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Droplet size influences division of mammalian cell factories in droplet microfluidic cultivation. | LitMetric

Droplet size influences division of mammalian cell factories in droplet microfluidic cultivation.

Electrophoresis

Division of Proteomics and Nanobiotechnology, Science for Life Laboratory, KTH Royal Institute of Technology, Stockholm, Sweden.

Published: January 2017

AI Article Synopsis

  • This study investigates how droplet size affects the division and viability of Chinese Hamster Ovary (CHO) cells during cultivation in microfluidic droplets.
  • The research found that CHO cells in smaller 33 pL droplets stopped dividing after 24 hours and experienced a drastic decline in viability, while those in larger 180 and 320 pL droplets continued to divide and remained over 90% viable for 72 hours.
  • The results emphasize the need to choose the appropriate droplet size for optimizing mammalian cell factory screening assays.

Article Abstract

The potential of using droplet microfluidics for screening mammalian cell factories has been limited by the difficulty in achieving continuous cell division during cultivation in droplets. Here, we report the influence of droplet size on mammalian cell division and viability during cultivation in droplets. Chinese Hamster Ovary (CHO) cells, the most widely used mammalian host cells for biopharmaceuticals production were encapsulated and cultivated in 33, 180 and 320 pL droplets for 3 days. Periodic monitoring of the droplets during incubation showed that the cell divisions in 33 pL droplets stopped after 24 h, whereas continuous cell division was observed in 180 and 320 pL droplets for 72 h. The viability of the cells cultivated in the 33 pL droplets also dropped to about 50% in 72 h. In contrast, the viability of the cells in the larger droplets was above 90% even after 72 h of cultivation, making them a more suitable droplet size for 72-h cultivation. This study shows a direct correlation of microfluidic droplet size to the division and viability of mammalian cells. This highlights the importance of selecting suitable droplet size for mammalian cell factory screening assays.

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Source
http://dx.doi.org/10.1002/elps.201600316DOI Listing

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