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软骨周转率高的骨关节炎患者对硫酸葡萄糖胺的软骨保护作用反应性增强。

Osteoarthritic patients with high cartilage turnover show increased responsiveness to the cartilage protecting effects of glucosamine sulphate.

作者信息

Christgau S, Henrotin Y, Tankó L B, Rovati L C, Collette J, Bruyere O, Deroisy R, Reginster J Y

机构信息

Nordic Bioscience A/S, Herlev, Denmark.

出版信息

Clin Exp Rheumatol. 2004 Jan-Feb;22(1):36-42.

Abstract

OBJECTIVE

Glucosamine sulphate has been shown in a large double-blind, placebo-controlled clinical trial to prevent structural damage and improve clinical symptoms of osteoarthritis (OA). We investigated whether early response in a newly developed biochemical marker of collagen type II degradation (CTX-II, CartiLaps ELISA) could reflect the long-term preservation of hyaline cartilage.

METHODS

Study subjects comprised 212 knee OA patients participating in a clinical trial of the effects of glucosamine sulphate. Disease symptoms were assessed quarterly by WOMAC scoring and X-ray analysis was performed at baseline and after 3 years. Urine samples were obtained at baseline and after 1, 2 and 3 years for measurement in the CartiLaps assay. The measurements were corrected for creatinine.

RESULTS

At baseline the patients had an average concentration of urinary CTX-II of 222.4 +/- 159.5 ng/mmol creatinine. This was significantly above the CTX-II levels measured in urine samples from 415 healthy controls (169.1 +/- 92.3 ng/mmol, p < 0.0001). There was no significant difference in the CTX-II response in the placebo group and the glucosamine treated group. However, those with high cartilage turnover presented a significant decrease in CTX-II after 12-month glucosamine treatment. Thus, three group with CTX II concentrations above normal average + 1SD decreased 15.5% after 12-month therapy. The 12 months change in CTX-II in OA patients with elevated CTX-II at baseline correlated with the change in average joint space width observed after 36 months (R = 0.43, p < 0.05). Increased baseline levels of CTX-II were associated with a worsening of the WOMAC index (p < 0.01).

CONCLUSION

The data indicate that measurement of urinary collagen type II C-telopeptide fragments enables the identification of OA patients with high cartilage turnover who at the same time are most responsive to therapy with structure modifying drugs.

摘要

目的

在一项大型双盲、安慰剂对照临床试验中已表明,硫酸氨基葡萄糖可预防骨关节炎(OA)的结构损伤并改善其临床症状。我们研究了新开发的II型胶原降解生化标志物(CTX-II,软骨检测酶联免疫吸附测定法)的早期反应是否能反映透明软骨的长期保存情况。

方法

研究对象包括212名参与硫酸氨基葡萄糖疗效临床试验的膝骨关节炎患者。每季度通过西安大略和麦克马斯特大学骨关节炎指数(WOMAC)评分评估疾病症状,并在基线和3年后进行X线分析。在基线以及1年、2年和3年后采集尿液样本,用于软骨检测分析。测量结果用肌酐进行校正。

结果

在基线时,患者尿CTX-II的平均浓度为222.4±159.5 ng/mmol肌酐。这显著高于415名健康对照者尿液样本中测得的CTX-II水平(169.1±92.3 ng/mmol,p<0.0001)。安慰剂组和氨基葡萄糖治疗组的CTX-II反应无显著差异。然而,软骨转换率高的患者在接受12个月氨基葡萄糖治疗后,CTX-II显著下降。因此,CTX-II浓度高于正常平均值+1标准差的三组患者在12个月治疗后下降了15.5%。基线时CTX-II升高的OA患者12个月内CTX-II的变化与36个月后观察到的平均关节间隙宽度变化相关(R=0.43,p<0.05)。CTX-II基线水平升高与WOMAC指数恶化相关(p<0.01)。

结论

数据表明,检测尿II型胶原C末端肽片段能够识别软骨转换率高的OA患者,这些患者同时对结构改善药物治疗反应最为敏感。

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