首页> 外文期刊>The Journal of rheumatology >Effects of etanercept on serum biochemical markers of cartilage metabolism in patients with spondyloarthropathy.
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Effects of etanercept on serum biochemical markers of cartilage metabolism in patients with spondyloarthropathy.

机译:依那西普对脊椎关节炎患者软骨代谢血清生化指标的影响。

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OBJECTIVE: Anti-tumor necrosis factor (TNF) therapies provide symptomatic benefit in patients with spondyloarthropathy (SpA). Their effect on structural lesions has not yet been assessed. Biochemical markers of cartilage turnover revealing type II collagen degradation and synthesis are associated with joint damage in rheumatoid arthritis; their role in SpA is unknown. We describe the effects of etanercept on biochemical markers of type II collagen synthesis and degradation in patients with SpA followed for 2 years. METHODS: A total of 29 patients with SpA aged 22-68 years were included in a prospective 2-year study. Each patient received etanercept (25 mg twice a week) because of active disease despite optimal treatment. Cartilage degradation was investigated by measuring serum levels of the type II collagen fragments Helix-II and C2C, whereas the C-terminal propeptide of type II collagen (PIICP) was used as a marker of type II collagen synthesis. These markers were measured at baseline and after 1, 3,6, 12, and 24 months of treatment. RESULTS: Over 2 years, there was a significant decrease of serum C2C (p = 0.0035 by repeated Friedman's test) and serum Helix-II (p = 0.004). Compared to baseline, the decrease of serum C2C was significant at Month 12 (-12.1%; p = 0.004), whereas the decrease of serum Helix-II was observed as early as 1 month (-18.1%; p = 0.015) after start of therapy, reaching a maximum decrease of -33.4% (p = 0.0079) at Month 12. Conversely, PIICP increased significantly by 17% (p = 0.006) at 24 months. CONCLUSION: These data suggest that etanercept may have beneficial effects on cartilage metabolism in patients with SpA.
机译:目的:抗肿瘤坏死因子(TNF)治疗可为脊柱关节炎(SpA)的患者带来症状。尚未评估其对结构性病变的影响。类风湿关节炎的关节损伤与软骨周转的生化标志物揭示II型胶原蛋白的降解和合成有关。它们在SpA中的作用尚不清楚。我们描述依那西普对SpA患者随访2年的II型胶原合成和降解的生化标志物的影响。方法:前瞻性两年研究共纳入29例22-68岁的SpA患者。尽管进行了最佳治疗,但由于活动性疾病,每位患者均接受依那西普(25毫克每周两次)治疗。通过测量II型胶原蛋白片段Helix-II和C2C的血清水平研究了软骨的降解,而II型胶原蛋白的C末端前肽(PIICP)被用作II型胶原蛋白合成的标志物。这些标记物是在基线以及治疗1、3、6、12和24个月后测量的。结果:在过去的两年中,血清C2C(通过重复的弗里德曼检验(Priedman's test),p = 0.0035)和血清Helix-II(p = 0.004)显着降低。与基线相比,在第12个月时血清C2C下降显着(-12.1%; p = 0.004),而在开始后1个月就观察到血清Helix-II下降(-18.1%; p = 0.015)。的治疗,在第12个月达到最大降低-33.4%(p = 0.0079)。相反,PIICP在24个月时显着增加了17%(p = 0.006)。结论:这些数据表明依那西普可能对SpA患者的软骨代谢产生有益作用。

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