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开发一种体外模型以测试治疗椎间盘退变新疗法的疗效。

Development of an in vitro model to test the efficacy of novel therapies for IVD degeneration.

作者信息

Le Maitre Christine L, Fotheringham Andrew P, Freemont Anthony J, Hoyland Judith A

机构信息

Biomedical Research Centre, Biosciences, Sheffield Hallam University, City Campus, Owen Building, Howard Street, Sheffield S1 1WB, UK.

出版信息

J Tissue Eng Regen Med. 2009 Aug;3(6):461-9. doi: 10.1002/term.180.

Abstract

Low back pain (LBP) is a major cause of disability worldwide that has been linked to intervertebral disc (IVD) degeneration. An improved understanding of the pathogenesis of disc degeneration is now developing, which is leading to the development of a number of possible future therapies targeted at the underlying pathology and regeneration strategies. Although results thus far are promising, the investigation of such therapies in an environment that mimics the mechanical environment of the human disc in vivo is problematic. The development of an in vitro model system that can maintain metabolically active IVD tissue within a loading environment pertaining to that of the human spine is crucial for testing the efficacy of future cell-based and tissue-engineering therapies for IVD degeneration. Here, using our novel loading rig, capable of mimicking the loading environment experienced within the human spine, we have cultured nucleus pulposus tissue explants, applied a daily hydrostatic loading regime for up to 2 weeks and investigated proteoglycan retention, metabolic activity and cellular phenotype. IVD tissue cultured under a loading environment pertaining to the in vivo loading environment maintained metabolic cell activity, proteoglycan content and cellular phenotype. Indeed, all parameters were improved in IVD tissue cultured with load compared to unloaded controls. Such a model is invaluable for investigations assessing the feasibility and efficacy of future therapeutic approaches to inhibiting degeneration or stimulating regeneration of the IVD, where the in vivo loading environment may be crucial to their success or failure.

摘要

下背痛(LBP)是全球致残的主要原因,与椎间盘(IVD)退变有关。目前人们对椎间盘退变的发病机制有了更深入的了解,这促使了一些针对潜在病理和再生策略的未来可能疗法的发展。尽管目前的结果很有前景,但在模拟人体椎间盘体内力学环境的条件下研究此类疗法存在问题。开发一种能够在与人类脊柱相关的加载环境中维持代谢活跃的IVD组织的体外模型系统,对于测试未来基于细胞和组织工程的IVD退变疗法的疗效至关重要。在此,我们使用能够模拟人体脊柱内加载环境的新型加载装置,培养了髓核组织外植体,施加了长达2周的每日静水压力加载方案,并研究了蛋白聚糖保留、代谢活性和细胞表型。在与体内加载环境相关的加载环境下培养的IVD组织保持了代谢细胞活性、蛋白聚糖含量和细胞表型。事实上,与未加载的对照组相比,加载培养的IVD组织中所有参数都有所改善。这样的模型对于评估未来抑制IVD退变或刺激其再生的治疗方法的可行性和疗效的研究非常宝贵,因为体内加载环境可能对其成败至关重要。

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