Development of a scalable AAV production process in suspension cells

Ann-Christin Magnusson

doi:10.18609/cgti.2021.176

Development of a scalable AAV production process in suspension cells

Cell & Gene Therapy Insights 2021; 7(9), 1337

10.18609/cgti.2021.176

Published: 11 November 2021

FastFacts

Ann-Christin Magnusson

Watch the video or read the poster to learn about:

Optimization of AAV2 triple plasmid transfection using design of experiment (DoE)
An optimized transient transfection protocol that can be used for several different AAV serotypes to achieve high titers
Scale up of production using XDR-10 and the ReadyToProcess WAVE™ 25 bioreactor systems

Ann-Christin holds a degree in Biomedical Engineering from Uppsala University, Sweden and has over 30 years of hands-on experience in cell culture of different cell lines. In her previous function, Ann-Christin developed different stable CHO cell lines from DNA construction to a final cell line for GMP production of recombinant protein. Ann-Christin joined Cytiva in 2008, and currently leads the upstream teams for cell culture, development of solutions for virus production for vaccine manufacturing and gene therapy applications.