Nature and timing of post-approval manufacturing changes of tumour necrosis factor α inhibitor products: A 20-year follow-up study of originators and biosimilars

Ali M Alsamil; Thijs J Giezen; Toine C Egberts; Erik Doevendans; Hubert G Leufkens; Helga Gardarsdottir

doi:10.1016/j.ejps.2022.106227

Nature and timing of post-approval manufacturing changes of tumour necrosis factor α inhibitor products: A 20-year follow-up study of originators and biosimilars

Eur J Pharm Sci. 2022 Aug 1:175:106227. doi: 10.1016/j.ejps.2022.106227. Epub 2022 May 27.

Authors

Ali M Alsamil¹, Thijs J Giezen², Toine C Egberts³, Erik Doevendans⁴, Hubert G Leufkens⁵, Helga Gardarsdottir⁶

Affiliations

¹ Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences, Department of Pharmaceutical Sciences, Faculty of Science, Utrecht University, P.O. Box 80082, Utrecht 3508 TB, the Netherlands; Pharmaceutical Product Evaluation Directorate, Drug sector, Saudi Food, and Drug Authority, Riyadh, Saudi Arabia.
² Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences, Department of Pharmaceutical Sciences, Faculty of Science, Utrecht University, P.O. Box 80082, Utrecht 3508 TB, the Netherlands; Foundation Pharmacy for Hospitals in Haarlem, Haarlem, the Netherlands; Department of Clinical Pharmacy, Spaarne Gasthuis, Haarlem/ Hoofddorp, the Netherlands.
³ Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences, Department of Pharmaceutical Sciences, Faculty of Science, Utrecht University, P.O. Box 80082, Utrecht 3508 TB, the Netherlands; Department of Clinical Pharmacy, University Medical Center Utrecht, Utrecht, the Netherlands.
⁴ Division of Pharmaceutics, Utrecht Institute for Pharmaceutical Sciences, Department of Pharmaceutical Sciences, Faculty of Science, Utrecht University, Utrecht, the Netherlands.
⁵ Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences, Department of Pharmaceutical Sciences, Faculty of Science, Utrecht University, P.O. Box 80082, Utrecht 3508 TB, the Netherlands.
⁶ Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences, Department of Pharmaceutical Sciences, Faculty of Science, Utrecht University, P.O. Box 80082, Utrecht 3508 TB, the Netherlands; Department of Clinical Pharmacy, University Medical Center Utrecht, Utrecht, the Netherlands; Department of Pharmaceutical Sciences, University of Iceland, Reykjavik, Iceland. Electronic address: h.gardarsdottir@uu.nl.

PMID: 35636657
DOI: 10.1016/j.ejps.2022.106227

Abstract

The manufacturing of biopharmaceuticals is complex, and minor changes in the process may affect quality attributes (QAs) that may, in turn, impact clinical outcomes. Regulatory documents from the European Medicines Agency were used to characterize two aspects, nature and timing, of post-approval MCs for originators and biosimilars TNF-α inhibitors that were on the European market up to May 2021. The nature of MCs was evaluated in two ways: (1) the type of MCs related to the drug substance (DS) or drug product (DP), classified as manufacturing, quality control, composition, packaging, or stability with various subtypes; and (2) the risk level according to the potential impact of the MCs on QAs, classified as low, medium, or high. Timing was defined as the date of the regulatory decision on the MC in relation to the approval date. We identified 801 post-approval MCs implemented to originators (mean: 137, range: 112-175) and biosimilars (mean: 30, range: 0-133). Most of implemented MCs for originators and biosimilars were classified as low and medium risk (88.1%), and a small fraction were considered high-risk (11.9%). The average incidence rates were comparable for both originators and biosimilars (7.0/year for MCs, 0.8/year for high-risk MCs). In 20% of MCs introduced to biosimilars, the DP manufacturing site was involved (9% for originators). In contrast, 16% of MCs introduced to originators were related to the DS manufacturing processes (only 7% for biosimilars). In conclusion, while the overall MC incidence rate and the risk level of MCs was not substantially different between TNF-α inhibitor products, we observed some differences in a few types of MCs related to DS manufacturing process and DP manufacturing site between originators and biosimilars. As far as our data shows there is no reasons to assume that post-approval MCs will lead to differences between TNF-α-i originators and biosimilars in clinical practice.

Keywords: Biopharmaceuticals; Biosimilars; Comparability; Consistency; Manufacturing changes; Originators; Quality attributes; Reference products; Tumour necrosis factor alpha inhibitors.

Publication types

Review

MeSH terms

Biosimilar Pharmaceuticals*
Drug Approval
Follow-Up Studies
Immunologic Factors
Quality Control
Tumor Necrosis Factor-alpha

Substances

Biosimilar Pharmaceuticals
Immunologic Factors
Tumor Necrosis Factor-alpha