首页> 外文期刊>Annals of the Rheumatic Diseases: A Journal of Clinical Rheumatology and Connective Tissue Research >Induction therapy with a combination of DMARDs is better than methotrexate monotherapy: First results of the tREACH trial
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Induction therapy with a combination of DMARDs is better than methotrexate monotherapy: First results of the tREACH trial

机译:结合DMARD的诱导治疗优于甲氨蝶呤单药治疗:tREACH试验的首个结果

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Objective: To determine the most effective induction disease-modifying antirheumatic drug (DMARD) strategy in early rheumatoid arthritis (RA), second to compare one single dose of intramuscular glucocorticoids (GCs) with daily oral GCs during the induction phase. Methods: The 3-month data of a single-blinded clinical trial in patients with recent-onset arthritis (tREACH) were used. Patients were included who had a high probability (>70%) of progressing to persistent arthritis, based on the prediction model of Visser. Patients were randomised into three induction therapy strategies: (A) combination therapy (methotrexate (MTX) + sulfasalazine + hydroxychloroquine) with GCs intramuscularly; (B) combination therapy with an oral GC tapering scheme and (C) MTX with oral GCs similar to B. A total of 281 patients were randomly assigned to strategy (A) (n=91), (B) (n=93) or (C) (n=97). Results: The Disease Activity Score (DAS) after 3 months was lower in patients receiving initial combination therapy than in those receiving MTX monotherapy (0.39 (0.67 to 0.11, 95% CI)). DAS did not differ between the different GC bridging treatments. After 3 months 50% fewer biological agents were prescribed in the combination therapy groups. Although the proportion of patients with medication adjustments differed significantly between the treatment arms, no differences were seen in these adjustments due to adverse events after stratification for drug. Conclusion: Triple DMARD induction therapy is better than MTX monotherapy in early RA. Furthermore, no differences were seen in medication adjustments due to adverse events after stratification for drug. Intramuscular and oral GCs are equally effective as bridging treatments and both can be used.
机译:目的:确定早期类风湿关节炎(RA)中最有效的诱导疾病改变型抗风湿药(DMARD)策略,其次是比较在诱导期将单剂量肌注糖皮质激素(GC)与每日口服GC进行比较。方法:使用最近发作的关节炎(tREACH)患者的单盲临床试验的3个月数据。根据Visser的预测模型,纳入有发展为持续性关节炎的可能性很高(> 70%)的患者。将患者随机分为三种诱导治疗策略:(A)肌内联合应用GC联合治疗(甲氨蝶呤(MTX)+柳氮磺吡啶+羟氯喹); (B)采用口服GC渐缩方案的联合治疗,以及(C)使用与B类似的口服GC的MTX。总共281例患者被随机分配到策略(A)(n = 91),(B)(n = 93)或(C)(n = 97)。结果:接受初始联合治疗的患者3个月后的疾病活动评分(DAS)低于接受MTX单药治疗的患者(0.39(0.67至0.11,95%CI))。在不同的GC桥接处理之间,DAS没有差异。 3个月后,在联合治疗组中减少了50%的生物制剂处方。尽管在治疗组之间进行药物调整的患者比例存在显着差异,但由于药物分层后的不良事件,在这些调整中未见差异。结论:在早期RA中,三重DMARD诱导疗法优于MTX单一疗法。此外,由于药物分层后的不良事件,药物调整没有差异。肌内和口服GC与桥接治疗同样有效,两者均可使用。

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