首页> 美国卫生研究院文献>PLoS Clinical Trials >Circulating Protein Fragments of Cartilage and Connective Tissue Degradation Are Diagnostic and Prognostic Markers of Rheumatoid Arthritis and Ankylosing Spondylitis
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Circulating Protein Fragments of Cartilage and Connective Tissue Degradation Are Diagnostic and Prognostic Markers of Rheumatoid Arthritis and Ankylosing Spondylitis

机译:软骨循环蛋白片段和结缔组织降解是类风湿关节炎和强直性脊柱炎的诊断和预后标志

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摘要

Inflammation driven connective tissue turnover is key in rheumatic diseases, such as ankylosing spondylitis (AS). Few biomarkers are available for measuring disease prognosis or the efficacy of interventions applied in these tissue-related conditions. Type II collagen is the primary structural protein of cartilage and type III collagen of connective tissues, and obvious targets for the collagenalytic, which increase during tissue inflammation. The objective of the study was to investigate the diagnostic and prognostic utility of cartilage, C2M, and synovial, C3M, turnover biomarkers in AS. Serum samples were retrieved from patients suffering from AS (n = 103), RA (n = 47) and healthy controls (n = 56). AS progressors were defined as having new vertebral syndesmophytes or more that 3 unit change in mSASSS over a two-year period. Type II collagen degradation markers in serum were measured by the C2M ELISA, and type III collagen degradation by the C3M ELISA. Logistic regression and dichotomized decision tree were used to analyze the prognostic value of the markers individually or in combination. Both C2M and C3M levels were significantly higher in RA patients than in healthy controls (p<0.0001). Diagnostic utility was analyzed by ROC and areas under the curve (AUCs) were 72% and 89% for C2M and C3M, respectively. Both C2M and C3M, were significantly higher in serum samples from AS patient than from healthy controls (p<0.0001). The AUCs of C2M and C3M, respectively, were 70% and 81% for AS. A combination of C2M and C3M, dichotomized according to best cut-offs for individual markers, could correctly identify 80% of the progressors and 61% of the non-progressors. The present study is the first to show that specific biomarkers of cartilage and connective tissue degradation facilitate both diagnosis and prediction of progression of RA and AS.
机译:炎症驱动的结缔组织更新是风湿性疾病(例如强直性脊柱炎(AS))的关键。很少有生物标志物可用于测量疾病预后或在这些组织相关病症中应用干预措施的功效。 II型胶原蛋白是结缔组织软骨的主要结构蛋白和结缔组织的III型胶原蛋白,是胶原分解的明显靶标,在组织炎症过程中会增加。这项研究的目的是调查软骨,C2M和滑膜,C3M,周转生物标志物在AS中的诊断和预后效用。从患有AS(n = 103),RA(n = 47)和健康对照(n = 56)的患者中获取血清样品。 AS进展者的定义是在两年的时间内mSASSS中有新的椎间突或超过3个单位的变化。通过C2M ELISA测定血清中的II型胶原降解标记,并通过C3M ELISA测定III型胶原降解。使用逻辑回归和二分决策树分析标记物的单独或组合的预后价值。 RA患者的C2M和C3M水平均显着高于健康对照组(p <0.0001)。通过ROC分析了诊断效用,C2M和C3M的曲线下面积(AUC)分别为72%和89%。 AS患者血清样品中的C2M和C3M均显着高于健康对照者(p <0.0001)。对于AS,C2M和C3M的AUC分别为70%和81%。 C2M和C3M的组合(根据单个标记的最佳分界线分为两部分)可以正确识别80%的进展者和61%的非进展者。本研究是第一个显示软骨和结缔组织降解的特定生物标志物有助于RA和AS的诊断和预测进展的研究。

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