Selection of chemically defined media for CHO cell fed-batch culture processes
Two CHO cell clones derived from the same parental CHOBC cell line and producing the same monoclonal antibody (BC-G, a low producing clone; BC-P, a high producing clone) were tested in four basal media in all possible combinations with three feeds (=12 conditions) in fed-batch cultures.Higher amino acid feeding did not always lead to igher mAb production. The two clones showed differences in cell physiology, metabolism and optimal medium-feed combinations. During the phase transitions of all cultures, cell metabolism showed a shift represented by lower specific consumption and roduction rates, except for the specific glucose consumption rate in cultures fed by Actifeed A/B.The BC-P clone fed by Actifeed A/B showed a threefold cell volume increase and an increase of the specific consumption rate of glucose in the stationaryphase. Since feeding was based on glucose this resulted in accumulation of amino acids for this feed, while this did not occur for the poorer feed (EFA/B).The same feed also led to an increase of cell size for the BC-G clone, but to a lesser extent.
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| Format: | Article/Letter to editor biblioteca |
| Language: | English |
| Subjects: | Antibody production, Cell culture medium, Chinese hamster ovary (CHO) cell, Fed-batch, Metabolite profile, Phase transition, |
| Online Access: | https://research.wur.nl/en/publications/selection-of-chemically-defined-media-for-cho-cell-fed-batch-cult |
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dig-wur-nl-wurpubs-5107112025-01-17 Pan, X. Streefland, M. Dalm, C. Wijffels, R.H. Martens, D.E. Article/Letter to editor Cytotechnology 69 (2017) 1 ISSN: 0920-9069 Selection of chemically defined media for CHO cell fed-batch culture processes 2017 Two CHO cell clones derived from the same parental CHOBC cell line and producing the same monoclonal antibody (BC-G, a low producing clone; BC-P, a high producing clone) were tested in four basal media in all possible combinations with three feeds (=12 conditions) in fed-batch cultures.Higher amino acid feeding did not always lead to igher mAb production. The two clones showed differences in cell physiology, metabolism and optimal medium-feed combinations. During the phase transitions of all cultures, cell metabolism showed a shift represented by lower specific consumption and roduction rates, except for the specific glucose consumption rate in cultures fed by Actifeed A/B.The BC-P clone fed by Actifeed A/B showed a threefold cell volume increase and an increase of the specific consumption rate of glucose in the stationaryphase. Since feeding was based on glucose this resulted in accumulation of amino acids for this feed, while this did not occur for the poorer feed (EFA/B).The same feed also led to an increase of cell size for the BC-G clone, but to a lesser extent. en application/pdf https://research.wur.nl/en/publications/selection-of-chemically-defined-media-for-cho-cell-fed-batch-cult 10.1007/s10616-016-0036-5 https://edepot.wur.nl/401316 Antibody production Cell culture medium Chinese hamster ovary (CHO) cell Fed-batch Metabolite profile Phase transition https://creativecommons.org/licenses/by/4.0/ Wageningen University & Research |
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Antibody production Cell culture medium Chinese hamster ovary (CHO) cell Fed-batch Metabolite profile Phase transition Antibody production Cell culture medium Chinese hamster ovary (CHO) cell Fed-batch Metabolite profile Phase transition |
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Antibody production Cell culture medium Chinese hamster ovary (CHO) cell Fed-batch Metabolite profile Phase transition Antibody production Cell culture medium Chinese hamster ovary (CHO) cell Fed-batch Metabolite profile Phase transition Pan, X. Streefland, M. Dalm, C. Wijffels, R.H. Martens, D.E. Selection of chemically defined media for CHO cell fed-batch culture processes |
| description |
Two CHO cell clones derived from the same parental CHOBC cell line and producing the same monoclonal antibody (BC-G, a low producing clone; BC-P, a high producing clone) were tested in four basal media in all possible combinations with three feeds (=12 conditions) in fed-batch cultures.Higher amino acid feeding did not always lead to igher mAb production. The two clones showed differences in cell physiology, metabolism and optimal medium-feed combinations. During the phase transitions of all cultures, cell metabolism showed a shift represented by lower specific consumption and roduction rates, except for the specific glucose consumption rate in cultures fed by Actifeed A/B.The BC-P clone fed by Actifeed A/B showed a threefold cell volume increase and an increase of the specific consumption rate of glucose in the stationaryphase. Since feeding was based on glucose this resulted in accumulation of amino acids for this feed, while this did not occur for the poorer feed (EFA/B).The same feed also led to an increase of cell size for the BC-G clone, but to a lesser extent. |
| format |
Article/Letter to editor |
| topic_facet |
Antibody production Cell culture medium Chinese hamster ovary (CHO) cell Fed-batch Metabolite profile Phase transition |
| author |
Pan, X. Streefland, M. Dalm, C. Wijffels, R.H. Martens, D.E. |
| author_facet |
Pan, X. Streefland, M. Dalm, C. Wijffels, R.H. Martens, D.E. |
| author_sort |
Pan, X. |
| title |
Selection of chemically defined media for CHO cell fed-batch culture processes |
| title_short |
Selection of chemically defined media for CHO cell fed-batch culture processes |
| title_full |
Selection of chemically defined media for CHO cell fed-batch culture processes |
| title_fullStr |
Selection of chemically defined media for CHO cell fed-batch culture processes |
| title_full_unstemmed |
Selection of chemically defined media for CHO cell fed-batch culture processes |
| title_sort |
selection of chemically defined media for cho cell fed-batch culture processes |
| url |
https://research.wur.nl/en/publications/selection-of-chemically-defined-media-for-cho-cell-fed-batch-cult |
| work_keys_str_mv |
AT panx selectionofchemicallydefinedmediaforchocellfedbatchcultureprocesses AT streeflandm selectionofchemicallydefinedmediaforchocellfedbatchcultureprocesses AT dalmc selectionofchemicallydefinedmediaforchocellfedbatchcultureprocesses AT wijffelsrh selectionofchemicallydefinedmediaforchocellfedbatchcultureprocesses AT martensde selectionofchemicallydefinedmediaforchocellfedbatchcultureprocesses |
| _version_ |
1822270097061838848 |