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向 FDA 报告的严重药物不良事件:FDA 不良事件报告系统 2006-2014 年数据库分析。

Serious Adverse Drug Events Reported to the FDA: Analysis of the FDA Adverse Event Reporting System 2006-2014 Database.

机构信息

1 Department of Health Services Research, Management and Policy, University of Florida, Gainesville.

2 Department of Health Outcomes Research and Policy, Auburn University, Auburn, Alabama.

出版信息

J Manag Care Spec Pharm. 2018 Jul;24(7):682-690. doi: 10.18553/jmcp.2018.24.7.682.

DOI:10.18553/jmcp.2018.24.7.682
PMID:29952714
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10397884/
Abstract

BACKGROUND

Data on adverse drug events (ADEs) observed at the population level provide important evidence regarding the safety of a pharmaceutical product in real-world settings. Recent patterns in serious and fatal ADE reporting have not been documented.

OBJECTIVE

To assess recent patterns in serious and fatal ADE reports in the United States.

METHODS

We conducted a retrospective analysis of the publicly available 2006-2014 FDA Adverse Event Reporting System database. Non-U.S. reports, reports from clinical trials, and reports with missing outcome data were excluded. The annual numbers of ADEs with reported outcome of death, disability, and other serious outcomes were determined. Types (direct, manufacturer expedited, or manufacturer periodic) and sources (consumer, health professional, or other) of these serious ADE reports were also identified. The distribution of serious ADE reports by patient age groups (< 18, 18-44, 45-64, and ≥ 65 years) was determined. Drugs listed as primary suspects in serious ADEs (death, disability, and other serious outcomes) were identified and ranked. Descriptive statistics were used to characterize the patterns in serious or fatal ADE reporting.

RESULTS

From 2006 to 2014, the number of serious ADEs reported to the FDA increased 2-fold. A total of 902,323 serious outcomes were reported over the 9-year study period: 244,408 deaths, 72,141 disabilities, and 585,774 other serious outcomes. The relative percentage of reports of deaths was highest during 2012 (32.4%). The percentage of reports of disability was highest during 2006 (12.1%). Overall, the "other serious outcomes" category accounted for almost 65% of serious ADEs reports. Expedited reports from drug manufacturers were most common (about 72%) of the serious ADEs with available data on report type. Health professionals (47.3%) were the most common source of report followed by consumers (36.1%) and other sources (16.6%). A disproportionately high number of reported ADEs was among patients aged 45-64 years (40%) and ≥ 65 years (32.6%). Antineoplastic drugs were more frequently reported with deaths. Three antidepressant drugs were among the top 10 drugs reported with disability. During 2006-2014, there were 38 drugs with more than 1,000 reports of serious ADEs in a given year: 2 drugs currently withdrawn from the market (rofecoxib and parecoxib), 10 drugs with an FDA risk evaluation and mitigation strategies (REMS) program, 13 biologic or specialty drugs, and 14 others.

CONCLUSIONS

An overall increase in the trend of the number of serious ADE reports was observed from 2006 to 2014. Drugs with a REMS program and biologic and specialty drugs were involved in a significant number of reported serious ADEs. Data on reporting patterns can guide surveillance and pharmacoepidemiological studies to understand the public health burden of serious ADEs.

DISCLOSURES

No outside funding supported this study. Hansen has received consulting fees from and has provided expert testimony for Daichii Sankyo and Takeda. The other authors have nothing to disclose.

摘要

背景

在人群水平上观察到的药物不良反应 (ADE) 数据为了解药物在真实环境中的安全性提供了重要证据。最近严重和致命 ADE 报告的模式尚未记录。

目的

评估美国最近严重和致命 ADE 报告的模式。

方法

我们对公开的 2006-2014 年 FDA 不良事件报告系统数据库进行了回顾性分析。排除非美国报告、临床试验报告和缺少结局数据的报告。确定了报告结局为死亡、残疾和其他严重结局的 ADE 年度数量。还确定了这些严重 ADE 报告的类型(直接、制造商加速或制造商定期)和来源(消费者、卫生专业人员或其他)。按患者年龄组(<18 岁、18-44 岁、45-64 岁和≥65 岁)确定严重 ADE 报告的分布情况。确定并对严重 ADE 中列为主要嫌疑药物(死亡、残疾和其他严重结局)进行排名。使用描述性统计来描述严重或致命 ADE 报告的模式。

结果

2006 年至 2014 年,向 FDA 报告的严重 ADE 数量增加了两倍。在 9 年的研究期间,共报告了 902,323 例严重结局:244,408 例死亡、72,141 例残疾和 585,774 例其他严重结局。2012 年报告死亡的比例最高(32.4%)。2006 年报告残疾的比例最高(12.1%)。总体而言,“其他严重结局”类别占严重 ADE 报告的近 65%。关于报告类型,有可用数据的严重 ADE 中,制造商加速报告最常见(约 72%)。卫生专业人员(47.3%)是报告的最常见来源,其次是消费者(36.1%)和其他来源(16.6%)。45-64 岁(40%)和≥65 岁(32.6%)患者报告的 ADE 数量不成比例地高。抗肿瘤药物更频繁地与死亡相关。三种抗抑郁药是报告残疾的十大药物之一。2006-2014 年期间,每年有 38 种药物报告严重 ADE 超过 1000 例:2 种药物目前已从市场撤出(罗非昔布和帕瑞昔布),10 种药物有 FDA 风险评估和缓解策略(REMS)计划,13 种生物或专科药物和 14 种其他药物。

结论

从 2006 年到 2014 年,严重 ADE 报告数量的总体趋势呈上升趋势。有 REMS 计划和生物和专科药物的药物涉及大量报告的严重 ADE。报告模式数据可指导监测和药物流行病学研究,以了解严重 ADE 的公共卫生负担。

披露

本研究没有外部资金支持。Hansen 曾为 Daiichi Sankyo 和 Takeda 提供咨询费并提供专家证词。其他作者没有任何要披露的内容。