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大麻素用于进行性炎症性脑病(CUPID)试验:一项随机双盲安慰剂对照平行组多中心试验及大麻素延缓多发性硬化症进展的经济学评估。

The Cannabinoid Use in Progressive Inflammatory brain Disease (CUPID) trial: a randomised double-blind placebo-controlled parallel-group multicentre trial and economic evaluation of cannabinoids to slow progression in multiple sclerosis.

作者信息

Ball Susan, Vickery Jane, Hobart Jeremy, Wright Dave, Green Colin, Shearer James, Nunn Andrew, Cano Mayam Gomez, MacManus David, Miller David, Mallik Shahrukh, Zajicek John

机构信息

Centre for Biostatistics, Bioinformatics and Biomarkers, Plymouth University Peninsula Schools of Medicine and Dentistry, Plymouth, UK.

Peninsula Clinical Trials Unit, Plymouth University Peninsula Schools of Medicine and Dentistry, Plymouth, UK.

出版信息

Health Technol Assess. 2015 Feb;19(12):vii-viii, xxv-xxxi, 1-187. doi: 10.3310/hta19120.

DOI:10.3310/hta19120
PMID:25676540
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4781163/
Abstract

BACKGROUND

The Cannabinoid Use in Progressive Inflammatory brain Disease (CUPID) trial aimed to determine whether or not oral Δ(9)-tetrahydrocannabinol (Δ(9)-THC) slowed the course of progressive multiple sclerosis (MS); evaluate safety of cannabinoid administration; and, improve methods for testing treatments in progressive MS.

OBJECTIVES

There were three objectives in the CUPID study: (1) to evaluate whether or not Δ(9)-THC could slow the course of progressive MS; (2) to assess the long-term safety of Δ(9)-THC; and (3) to explore newer ways of conducting clinical trials in progressive MS.

DESIGN

The CUPID trial was a randomised, double-blind, placebo-controlled, parallel-group, multicentre trial. Patients were randomised in a 2 : 1 ratio to Δ(9)-THC or placebo. Randomisation was balanced according to Expanded Disability Status Scale (EDSS) score, study site and disease type. Analyses were by intention to treat, following a pre-specified statistical analysis plan. A cranial magnetic resonance imaging (MRI) substudy, Rasch measurement theory (RMT) analyses and an economic evaluation were undertaken.

SETTING

Twenty-seven UK sites.

PARTICIPANTS

Adults aged 18-65 years with primary or secondary progressive MS, 1-year evidence of disease progression and baseline EDSS 4.0-6.5.

INTERVENTIONS

Oral Δ(9)-THC (maximum 28 mg/day) or matching placebo.

ASSESSMENT VISITS

Three and 6 months, and then 6-monthly up to 36 or 42 months.

MAIN OUTCOME MEASURES

Primary outcomes were time to EDSS progression, and change in Multiple Sclerosis Impact Scale-29 version 2 (MSIS-29v2) 20-point physical subscale (MSIS-29phys) score. Various secondary patient- and clinician-reported outcomes and MRI outcomes were assessed. RMT analyses examined performance of MS-specific rating scales as measurement instruments and tested for a symptomatic or disease-modifying treatment effect. Economic evaluation estimated mean incremental costs and quality-adjusted life-years (QALYs).

RESULTS

Effectiveness - recruitment targets were achieved. Of the 498 randomised patients (332 to active and 166 to placebo), 493 (329 active and 164 placebo) were analysed.

PRIMARY OUTCOMES

no significant treatment effect; hazard ratio EDSS score progression (active : placebo) 0.92 [95% confidence interval (CI) 0.68 to 1.23]; and estimated between-group difference in MSIS-29phys score (active-placebo) -0.9 points (95% CI -2.0 to 0.2 points). Secondary clinical and MRI outcomes: no significant treatment effects. Safety - at least one serious adverse event: 35% and 28% of active and placebo patients, respectively. RMT analyses - scale evaluation: MSIS-29 version 2, MS Walking Scale-12 version 2 and MS Spasticity Scale-88 were robust measurement instruments. There was no clear symptomatic or disease-modifying treatment effect. Economic evaluation - estimated mean incremental cost to NHS over usual care, over 3 years £27,443.20 per patient. No between-group difference in QALYs.

CONCLUSIONS

The CUPID trial failed to demonstrate a significant treatment effect in primary or secondary outcomes. There were no major safety concerns, but unwanted side effects seemed to affect compliance. Participants were more disabled than in previous studies and deteriorated less than expected, possibly reducing our ability to detect treatment effects. RMT analyses supported performance of MS-specific rating scales as measures, enabled group- and individual person-level examination of treatment effects, but did not influence study inferences. The intervention had significant additional costs with no improvement in health outcomes; therefore, it was dominated by usual care and not cost-effective. Future work should focus on determining further factors to predict clinical deterioration, to inform the development of new studies, and modifying treatments in order to minimise side effects and improve study compliance. The absence of disease-modifying treatments in progressive MS warrants further studies of the cannabinoid pathway in potential neuroprotection.

