Rapid high-throughput characterisation, classification and selection of recombinant mammalian cell line phenotypes using intact cell MALDI-ToF mass spectrometry fingerprinting and PLS-DA modelling

Rapid high-throughput characterisation, classification and selection of recombinant mammalian cell line phenotypes using intact cell MALDI-ToF mass spectrometry fingerprinting and PLS-DA modelling

•Methodology for prediction of CHO cell productivity early in cell line development.•Development of a CHO cell MALDI-ToF fingerprint database.•Evaluation of novel cell line development methodology at industrial scale. Despite many advances in the generation of high producing recombinant mammalian ce...

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Veröffentlicht in:Journal of biotechnology 2014-08, Vol.184, p.84-93
Hauptverfasser: Povey, Jane F., O’Malley, Christopher J., Root, Tracy, Martin, Elaine B., Montague, Gary A., Feary, Marc, Trim, Carol, Lang, Dietmar A., Alldread, Richard, Racher, Andrew J., Smales, C. Mark
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Batch Cell Culture Techniques - methods
Bioreactors
Biotechnology
Cell line development
Cell line prediction
Chinese hamster ovary cells
CHO Cells - classification
Cricetinae
Cricetulus
DNA Fingerprinting - methods
Fingerprints
Least-Squares Analysis
Mammals - immunology
Mass spectrometry
Mathematical models
PLS-DA modelling
Productivity
Recombinant
Scale (ratio)
Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization - methods
Whole cell MALDI-ToF mass spectrometry
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Zusammenfassung:•Methodology for prediction of CHO cell productivity early in cell line development.•Development of a CHO cell MALDI-ToF fingerprint database.•Evaluation of novel cell line development methodology at industrial scale. Despite many advances in the generation of high producing recombinant mammalian cell lines over the last few decades, cell line selection and development is often slowed by the inability to predict a cell line's phenotypic characteristics (e.g. growth or recombinant protein productivity) at larger scale (large volume bioreactors) using data from early cell line construction at small culture scale. Here we describe the development of an intact cell MALDI-ToF mass spectrometry fingerprinting method for mammalian cells early in the cell line construction process whereby the resulting mass spectrometry data are used to predict the phenotype of mammalian cell lines at larger culture scale using a Partial Least Squares Discriminant Analysis (PLS-DA) model. Using MALDI-ToF mass spectrometry, a library of mass spectrometry fingerprints was generated for individual cell lines at the 96 deep well plate stage of cell line development. The growth and productivity of these cell lines were evaluated in a 10L bioreactor model of Lonza's large-scale (up to 20,000L) fed-batch cell culture processes. Using the mass spectrometry information at the 96 deep well plate stage and phenotype information at the 10L bioreactor scale a PLS-DA model was developed to predict the productivity of unknown cell lines at the 10L scale based upon their MALDI-ToF fingerprint at the 96 deep well plate scale. This approach provides the basis for the very early prediction of cell lines’ performance in cGMP manufacturing-scale bioreactors and the foundation for methods and models for predicting other mammalian cell phenotypes from rapid, intact-cell mass spectrometry based measurements.
ISSN:0168-1656
1873-4863
DOI:10.1016/j.jbiotec.2014.04.028