关于孤儿药研究与欧洲药品管理局(EMA)在欧洲的授权上市决定相关的临床评估。
The clinical assessment of studies on orphan drugs in relation to the EMA's authorization marketing decisions in Europe.
作者信息
Jakubowski Szczepan, Malinowski Krzysztof Piotr, Kawalec Paweł
机构信息
Department of Health Promotion and e-Health, Faculty of Health of Science, Jagiellonian University Medical College, Kraków, Poland.
Department of Bioinformatics and Telemedicine, Faculty of Medicine, Jagiellonian University Medical College, Kraków, Poland.
出版信息
Front Pharmacol. 2025 Mar 31;16:1558987. doi: 10.3389/fphar.2025.1558987. eCollection 2025.
INTRODUCTION
The main objective of this study was to assess the correlation between the methodological characteristics of clinical trials on orphan drugs and the special statuses granted by the European Medicines Agency (EMA).
MATERIAL AND METHODS
Data were collected for all medicines with orphan designation assigned by 2020. From August 2019 to June 2020, special statuses (authorization statuses and registration requirements) and general information on orphan drugs were obtained from the EMA's web-based registry. The following clinical data were collected: number of patients, clinical phase, randomization, masking, control group, treatment durations, and safety and efficacy follow-ups. Descriptive, comparative, multivariate, and univariate analyses of data were conducted.
RESULTS
Results were provided for 105 medicines with orphan designation. The odds of an orphan drug receiving conditional approval were lower for studies with randomization (p = 0.002) and active controlled trials (p = 0.010), but they increased in those with a treatment duration of 3-12 months (p = 0.002) and those with a safety and efficacy follow-up of 2-6 months (p = 0.008 and p = 0.035, respectively). Approval under exceptional circumstances was less likely for each additional 1,000 patients included in reference (p = 0.002), randomization (p = 0.024), double blinding (p = 0.033), and active-controlled trials (p = 0.006). However, it was more likely for phase II/III trials (p = 0.039), those with a treatment duration of 3-12 months (p = 0.03), and those with a safety and efficacy follow-up longer than 6 months (p = 0.022 and p = 0.047, respectively).
CONCLUSION
The types of clinical trials and their methodological characteristics are correlated with the EMA's decisions. Randomization, double blinding, and active-controlled trials reduce the odds of ODs receiving EMA special statuses. In contrast, phase II/III trials, specific durations of treatment, and specific safety and efficacy follow-ups increased these odds.
引言
本研究的主要目的是评估孤儿药临床试验的方法学特征与欧洲药品管理局(EMA)授予的特殊地位之间的相关性。
材料与方法
收集了截至2020年获得孤儿药指定的所有药物的数据。2019年8月至2020年6月,从EMA的基于网络的注册中心获取了孤儿药的特殊地位(批准状态和注册要求)及一般信息。收集了以下临床数据:患者数量、临床阶段、随机分组、设盲、对照组、治疗持续时间以及安全性和疗效随访。对数据进行了描述性、比较性、多变量和单变量分析。
结果
提供了105种获得孤儿药指定药物的结果。对于采用随机分组的研究(p = 0.002)和活性药物对照试验(p = 0.010),孤儿药获得有条件批准的几率较低,但在治疗持续时间为3至12个月的研究中(p = 0.002)以及安全性和疗效随访时间为2至6个月的研究中(分别为p = 0.008和p = 0.035),该几率有所增加。每增加1000名纳入参考的患者(p = 0.002)、随机分组(p = 0.024)、双盲(p = 0.033)和活性药物对照试验(p = 0.006),在特殊情况下获得批准的可能性就越小。然而,对于II/III期试验(p = 0.039)、治疗持续时间为3至12个月的试验(p = 0.03)以及安全性和疗效随访时间超过6个月的试验(分别为p = 0.022和p = 0.047),获得批准的可能性更大。
结论
临床试验的类型及其方法学特征与EMA的决策相关。随机分组、双盲和活性药物对照试验降低了孤儿药获得EMA特殊地位的几率。相比之下,II/III期试验、特定的治疗持续时间以及特定的安全性和疗效随访增加了这些几率。
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