从中度至重度类风湿关节炎的即释型泼尼松转换为缓释型泼尼松:一项基于实践的临床研究。
Switching From Immediate-Release to Delayed-Release Prednisone in Moderate to Severe Rheumatoid Arthritis: A Practice-Based Clinical Study.
作者信息
Dikranian Ara H, Mallay Rubaiya, Marshall Mike, Francis-Sedlak Megan, Holt Robert J
机构信息
Cabrillo Center for Rheumatic Disease, San Diego, CA, USA.
Suncoast Internal Medicine Consultants and Largo Medical Center, Largo, FL, USA.
出版信息
Rheumatol Ther. 2017 Dec;4(2):363-374. doi: 10.1007/s40744-017-0075-1. Epub 2017 Aug 17.
INTRODUCTION
Rheumatoid arthritis (RA) produces debilitating morning stiffness. Exogenous glucocorticoids can help with these symptoms when timed appropriately. Bedtime dosing of delayed-release prednisone (DR-prednisone) matches the rise of inflammatory cytokines before awakening and can improve stiffness and other RA symptoms. A prospective open-label study was conducted in patients currently on stable doses of immediate-release prednisone (IR-prednisone) who were switched to DR-prednisone to analyze the incremental benefit of better timed and lower dose glucocorticoid therapy.
METHODS
Twelve US sites enrolled patients with moderate-severe RA into a 12-week prospective study. Patients were switched from IR- to DR-prednisone while maintaining other existing background therapies. Change from baseline in morning stiffness severity, morning stiffness duration, swollen and tender joint counts (S-TJC), 28 joint disease activity score (DAS28), and patient/physician global assessment (PGA/PhGA), among others, were measured. Post-hoc analyses were performed on those completing 10 weeks of treatment and those with >60 min of morning stiffness at baseline.
RESULTS
Fifty-six patients had at least one follow-up visit and were similar in demographics to previous controlled trials with DR-prednisone with regard to baseline age and DAS28-CRP but had lower morning stiffness and RA duration. DR-prednisone produced a trend toward lower morning stiffness severity and duration with a reduction in daily prednisone dose of almost 1 mg. Patients treated with DR-prednisone for ≥10 weeks demonstrated significant reductions in morning stiffness duration, SJC, TJC, DAS28-CRP, and PhGA (all p ≤ 0.04). Patients treated for ≥10 weeks with >60 min of baseline morning stiffness produced similar results in these measures as well as a 21% reduction in morning stiffness severity (p = 0.02).
CONCLUSION
Patients switched to DR-prednisone from IR-prednisone in this practice-based study maintained or improved their outcomes across a variety of domains, and results were comparable to previous controlled trials in which patients completed at least 10 weeks of treatment.
FUNDING
Horizon Pharma USA, Inc.
TRIAL REGISTRATION
ClinicalTrials.gov identifier, NCT02287610.
引言
类风湿性关节炎(RA)会导致使人虚弱的晨僵。外源性糖皮质激素在适当的时间给药时可缓解这些症状。睡前服用缓释泼尼松(DR-泼尼松)与觉醒前炎症细胞因子的升高相匹配,可改善僵硬及其他RA症状。对目前正在服用稳定剂量速释泼尼松(IR-泼尼松)且转而服用DR-泼尼松的患者进行了一项前瞻性开放标签研究,以分析时间安排更佳且剂量更低的糖皮质激素治疗的额外益处。
方法
美国12个研究点招募了中重度RA患者参与一项为期12周的前瞻性研究。患者从IR-泼尼松转换为DR-泼尼松,同时维持其他现有的背景治疗。测量了晨僵严重程度、晨僵持续时间、肿胀和压痛关节计数(S-TJC)、28关节疾病活动评分(DAS28)以及患者/医生整体评估(PGA/PhGA)等相对于基线的变化。对完成10周治疗的患者以及基线时晨僵超过60分钟的患者进行了事后分析。
结果
56例患者至少进行了一次随访,在人口统计学方面,其基线年龄和DAS28-CRP与之前使用DR-泼尼松的对照试验相似,但晨僵程度和RA病程较短。DR-泼尼松使晨僵严重程度和持续时间呈降低趋势,每日泼尼松剂量减少了近1毫克。接受DR-泼尼松治疗≥10周的患者晨僵持续时间、SJC、TJC、DAS28-CRP和PhGA均显著降低(所有p≤0.04)。基线晨僵超过60分钟且接受≥10周治疗的患者在这些指标上也产生了类似结果,晨僵严重程度降低了21%(p=0.02)。
结论
在这项基于实践的研究中,从IR-泼尼松转换为DR-泼尼松的患者在多个领域维持或改善了其治疗效果,结果与之前患者至少完成10周治疗的对照试验相当。
资助
美国地平线制药公司
试验注册
ClinicalTrials.gov标识符,NCT02287610
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