Donahue Katrina E, Gartlehner Gerald, Jonas Daniel E, Lux Linda J, Thieda Patricia, Jonas Beth L, Hansen Richard A, Morgan Laura C, Lohr Kathleen N
University of North Carolina and Cecil G. Sheps Center for Health Services Research, Chapel Hill, North Carolina 27599, USA.
Ann Intern Med. 2008 Jan 15;148(2):124-34. doi: 10.7326/0003-4819-148-2-200801150-00192. Epub 2007 Nov 19.
The comparative effectiveness of rheumatoid arthritis therapies is uncertain.
To compare the benefits and harms of disease-modifying antirheumatic drugs (DMARDs) for adults with rheumatoid arthritis.
Records limited to the English language and studies of adults were identified by using MEDLINE, EMBASE, The Cochrane Library, and International Pharmaceutical Abstracts from 1980 to September 2007.
Two persons independently selected relevant head-to-head trials and prospective cohort studies with at least 100 participants and 12-week follow-up and relevant good- or fair-quality meta-analyses that compared benefits or harms of 11 drug therapies. For harms, they included retrospective cohort studies.
Information on study design, interventions, outcomes, and quality were extracted according to a standard protocol.
Head-to-head trials (n = 23), mostly examining synthetic DMARDs, showed no clinically important differences in efficacy among synthetic DMARDs (limited to methotrexate, leflunomide, and sulfasalazine) or among anti-tumor necrosis factor drugs (adalimumab, etanercept, and infliximab). Monotherapy with anti-tumor necrosis factor drugs resulted in better radiographic outcomes than did methotrexate but no important differences in clinical outcomes (for example, 20%, 50%, or 70% improvement according to American College of Rheumatology response criteria). Various combinations of biological DMARDs plus methotrexate improved clinical response rates and functional outcomes more than monotherapy with either methotrexate or biological DMARDs. In patients whose monotherapy failed, combination therapy with synthetic DMARDs improved response rates. Numbers and types of short-term adverse events were similar for biological and synthetic DMARDs. The evidence was insufficient to draw conclusions about differences for rare but serious adverse events for biological DMARDs.
Most studies were short-term efficacy trials conducted in selected populations with few comorbid conditions.
Limited available comparative evidence does not support one monotherapy over another for adults with rheumatoid arthritis. Although combination therapy is more effective for patients whose monotherapy fails, the evidence is insufficient to draw firm conclusions about whether one combination or treatment strategy is better than another or is the best treatment for early rheumatoid arthritis.
类风湿关节炎治疗方法的相对疗效尚不确定。
比较改善病情抗风湿药(DMARDs)对成年类风湿关节炎患者的益处和危害。
通过使用MEDLINE、EMBASE、Cochrane图书馆和国际药学文摘,检索1980年至2007年9月期间仅限于英文且针对成年人的研究记录。
两人独立选择相关的直接比较试验和前瞻性队列研究,这些研究至少有100名参与者且随访12周,以及比较11种药物疗法益处或危害的相关高质量或中等质量的荟萃分析。对于危害方面,纳入了回顾性队列研究。
根据标准方案提取有关研究设计、干预措施、结局和质量的信息。
直接比较试验(n = 23),大多研究合成DMARDs,结果显示合成DMARDs(限于甲氨蝶呤、来氟米特和柳氮磺胺吡啶)之间或抗肿瘤坏死因子药物(阿达木单抗、依那西普和英夫利昔单抗)之间在疗效上无临床重要差异。抗肿瘤坏死因子药物单药治疗比甲氨蝶呤产生更好的放射学结局,但在临床结局方面无重要差异(例如,根据美国风湿病学会反应标准改善20%、50%或70%)。生物DMARDs加甲氨蝶呤的各种联合治疗比甲氨蝶呤或生物DMARDs单药治疗能提高临床缓解率和功能结局。在单药治疗失败的患者中,合成DMARDs联合治疗可提高缓解率。生物和合成DMARDs的短期不良事件数量和类型相似。关于生物DMARDs罕见但严重不良事件的差异,证据不足,无法得出结论。
大多数研究是在合并症较少的特定人群中进行的短期疗效试验。
有限的现有比较证据不支持对成年类风湿关节炎患者采用一种单药治疗优于另一种。虽然联合治疗对单药治疗失败的患者更有效,但关于一种联合治疗或治疗策略是否优于另一种或是否是早期类风湿关节炎的最佳治疗方法,证据不足,无法得出确切结论。