TRIAL REGISTRATION

Current Controlled Trials ISRCTN62942668.

FUNDING

The National Institute for Health Research Health Technology Assessment programme, the Medical Research Council Efficacy and Mechanism Evaluation programme, Multiple Sclerosis Society and Multiple Sclerosis Trust. The report will be published in full in Health Technology Assessment; Vol. 19, No. 12. See the NIHR Journals Library website for further project information.

摘要

背景

大麻素用于进行性炎症性脑病(CUPID)试验旨在确定口服Δ⁹ - 四氢大麻酚(Δ⁹ - THC)是否能减缓进展型多发性硬化症(MS)的病程;评估大麻素给药的安全性;并改进进展型MS治疗方法的测试。

目的

CUPID研究有三个目标:(1)评估Δ⁹ - THC是否能减缓进展型MS的病程;(2)评估Δ⁹ - THC的长期安全性;(3)探索进展型MS临床试验的新方法。

设计

CUPID试验是一项随机、双盲、安慰剂对照、平行组、多中心试验。患者按2∶1的比例随机分配至Δ⁹ - THC组或安慰剂组。随机化根据扩展残疾状态量表(EDSS)评分、研究地点和疾病类型进行平衡。分析采用意向性分析,遵循预先指定的统计分析计划。进行了一项头颅磁共振成像(MRI)子研究、拉施测量理论(RMT)分析和一项经济评估。

地点

英国27个地点。

参与者

年龄在18 - 65岁之间,患有原发性或继发性进展型MS,有1年疾病进展证据且基线EDSS为4.0 - 6.5的成年人。

干预措施

口服Δ⁹ - THC(最大剂量28毫克/天)或匹配的安慰剂。

评估访视

3个月和6个月时进行评估,然后每6个月评估一次,直至36或42个月。

主要结局指标

主要结局为EDSS进展时间以及多发性硬化症影响量表29版本2(MSIS - 29v2)20分身体亚量表(MSIS - 29phys)评分的变化。评估了各种次要的患者和临床医生报告的结局以及MRI结局。RMT分析检查了MS特异性评定量表作为测量工具的性能,并测试了对症或疾病修饰治疗效果。经济评估估计了平均增量成本和质量调整生命年(QALYs)。

结果

有效性 - 达到了招募目标。在498名随机分组的患者中(332名接受活性药物治疗,166名接受安慰剂治疗),对493名患者(329名接受活性药物治疗,164名接受安慰剂治疗)进行了分析。

主要结局

无显著治疗效果;EDSS评分进展的风险比(活性药物∶安慰剂)为0.92 [95%置信区间(CI)0.68至1.23];MSIS - 29phys评分的组间估计差异(活性药物 - 安慰剂)为 - 0.9分(95% CI - 2.0至0.2分)。次要临床和MRI结局:无显著治疗效果。安全性 - 至少发生一次严重不良事件:活性药物组和安慰剂组患者分别为35%和28%。RMT分析 - 量表评估:MSIS - 29版本2、MS步行量表12版本2和MS痉挛量表88是可靠的测量工具。没有明显的对症或疾病修饰治疗效果。经济评估 - 估计国民健康服务体系(NHS)在3年期间每位患者相对于常规护理的平均增量成本为27,443.20英镑。QALYs在组间无差异。

结论

CUPID试验未能在主要或次要结局中证明显著的治疗效果。没有重大安全问题,但不良副作用似乎影响了依从性。参与者比以往研究中的患者残疾程度更高,病情恶化程度低于预期,这可能降低了我们检测治疗效果的能力。RMT分析支持MS特异性评定量表作为测量工具的性能,能够在组和个体层面检查治疗效果,但不影响研究推断。该干预措施有显著的额外成本,且健康结局无改善;因此,它被常规护理所主导,不具有成本效益。未来的工作应侧重于确定进一步预测临床恶化的因素,为新研究的开展提供信息,并调整治疗方法以尽量减少副作用并提高研究依从性。进展型MS缺乏疾病修饰治疗方法,这使得有必要进一步研究大麻素途径在潜在神经保护中的作用。

试验注册

当前受控试验ISRCTN62942668。

资助

英国国家卫生研究院健康技术评估项目、医学研究理事会疗效与机制评估项目、多发性硬化症协会和多发性硬化症信托基金。该报告将全文发表在《健康技术评估》;第19卷,第12期。有关进一步的项目信息,请参阅NIHR期刊图书馆网站。