Do the Outcomes of Clinical Efficacy Trials Matter in Regulatory Decision-Making for Biosimilars?

IF 5.4 2区 医学 Q1 IMMUNOLOGY BioDrugs Pub Date : 2023-11-01 Epub Date: 2023-10-13 DOI:10.1007/s40259-023-00631-4
Nadine Kirsch-Stefan, Elena Guillen, Niklas Ekman, Sean Barry, Verena Knippel, Sheila Killalea, Martina Weise, Elena Wolff-Holz
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引用次数: 2

Abstract

Background: There is an increasing body of evidence supporting a more flexible approach in clinical data requirements for the approval of more complex biosimilar substances such as monoclonal antibodies (mAbs).

Objective: The aim of this paper is to further analyse the role of quality/chemistry, manufacturing and controls (CMC) and clinical data for the conclusion on biosimilarity and the decision on marketing authorisation (MA).

Methods: In the present study, we analysed the MA applications (MAAs) of all 33 mAbs and three fusion proteins evaluated by the European Medicines Agency (EMA) between July 2012 and November 2022 with special emphasis on all submitted rituximab (four products) and trastuzumab (seven products) biosimilar candidates, including withdrawn applications. For the two withdrawn applications, the comparative efficacy trials suggested biosimilarity, but the quality/CMC package was not accepted by EMA. We therefore investigated whether a negative MAA outcome could have been predicted based on the evidence generated in the quality/CMC packages, regardless of clinical trial data. For this purpose, we reviewed the respective European Public Assessment Reports (EPARs) or withdrawal assessment reports, and the first regulatory assessments for all these 36 MAAs (i.e. day 120 of the centralized procedure), which are not publicly available. During EMA review, where significant issues are identified which would preclude a marketing authorisation, these issues are raised as questions to the applicant and are classified as major objections (MO).

Results: In 67% of cases, the outcome of the quality and clinical assessment was the same, i.e. both the quality and clinical assessments either supported approval or did not support approval. In 11% of cases, MO were identified in the quality part of the submission but not in the clinical data. In 22% of cases, MO were raised on the clinical data package but not on the quality data. However, we found no instance where seemingly negative clinical data, including failed efficacy trials, led to a negative overall decision. In each instance, the failure to confirm similar clinical performance in all investigated aspects was eventually viewed as not being related to the biosimilar per se but as being due to imbalances in the trial arms, immaturity of secondary endpoint results, change in the reference product, or even chance findings. Furthermore, when performing an in-depth analysis of the quality and clinical packages of trastuzumab and rituximab biosimilars, we found that in no case were clinical trial data necessary to resolve residual uncertainties regarding the quality part.

Conclusion: The results further support the argument that sufficient evidence for biosimilarity can be obtained from a combination of analytical and functional testing and pharmacokinetic studies which may also generate immunogenicity data. This calls into question the usefulness of comparative efficacy studies for the purposes of regulatory decision-making when approving biosimilar mAbs and fusion proteins.

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临床疗效试验的结果在生物仿制药的监管决策中重要吗?
背景:越来越多的证据支持在临床数据要求中采用更灵活的方法来批准更复杂的生物类似物质,如单克隆抗体。目的:本文的目的是进一步分析质量/化学的作用,生产和对照(CMC)和临床数据,以得出生物相似性结论和上市许可决定(MA)。方法:在本研究中,我们分析了欧洲药品管理局(EMA)在2012年7月至2022年11月期间评估的所有33种单克隆抗体和三种融合蛋白的MA应用(MAA),特别强调了所有提交的利妥昔单抗(四种产品)和曲妥珠单抗(七种产品)候选生物仿制药,包括撤回的应用。对于两份撤回的申请,疗效比较试验表明其生物相似性,但EMA不接受质量/CMC包。因此,我们调查了是否可以根据质量/CMC包中产生的证据预测MAA阴性结果,而不考虑临床试验数据。为此,我们审查了各自的欧洲公共评估报告(EPAR)或退出评估报告,以及所有这36个MAA的第一次监管评估(即集中程序的第120天),这些报告均未公开。在EMA审查期间,如果发现重大问题会阻碍上市授权,这些问题会作为问题向申请人提出,并被归类为主要异议(MO)。结果:在67%的病例中,质量和临床评估的结果是相同的,即质量和临床评估要么支持批准,要么不支持批准。在11%的病例中,MO在提交的质量部分被确定,但在临床数据中没有。在22%的病例中,MO在临床数据包中提出,但在质量数据中没有提出。然而,我们没有发现任何看似负面的临床数据,包括失败的疗效试验,导致负面的总体决定。在每一种情况下,未能在所有研究方面确认类似的临床表现最终被视为与生物仿制药本身无关,而是由于试验组的不平衡、次要终点结果的不成熟、参考产品的变化,甚至偶然发现。此外,在对曲妥珠单抗和利妥昔单抗生物仿制药的质量和临床包进行深入分析时,我们发现在任何情况下都没有必要的临床试验数据来解决质量部分的残余不确定性。结论:该结果进一步支持了这样一种论点,即通过分析和功能测试以及药代动力学研究的结合,可以获得足够的生物相似性证据,这也可能产生免疫原性数据。这就对比较疗效研究在批准生物类似mAb和融合蛋白时用于监管决策的有用性提出了质疑。
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来源期刊
BioDrugs
BioDrugs 医学-免疫学
CiteScore
12.60
自引率
2.90%
发文量
50
审稿时长
>12 weeks
期刊介绍: An essential resource for R&D professionals and clinicians with an interest in biologic therapies. BioDrugs covers the development and therapeutic application of biotechnology-based pharmaceuticals and diagnostic products for the treatment of human disease. BioDrugs offers a range of additional enhanced features designed to increase the visibility, readership and educational value of the journal’s content. Each article is accompanied by a Key Points summary, giving a time-efficient overview of the content to a wide readership. Articles may be accompanied by plain language summaries to assist patients, caregivers and others in understanding important medical advances. The journal also provides the option to include various other types of enhanced features including slide sets, videos and animations. All enhanced features are peer reviewed to the same high standard as the article itself. Peer review is conducted using Editorial Manager®, supported by a database of international experts. This database is shared with other Adis journals.
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