首页> 外文期刊>The Journal of arthroplasty >Particle bioreactivity and wear-mediated osteolysis.
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Particle bioreactivity and wear-mediated osteolysis.

机译:颗粒生物反应性和磨损介导的骨溶解。

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摘要

This review focuses on wear debris-mediated osteolysis, a major factor compromising the long-term success of total joint arthroplasty. Studies on retrieved implants and animal models, as well as in vitro studies on particle bioreactivity, suggest that wear-mediated periprosthetic osteolysis is unlikely to be caused solely by 1 particular cell type or particulate species, but is rather the cumulative consequence of a number of biological reactions. Our recent findings suggest 3 novel mechanisms of particle bioreactivity that may contribute to osteolysis: 1) exacerbated inflammation caused by elevated reactive oxygen species production by activated macrophages and osteoclasts, (2) impaired periprosthetic bone formation secondary to disrupted osteogenesis, and (3) compromised bone regeneration resulting from increased cytotoxic response of mesenchymal osteoprogenitor cells. Understanding the pathogenesis of wear-mediated osteolysis is needed to improve orthopedic implant biocompatibility and wear reduction, and to develop effective pharmacotherapies.
机译:这篇综述的重点是磨损碎片介导的骨溶解,这是影响全关节置换术长期成功的主要因素。对取回的植入物和动物模型的研究以及对颗粒生物反应性的体外研究表明,磨损介导的假体周围骨质溶解不太可能仅由一种特定的细胞类型或颗粒种类引起,而是许多特定类型的细胞或颗粒物的累积结果。生物反应。我们最近的发现表明3种可能导致骨溶解的新型生物反应机制:1)活化的巨噬细胞和破骨细胞增加了活性氧产生的炎症,加剧了炎症;(2)继发于成骨作用的假体周围骨形成受损;(3)受损间充质骨祖细胞的细胞毒性反应增强导致骨骼再生。需要了解磨损介导的骨溶解的发病机理,以改善骨科植入物的生物相容性和减少磨损,并开发有效的药物疗法。

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