Riera Rachel, Porfírio Gustavo J M, Torloni Maria R
Centro de Estudos em Medicina Baseada em Evidências e Avaliação Tecnológica em Saúde, Brazilian Cochrane Centre, Rua Borges Lagoa, 564 cj 63, São Paulo, SP, Brazil, 04038-000.
Cochrane Database Syst Rev. 2016 Apr 15;4(4):CD011203. doi: 10.1002/14651858.CD011203.pub2.
Multiple sclerosis (MS) is an autoimmune, T-cell-dependent, inflammatory, demyelinating disease of the central nervous system, with an unpredictable course. Current MS therapies focus on treating exacerbations, preventing new exacerbations and avoiding the progression of disability. However, at present there is no effective treatment that is capable of safely and effectively reaching these objectives. This has led to the development and investigation of new drugs. Recent clinical trials suggest that alemtuzumab, a humanised monoclonal antibody against cell surface CD52, could be a promising option for MS.
To assess the safety and effectiveness of alemtuzumab used alone or associated with other treatments to decrease disease activity in patients with any form of MS.
We searched the Trials Register of the Cochrane Multiple Sclerosis and Rare Diseases of the CNS Group (30 April 2015), which contains trials from the Cochrane Central Register of Controlled Trials (CENTRAL), MEDLINE, EMBASE, CINAHL, LILACS and the trial registry databases ClinicalTrials.gov and WHO International Clinical Trials Registry Platform. There was no restriction on the source, publication date or language.
All randomised clinical trials (RCTs) involving adults diagnosed with any form of MS according to the McDonald criteria, comparing alemtuzumab alone or associated with other medications, at any dose and for any duration, versus placebo or any other active drug therapy or alemtuzumab in other dose, regimen or duration. The co-primary outcomes were relapse-free survival, sustained disease progression and number of participants with at least one of any adverse events, including serious adverse events.
Two independent review authors performed study selection, data extraction and 'Risk of bias' assessment. A third review author checked the process for accuracy. We used the Cochrane 'Risk of bias' tool to assess the risk of bias of the studies included in the review. We used the GRADE system to assess the quality of the body of evidence. To measure the treatment effect on dichotomous outcomes we used the risk ratio (RR); for the treatment effect on continuous outcomes, we used the mean difference (MD) and for time-to-event outcomes we used hazard ratio (HR). We calculated 95% confidence intervals (CI) for these measures. When there was no heterogeneity, we used a fixed-effect model to pool data.
Three RCTs (1713 participants) fulfilled the selection criteria and we included them in the review. All three trials compared alemtuzumab versus subcutaneous interferon beta-1a for patients with relapsing-remitting MS. Patients were treatment-naive in the CARE-MS and CAMMS223 studies. The CARE-MS II study included patients with at least one relapse while being treated with interferon beta or glatiramer acetate. Alemtuzumab was given for 12 or 24 months; for some outcomes, the follow-up period reached 36 months. The regimens were (a) 12 mg or 24 mg per day administered intravenously, once a day for five consecutive days at month 0 and 12 or (b) 24 mg per day, intravenously, once a day for three consecutive days at month 12 and 24. The patients in the other arm of the trials received interferon beta-1a 44 μg subcutaneously three times weekly after dose titration.At 24 months, alemtuzumab 12 mg was associated with: (a) higher relapse-free survival (hazard ratio (HR) 0.50, 95% CI 0.41 to 0.60; 1248 participants, two studies, moderate quality evidence); (b) higher sustained disease progression-free survival (HR 0.62, 95% CI 0.44 to 0.87; 1191 participants; two studies; moderate quality evidence); (c) a slightly higher number of participants with at least one adverse event (RR 1.04, 95% CI 1.01 to 1.06; 1248 participants; two studies; moderate quality evidence); (d) a lower number of participants with new or enlarging T2-hyperintense lesions on magnetic resonance imaging (MRI) (RR 0.74, 95% CI 0.59 to 0.91; 1238 participants; two studies; I(2) = 80%); and (e) a lower number of dropouts (RR 0.31, 95% CI 0.23 to 0.41; 1248 participants; two studies, I(2) = 29%; low quality evidence).At 36 months, alemtuzumab 24 mg was associated with: (a) higher relapse-free survival (45 versus 17; HR 0.21, 95% CI 0.11 to 0.40; one study; 221 participants); (b) a higher sustained disease progression-free survival (HR 0.33, 95% CI 0.16 to 0.69; one study; 221 participants); and (c) no statistical difference in the rate of participants with at least one adverse event. We did not find any study that reported any of the following outcomes: rate of participants free of clinical disease activity, quality of life, fatigue or change in the numbers of MRI T2- and T1-weighted lesions after treatment. It was not possible to perform subgroup analyses according to disease type and disability at baseline due to lack of data.
