Structural damage progression in patients with early rheumatoid arthritis treated with methotrexate, baricitinib, or baricitinib plus methotrexate based on clinical response in the phase 3 RA-BEGIN study

van der Heijde Desiree; Durez Patrick; Schett Georg; Naredo Esperanza; Ostergaard Mikkel; Meszaros Gabriella; De Leonardis Francesco; de la Torre Inmaculada; Lopez-Romero Pedro; Schlichting Douglas; Nantz Eric; Fleischmann Roy

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Structural damage progression in patients with early rheumatoid arthritis treated with methotrexate, baricitinib, or baricitinib plus methotrexate based on clinical response in the phase 3 RA-BEGIN study

机译：基于临床反应的甲氨蝶呤，白藜芦醇尿嘧啶及甲氨蝶呤治疗早期类风湿性关节炎患者的结构损伤进展

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The objective of this study was to evaluate structural damage progression based on clinical response in rheumatoid arthritis patients with no or limited prior disease-modifying anti-rheumatic drug treatment receiving the Janus kinase (JAK)1/JAK2 inhibitor baricitinib 4 mg, methotrexate (MTX), or the combination. Data from the phase 3 RA-BEGIN study were analysed post hoc. Proportions of patients with structural damage progression (change from baseline greater than the smallest detectable change in modified total Sharp score) at week 52 were evaluated based on sustained Disease Activity Score for 28-joint count with serum high-sensitivity C-reactive protein (DAS28-hsCRP) = 3.2 or Simplified Disease Activity Index (SDAI) scow = 11; no formal statistical comparisons between treatments were performed to test these proportions. Baseline factors associated with risk of structural damage progression, including Clinical Disease Activity Index (CDAI) score, were identified using multivariate analysis. Patients achieving versus not achieving sustained DAS28-hsCRP = 3.2 or SDAI score = 11 were less likely to experience structural damage progression at week 52. In patients achieving these responses, structural damage progression was less likely with baricitinib monotherapy or plus MTX than with MTX monotherapy. In patients not achieving these sustained clinical thresholds, structural damage progression was less likely with baricitinib plus MTX than with either monotherapy. Independent of treatment, baseline factors significantly associated with increased risk of structural damage progression included higher hsCRP and CDAI score, smoking, female sex, and lower body mass index. In conclusion, patients achieving versus not achieving sustained DAS28-hsCRP = 3.2 or SDAI score = 11 were less likely to show structural damage progression, irrespective of treatment.

机译：本研究的目的是评估基于类风湿性关节炎患者的临床反应的结构损伤进展，其患者没有或有限的疾病 - 改性抗风湿药物治疗接受Janus激酶（Jak）1 / Jak2抑制剂Baricitinib 4mg，甲氨蝶呤（MTX或者组合。分析了第3阶段RA-BEGIN研究的数据。在第52周评估第52周的结构损伤进展患者（从改性总尖锐评分的最小可检测变化的基线的变化）的比例基于血清高敏感性C反应蛋白的28关节计数（DAS28 -hscrp）＆ = 3.2或简化疾病活动指数（sdai）污染物＆ = 11;未进行治疗之间的正式统计比较以测试这些比例。使用多变量分析鉴定了与结构损伤进展相关的基线因素，包括临床疾病活动指数（CDAI）评分。实现与持续的DAS28-HSCRP患者的患者或SDAI得分均不太可能在第52周内体验结构损伤进展的可能性损伤。在实现这些反应的患者中，结构损伤进展不太可能与MYOTINIB单一疗法或加号不太可能而不是mtx单疗法。在未实现这些持续临床阈值的患者中，Baricitinib Plus MTX的结构损伤进展比单药治疗不太可能。独立于治疗，与结构损伤进展的风险显着相关的基线因素包括较高的HSCRP和CDAI得分，吸烟，女性性别和降低体重指数。总之，无论治疗如何，都达到了患者，而不是实现持续的DAS28-HSCRP = 3.2或SDAI得分。

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来源
《Clinical rheumatology》 |2018年第9期|共10页
作者
van der Heijde Desiree; Durez Patrick; Schett Georg; Naredo Esperanza; Ostergaard Mikkel; Meszaros Gabriella; De Leonardis Francesco; de la Torre Inmaculada; Lopez-Romero Pedro; Schlichting Douglas; Nantz Eric; Fleischmann Roy;
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作者单位

Leiden Univ Med Ctr Albinusdreef 2 NL-2333 ZA Leiden Netherlands;

Catholic Univ Louvain Pole Pathol Rhumatismales Inflammatoires &

Syst Inst Rech Expt &

Clin;

Friedrich Alexander Univ Erlangen Nuremberg Erlangen Germany;

Hosp Univ Fdn Jimenez Diaz Madrid Spain;

