School of Public Health, University of the Witwatersrand, Johannesburg, South Africa.
University of Malawi, College of Medicine, Blantyre, Malawi.
Malar J. 2020 Mar 20;19(1):119. doi: 10.1186/s12936-020-03190-z.
Drug safety assessments in clinical trials present unique analytical challenges. Some of these include adjusting for individual follow-up time, repeated measurements of multiple outcomes and missing data among others. Furthermore, pre-specifying appropriate analysis becomes difficult as some safety endpoints are unexpected. Although existing guidelines such as CONSORT encourage thorough reporting of adverse events (AEs) in clinical trials, they provide limited details for safety data analysis. The limited guidelines may influence suboptimal analysis by failing to account for some analysis challenges above. A typical example where such challenges exist are trials of anti-malarial drugs for malaria prevention during pregnancy. Lack of proper standardized evaluation of the safety of antimalarial drugs has limited the ability to draw conclusions about safety. Therefore, a systematic review was conducted to establish the current practice in statistical analysis for preventive antimalarial drug safety in pregnancy.
The search included five databases (PubMed, Embase, Scopus, Malaria in Pregnancy Library and Cochrane Central Register of Controlled Trials) to identify original English articles reporting Phase III randomized controlled trials (RCTs) on anti-malarial drugs for malaria prevention in pregnancy published from January 2010 to July 2019.
Eighteen trials were included in this review that collected multiple longitudinal safety outcomes including AEs. Statistical analysis and reporting of the safety outcomes in all the trials used descriptive statistics; proportions/counts (n = 18, 100%) and mean/median (n = 2, 11.1%). Results presentation included tabular (n = 16, 88.9%) and text description (n = 2, 11.1%). Univariate inferential methods were reported in most trials (n = 16, 88.9%); including Chi square/Fisher's exact test (n = 12, 66.7%), t test (n = 2, 11.1%) and Mann-Whitney/Wilcoxon test (n = 1, 5.6%). Multivariable methods, including Poisson and negative binomial were reported in few trials (n = 3, 16.7%). Assessment of a potential link between missing efficacy data and safety outcomes was not reported in any of the trials that reported efficacy missing data (n = 7, 38.9%).
The review demonstrated that statistical analysis of safety data in anti-malarial drugs for malarial chemoprevention in pregnancy RCTs is inadequate. The analyses insufficiently account for multiple safety outcomes potential dependence, follow-up time and informative missing data which can compromise anti-malarial drug safety evidence development, based on the available data.
临床试验中的药物安全性评估带来了独特的分析挑战。其中一些挑战包括调整个体随访时间、多次测量多个结局以及数据缺失等。此外,由于某些安全性终点是意外的,因此预先指定适当的分析变得困难。尽管现有的指南(如 CONSORT)鼓励在临床试验中全面报告不良事件(AE),但它们为安全性数据分析提供的细节有限。这些有限的指南可能会因为没有考虑到上述某些分析挑战而导致分析结果不理想。一个典型的例子是在预防妊娠疟疾期间使用抗疟药物的临床试验。缺乏对抗疟药物安全性的适当标准化评估,限制了我们对安全性的结论。因此,我们进行了一项系统评价,以确定当前预防妊娠疟疾中抗疟药物安全性的统计分析实践。
该检索包括五个数据库(PubMed、Embase、Scopus、妊娠疟疾文库和 Cochrane 对照试验中心注册库),以确定 2010 年 1 月至 2019 年 7 月期间发表的预防妊娠疟疾的抗疟药物 III 期随机对照试验(RCT)的原始英文文章。
本综述共纳入 18 项试验,这些试验均收集了多个纵向安全性结局,包括 AE。所有试验均使用描述性统计方法对安全性结局进行统计分析和报告;比例/计数(n=18,100%)和均值/中位数(n=2,11.1%)。结果展示包括表格(n=16,88.9%)和文本描述(n=2,11.1%)。大多数试验报告了单变量推论方法(n=16,88.9%);包括卡方/ Fisher 精确检验(n=12,66.7%)、t 检验(n=2,11.1%)和 Mann-Whitney/Wilcoxon 检验(n=1,5.6%)。少数试验报告了多变量方法,包括泊松分布和负二项分布(n=3,16.7%)。在报告疗效缺失数据的试验中(n=7,38.9%),没有报告缺失疗效数据与安全性结局之间潜在关联的评估。
本综述表明,预防妊娠疟疾的抗疟药物 RCT 中安全性数据分析不充分。根据现有数据,分析未能充分考虑多个安全性结局的潜在依赖性、随访时间和信息性缺失数据,这可能会影响抗疟药物安全性证据的发展。
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