Landscape of Post-Marketing Requirements Under the Pediatric Research Equity Act for Antibiotics from 2009-2024.

IF 4.6 2区医学 Q1 INFECTIOUS DISEASES

Antibiotics-Basel Pub Date : 2025-06-06 DOI:10.3390/antibiotics14060583

Daniel Selig, Funmi Aminu, Sue Cammarata, Ting Chen, Lauren Dolak, Stephen Duprez, Stephanie Ecker, Lisa Gault, Sandra George, Margaret Harkins, Clayton Litchmore, Michael Serenko, William Waverczak, Doug Girgenti

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引用次数: 0

Abstract

Background/Objectives: We reviewed Post-Marketing Requirements (PMRs) under the Pediatric Research Equity Act (PREA) for antibiotics approved in adults from 2009 to 2024 to better understand factors associated with PMR study completion. Methods: Initial PMRs, including study design and completion timelines were extracted from Food and Drug Administration (FDA) approval letters. Studies were cross-referenced at clinicaltrials.gov, with follow-up from adult approval to study completion or through 31 December 2024. Results: Eighteen antibiotics were approved in adults from 2009 to 2024, with 53 associated PREA PMRs. A total of nine PMRs were excluded from analysis (six exclusions for projected study completion dates on or after 12/31/2024, one exclusion due to lack of information, and two exclusions because the study type was not categorizable as Phase 1 or Phase 2). Of the 44 remaining PMRs in the analysis set, the median pediatric study follow-up time from adult approval was 5.3 years (range 0.94 to 11.5 years), with a study completion rate of 54.5% (N = 24). Small- and medium-sized companies had a study completion rate of 10% (N = 2/20) over a median of 6.44 years of follow-up, with no pediatric approvals. Large pharmaceutical corporations had a significantly higher study completion rate of 91.6% (N = 22/24; adjusted hazard ratio 20.3 95%CI, 5.02 to 82.4) over a median follow-up time of 4.7 years and achieved pediatric approval with labelling updates for 75% of antibiotics (N = 6/8). Conclusions: Compared to larger organizations, smaller pharmaceutical companies have experienced difficulty in PREA PMR antibiotic study completion, which may be related to financial difficulties in the challenging market for antibiotics. To improve PMR study completion, smaller companies require continued financial support and innovation in study design. For pediatric antibiotic development, the FDA accepts the extrapolation of efficacy from well-conducted randomized adult trials (i.e., pharmacokinetics (PK) and the safety approach). Therefore, sponsors should consider the use of single-arm, non-comparative PK and safety study designs to reduce the size and scope of trials. Sponsors should also assess whether the evaluation of an antibiotic is necessary in adolescents, or if data in a surrogate population of adults (e.g., low-weight adults) may serve as adequate evidence for adolescent approval.

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2009-2024年儿科研究公平法案下抗生素上市后要求的景观。

背景/目的：我们回顾了2009年至2024年儿科研究公平法案（PREA）下批准的成人抗生素上市后要求（PMR），以更好地了解与PMR研究完成相关的因素。方法：从美国食品和药物管理局（FDA）的批准信中提取初始pmr，包括研究设计和完成时间。研究在clinicaltrials.gov上进行了交叉参考，从成人批准到研究完成或到2024年12月31日进行了随访。结果：2009年至2024年，18种抗生素被批准用于成人，53种相关PREA pmr。共有9例pmr被排除在分析之外（6例因预计研究完成日期为2024年12月31日或之后而排除，1例因缺乏信息而排除，2例因研究类型不能划分为1期或2期而排除）。在分析集中剩余的44个pmr中，从成人批准开始的中位儿科研究随访时间为5.3年（范围0.94至11.5年），研究完成率为54.5% （N = 24）。中小型公司的研究完成率为10% (N = 2/20)，随访中位数为6.44年，没有儿科批准。大型制药公司的研究完成率为91.6% (N = 22/24；调整后的风险比为20.3 (95%CI, 5.02 - 82.4)，中位随访时间为4.7年，75%的抗生素标签更新后获得儿科批准（N = 6/8）。结论：与大型组织相比，小型制药公司在完成PREA PMR抗生素研究方面遇到了困难，这可能与抗生素挑战性市场中的资金困难有关。为了提高PMR研究的完成率，小型公司需要持续的财政支持和研究设计的创新。对于儿科抗生素的开发，FDA接受从进行良好的随机成人试验（即药代动力学（PK）和安全性方法）中推断出的疗效。因此，申办者应考虑使用单臂、非比较性PK和安全性研究设计来减少试验的规模和范围。申办者还应评估是否有必要对青少年进行抗生素评估，或者成人替代人群（如低体重成年人）的数据是否可以作为青少年批准的充分证据。

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来源期刊

Antibiotics-Basel Pharmacology, Toxicology and Pharmaceutics-General Pharmacology, Toxicology and Pharmaceutics

CiteScore

7.30

自引率

14.60%

发文量

1547

审稿时长

11 weeks

期刊介绍： Antibiotics (ISSN 2079-6382) is an open access, peer reviewed journal on all aspects of antibiotics. Antibiotics is a multi-disciplinary journal encompassing the general fields of biochemistry, chemistry, genetics, microbiology and pharmacology. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. Therefore, there is no restriction on the length of papers.