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Treatment of polymyalgia rheumatica: a systematic review.

机译:治疗风湿性多肌痛:一个系统审查。

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BACKGROUND: Polymyalgia rheumatica (PMR) treatment is based on low-dose glucocorticoids. Glucocorticoid-sparing agents have also been tested. Our objective was to systematically examine the peer-reviewed literature on PMR therapy, particularly the optimal glucocorticoid type, starting doses, and subsequent reduction regimens as well as glucocorticoid-sparing medications. METHODS: We searched Cochrane Databases and MEDLINE (1957 through December 2008) for English-language articles on PMR treatment (randomized trials, prospective cohorts, case-control trials, and case series) that included 20 or more patients. All data on study design, PMR definition criteria, medical therapy, and disease outcomes were collected using a standardized protocol. RESULTS: Thirty studies (13 randomized trials and 17 observational studies) were analyzed. No meta-analyses or systematic reviews were found. The PMR definition criteria, treatment protocols, and outcome measures differed widely among the trials. Starting prednisone doses higher than 10 mg/d were associated with fewer relapses and shorter therapy than were lower doses; starting prednisone doses of 15 mg/d or lower were associated with lower cumulative glucocorticoid doses than were higher starting prednisone doses; and starting prednisone doses higher than 15 mg/d were associated with more glucocorticoid-related adverse effects. Slow prednisone dose tapering (<1 mg/mo) was associated with fewer relapses and more frequent glucocorticoid treatment cessation than faster tapering regimens. Initial addition of oral or intramuscular methotrexate provided efficacy at doses of 10 mg/wk or higher. Infliximab was ineffective as initial cotreatment. CONCLUSIONS: The scarcity of randomized trials and the high level of heterogeneity of studies on PMR therapy do not allow firm conclusions to be drawn. However, PMR remission seems to be achieved with prednisone treatment at a dose of 15 mg/d in most patients, and reductions below 10 mg/d should preferably follow a tapering rate of less than 1 mg/mo. Methotrexate seems to exert glucocorticoid-sparing properties.
机译:背景:风湿性多肌痛(PMR)治疗基于低剂量的糖皮质激素。Glucocorticoid-sparing代理也测试。检查同行评议的文献PMR治疗,特别是最佳的糖皮质激素类型、起始剂量和随后的减少方案以及glucocorticoid-sparing的药物。数据库和MEDLINE(1957年12月通过2008)对PMR英文文章治疗(随机试验、勘察军团,病例对照试验和病例分析),其中包括20或更多的病人。研究设计,PMR定义标准,医疗治疗,收集和疾病的结果使用一个标准化的协议。研究(13个随机试验和17观察性研究)进行了分析。荟萃分析或系统的评论被发现。PMR定义标准,治疗方案,和结果的措施各不相同试用用更少的复发和mg / d有关更短的治疗比低剂量;强的松的剂量15毫克/天或更低降低累积糖皮质激素开始比高剂量强的松的剂量;和启动强的松的剂量高于15毫克/天有关更多glucocorticoid-related不利影响。(< 1毫克/ mo)和减少复发有关更频繁的糖皮质激素治疗停止比速度逐渐减少方案。口服或肌肉注射甲氨蝶呤疗效剂量的10毫克/周或更高。英夫利昔单抗最初是无效的cotreatment。随机试验和高水平的异质性的研究不PMR治疗让公司的结论。缓解似乎取得了与强的松治疗15毫克/天的剂量在大多数患者中,和减少低于10 mg / d应该最好遵循一个圆锥形的速度小于1毫克/ mo。甲氨蝶呤似乎发挥glucocorticoid-sparing属性。

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