THE PLACE OF LEFLUNOMIDE IN DISEASE-MODIFYING THERAPY OF RHEUMATOID ARTHRITIS: NEW ASPECTS

O. Iaremenko, G. Mikitenko
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Abstract

A new mechanism of lefl unomide (LEF) action was recently discovered, namely its ability to infl uence the intracellular mechanism of the infl ammatory process by inhibiting JAK kinases, which brings it closer to the new most eff ective group for treatment of rheumatoid arthritis (RA) – Janus kinase inhibitors. The article presents data from both our own and other authors’ studies on the eff ectiveness and safety of the drug in comparison with other synthetic and biological basic agents. The aim of our study was a comparative evaluation of LEF, methotrex- ate (MTX), sulfasalazine (SS) and their combinations (CDT) in 402 patients with RA. Obtained results showed advantages of LEF and СDT over the use of SS (at any RA duration) and MTX (at late RA). Adverse events were the lowest in the SS group, and disease-modifying anti-rheumatic drug (DMARD) discontinuation due to complications was the lowest in the LEF group. Based on the results of multifactor regression analysis, we developed a scheme of individualized selection of the most eff ective DMARD depending on the initial characteristics of RA patients. The article also presents international study data. It analyses the comparative effi cacy of LEF (10-20 mg/d) and low doses of rituximab (500 mg twice daily) in patients refractory to MTX therapy; effi cacy of LEF in monotherapy (5-40 mg/d) and combination with other DMARD; LEF at a dose of 100 mg/week and MTX at a dose of 10 mg/week; LEF at a dose of 50 mg once a week and 10 mg daily. The eff ect of LEF on uric acid levels and bone mineral density of the lumbar spine in patients with RA was studied.
来氟米特在类风湿关节炎疾病改善治疗中的地位:新的方面
最近发现了lefl unomide (LEF)作用的新机制,即通过抑制JAK激酶影响炎症过程的细胞内机制,使其更接近治疗类风湿关节炎(RA)的新的最有效组- Janus激酶抑制剂。本文介绍了我们自己和其他作者对该药的有效性和安全性的研究数据,并与其他合成和生物基础药物进行了比较。本研究的目的是比较评价402例RA患者的LEF、甲氨蝶呤(MTX)、磺胺嘧啶(SS)及其联合用药(CDT)。所获得的结果显示LEF和СDT优于使用SS(在任何RA持续时间)和MTX(在RA晚期)。不良事件在SS组中最低,因并发症而停药的情况在LEF组中最低。基于多因素回归分析的结果,我们根据RA患者的初始特征制定了最有效的DMARD的个性化选择方案。文章还提供了国际研究数据。它分析了LEF (10- 20mg /d)和低剂量利妥昔单抗(500mg,每日两次)对MTX治疗难治性患者的比较疗效;LEF单药(5- 40mg /d)及与其他DMARD合用的疗效;LEF剂量为100毫克/周,MTX剂量为10毫克/周;左旋肾上腺素的剂量为50毫克,每周一次,每天10毫克。研究左旋肾上腺素对风湿性关节炎患者腰椎尿酸水平和骨密度的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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