Metabolomic characterization of monoclonal antibody‐producing Chinese hamster lung (CHL)‐YN cells in glucose‐controlled serum‐free fed‐batch operation

Author:

Sukwattananipaat Puriwat1ORCID,Kuroda Hirotaka123ORCID,Yamano‐Adachi Noriko145ORCID,Omasa Takeshi145ORCID

Affiliation:

1. Graduate School of Engineering Osaka University Osaka Japan

2. Shimadzu Corp. Kyoto Japan

3. Shimadzu Analytical Innovation Research Laboratories Osaka Japan

4. Institute for Open and Transdisciplinary Research Initiatives Osaka University Osaka Japan

5. Manufacturing Technology Association of Biologics (MAB) Hyogo Japan

Abstract

AbstractThe fast‐growing Chinese hamster lung (CHL)‐YN cell line was recently developed for monoclonal antibody production. In this study, we applied a serum‐free fed‐batch cultivation process to immunoglobulin (Ig)G1‐producing CHL‐YN cells, which were then used to design a dynamic glucose supply system to stabilize the extracellular glucose concentration based on glucose consumption. Glucose consumption of the cultures rapidly oscillated following three phases of glutamine metabolism: consumption, production, and re‐consumption. Use of the dynamic glucose supply prolonged the viability of the CHL‐YN‐IgG1 cell cultures and increased IgG1 production. Liquid chromatography with tandem mass spectrometry‐based target metabolomics analysis of the extracellular metabolites during the first glutamine shift was conducted to search for depleted compounds. The results suggest that the levels of four amino acids, namely arginine, aspartate, methionine, and serine, were sharply decreased in CHL‐YN cells during glutamine production. Supporting evidence from metabolic and gene expression analyses also suggest that CHL‐YN cells acquired ornithine‐ and cystathionine‐production abilities that differed from those in Chinese hamster ovary‐K1 cells, potentially leading to proline and cysteine biosynthesis.

Publisher

Wiley

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