Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor
Stiens LR, Büntemeyer H, Lütkemeyer D, Lehmann J, Bergmann A, Weglohner W (2000)
BIOTECHNOLOGY PROGRESS 16(5): 703-709.
Zeitschriftenaufsatz
| Veröffentlicht | Englisch
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Autor*in
Stiens, LR;
Büntemeyer, HeinoUniBi;
Lütkemeyer, DirkUniBi;
Lehmann, J;
Bergmann, A;
Weglohner, W
Einrichtung
Abstract / Bemerkung
For the detection of autoantibodies to thyroid stimulating hormone receptors (TSH-R) in Graves' disease based on a novel coated tube assay system, human TSH-R is needed in large amounts. Whereas expression of TSH-R in bacteria, yeast, or insect cells results in nonfunctional, denaturated receptor, mammalian cells such as COS, CHO, and HeLa are able to express functional TSH-R, but only in very low amounts. Furthermore, for all of these cultivations expensive standard media containing 10% fetal calf serum are needed to obtain functional receptor. Here we report on the development of a serum-free production-scale process based on a stable transformed and highly productive human leukemia cell line K562 (1). Starting with K562-TSH-R cells growing in medium containing 10% fetal calf serum the cell line was adapted to serum-free medium. The adaptation medium was optimized in regards to amino acid and protein concentrations, since the use of unadjusted medium caused cell death after 2 days. The adapted cells were stable and could be cultivated without antibiotics for more than 50 cell doublings without losing their productivity. The obtained receptor showed improved TSH binding. The process development was based on cultivations in a 2-L bench-scale bioreactor. Cultivations in batch mode and chemostat mode and perfusion cultivation with the usage of an internal microfiltration device and a spin-filter device were compared. After process optimization a continuous process using spin-filter was set up and run in a 20 L-pilot-scale bioreactor. The presented results were the prerequisite for the production of the novel assay for the diagnosis of autoantibodies to TSH-R in Graves' disease.
Erscheinungsjahr
2000
Zeitschriftentitel
BIOTECHNOLOGY PROGRESS
Band
16
Ausgabe
5
Seite(n)
703-709
ISSN
8756-7938
Page URI
https://pub.uni-bielefeld.de/record/1618879
Zitieren
Stiens LR, Büntemeyer H, Lütkemeyer D, Lehmann J, Bergmann A, Weglohner W. Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor. BIOTECHNOLOGY PROGRESS. 2000;16(5):703-709.
Stiens, L. R., Büntemeyer, H., Lütkemeyer, D., Lehmann, J., Bergmann, A., & Weglohner, W. (2000). Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor. BIOTECHNOLOGY PROGRESS, 16(5), 703-709. https://doi.org/10.1021/bp000103l
Stiens, LR, Büntemeyer, Heino, Lütkemeyer, Dirk, Lehmann, J, Bergmann, A, and Weglohner, W. 2000. “Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor”. BIOTECHNOLOGY PROGRESS 16 (5): 703-709.
Stiens, L. R., Büntemeyer, H., Lütkemeyer, D., Lehmann, J., Bergmann, A., and Weglohner, W. (2000). Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor. BIOTECHNOLOGY PROGRESS 16, 703-709.
Stiens, L.R., et al., 2000. Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor. BIOTECHNOLOGY PROGRESS, 16(5), p 703-709.
L.R. Stiens, et al., “Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor”, BIOTECHNOLOGY PROGRESS, vol. 16, 2000, pp. 703-709.
Stiens, L.R., Büntemeyer, H., Lütkemeyer, D., Lehmann, J., Bergmann, A., Weglohner, W.: Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor. BIOTECHNOLOGY PROGRESS. 16, 703-709 (2000).
Stiens, LR, Büntemeyer, Heino, Lütkemeyer, Dirk, Lehmann, J, Bergmann, A, and Weglohner, W. “Development of serum-free bioreactor production of recombinant human thyroid stimulating hormone receptor”. BIOTECHNOLOGY PROGRESS 16.5 (2000): 703-709.
Daten bereitgestellt von European Bioinformatics Institute (EBI)
3 Zitationen in Europe PMC
Daten bereitgestellt von Europe PubMed Central.
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