Identifying Pediatric Drug Safety Knowledge Gaps: An Integrated Approach Leveraging Real-World Data, a Biomedical Knowledge Base, and Postmarketing Surveillance Data.

IF 3.4 3区医学 Q2 PHARMACOLOGY & PHARMACY

Pharmacotherapy Pub Date : 2025-10-01 DOI:10.1002/phar.70061

Saurabh Rahurkar, Jiayi Ouyang, Pallavi Jonnalagadda, Xiaofu Liu, Shijun Zhang, Chien-Wei Chiang, Lei Wang, Aditi Shendre, Lang Li

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引用次数: 0

Abstract

Background: Drug safety has historically been understudied in pediatric populations, rendering them "therapeutic orphans." Pediatric drug indications and dosages are often inferred by extrapolating safety, efficacy, and dosing data from adult studies, leading to widespread off-label use. However, this approach fails to account for age-specific differences in disease pathophysiology and developmental pharmacokinetics (PK). Despite evidence that adverse drug events (ADEs) manifest with greater severity in pediatric populations than in adults, fewer than 50% of drugs have been systematically studied for pediatric use. The lack of robust drug safety data may result in suboptimal or harmful treatment strategies.

Methods: We used a data-driven approach that integrated three databases -including Merative MarketScan claims, the Maternal and Pediatric Precision in Therapeutics (MPRINT) Knowledgebase (including 670,185 pediatric pharmacoepidemiology, PK, and clinical trial publications on 5062 drugs), the United States Food and Drug Administration (FDA) Adverse Event Reporting System (FAERS, a postmarketing safety surveillance database), and FDA drug label data- to identify high-impact target. High-impact targets were defined as drugs that have a high prescription volume, limited safety evidence and high risk of serious ADEs.

Results: With 229,550 prescriptions in MarketScan, only 9 studies, and almost 50 high risk serious ADEs benzonatate was identified as a high-impact drug of concern. Serious ADEs included seizure, death, and arrhythmia with proportional reportion ratios (PRRs) ranging from 4.3 to 477.8.

Conclusion: Approved in 1958, Benzonatate, a nonnarcotic antitussive agent has a limited safety evidence with only nine PE/PK publications in six decades. Moreover, it is frequently prescribed off-label for cough relief despite questionable effectiveness, and high-risk of serious ADEs. Our findings reveal a disconnect between clinical practice and suppporting safety evidence. As such, there is critical need to study the safety of this drug using emerging real-world data for real-world evidence. In summary, this study presents an approach that is systematic, objective, reproducible, and data driven to identify and prioritize drug-ADE combinations with limited evidence.

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识别儿科药物安全知识缺口：利用真实世界数据、生物医学知识库和上市后监测数据的综合方法。

背景：药物安全性在儿科人群中的研究一直不足，使他们成为“治疗孤儿”。儿童药物的适应症和剂量通常是通过推断成人研究的安全性、有效性和剂量数据来推断的，导致广泛的标签外使用。然而，这种方法无法解释疾病病理生理和发育药代动力学（PK）的年龄特异性差异。尽管有证据表明，儿童人群的药物不良事件（ADEs）比成人更严重，但针对儿童使用的药物进行了系统研究的药物还不到50%。缺乏可靠的药物安全性数据可能导致次优或有害的治疗策略。方法：我们采用数据驱动的方法，整合了三个数据库，包括Merative MarketScan声明、母婴精准治疗（MPRINT）知识库（包括670,185个儿科药物流行病学、PK和5062种药物的临床试验出版物）、美国食品和药物管理局（FDA）不良事件报告系统（FAERS，一个上市后安全监测数据库）和FDA药物标签数据，以确定高影响目标。高影响靶点被定义为处方量大、安全性证据有限和严重ade风险高的药物。结果：在MarketScan的229,550张处方中，只有9项研究和近50项高风险严重ade苯甲酸酯被确定为高影响药物。严重的不良事件包括癫痫发作、死亡和心律失常，比例报告比（PRRs）从4.3到477.8不等。结论：苯并酸盐是一种非麻醉性止咳剂，于1958年获得批准，其安全性证据有限，60年来仅有9篇PE/PK出版物。此外，尽管它的有效性值得怀疑，但它经常被用于治疗咳嗽，并有严重不良反应的高风险。我们的发现揭示了临床实践和支持安全性证据之间的脱节。因此，迫切需要使用新兴的真实世界数据来研究这种药物的安全性。总之，本研究提出了一种系统、客观、可重复性和数据驱动的方法，以有限的证据识别和优先考虑药物- ade组合。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Pharmacotherapy 医学-药学

CiteScore

7.80

自引率

2.40%

发文量

审稿时长

4-8 weeks

期刊介绍： Pharmacotherapy is devoted to publication of original research articles on all aspects of human pharmacology and review articles on drugs and drug therapy. The Editors and Editorial Board invite original research reports on pharmacokinetic, bioavailability, and drug interaction studies, clinical trials, investigations of specific pharmacological properties of drugs, and related topics.