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首页> 外文期刊>Journal of orthopaedic research >Microencapsulation of rifampicin: A technique to preserve the mechanical properties of bone cement
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Microencapsulation of rifampicin: A technique to preserve the mechanical properties of bone cement

机译:利福平的微胶囊化:一种保持骨水泥机械性能的技术

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Two-stage exchange with antibiotic-loaded bone cement spacers remains the gold standard for chronic periprosthetic joint infection (PJI). Rifampicin is highly efficient on stationary-phase staphylococci in biofilm; however, its addition to PMMA to manufacture spacers prevents polymerization and reduces mechanical properties. Isolation of rifampicin during polymerization by microencapsulation could allow manufacturing rifampicin-loaded bone cement maintaining elution and mechanical properties. Microcapsules of rifampicin with alginate, polyhydroxybutyratehydroxyvalerate (PHBV), ethylcellulose and stearic acid (SA) were synthesized. Alginate and PHBV microcapsules were added to bone cement and elution, compression, bending, hardness, setting time and microbiological tests were performed. Repeated measures ANOVA and Bonferroni post-hoc test were performed, considering a p0.05 as statistical significance. Bone cement specimens containing alginate microcapsules eluted more rifampicin than PHBV microcapsules or non-encapsulated rifampicin over time (p0.012). Microencapsulation of rifampicin allowed PMMA to preserve mechanical properties in compression and bending tests. Cement with alginate microcapsules showed similar behavior in hardness tests to control cement over the study period (73 +/- 1.68H(D)). PMMA with alginate microcapsules exhibited the largest zones of inhibition in microbiological tests. Statistically significant differences in mean diameters of zones of inhibition between PMMA loaded with alginate-rifampicin (p=0.0001) and alginate-PHBV microcapsules (p=0.0001) were detected. Rifampicin microencapsulation with alginate is the best choice to introduce rifampicin in PMMA preserving mechanical properties, setting time, elution, and antimicrobial properties. The main applicability of this study is the opportunity for obtaining rifampicin-loaded PMMA by microencapsulation of rifampicin in alginate microparticles, achieving high doses of rifampicin in infected tissues, increasing the successful of PJI treatment. (c) 2017 Orthopaedic Research Society. Published by Wiley Periodicals, Inc. J Orthop Res 36:459-466, 2018.
机译:含有抗生素的骨水泥间隔物的两级交换仍然是慢性跨越关节感染(PJI)的金标准。利福平在生物膜的固定相葡萄球菌上高效;然而,它添加到PMMA以制造间隔物防止聚合并降低机械性能。通过微胶囊化聚合过程中利福平的分离可以允许制造利福平装载的骨水泥保持洗脱和机械性能。合成了利福平的利福平,聚羟基丁酸盐羟基苯甲酸盐(PHBV),乙基纤维素和硬脂酸(SA)的微胶囊。藻酸盐和PHBV微胶囊加入骨水泥和洗脱,压缩,弯曲,硬度,设定时间和微生物测试。考虑到P <0.05作为统计显着性,进行重复措施Anova和Bonferroni后Hoc测试。含有藻酸盐微胶囊的骨水泥样本比pHBV微胶囊或非封装的利福平随时间洗脱更多的利福平细胞(P <0.012)。利福平的微胶囊储能允许PMMA保持压缩和弯曲试验中的机械性能。具有藻酸盐微胶囊的水泥在硬度试验中显示出类似的行为,以在研究期间控制水泥(73 +/- 1.68H(D))。具有藻酸盐微胶囊的PMMA表现出微生物试验中最大的抑制区域。检测到具有藻酸盐 - 利福平(P = 0.0001)和藻酸盐-PHBV微胶囊(P = 0.0001)的PMMA之间的抑制区的平均直径差异。利福平微胶囊含有藻酸盐是在PMMA中引入利福平的最佳选择,保存机械性能,设定时间,洗脱和抗微生物性能。本研究的主要适用性是通过在海藻酸盐微粒中通过利福平微脉状物获得利福平装载的PMMA的机会,在感染组织中达到高剂量的利福平,增加了PJI治疗的成功。 (c)2017年骨科研究会。由Wiley期刊出版,Inc.J Orthop Res 36:459-466,2018。

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