterial properties of a composite drug delivery system consisting of PMMA/calcium sulfate carrying vancomycin (dual carrier‐v) against Staphylococcus?aureus , with PMMA loaded with vancomycin (PMMA‐v) as a control. Vancomycin gradually degraded from dual carrier‐v and PMMA‐v up to about 8 and 6?weeks, respectively. At different elution time points, the inhibition zones of the dual carrier‐v were larger than the inhibition zones of the PMMA‐v ( P ?0.05). The colony inhibition rate of the dual carrier‐v was 95.57%, whereas it was 77.87% for PMMA‐v. Scanning electron microscopy was used to demonstrate biofilm formation on the surface of plates treated with vancomycin‐unloaded PMMA, whereas there was no biofilm formation on the surface of plates treated with dual carrier‐v or PMMA‐v. The dual carrier‐v was more effective at antibacterial adhesion at each time point after immersion in simulated body fluid as compared with PMMA‐v ( P ?0.05). In conclusion, our results suggest that the dual carrier‐v can release higher concentrations of antibiotics and inhibit bacteria growth more effectively in?vitro as compared with PMMA‐v. The dual carrier‐v thus may have potential as an alternative strategy for osteomyelitis management.
机译:抗生素浸渍的聚(丙烯酸甲酯,甲基丙烯酸甲酯)(PMMA)和抗生素浸渍的硫酸钙已成功用作急性骨髓炎的局部抗生素递送载体。在这里,我们研究了由对葡萄球菌(双载体-V)的PMMA /硫酸钙含有对葡萄球菌(双载体-V)组成的复合药物输送系统的抗生素洗脱特性和抗菌性质,用Vancomycin(PMMA-V)负载的PMMA作为对照。万古霉素分别从双载体-V和PMMA-v逐渐降解,分别为约8和6?周。在不同的洗脱时间点,双载体-V的抑制区大于PMMA-V的抑制区(P <0.05)。双载体-V的菌落抑制率为95.57%,而PMMA-V为77.87%。扫描电子显微镜用于在用万古霉素 - 卸载的PMMA处理的平板表面上显示生物膜形成,而用双载体-V或PMMA-V处理的平板表面没有生物膜形成。与PMMA-V相比,双载体-V在浸没在模拟体液中的每次时的抗菌粘附性更有效(P <0.05)。总之,我们的结果表明,与PMMA-V相比,双载体-V可以更有效地释放出更高浓度的抗生素并抑制细菌生长。因此,双载体-V可能具有作为骨髓炎管理的替代策略。

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