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在现实临床实践中,通过机会窗紧密控制策略用改善病情抗风湿药物治疗类风湿关节炎能否实现长期缓解和药物无缓解?一项队列研究。

Can treating rheumatoid arthritis with disease-modifying anti-rheumatic drugs at the window of opportunity with tight control strategy lead to long-term remission and medications free remission in real-world clinical practice? A cohort study.

机构信息

Connective Tissue Diseases Research Center, Tabriz University of Medical Sciences, Tabriz, Iran.

Autoimmune Diseases Research Center, Kashan University of Medical Sciences, Kashan, Iran.

出版信息

Clin Rheumatol. 2021 Nov;40(11):4485-4491. doi: 10.1007/s10067-021-05831-3. Epub 2021 Jun 23.

Abstract

OBJECTIVE

The aim of this retrospective study is to compare the results of starting rheumatoid arthritis (RA) treatment with tight control strategy in the window of opportunity and later phases of the disease in real-world clinical practice.

METHODS

In this cohort, 609 RA patients were divided into three groups: (i) very early treatment (VET): ≤ 3 months; (ii) early treatment (ET): 3-12 months; and (iii) late treatment (LT) > 12 months after the onset of the disease. Four levels of remission were defined: (i) sustained remission on treatment, (ii) sustained glucocorticoids free remission, (iii) sustained disease-modifying anti-rheumatic drugs (DMARDs) free remission, and (iv) long-term remission. Outcome was assessed based on the number of patients in sustained or long-term remission and patients with poor joint outcome and systemic involvement.

RESULTS

There were no significant differences in the remission rate between the groups. Time to sustained remission in VET group was shorter than ET and LT groups. There were no significant differences in the rate and duration of prednisolone discontinuation in the studied groups. DMARDs were discontinued in VET, ET, and LT groups in 8.7%, 10.2%, and 7% of the patients, respectively. Poor joint outcome occurred in 33.2%, 50.5%, and 59.4% of the patients in the VET, ET, and LT groups, respectively. Remission induction in the first year of the treatment was associated with long-term remission in the VET, ET, and LT groups.

CONCLUSIONS

Medications free remission in RA is rare, and although treatment with DMARDs within 3 months of the onset of the disease can prevent joint damage, it cannot lead to long-term remission and discontinuation of medications.

KEY POINTS

• Medications free remission in rheumatoid arthritis is rare. • Treatment with DMARDs within 3 months of the onset of the disease can prevent joint damage, but it cannot lead to long-term remission and discontinuation of medications.

摘要

目的

本回顾性研究旨在比较在机会窗口和疾病后期阶段采用严格控制策略开始治疗类风湿关节炎(RA)的结果,以观察真实世界中的临床实践。

方法

在该队列中,将 609 例 RA 患者分为三组:(i)早期治疗(ET):≤3 个月;(ii)早期治疗(ET):3-12 个月;(iii)晚期治疗(LT):疾病发作后超过 12 个月。定义了四个缓解水平:(i)治疗持续缓解,(ii)持续糖皮质激素缓解,(iii)持续缓解,(iv)长期缓解。基于持续缓解或长期缓解的患者数量和具有不良关节结局和全身受累的患者来评估结果。

结果

三组间缓解率无显著差异。VET 组达到持续缓解的时间短于 ET 和 LT 组。在研究组中,泼尼松龙停药的发生率和持续时间无显著差异。VET、ET 和 LT 组分别有 8.7%、10.2%和 7%的患者停用 DMARDs。VET、ET 和 LT 组分别有 33.2%、50.5%和 59.4%的患者出现关节预后不良。在 VET、ET 和 LT 组中,治疗第一年的缓解诱导与长期缓解相关。

结论

RA 中药物无缓解是罕见的,尽管在疾病发作后 3 个月内使用 DMARDs 治疗可以预防关节损伤,但它不能导致长期缓解和停药。

关键点

•RA 中药物无缓解是罕见的。•在疾病发作后 3 个月内使用 DMARDs 治疗可以预防关节损伤,但不能导致长期缓解和停药。

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