免疫性炎性风湿性疾病糖皮质激素治疗的二分法:循证观点和临床实践的见解。

IF 1.4 Q3 RHEUMATOLOGY
Reumatologia Pub Date : 2023-01-01 Epub Date: 2023-08-31 DOI:10.5114/reum/170845
Elvis Hysa, Tamara Vojinovic, Emanuele Gotelli, Elisa Alessandri, Carmen Pizzorni, Sabrina Paolino, Alberto Sulli, Vanessa Smith, Maurizio Cutolo
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引用次数: 0

摘要

目的:糖皮质激素(GC)是最常用的抗炎和免疫抑制药物,因为它们在许多免疫炎症性风湿性疾病(IRD)中有效地控制疼痛和疾病改变。然而,由于不良反应(AE),它们的使用受到限制。材料和方法:作者分析了最近的研究,包括随机对照试验(RCT)、观察性研究、转化研究和系统综述,对GC在风湿病中的应用的优缺点提供了深入的观点。结果:糖皮质激素在治疗危及生命的自身免疫性疾病方面至关重要,也是许多IRD的基石,因为它们的作用迅速,在发作时是必要的。几项随机对照试验和荟萃分析表明,当长期低剂量给药时,GC可以将早期类风湿性关节炎(RA)患者的放射学进展减缓至少50%,满足疾病改良抗风湿药物(DMARD)的传统定义。在RA治疗的背景下,夜间使用改性释放的泼尼松制剂可以提供尊重炎症反应和HPA激活的昼夜节律的选择,从而使低剂量GC给药能够减轻夜间炎症、延长的早晨疲劳和关节僵硬。长期GC的使用应根据患者的特点进行个体化,并因其潜在的AE而尽量减少。它们的长期使用,特别是中/高剂量,可能会由于代谢系统效应的负担和感染风险的增加而导致不可逆的器官损伤。许多国际指南建议在持续缓解的情况下逐渐减少/退出GC。靶向治疗(T2T)策略在设定疾病活动目标和一旦达到控制就减少/停止GC方面至关重要。结论:糖皮质激素在治疗IRD中的使用应该是明智的,重点是尽量减少使用,尽可能减少和停止治疗,以提高长期安全性。糖皮质激素仍然是许多治疗方案的一部分,特别是在低剂量下,老年RA患者,特别是患有相关慢性合并症的患者,可能受益于长期低剂量GC治疗。个性化的GC治疗对于获得最佳的长期结果至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The dichotomy of glucocorticosteroid treatment in immune-inflammatory rheumatic diseases: an evidence-based perspective and insights from clinical practice.

The dichotomy of glucocorticosteroid treatment in immune-inflammatory rheumatic diseases: an evidence-based perspective and insights from clinical practice.

Objectives: Glucocorticosteroids (GCs) are the most used anti-inflammatory and immunosuppressive drugs due to their effectiveness in managing pain and disease modification in many immune-inflammatory rheumatic diseases (IRDs). However, their use is limited because of adverse effects (AEs).

Material and methods: The authors analyzed recent studies, including randomized controlled trials (RCTs), observational, translational studies and systematic reviews, providing an in-depth viewpoint on the benefits and drawbacks of GC use in rheumatology.

Results: Glucocorticosteroids are essential in managing life-threatening autoimmune diseases and a cornerstone in many IRDs given their swift onset of action, necessary in flares. Several RCTs and meta-analyses have demonstrated that when administered over a long time and on a low-dose basis, GC can slow the radiographic progression in early rheumatoid arthritis (RA) patients by at least 50%, satisfying the conventional definition of a disease-modifying anti-rheumatic drug (DMARD). In the context of RA treatment, the use of modified-release prednisone formulations at night may offer the option of respecting circadian rhythms of both inflammatory response and HPA activation, thereby enabling low-dose GC administration to mitigate nocturnal inflammation and prolonged morning fatigue and joint stiffness. Long-term GC use should be individualized based on patient characteristics and minimized due to their potential AEs. Their chronic use, especially at medium/high dosages, might cause irreversible organ damage due to the burden of metabolic systemic effects and increased risk of infections. Many international guidelines recommend tapering/withdrawal of GCs in sustained remission. Treat-to-target (T2T) strategies are critical in setting targets for disease activity and reducing/discontinuing GCs once control is achieved.

Conclusions: Glucocorticosteroids' use in treating IRDs should be judicious, focused on minimizing use, tapering and discontinuing treatment, when possible, to improve long-term safety. Glucocorticosteroids remain part of many therapeutic regimens, particularly at low doses, and elderly RA patients, especially with associated chronic comorbidities, may benefit from long-term low-dose GC treatment. A personalized GC therapy is essential for optimal long-term outcomes.

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来源期刊
Reumatologia
Reumatologia Medicine-Rheumatology
CiteScore
2.70
自引率
0.00%
发文量
44
审稿时长
10 weeks
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