Departament de Farmacologia, de Terapèutica i de Toxicologia, Unitat Docent Parc Taulí, Universitat Autònoma de Barcelona, C/Parc Taulí, 1, 08208, Sabadell, Spain.
Unitat de Farmacologia Clínica, Institut d'Investigació i Innovació Parc Taulí I3PT, Parc Taulí Hospital Universitari, Universitat Autònoma de Barcelona, Parc Taulí 1, 08028, Sabadell, Barcelona, Spain.
Orphanet J Rare Dis. 2018 Nov 15;13(1):206. doi: 10.1186/s13023-018-0926-z.
To assess uncertainty in regulatory decision-making for orphan medicinal products (OMP), a summary of the current basis for approval is required; a systematic grouping of medical conditions may be useful in summarizing information and issuing recommendations for practice.
A grouping of medical conditions with similar characteristics regarding the potential applicability of methods and designs was created using a consensus approach. The 125 dossiers for authorised OMP published between 1999 and 2014 on the EMA webpage were grouped accordingly and data was extracted from European Public Assessment Reports (EPARs) to assess the extent and robustness of the pivotal evidence supporting regulatory decisions.
88% (110/125) of OMP authorizations were based on clinical trials, with 35% (38/110) including replicated pivotal trials. The mean (SD) number of pivotal trials per indication was 1.4 (0.7), and the EPARs included a median of three additional non-pivotal supportive studies. 10% of OMPs (13/125) were authorised despite only negative pivotal trials. One-third of trials (53/159) did not include a control arm, one-third (50/159) did not use randomisation, half the trials (75/159) were open-label and 75% (119/159) used intermediate or surrogate variables as the main outcome. Chronic progressive conditions led by multiple system/organs, conditions with single acute episodes and progressive conditions led by one organ/system were the groups where the evidence deviated most from conventional standards. Conditions with recurrent acute episodes had the most robust datasets. The overall size of the exposed population at the time of authorisation of OMP - mean(SD) 190.5 (202.5) - was lower than that required for the qualification of clinically-relevant adverse reactions.
The regulatory evidence supporting OMP authorization showed substantial uncertainties, including weak protection against errors, substantial use of designs unsuited for conclusions on causality, use of intermediate variables, lack of a priorism and insufficient safety data to quantify risks of relevant magnitude. Grouping medical conditions based on clinical features and their methodological requirements may facilitate specific methodological and regulatory recommendations for the study of OMP to strengthen the evidence base.
为了评估孤儿药监管决策的不确定性,需要对当前批准依据进行总结;对医学病症进行系统分组有助于对信息进行总结,并为实践提供建议。
采用共识方法创建了一个具有相似特征的医学病症分组,这些特征涉及到方法和设计的潜在适用性。根据这一分组,对 1999 年至 2014 年期间在 EMA 网页上公布的 125 份已批准的孤儿药档案进行分组,并从欧洲公共评估报告(EPAR)中提取数据,以评估支持监管决策的关键证据的充分性和稳健性。
88%(110/125)的孤儿药批准是基于临床试验的,其中 35%(38/110)包含重复的关键性试验。每个适应证的平均(SD)关键性试验数量为 1.4(0.7),EPAR 中包含中位数为 3 项额外的非关键性支持性研究。10%(13/125)的孤儿药是在仅有阴性关键性试验的情况下获得批准的。三分之一的试验(53/159)没有对照组,三分之一(50/159)没有随机分组,一半的试验(75/159)是开放性的,75%(119/159)使用中间或替代变量作为主要结局。多系统/器官慢性进行性疾病、单一急性发作疾病和单一器官/系统进行性疾病是证据与常规标准偏差最大的组。有反复发作急性发作的疾病具有最稳健的数据集。在孤儿药获得批准时,暴露人群的总体规模(平均值(SD)190.5(202.5))低于确定与临床相关不良反应所需的规模。
支持孤儿药批准的监管证据存在很大的不确定性,包括错误保护不足、大量使用不适合因果关系结论的设计、使用中间变量、缺乏优先性和不充分的安全性数据来量化相关规模的风险。基于临床特征及其方法学要求对医学病症进行分组,可能有助于为孤儿药研究提供具体的方法学和监管建议,以加强证据基础。
