Induction of Cure in Early Arthritis (I CEA): study protocol for an investigator-initiated randomized single-blind clinical trial with open-label extension to compare three treatment strategies in patients with newly diagnosed undifferentiated arthritis.
S A Bergstra, L van Ouwerkerk, I S Nevins, J A van der Pol, G S Helmich, I Hest, A van Veen, R Bos, Y P M Goekoop-Ruiterman, H E Vonkeman, J Bijsterbosch, P H P de Jong, M Güler-Yüksel, S Böhringer, T W J Huizinga, F A van Gaalen
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引用次数: 0
Abstract
Background: Undifferentiated arthritis (UA) is a term used to describe patients with inflammatory arthritis that has not differentiated into a specific rheumatic disease. UA may be a pre-stage of rheumatoid arthritis (RA) or another inflammatory disease or remain undifferentiated, but a substantial proportion of patients may also achieve spontaneous remission. As UA may be an early presentation of RA, rheumatologists often start methotrexate (or another csDMARD) as early as possible. There are however very little data on the potential benefits of early DMARD treatment, and longitudinal data suggests that long-term outcomes such as physical functioning hardly improved in these patients in the past decades. In the I CEA trial, we investigate if it is beneficial to start early treatment with MTX or baricitinib, a more rapidly acting drug with a broader mechanism of action, compared to waiting for spontaneous remission with symptomatic therapy in patients with UA.
Methods: The I CEA is a multicenter single-blind (independent assessor) randomized clinical trial with a 3-month interventional and 9-month observational follow-up period. The study includes patients with early (< 1 year symptom duration) DMARD-naïve undifferentiated arthritis. Patients with an increased risk of AEs with baricitinib treatment are excluded. Participants are randomized 1:1:1 to (1) symptom relief with NSAIDs and a single injection of glucocorticoids and (waiting for spontaneous remission); (2) methotrexate and a single injection of glucocorticoids, and NSAIDs are optional; and (3) baricitinib and a single injection of glucocorticoids and NSAIDs are optional. During the observational follow-up period, patients are treated in shared decision with their rheumatologist. The primary outcome will be the change in DAS at 3 months. Secondary outcomes include radiographic progression, physical functioning, patient-reported outcomes, cost utilities, safety, progression to classifiable RA, and disease activity over time.
Discussion: The 12-month I CEA trial studies early treatment of patients with UA with methotrexate, baricitinib, or NSAIDs. The study initially had a more complex design. Emerging safety warnings about baricitinib necessitated adjustment of the trial protocol including more extensive exclusion criteria. The number of included patients was lower than initially planned, supported by an updated sample size calculation.
背景:未分化关节炎(UA)是一个术语,用于描述尚未分化为特定风湿性疾病的炎症性关节炎患者。未分化关节炎可能是类风湿性关节炎(RA)或其他炎症性疾病的前期阶段,也可能仍处于未分化状态,但相当一部分患者也可能获得自发缓解。由于 UA 可能是 RA 的早期表现,风湿免疫科医生通常会尽早开始使用甲氨蝶呤(或其他 csDMARD)。然而,关于早期DMARD治疗的潜在益处的数据很少,而且纵向数据表明,在过去几十年中,这些患者的长期预后(如身体功能)几乎没有改善。在 I CEA 试验中,我们研究了早期开始使用 MTX 或巴利昔尼(一种作用机制更广、起效更快的药物)治疗与等待 UA 患者症状自发缓解相比是否有益:I CEA是一项多中心单盲(独立评估者)随机临床试验,具有3个月的干预期和9个月的观察随访期。研究对象包括早期(讨论:为期 12 个月的 I CEA 试验研究用甲氨蝶呤、巴利昔尼或非甾体抗炎药对 UA 患者进行早期治疗。该研究最初的设计较为复杂。由于巴利昔尼的安全性警告不断出现,因此有必要对试验方案进行调整,包括更广泛的排除标准。纳入的患者人数比最初计划的要少,这得到了最新样本量计算的支持:荷兰试验注册号:NL73202.058.20,EudraCT 2019-004359-35,注册时间:2020年6月10日。协议版本 1Q,06-05-2024。
期刊介绍:
Trials is an open access, peer-reviewed, online journal that will encompass all aspects of the performance and findings of randomized controlled trials. Trials will experiment with, and then refine, innovative approaches to improving communication about trials. We are keen to move beyond publishing traditional trial results articles (although these will be included). We believe this represents an exciting opportunity to advance the science and reporting of trials. Prior to 2006, Trials was published as Current Controlled Trials in Cardiovascular Medicine (CCTCVM). All published CCTCVM articles are available via the Trials website and citations to CCTCVM article URLs will continue to be supported.