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Directed evolution of biomass intensive CHO cells by adaptation to sub-physiological temperature.

Authors :
Syddall, Katie L.
Fernandez–Martell, Alejandro
Cartwright, Joseph F.
Alexandru-Crivac, Cristina N.
Hodgson, Adam
Racher, Andrew J.
Young, Robert J.
James, David C.
Source :
Metabolic Engineering. Jan2024, Vol. 81, p53-69. 17p.
Publication Year :
2024

Abstract

We report a simple and effective means to increase the biosynthetic capacity of host CHO cells. Lonza proprietary CHOK1SV® cells were evolved by serial sub-culture for over 150 generations at 32 °C. During this period the specific proliferation rate of hypothermic cells gradually recovered to become comparable to that of cells routinely maintained at 37 °C. Cold-adapted cell populations exhibited (1) a significantly increased volume and biomass content (exemplified by total RNA and protein), (2) increased mitochondrial function, (3) an increased antioxidant capacity, (4) altered central metabolism, (5) increased transient and stable productivity of a model IgG4 monoclonal antibody and Fc-fusion protein, and (6) unaffected recombinant protein N-glycan processing. This phenotypic transformation was associated with significant genome-scale changes in both karyotype and the relative abundance of thousands of cellular mRNAs across numerous functional groups. Taken together, these observations provide evidence of coordinated cellular adaptations to sub-physiological temperature. These data reveal the extreme genomic/functional plasticity of CHO cells, and that directed evolution is a viable genome-scale cell engineering strategy that can be exploited to create host cells with an increased cellular capacity for recombinant protein production. • Long-term adaptive evolution of mammalian (CHO) cells to hypothermic growth. • Increased biomass synthesis and recombinant protein production by cold-adapted cells. • Cellular adaptation (karyotypic, metabolic, bioenergetic, transcriptomic) was extensive and conserved. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
10967176
Volume :
81
Database :
Academic Search Index
Journal :
Metabolic Engineering
Publication Type :
Academic Journal
Accession number :
174917340
Full Text :
https://doi.org/10.1016/j.ymben.2023.11.005