首页> 外文期刊>Arthritis and Rheumatism >The combination of the biomarkers urinary C-terminal telopeptide of type II collagen, serum cartilage oligomeric matrix protein, and serum chondroitin sulfate 846 reflects cartilage damage in hemophilic arthropathy.
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The combination of the biomarkers urinary C-terminal telopeptide of type II collagen, serum cartilage oligomeric matrix protein, and serum chondroitin sulfate 846 reflects cartilage damage in hemophilic arthropathy.

机译:II型胶原蛋白尿液C端端肽生物标志物,血清软骨低聚基质蛋白和血清硫酸软骨素846的组合反映了血友病性关节炎中的软骨损伤。

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OBJECTIVE: Hemophilic arthropathy, with characteristics of inflammatory (rheumatoid arthritis) and degenerative (osteoarthritis) joint damage, occurs at an early age, is associated with minor comorbidity, and is restricted to 3 pairs of large joints. The aim of this study was to determine whether commonly used serum and/or urinary biomarkers of cartilage and bone turnover for which assay kits are commercially available are associated with the severity of joint damage in patients with various degrees of hemophilic arthropathy and, thus, whether this disease could be useful in the identification and evaluation of such biomarkers. METHODS: Blood and urine samples were collected from 36 patients with various degrees of hemophilic arthropathy. Commercially available assays for the most frequently investigated serum and urine biomarkers were performed: urinary C-terminal telopeptide of type I collagen (CTX-I), urinary CTX-II, serum CTX-I, serum CTX-II, serum cartilage oligomeric matrix protein (COMP), serum cartilage cleavage products C1,2C and C2C, and serum chondroitin sulfate 846 (CS-846). Radiographs of the ankles, knees, and elbows in all patients were evaluated for the degree of joint damage according to the Pettersson score, which is based on cartilage and periarticular bone changes and is specific for hemophilic arthropathy. RESULTS: Urinary CTX-II, serum C1,2C, and serum CS-846 levels correlated with the overall Pettersson score and with the joint space narrowing component. Regression analysis showed that combined indexes of different markers increased the degree of correlation for the combination of urinary CTX-II, serum COMP, and serum CS-846. Bone-specific markers (urinary/serum CTX-I and serum C1,2C) did not correlate with specific bone-related items of the Pettersson score (osteoporosis and erosions). CONCLUSION: These results support the idea that a combination of biomarkers relates significantly better to the severity of joint damage than do individual biomarkers. The combination of urinary CTX-II, serum COMP, and serum CS-846 correlated best with the degree of arthropathy. Because of its specific characteristics and restricted involvement, hemophilic arthropathy may prove useful in the screening of newly developed biomarkers of joint damage.
机译:目的:血友病性关节炎,具有炎症性(类风湿关节炎)和变性性(骨关节炎)的特点,发生于儿童早期,伴有轻微合并症,仅限于三对大关节。这项研究的目的是确定市售测定试剂盒的常用软骨和/或骨代谢的血清和/或尿液生物标志物是否与各种程度的血友病性关节炎患者的关节损伤严重程度有关,因此,是否这种疾病可能有助于鉴定和评估此类生物标志物。方法:从36例不同程度的血友病性关节病患者中采集血液和尿液样本。对最常研究的血清和尿液生物标志物进行了市售化验:I型胶原的尿C端端肽(CTX-I),尿CTX-II,血清CTX-I,血清CTX-II,血清软骨寡聚基质蛋白(COMP),血清软骨裂解产物C1,2C和C2C,以及血清硫酸软骨素846(CS-846)。根据Pettersson评分评估所有患者的脚踝,膝盖和肘部X光片的关节损伤程度,该评分基于软骨和关节周围骨的变化,并且对血友病性关节病具有特异性。结果:尿CTX-II,血清C1,2C和血清CS-846水平与总体Pettersson评分和关节间隙变窄相关。回归分析表明,不同标志物的综合指标增加了尿CTX-II,血清COMP和血清CS-846的相关度。骨特异性标志物(尿/血清CTX-1和血清C1,2C)与Pettersson评分的特定骨相关项目(骨质疏松和糜烂)不相关。结论:这些结果支持这样的观点,即生物标志物的组合与关节损伤严重程度的关系比单个生物标志物明显更好。尿液CTX-II,血清COMP和血清CS-846的组合与关节病的程度最相关。由于其特殊的特性和有限的参与,血友病性关节炎可能被证明可用于筛选新开发的关节损伤生物标志物。

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