Uppsala Monitoring Centre, Uppsala, Sweden.
Centre for Applied Philosophy of Science, Norwegian University of Life Sciences, Ås, Norway.
Drug Saf. 2021 Sep;44(9):987-998. doi: 10.1007/s40264-021-01091-x. Epub 2021 Aug 10.
The safety profile of remdesivir, conditionally approved for COVID-19, was limited at its 2020 introduction. Adverse drug reactions (ADRs) for medicines are collected in VigiBase, the WHO Global Database of Individual Case Safety Reports (ICSRs).
This study aimed to provide a descriptive analysis of COVID-19 ICSR data focusing on remdesivir, including a disproportionality analysis (DA) of ADRs.
A dedicated algorithm enabled retrieval of all COVID-19 treatment-specific ICSRs. A severity algorithm based on co-reported medicines and symptoms enabled selection of tocilizumab with its well established safety profile as comparator for remdesivir. Descriptive statistics were used for general ICSR demographics for all COVID-19-specific medicines, remdesivir and tocilizumab individually and furthermore to present treatment patterns of medicines co-reported with remdesivir. A COVID-19 indication-focused DA was deployed to minimize confounding from underlying polysymptomatic disease.
14,574 COVID-19-related ICSRs were entered into VigiBase during 2020. Remdesivir was the most common medicine reported. Of 4944 remdesivir ICSRs, where tocilizumab was not co-reported, 93% described remdesivir as the sole suspect medicine. Sixty percent of ICSRs concerned males, median age was 63 years and the majority originated from the Americas (72%). In 1089 (21%) of remdesivir ICSRs, data indicated severe/critical disease. Co-reported medicines peaked during the first 3 days of remdesivir treatment. The DA for the established tocilizumab and the new remdesivir were mainly in line with the safety profiles for both medicines but suggested new safety concerns. The most reported ADRs for remdesivir represented liver dysfunction, kidney injury, death and bradycardia.
Global COVID-19-related ADR reporting proved useful in providing information on ADRs as well as on treatment patterns in this patient group. Indication-focused disproportionality analysis, together with the use of a comparator with a known safety profile, proved effective in identifying known safety information and suggested new safety concerns for remdesivir.
瑞德西韦于 2020 年获得有条件批准用于治疗 COVID-19,其安全性数据有限。药品不良反应(ADR)在世界卫生组织全球个体病例安全报告数据库(VigiBase)中进行收集。
本研究旨在提供 COVID-19 个体病例安全报告数据的描述性分析,重点关注瑞德西韦,并对 ADR 进行比例失衡分析(DA)。
使用专用算法检索所有 COVID-19 治疗特异性个体病例安全报告。基于共同报告药物和症状的严重程度算法,选择已确立安全性的托珠单抗作为瑞德西韦的对照药物。采用描述性统计方法对所有 COVID-19 特异性药物、瑞德西韦和托珠单抗的一般个体病例安全报告数据进行分析,并进一步展示与瑞德西韦共同报告的药物的治疗模式。采用 COVID-19 适应证聚焦的 DA 以尽量减少基础多病症状的混杂影响。
2020 年期间,VigiBase 共收录了 14574 份 COVID-19 相关个体病例安全报告。瑞德西韦是报告最常见的药物。在 4944 份未共同报告托珠单抗的瑞德西韦个体病例安全报告中,93%的报告将瑞德西韦单独列为可疑药物。60%的报告涉及男性,中位年龄为 63 岁,大多数报告来自美洲(72%)。在 1089 份(21%)瑞德西韦个体病例安全报告中,数据表明疾病为严重/危重症。共同报告的药物在瑞德西韦治疗的前 3 天达到峰值。针对已确立的托珠单抗和新的瑞德西韦的 DA 主要与这两种药物的安全性概况一致,但提示了新的安全性问题。瑞德西韦最报告的 ADR 为肝功能障碍、肾损伤、死亡和心动过缓。
全球 COVID-19 相关 ADR 报告为了解该患者群体的 ADR 信息和治疗模式提供了有用的数据。适应证聚焦的比例失衡分析,以及使用具有已知安全性概况的对照药物,在确定已知安全性信息和提示瑞德西韦新的安全性问题方面是有效的。
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