首页> 外文期刊>Annals of the Rheumatic Diseases: A Journal of Clinical Rheumatology and Connective Tissue Research >Interactions between tenocytes and monosodium urate monohydrate crystals: Implications for tendon involvement in gout
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Interactions between tenocytes and monosodium urate monohydrate crystals: Implications for tendon involvement in gout

机译:肌腱细胞与尿酸钠一水合物晶体之间的相互作用:肌腱参与痛风的含义

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Objectives: Advanced imaging studies have demonstrated that urate deposition in periarticular structures, such as tendons, is common in gout. The aim of this study was to investigate the effects of monosodium urate monohydrate (MSU) crystals on tenocyte viability and function. Methods: The histological appearance of tendons in joints affected by advanced gout was examined using light microscopy. In vitro, colorimetric assays and flow cytometry were used to assess cell viability in primary rat and primary human tenocytes cultured with MSU crystals. Real-time PCR was used to determine changes in the relative mRNA expression levels of tendon-related genes, and Sirius red staining was used to measure changes in collagen deposition in primary rat tenocytes. Results: In joint samples from patients with gout, MSU crystals were identifi ed within the tendon, adjacent to and invading into tendon, and at the enthesis. MSU crystals reduced tenocyte viability in a dose-dependent manner. MSU crystals decreased the mRNA expression of tendon collagens, matrix proteins and degradative enzymes and reduced collagen protein deposition by tenocytes. Conclusions: These data indicate that MSU crystals directly interact with tenocytes to reduce cell viability and function. These interactions may contribute to tendon damage in people with advanced gout.
机译:目的:先进的影像学研究表明,痛风在尿道周围结构(如肌腱)中尿酸盐沉积很常见。这项研究的目的是调查尿酸一钠一水合物(MSU)晶体对肌腱细胞活力和功能的影响。方法:使用光学显微镜检查晚期痛风影响的关节中肌腱的组织学外观。在体外,用比色法和流式细胞仪评估了用MSU晶体培养的原代大鼠和原代人肌腱细胞的细胞活力。实时PCR用于确定肌腱相关基因的相对mRNA表达水平的变化,Sirius红染色用于测量原代大鼠肌腱细胞胶原沉积的变化。结果:在痛风患者的关节样本中,在肌腱内,肌腱附近并侵入肌腱以及在其上发现了MSU晶体。 MSU晶体以剂量依赖性方式降低肌腱细胞的生存能力。 MSU晶体降低了肌腱胶原蛋白,基质蛋白和降解酶的mRNA表达,并减少了肌腱细胞沉积的胶原蛋白。结论:这些数据表明MSU晶体直接与肌腱细胞相互作用,从而降低细胞活力和功能。这些相互作用可能导致痛风晚期的肌腱损伤。

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