Fed-batch performance profiles for mAb production using different intensified N - 1 seed strategies are CHO cell-line dependent.

Autor: Tang Y; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., Xu J; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., Xu M; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., Huang Z; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., Santos J; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., He Q; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., Borys M; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA., Khetan A; Global Product Development and Supply, Bristol Myers Squibb Company, Devens, Massachusetts, USA.
Jazyk: angličtina
Zdroj: Biotechnology progress [Biotechnol Prog] 2024 Jul-Aug; Vol. 40 (4), pp. e3446. Date of Electronic Publication: 2024 Feb 28.
DOI: 10.1002/btpr.3446
Abstrakt: Recent optimizations of cell culture processes have focused on the final seed scale-up step (N - 1 stage) used to inoculate the production bioreactor (N-stage bioreactor) to enable higher inoculation cell densities (2-20 × 10 6 cells/mL), which could shorten the production culture duration and/or increase the volumetric productivity. N - 1 seed process intensification can be achieved by either non-perfusion (enriched-batch or fed-batch) or perfusion culture to reach those higher final N - 1 viable cell densities (VCD). In this study, we evaluated how different N - 1 intensification strategies, specifically enriched-batch (EB) N - 1 versus perfusion N - 1, affect cell growth profiles and monoclonal antibody (mAb) productivity in the final N-stage production bioreactor operated in fed-batch mode. Three representative Chinese Hamster Ovary (CHO) cell lines producing different mAbs were cultured using either EB or perfusion N - 1 seeds and found that the N-stage cell growth and mAb productivities were comparable between EB N - 1 and perfusion N - 1 conditions for two of the cell lines but were very different for the third. In addition, within the two similar cell growth cell lines, differences in cell-specific productivity were observed. This suggests that the impact of the N - 1 intensification process on production was cell-line dependent. This study revealed that the N - 1 intensification strategy and the state of seeds from the different N - 1 conditions may affect the outcome of the N production stage, and thus, the choice of N - 1 intensification strategy could be a new target for future upstream optimization of mAb production.
(© 2024 American Institute of Chemical Engineers.)
Databáze: MEDLINE
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