Upstream process optimization and micro- and macrocarrier screening for large-scale production of the oncolytic H-1 protoparvovirus

Wohlfarth, Daniel; Frehtman, Veronika; Müller, Marcus; Vogel, M.; Phan, Linh M. P.; Brunecker, Adrian; Leuchs, Barbara

doi:10.1007/s00253-021-11642-y

Cited by 3 publications

(1 citation statement)

References 22 publications

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“…In this study, it was demonstrated that a seeding density of 5 × 10 3 cells/cm 2 led to the highest functional LVV titers at small scale when compared with 7 × 10 3 or 2.5 × 10 4 cells/cm 2 . This low seeding density was recently used in the iCELLis Nano bioreactor to generate oncolytic H-1 protoparvovirus for cancer treatments, 32 but was never previously used for LVV production in which the lowest seeding density published was 7 × 10 3 cells/cm 2 . 25 The reduction in the inoculation cell density resulted in a delay in transfection from 48 to 120 h, but we considered that an overall process of 7 days is an acceptable process length for the production of these viral vectors.…”

Section: Discussionmentioning

confidence: 99%

Optimizing and developing a scalable, chemically defined, animal component-free lentiviral vector production process in a fixed-bed bioreactor

Fiol¹,

Collignon²,

Welsh³

et al. 2023

Molecular Therapy - Methods & Clinical Development

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Section: Discussionmentioning

confidence: 99%

Optimizing and developing a scalable, chemically defined, animal component-free lentiviral vector production process in a fixed-bed bioreactor

Fiol¹,

Collignon²,

Welsh³

et al. 2023

Molecular Therapy - Methods & Clinical Development

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Upstream Processing of Viral Therapeutics: From Host Cell Expansion to Virus Production

Hamusics,

Loewe

2023

Bioprocess and Analytics Development for Virus-Based Advanced Therapeutics and Medicinal Products (ATMPs)

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Stability and safety key factors of the oncolytic protoparvovirus H-1 from manufacturing to human application

Frehtman

Wohlfarth

Müller

et al. 2023

Appl Microbiol Biotechnol

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The oncolytic rodent protoparvovirus H-1PV has been successfully used in phase I/II clinical trials to treat recurrent glioblastoma multiforme and pancreatic cancer. The present work focuses on the stability and environmental safety of the H-1PV drug product from production up to its use in patients. We identified hold-steps in manufacturing for up to 3 months and showed 7-years stability for the optimal product formulation. Stress testing via UV, temperature, and pH also determined that the drug product is stable. De- and rehydration for lyophilization simulation are possible without infectious virus loss. Furthermore, we prove in-use stability for 4 days at room temperature and show no virus adsorption to injection devices, guaranteeing the correct administration dose. Iodixanol in the formulation, resulting in high viscosity, protects H-1PV against UV and some disinfectants. Nonetheless, H-1PV is depleted with rapid heat deactivation, autoclavation, and nanofiltration. Assessment of chemical disinfectants that are currently recommended by the Robert Koch-Institute demonstrated that ethanol-based hand disinfectants are not effective; however, aldehyde-based disinfectants for surfaces and instruments demonstrate sufficient H-1PV deactivation in aqueous formulations by 4 to 6 log10. With these results, we could establish a specific hygiene plan for all involved facilities from manufacturing to patient application. Overall, using 48% Iodixanol in Visipaque/Ringer as a drug formulation stabilizes H-1PV infectivity over years and protects against virus loss from short-term UV, low pH, and temperature exposure. Key points • Optimal formulation of drug product protects the H-1PV protoparvovirus against UV, temperatures up to 50 °C, and low pH (> 1.25), stabilizing the virus during manufacturing, storage, transport, and application. • H-1PV is stable during in-use and does not adsorb to injection devices during patient administration. • Hygiene plan for H-1PV with physicochemical methods has been established.

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Upstream process optimization and micro- and macrocarrier screening for large-scale production of the oncolytic H-1 protoparvovirus

Cited by 3 publications

References 22 publications

Optimizing and developing a scalable, chemically defined, animal component-free lentiviral vector production process in a fixed-bed bioreactor

Optimizing and developing a scalable, chemically defined, animal component-free lentiviral vector production process in a fixed-bed bioreactor

Upstream Processing of Viral Therapeutics: From Host Cell Expansion to Virus Production

Stability and safety key factors of the oncolytic protoparvovirus H-1 from manufacturing to human application

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