Hughes R A, van der Meché F G
Department of Neuroimmunology, Guy's, King's and St Thomas' School of Medicine, Hodgkin Building, Guy's Hospital, London, UK, SE1 9RT.
Cochrane Database Syst Rev. 2000(2):CD001446. doi: 10.1002/14651858.CD001446.
The cause of Guillain-Barré syndrome (GBS) is inflammation of the peripheral nerves which corticosteroids would be expected to benefit.
To examine the efficacy of corticosteroids in hastening recovery and reducing the long term morbidity from Guillain-Barré syndrome (GBS).
Search of the Cochrane Neuromuscular Disease Group register for randomised trials and enquiry from authors of trials and other experts in the field.
Types of studies: quasi-randomised or randomised controlled trials
patients with GBS of all ages and all degrees of severity Types of interventions: any form of corticosteroid or adrenocorticotrophic hormone Types of outcome measures: Primary: improvement in disability grade on a commonly used seven point scale four weeks after randomisation Secondary: time from randomisation until recovery of unaided walking, time from randomisation until discontinuation of ventilation (for those ventilated), mortality, proportion of patients dead or disabled (unable to walk without aid) after 12 months, improvement in disability grade after six months, improvement in disability grade after 12 months, proportion of patients who relapse, and proportion of patients with adverse events related to corticosteroid treatment
We identified six randomised trials. One author extracted the data and the other checked them. We obtained some missing data from investigators.
The six eligible trials included a total of 195 corticosteroid treated patients and 187 control subjects. One trial of intravenous methylprednisolone accounted for 243 of the total 382 subjects studied (63%). This trial did not show a significant difference in any disability related outcome between the corticosteroid and placebo groups. There was no significant difference between the corticosteroid and control groups for the primary outcome measure, improvement in disability grade four weeks after randomisation. The weighted mean difference of the three trials for which this outcome was available showed no difference. The actual figure was 0.01 (95% CI -0.27 to 0.29) grade in favour of the corticosteroid group. There was also no significant difference between the groups for most of the secondary outcome measures. However in the largest trial hypertension developed less often in the intravenous methylprednisolone group (2/124, 1.6%) than in the control group (12/118, 10.2%), a significant difference in favour of corticosteroid treatment (relative risk 0.20, 95% CI 0.04 to 0.66).
REVIEWER'S CONCLUSIONS: Corticosteroids should not be used in the treatment of Guillain-Barré syndrome. If a patient with Guillain-Barré syndrome needs corticosteroid treatment for some other reason its use will probably not do harm. The effect of intravenous methylprednisolone combined with intravenous immunoglobulin in Guillain-Barré syndrome is being tested with a randomised trial.
吉兰 - 巴雷综合征(GBS)的病因是周围神经炎症,皮质类固醇有望对此有益。
研究皮质类固醇在加速吉兰 - 巴雷综合征(GBS)恢复及降低长期发病率方面的疗效。
检索Cochrane神经肌肉疾病组登记库中的随机试验,并向试验作者及该领域其他专家咨询。
研究类型:半随机或随机对照试验
所有年龄和严重程度的GBS患者 干预措施类型:任何形式的皮质类固醇或促肾上腺皮质激素 结局指标类型:主要指标:随机分组后四周,采用常用的七点量表评估残疾等级的改善情况 次要指标:从随机分组到独立行走恢复的时间、从随机分组到停止通气的时间(对于需要通气的患者)、死亡率、12个月后死亡或残疾(无法独立行走)的患者比例、六个月后残疾等级的改善情况、12个月后残疾等级的改善情况、复发患者比例以及与皮质类固醇治疗相关的不良事件患者比例
我们识别出六项随机试验。一位作者提取数据,另一位进行核对。我们从研究者处获取了一些缺失数据。
六项符合条件的试验共纳入195名接受皮质类固醇治疗的患者和187名对照受试者。一项静脉注射甲基泼尼松龙的试验纳入了总共382名受试者中的243名(63%)。该试验未显示皮质类固醇组与安慰剂组在任何与残疾相关的结局上有显著差异。对于主要结局指标,即随机分组后四周残疾等级的改善情况,皮质类固醇组与对照组之间无显著差异。有该结局数据的三项试验的加权平均差显示无差异。实际数值为0.01(95%可信区间 -0.27至0.29)级,有利于皮质类固醇组。在大多数次要结局指标上,两组之间也无显著差异。然而,在最大的试验中,静脉注射甲基泼尼松龙组发生高血压的频率(2/124,1.6%)低于对照组(12/118,10.2%),这一显著差异有利于皮质类固醇治疗(相对风险0.20,95%可信区间0.04至0.66)。
皮质类固醇不应被用于治疗吉兰 - 巴雷综合征。如果患有吉兰 - 巴雷综合征的患者因其他原因需要皮质类固醇治疗,使用它可能无害。一项随机试验正在测试静脉注射甲基泼尼松龙联合静脉注射免疫球蛋白在吉兰 - 巴雷综合征中的效果。
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