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首页> 外文期刊>Acta biomaterialia >Effects of gentamicin and gentamicin-RGD coatings on bone ingrowth and biocompatibility of cementless joint prostheses: an experimental study in rabbits.
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Effects of gentamicin and gentamicin-RGD coatings on bone ingrowth and biocompatibility of cementless joint prostheses: an experimental study in rabbits.

机译:庆大霉素和庆大霉素-RGD涂层对非骨水泥关节假体的骨长入和生物相容性的影响:在兔中的实验研究。

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摘要

Antimicrobial coatings are of interest as a means to improve infection prophylaxis in cementless joint arthroplasty. However, those coatings must not interfere with the essential bony integration of the implants. Gentamicin-hydroxyapatite (gentamicin-HA) and gentamicin-RGD (arginine-glycine-aspartate)-HA coatings have recently been shown to significantly reduce infection rates in a rabbit infection prophylaxis model. The purpose of the current study was to investigate the in vitro elution kinetics and in vivo effects of gentamicin-HA and gentamicin-RGD-HA coatings on new bone formation, implant integration and biocompatibility in a rabbit model. In vitro elution testing showed that 95% and 99% of the gentamicin was released after 12 and 24 h, respectively. The in vivo study comprised 45 rabbits in total, with six animals for each of the gentamicin-HA, gentamicin-RGD-HA group and control pure HA coating groups for the 4 week time period, and nine animals for each of the three groups for the 12 week observation period. A 2.0 mm steel K-wire with one of the coatings under test was placed in the intramedullary canal of the tibia. After 4 and 12 weeks the tibiae were harvested and three different areas (proximal metaphysis, shaft area, distal metaphysis) were assessed by quantitative and qualitative histology for new bone formation, direct implant-bone contact and the formation of multinucleated giant cells. The results exhibited high standard deviations in all subgroups. There was a trend towards better bone formation and better direct implant contact in the pure HA coating group compared with both gentamicin coatings after 4 and 12 weeks, which was, however, not statistically significant. The number of multinucleated giant cells did not differ significantly between the three groups at both time points. In summary, both gentamicin coatings with 99% release of gentamicin within 24 h revealed good biocompatibility and bony integration, which was not statistically significant different compared with pure HA coating. Limitations of the study are the high standard deviation of the results and the limited number of animals per time point.
机译:抗菌涂层作为改善非骨水泥关节置换术中感染预防的手段而受到关注。但是,这些涂层不得干扰植入物的基本骨整合。庆大霉素-羟基磷灰石(庆大霉素-HA)和庆大霉素-RGD(精氨酸-甘氨酸-天冬氨酸)-HA涂层最近在兔感染预防模型中显示出大大降低了感染率。本研究的目的是研究庆大霉素-HA和庆大霉素-RGD-HA涂层对兔模型中新骨形成,植入物整合和生物相容性的体外洗脱动力学和体内作用。体外洗脱试验表明,分别在12和24小时后释放了95%和99%的庆大霉素。体内研究总共包括45只兔子,在4周的时间内,庆大霉素-HA,庆大霉素-RGD-HA组和对照组纯HA包被组各有6只动物,三组各有9只动物。 12周的观察期。将带有被测涂层之一的2.0 mm钢K线置于胫骨的髓内管中。 4和12周后,收集胫骨并通过定量和定性组织学评估三个不同的区域(近端干physi端,干区,远端干meta端),以评估新骨的形成,植入物与骨的直接接触以及多核巨细胞的形成。结果在所有亚组中均显示出高标准偏差。与庆大霉素涂层相比,纯HA涂层组在4周和12周后有更好的骨形成和更好的直接植入物接触的趋势,但是,这在统计学上并不显着。在两个时间点,三组之间的多核巨细胞数量没有显着差异。总之,两种庆大霉素涂层均在24小时内释放出99%的庆大霉素,显示出良好的生物相容性和骨整合性,与纯HA涂层相比在统计学上无显着差异。研究的局限性是结果的高标准偏差和每个时间点的动物数量有限。

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