南非保健品管理局(SAHPRA)实施基于风险的评估方法。

IF 3.1 Q2 PHARMACOLOGY & PHARMACY
Pharmaceutical Medicine Pub Date : 2023-01-01 Epub Date: 2023-01-04 DOI:10.1007/s40290-022-00452-w
Lerato Moeti, Madira Litedu, Jacques Joubert
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引用次数: 0

摘要

背景:大量积压的未决监管决定是南非健康产品管理局(SAHPRA)从药品管制委员会(MCC)继承下来的主要历史挑战之一。修订和实施新的监管途径是南非保健品监管局规避这一问题的战略机制之一:为缓解积压问题,我们探索了一种新的审查途径,即对科学质量和生物等效性评估进行基于风险的审查。该研究的目的是阐明基于风险的评估(RBA)途径,确定药品风险等级分类的可靠标准,并确定药品评估和审批过程中应遵循的改进流程:2015 年,SAHPRA 开展了一项广泛的工作,以确定流程中申请的未知状态。RBA 试点项目于 2016 年启动,并利用 2016 年研究中获得的知识在 2021 年进一步试点,以优化效率:截至 2015 年,处于预注册阶段的积压申请数量为 7902 份。2015 年的项目包括两个阶段。第一阶段是确定 3505 份正在处理的申请的状态,最终登记了 198 份申请。第二阶段于 2016 年开始,对 4397 份尚未审查的申请进行了审查,并据此探索了 RBA 方法。由于制定了风险分类标准并完善了端到端注册流程,试点的最终确定时间中值为 90 个日历日,审批时间中值为 109 个日历日。在 2021 年进行的《风险评估》试点研究中,63 项申请的最终审批时间为 68 个日历日。与SAHPRA为2019年启动的积压清理计划所采用的现行流程的501个日历日相比,这些审批时间较短。从科学评估分配之日起计算,2016 年和 2021 年研究的批准时间相似。据报告,两项研究的评估时间分别为:低风险质量评估6-7小时,高风险质量评估9-10小时,生物等效性评估7-8小时,生物豁免和初步反应评估2-3小时:结论:本文详细介绍了为缓解 SAHPRA 积压而在基于风险的试点研究中采用的改进流程。与SAHPRA在2019年启动的积压清除计划中采用的现行流程所需的501个日历日相比,该流程可将最终确定时间缩短至68个日历日。因此,RBA 方法缩短了监管机构质量和生物等效性评估的最终确定和审批时间,同时又不影响医药产品的质量、安全性和有效性。此外,该方法还提供了一个原型解决方案,以应对监管机构收到的大量医药产品申请。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The Implementation of a Risk-Based Assessment Approach by the South African Health Products Regulatory Authority (SAHPRA).

The Implementation of a Risk-Based Assessment Approach by the South African Health Products Regulatory Authority (SAHPRA).

The Implementation of a Risk-Based Assessment Approach by the South African Health Products Regulatory Authority (SAHPRA).

The Implementation of a Risk-Based Assessment Approach by the South African Health Products Regulatory Authority (SAHPRA).

Background: An extensive backlog of pending regulatory decisions is one of the major historical challenges that the South African Health Products Regulatory Authority (SAHPRA) inherited from the Medicine Control Council (MCC). Revising and implementing new regulatory pathways is one of the strategic mechanisms that SAHPRA employs to circumvent this problem.

Objectives: To alleviate the backlog, the use of a new review pathway termed the risk-based review on the scientific quality and bioequivalence assessments was explored. The objective of the study was to articulate the risk-based assessment (RBA) pathway, to determine robust criteria for the classification of the levels of risk for medicines, and to define the improved process to be followed in the assessment and approval of medicines.

Methods: In 2015, an extensive exercise was conducted by SAHPRA to identify the unknown status of in-process applications. The RBA pilot project commenced in 2016 and further piloted in 2021 using the knowledge gained from the 2016 study for optimisation of efficiency.

Results: By 2015 the backlog was quantified as 7902 applications in the pre-registration phase. The 2015 project entailed two phases. The initial phase was conducted to identify the status of 3505 in-process applications, which resulted in the registration of 198 applications. The second phase commenced in 2016 on 4397 applications not yet reviewed whereby the RBA approach was explored. With the developed criteria for risk classification and refined end-to-end registration process, the pilot resulted in a finalisation time with a median value of 90 calendar days and a median approval time of 109 calendar days. The throughput of the RBA pilot study conducted in 2021 was 68 calendar days finalisation time for the 63 applications used. These finalisation times are lower in comparison to the 501 calendar days for the current process employed by SAHPRA for the backlog clearance programme initiated in 2019. Both the 2016 and 2021 studies had similar approval times calculated from the date of allocation of scientific assessments. The reported evaluation timelines for both studies were within 6-7 h for a low-risk quality assessment, 9-10 h for a high-risk quality assessment, 7-8 h for a bioequivalence assessment, and 2-3 h for a biowaiver and initial response assessment.

Conclusions: The refined processes used in the risk-based pilot studies to alleviate the SAHPRA backlog are described in detail. The process managed a reduction of the finalisation time to 68 calendar days in comparison to 501 calendar days for the current process that was employed by SAHPRA for the backlog clearance programme initiated in 2019. The RBA approach, therefore, reduces the finalisation and approval times for quality and bioequivalence assessments for regulatory authorities without compromising on the quality, safety and efficacy of the medicinal products. In addition, the approach provides a prototype solution to counteract the influx of medicinal product applications received by the regulatory authorities.

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来源期刊
Pharmaceutical Medicine
Pharmaceutical Medicine PHARMACOLOGY & PHARMACY-
CiteScore
5.10
自引率
4.00%
发文量
36
期刊介绍: Pharmaceutical Medicine is a specialist discipline concerned with medical aspects of the discovery, development, evaluation, registration, regulation, monitoring, marketing, distribution and pricing of medicines, drug-device and drug-diagnostic combinations. The Journal disseminates information to support the community of professionals working in these highly inter-related functions. Key areas include translational medicine, clinical trial design, pharmacovigilance, clinical toxicology, drug regulation, clinical pharmacology, biostatistics and pharmacoeconomics. The Journal includes:Overviews of contentious or emerging issues.Comprehensive narrative reviews that provide an authoritative source of information on topical issues.Systematic reviews that collate empirical evidence to answer a specific research question, using explicit, systematic methods as outlined by PRISMA statement.Original research articles reporting the results of well-designed studies with a strong link to wider areas of clinical research.Additional digital features (including animated abstracts, video abstracts, slide decks, audio slides, instructional videos, infographics, podcasts and animations) can be published with articles; these are designed to increase the visibility, readership and educational value of the journal’s content. In addition, articles published in Pharmaceutical Medicine may be accompanied by plain language summaries to assist readers who have some knowledge of, but not in-depth expertise in, the area to understand important medical advances.All manuscripts are subject to peer review by international experts. Letters to the Editor are welcomed and will be considered for publication.
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