首页> 外文期刊>Osteoarthritis and cartilage >Relationships between biochemical markers of bone and cartilage degradation with radiological progression in patients with knee osteoarthritis receiving risedronate: the Knee Osteoarthritis Structural Arthritis randomized clinical trial.
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Relationships between biochemical markers of bone and cartilage degradation with radiological progression in patients with knee osteoarthritis receiving risedronate: the Knee Osteoarthritis Structural Arthritis randomized clinical trial.

机译:接受利塞膦酸盐治疗的膝骨关节炎患者的骨和软骨降解的生化标志物与放射学进展之间的关系:膝骨关节炎结构性关节炎随机临床试验。

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OBJECTIVE: To investigate whether early changes in biochemical markers of bone (NTX-I) and cartilage (CTX-II [C-terminal crosslinking telopeptide of type II collagen]) degradation are associated with radiological progression in patients with knee osteoarthritis (OA) receiving risedronate. DESIGN: Two thousand four hundred and eighty three patients with medial compartment knee OA were randomized in two 24-month studies in North America (NA) and European Union (EU). Studies evaluated risedronate 5mg/day, 35mg/week (EU), 50mg/week (NA), and 15mg/day (NA and EU), compared to placebo in reducing signs and symptoms and in slowing radiographic progression. One thousand eight hundred and eighty five patients from the pooled EU and NA studies with available NTX-I/CTX-II at both baseline and 6 months and radiographs at baseline and at 24 months were analyzed. RESULTS: Risedronate produced a dose-dependent reduction of NTX-I and CTX-II observed at 6 months which continued up to 24 months. Patients who had CTX-II levels returned to low levels (<150ng/mmol creatinine) at 6 months had a lower risk of radiographic progression at 24 months than patients whose CTX-II levels were increased both at baseline and 6 months [odds-ratio (95% confidence interval): 0.57 (0.39-0.85) after adjustment for demographics and joint space width]. The lowest risk of progression was observed in patients who had low CTX-II levels both at baseline and at 6 months [odds-ratio 0.36 (0.21-0.63)]. No significant association between NTX-I levels and radiological progression was observed. CONCLUSION: CTX-II decreased with risedronate in patients with knee OA and levels reached after 6 months were associated with radiological progression at 24 months. Monitoring a marker of cartilage degradation 6 months after initiating treatment may be instructive in identifying patients with low progression.
机译:目的:研究接受膝骨关节炎(OA)的患者骨(NTX-I)和软骨(CTX-II [II型胶原的C端交联端肽]]的生化标志的早期变化是否与放射学进展有关利塞膦酸盐。设计:在北美洲(NA)和欧盟(EU)的两项为期24个月的研究中,将243例内侧膝关节OA患者随机分配。与安慰剂相比,研究评估了利舍膦酸盐5mg /天,35mg /周(EU),50mg /周(NA和EU)和15mg /天(NA和EU)与安慰剂相比,在减轻体征和症状以及放慢影像学进展方面的作用。分析了来自欧盟和北美研究的185例患者,在基线和6个月时都有可用的NTX-I / CTX-II,并对基线和24个月时的X光片进行了分析。结果:瑞斯膦酸钠在6个月时观察到剂量依赖性的NTX-I和CTX-II减少,持续到24个月。与基线和6个月时CTX-II水平均升高的患者相比,CTX-II水平在6个月恢复至低水平(<150ng / mmol肌酐)的患者在24个月时的影像学进展风险较低。 (95%置信区间):根据人口统计和关节间隙宽度调整后为0.57(0.39-0.85)。在基线和6个月时CTX-II水平低的患者中进展风险最低[比值比为0.36(0.21-0.63)]。没有观察到NTX-1水平与放射学进展之间的显着关联。结论:膝骨关节炎患者中,利塞膦酸盐的CTX-II水平降低,且6个月后达到的水平与24个月时的放射学进展有关。在开始治疗后6个月监测软骨降解的标志物可能对鉴别低进展的患者有指导意义。

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