Rigshosp Copenhagen Ctr Arthrit Res Ctr Rheumatol &

Spine Dis Glostrup Denmark;

Eli Lilly &

Co Indianapolis IN 46285 USA;

Eli Lilly &

Co Indianapolis IN 46285 USA;

Eli Lilly &

Co Indianapolis IN 46285 USA;

Eli Lilly &

Co Indianapolis IN 46285 USA;

Eli Lilly &

Co Indianapolis IN 46285 USA;

Eli Lilly &

Co Indianapolis IN 46285 USA;

Univ Texas Southwestern Med Ctr Dallas Metroplex Clin Res Ctr Dallas TX 75390 USA;

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原文格式 PDF
正文语种 eng
中图分类内科学;
关键词
Baricitinib; Joint damage; Methotrexate; RA-BEGIN study; Rheumatoid arthritis; Structural progression;

机译：Baricitinib;关节损伤;甲氨蝶呤;RA-BEGIN学习;类风湿性关节炎;结构进展;

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1. Structural damage progression in patients with early rheumatoid arthritis treated with methotrexate, baricitinib, or baricitinib plus methotrexate based on clinical response in the phase 3 RA-BEGIN study [J] . van der Heijde Desiree, Durez Patrick, Schett Georg, Clinical rheumatology . 2018,第9期

机译：基于临床反应的甲氨蝶呤，白藜芦醇尿嘧啶及甲氨蝶呤治疗早期类风湿性关节炎患者的结构损伤进展
2. Patient-reported outcomes from a randomized, double-blind, placebo controlled, phase III study of baricitinib versus placebo in patients with moderately to severely active rheumatoid arthritis and an inadequate response to methotrexate therapy: results from the RA-BALANCE study [J] . Yue Yang, Jianhua Xu, Jian Xu, Therapeutic advances in musculoskeletal disease. . 2021,第a期

机译：患者报告从随机，双盲，安慰剂控制的结果，对患者的患者的患者患者的AICA III研究，以严重活跃的类风湿性关节炎和对甲氨蝶呤治疗的反应不足：RA-BALLAGE研究结果
3. Attainment and characteristics of clinical remission according to the new ACR-EULAR criteria in abatacept-treated patients with early rheumatoid arthritis: new analyses from the Abatacept study to Gauge Remission and joint damage progression in methotrexate (MTX)-naive patients with Early Erosive rheumatoid arthritis (AGREE) [J] . Josef S. Smolen, Jürgen Wollenhaupt, Juan J. Gomez-Reino, Arthritis Research . 2015,第1期

机译：根据新的ACR-EULAR标准，在接受abatacept治疗的早期类风湿性关节炎患者中达到和达到临床缓解的特征：从Abatacept研究到未接受甲氨蝶呤（MTX）的早期侵蚀性类风湿性关节炎患者的量表缓解和关节损伤进展的新分析（同意）
4. Brain cortical structural differences between non-central nervous system cancer patients treated with and without chemotherapy compared to non-cancer controls: a cross-sectional pilot MRI study using clinically-indicated scans [C] . Mark S. Shiroishi, Vikash Gupta, Bavrina Bigjahan, 13th international conference on medical information processing and analysis . 2017

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5. Clinical studies of immunomodulatory activities of Yunzhi -Danshen in breast cancer and nasopharyngeal carcinoma patients, and Lingzhi-San Miao San in rheumatoid arthritis patients. [D] . Bao, Yixi. 2005

机译：云芝丹参对乳腺癌和鼻咽癌患者及类风湿关节炎灵芝三妙散的免疫调节活性的临床研究。
6. Structural damage progression in patients with early rheumatoid arthritis treated with methotrexate baricitinib or baricitinib plus methotrexate based on clinical response in the phase 3 RA-BEGIN study [O] . Désirée van der Heijde, Patrick Durez, Georg Schett, -1

机译：根据3期RA-BEGIN研究的临床反应接受甲氨蝶呤巴西替尼或巴西替尼加甲氨蝶呤治疗的早期类风湿关节炎患者的结构损伤进展
7. Assessment of the association of baseline anti-CarbV and anti-MCV antibodies with response to treatment and radiographic progression in an RA population treated with either methotrexate or baricitinib: post-hoc analyses from RA-BEGIN [O] . Pedro López-Romero, Lorena Martinez-Gamboa, Holger Bang, 2020

机译：评估基线抗CARBV和抗MCV抗体的响应与甲氨蝶呤或BARICINIB治疗的RA人群治疗和放射线进展的响应：HOC从RA-BEGIN分析

Structural damage progression in patients with early rheumatoid arthritis treated with methotrexate, baricitinib, or baricitinib plus methotrexate based on clinical response in the phase 3 RA-BEGIN study

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