含利福平复合物的加工和体外持续释放以增强骨髓炎的治疗。

Biomatter Pub Date : 2012-10-01 DOI:10.4161/biom.22793
Niina Ahola, Minna Veiranto, Noora Männistö, Matti Karp, Jaana Rich, Alexander Efimov, Jukka Seppälä, Minna Kellomäki
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引用次数: 11

摘要

这项研究的目的是开发一种骨导电性、可生物降解和释放利福平的骨填充复合材料,用于治疗骨髓炎,这是一种非常困难和昂贵的骨细菌感染。复合材料将与环丙沙星释放复合材料一起使用,因为当利福平单独使用时,耐药细菌会迅速发展。采用双螺杆挤压法制备了三种复合材料。复合材料的聚合物基体为聚l -丙交酯-co-ε-己内酯)70/30,所有复合材料的利福平抗生素含量为8wt %(重量%)。复合材料的β-TCP含量分别为0 wt%、50 wt%和60 wt%。在体外降解和药物释放试验前,对复合材料进行γ辐照灭菌。所研究的复合材料的水解降解速度快,聚合物组分的分子量迅速下降。利福平的释放分4个相,样品中β-TCP的高含量、聚合物的降解和质量损失都是决定其释放相的因素。陶瓷成分被认为对药物释放有积极的影响。含有50% β-TCP的复合物显示出最有希望的利福平释放谱,并显示出对一种常见的铜绿假单胞菌的活性。16 h后形成明显的抑制带。总的来说,所测试的材料显示出与环丙沙星释放材料联合开发成治疗骨髓炎或其他骨相关感染的骨填充材料的巨大潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Processing and sustained in vitro release of rifampicin containing composites to enhance the treatment of osteomyelitis.

Processing and sustained in vitro release of rifampicin containing composites to enhance the treatment of osteomyelitis.

Processing and sustained in vitro release of rifampicin containing composites to enhance the treatment of osteomyelitis.

Processing and sustained in vitro release of rifampicin containing composites to enhance the treatment of osteomyelitis.

The objective in this study was to develop an osteoconductive, biodegradable and rifampicin releasing bone filling composite material for the treatment of osteomyelitis, a bacterial infection of bone that is very difficult and expensive to treat. The composite material will be used together with a ciprofloxacin releasing composite, because of the rapid development of resistant bacteria when rifampicin is used alone. Three composites were manufactured by twin-screw extrusion. The polymer matrix for the composites was poly(L-lactide-co-ε-caprolactone) 70/30 and all the composites contained 8 wt% (weight percent) of rifampicin antibiotic. The β-TCP contents of the composites were 0 wt%, 50 wt% and 60 wt%. The composites were sterilized by gamma irradiation before in vitro degradation and drug release tests. The hydrolytical degradation of the studied composites proceeded quickly and the molecular weight of the polymer component of the composites decreased rapidly. Rifampicin release occurred in four phases in which the high β-TCP content of the samples, polymer degradation and mass loss all played a role in determining the phases. The ceramic component was seen to have a positive effect on the drug release. The composite with 50 wt% of β-TCP showed the most promising rifampicin release profile and it also showed activity against a common osteomyelitis causing bacteria Pseudomonas aeruginosa. A clear inhibition zone was formed in 16 h incubation. Overall, the tested materials showed great potential to be developed into a bone filler material for the treatment of osteomyelitis or other bone related infections in combination with the ciprofloxacin releasing materials.

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