A CHO stable pool production platform for rapid clinical development of trimeric SARS‐CoV‐2 spike subunit vaccine antigens

Par Conseil national de recherches du Canada

Téléchargement	Voir la version finale : A CHO stable pool production platform for rapid clinical development of trimeric SARS‐CoV‐2 spike subunit vaccine antigens (PDF, 6.0 Mio)
DOI	Trouver le DOI : https://doi.org/10.1002/bit.28387
Auteur	Rechercher : Joubert, Simon¹Identifiant ORCID : https://orcid.org/0009-0007-0405-8946; Rechercher : Stuible, Matthew¹Identifiant ORCID : https://orcid.org/0009-0002-4403-0677; Rechercher : Lord‐Dufour, Simon; Rechercher : Lamoureux, Linda¹; Rechercher : Vaillancourt, François¹; Rechercher : Perret, Sylvie¹; Rechercher : Ouimet, Manon¹; Rechercher : Pelletier, Alex¹; Rechercher : Bisson, Louis¹; Rechercher : Mahimkar, Rohan¹; Rechercher : Pham, Phuong Lan¹; Rechercher : L'Ecuyer-Coelho, Helene¹; Rechercher : Roy, Marjolaine¹; Rechercher : Voyer, Robert¹; Rechercher : Baardsnes, Jason¹; Rechercher : Sauvageau, Janelle¹; Rechercher : St-Michael, Frank¹; Rechercher : Robotham, Anna¹; Rechercher : Kelly, John¹; Rechercher : Acel, Andrea¹; Rechercher : Schrag, Joseph D.¹; Rechercher : El Bakkouri, Majida¹; Rechercher : Durocher, Yves¹Identifiant ORCID : https://orcid.org/0000-0002-2268-4111
Affiliation du nom	Conseil national de recherches du Canada. Thérapeutique en santé humaine
Format	Texte, Article
Sujet	CHO clones; CHO pools; product comparability; quality attributes; SARS‐CoV‐2 spike protei
Résumé	Protein expression from stably transfected Chinese hamster ovary (CHO) clones is an established but time-consuming method for manufacturing therapeutic recombinant proteins. The use of faster, alternative approaches, such as non-clonal stable pools, has been restricted due to lower productivity and longstanding regulatory guidelines. Recently, the performance of stable pools has improved dramatically, making them a viable option for quickly producing drug substance for GLP-toxicology and early-phase clinical trials in scenarios such as pandemics that demand rapid production timelines. Compared to stable CHO clones which can take several months to generate and characterize, stable pool development can be completed in only a few weeks. Here, we compared the productivity and product quality of trimeric SARS-CoV-2 spike protein ectodomains produced from stable CHO pools or clones. Using a set of biophysical and biochemical assays we show that product quality is very similar and that CHO pools demonstrate sufficient productivity to generate vaccine candidates for early clinical trials. Based on these data, we propose that regulatory guidelines should be updated to permit production of early clinical trial material from CHO pools to enable more rapid and cost-effective clinical evaluation of potentially life-saving vaccines.
Date de publication	2023-07
Licence	Attribution - Pas d'Utilisation Commerciale - Pas de Modification 4.0 International (CC BY-NC-ND 4.0) https://creativecommons.org/licenses/by-nc-nd/4.0/deed.fr
Dans	Biotechnology and Bioengineering 120, nº 7 (juillet 2023) : 1746–1761.
Langue	anglais
Publications évaluées par des pairs	Oui
Exporter la notice	Exporter en format RIS
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Identificateur de l’enregistrement	9878ecec-3c5a-4407-a26b-7b719b074767
Enregistrement créé	2023-07-17
Enregistrement modifié	2023-07-17

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Date de modification :: 2023-12-02