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An arginase-based system for selection of transfected CHO cells without the use of toxic chemicals

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논문

An arginase-based system for selection of transfected CHO cells without the use of toxic chemicals

학술지

The Journal of biological chemistry

저자명

Capella Roca, Berta; Lao, Nga; Barron, Niall; Doolan, Padraig; Clynes, Martin

초록

<P>Polyamines have essential roles in cell proliferation, DNA replication, transcription, and translation processes, with intracellular depletion of putrescine, spermidine, and spermine resulting in cellular growth arrest and eventual death. Serum-free media for CHO-K1 cells require putrescine supplementation, because these cells lack the first enzyme of the polyamine production pathway, arginase. On the basis of this phenotype, we developed an arginase-based selection system. We transfected CHO-K1 cells with a bicistronic vector co-expressing GFP and arginase and selected cells in media devoid of <SMALL>L</SMALL>-ornithine and putrescine, resulting in mixed populations stably expressing GFP. Moreover, single clones in these selective media stably expressed GFP for a total of 42 generations. Using this polyamine starvation method, we next generated recombinant CHO-K1 cells co-expressing arginase and human erythropoietin (hEPO), which also displayed stable expression and healthy growth. The hEPO-expressing clones grew in commercial media, such as BalanCD and CHO-S serum-free media (SFM)&#x2013;II, as well as in a defined serum-free, putrescine-containing medium for at least 9 passages (27 generations), with a minimal decrease in hEPO titer by the end of the culture. We observed a lack of arginase activity also in several CHO cell strains (CHO-DP12, CHO-S, and DUXB11) and other mammalian cell lines, including BHK21, suggesting broader utility of this selection system. In conclusion, we have established an easy-to-apply alternative selection system that effectively generates mammalian cell clones expressing biopharmaceutically relevant or other recombinant proteins without the need for any toxic selective agents. We propose that this system is applicable to mammalian cell lines that lack arginase activity.</P>

발행연도

2019

발행기관

American Society for Biochemistry and Molecular Biology

라이선스

cc-by

ISSN

0021-9258

ISSN

1083-351x

294

49

페이지

pp.18756-18768

주제어

mammal; recombinant protein expression; polyamine; erythropoietin; cloning; arginase; Chinese Hamster Ovary (CHO); putrescine; selection system

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1 2023-12-11

논문; 2019-12-01

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