AUTHORS' CONCLUSIONS: In patients with relapsing-remitting MS, alemtuzumab 12 mg was better than subcutaneous interferon beta-1a for the following outcomes assessed at 24 months: relapse-free survival, sustained disease progression-free survival, number of participants with at least one adverse event and number of participants with new or enlarging T2-hyperintense lesions on MRI. The quality of the evidence for these results was low to moderate. Alemtuzumab 24 mg seemed to be better than subcutaneous interferon beta-1a for relapse-free survival and sustained disease progression-free survival, at 36 months.More randomised clinical trials are needed to evaluate the effects of alemtuzumab on other forms of MS and compared with other therapeutic options. These new studies should assess additional relevant outcomes such as the rate of participants free of clinical disease activity, quality of life, fatigue and adverse events (individual rates, serious adverse events and long-term adverse events). Moreover, these new studies should evaluate other doses and durations of alemtuzumab course.
多发性硬化症(MS)是一种中枢神经系统的自身免疫性、T细胞依赖性、炎症性脱髓鞘疾病,病程不可预测。目前MS治疗主要集中于治疗病情加重、预防新的病情加重以及避免残疾进展。然而,目前尚无能够安全有效地实现这些目标的有效治疗方法。这促使了新药的研发和研究。近期临床试验表明,阿仑单抗,一种抗细胞表面CD52的人源化单克隆抗体,可能是MS治疗的一个有前景的选择。
评估单独使用阿仑单抗或与其他治疗联合使用以降低任何形式MS患者疾病活动度的安全性和有效性。
我们检索了Cochrane多发性硬化症和中枢神经系统罕见病小组试验注册库(2015年4月30日),其中包含来自Cochrane对照试验中心注册库(CENTRAL)、MEDLINE、EMBASE、CINAHL、LILACS以及试验注册数据库ClinicalTrials.gov和世界卫生组织国际临床试验注册平台的试验。对文献来源、发表日期或语言无限制。
所有根据麦克唐纳标准诊断为任何形式MS的成人随机临床试验(RCT),比较单独使用阿仑单抗或与其他药物联合使用,任何剂量和疗程,与安慰剂或任何其他活性药物治疗或其他剂量、方案或疗程的阿仑单抗。共同主要结局为无复发生存、持续疾病进展以及至少发生一项不良事件(包括严重不良事件)的参与者数量。
两名独立的综述作者进行研究选择、数据提取和“偏倚风险”评估。第三名综述作者检查该过程的准确性。我们使用Cochrane“偏倚风险”工具评估纳入综述研究的偏倚风险。我们使用GRADE系统评估证据体的质量。为衡量对二分结局的治疗效果,我们使用风险比(RR);对连续结局的治疗效果,我们使用平均差(MD);对事件发生时间结局,我们使用风险比(HR)。我们计算这些测量值的95%置信区间(CI)。当不存在异质性时,我们使用固定效应模型合并数据。
三项RCT(1713名参与者)符合选择标准,我们将其纳入综述。所有三项试验均比较了阿仑单抗与皮下注射干扰素β-1a治疗复发缓解型MS患者的疗效。在CARE-MS和CAMMS223研究中,患者此前未接受过治疗。CARE-MS II研究纳入了在接受干扰素β或醋酸格拉替雷治疗期间至少发生一次复发的患者。阿仑单抗给药12或24个月;对于某些结局,随访期长达36个月。给药方案为:(a)每月0月和12月静脉注射12mg或24mg/d,连续5天,每日1次;或(b)在第12个月和第24个月静脉注射24mg/d,连续3天,每日1次。试验另一组的患者在剂量滴定后每周皮下注射3次44μg干扰素β-1a。在24个月时,12mg阿仑单抗与以下情况相关:(a)更高的无复发生存(风险比(HR)0.50,95%CI 0.41至0.60;1248名参与者,两项研究,中等质量证据);(b)更高的持续无疾病进展生存(HR 0.62,95%CI 0.44至0.87;1191名参与者;两项研究;中等质量证据);(c)至少发生一项不良事件的参与者数量略高(RR 1.04,95%CI 1.01至1.06;1248名参与者;两项研究;中等质量证据);(d)磁共振成像(MRI)上新发或扩大的T2高信号病变的参与者数量更低(RR 0.
