Literature DB >> 30299005

Transient CHO expression platform for robust antibody production and its enhanced N-glycan sialylation on therapeutic glycoproteins.

Xiaotian Zhong1, Weijun Ma1, Caryl L Meade1, Amy S Tam1, Eliza Llewellyn1, Richard Cornell2, Kaffa Cote2, John J Scarcelli3, Jeffrey K Marshall2, Boriana Tzvetkova2, Bruno Figueroa4, Dana DiNino2, Annette Sievers1, Christopher Lee1, Jane Guo1, Evan Mahan1, Christopher Francis1, Khetemenee Lam1, Aaron M D'Antona1, Richard Zollner1, Hongli L Zhu1, Ron Kriz1, Will Somers1, Laura Lin1.   

Abstract

Large-scale transient expression in mammalian cells is a rapid protein production technology often used to shorten overall timelines for biotherapeutics drug discovery. In this study we demonstrate transient expression in a Chinese hamster ovary (CHO) host (ExpiCHO-S™) cell line capable of achieving high recombinant antibody expression titers, comparable to levels obtained using human embryonic kidney (HEK) 293 cells. For some antibodies, ExpiCHO-S™ cells generated protein materials with better titers and improved protein quality characteristics (i.e., less aggregation) than those from HEK293. Green fluorescent protein imaging data indicated that ExpiCHO-S™ displayed a delayed but prolonged transient protein expression process compared to HEK293. When therapeutic glycoproteins containing non-Fc N-linked glycans were expressed in transient ExpiCHO-S™, the glycan pattern was unexpectedly found to have few sialylated N-glycans, in contrast to glycans produced within a stable CHO expression system. To improve N-glycan sialylation in transient ExpiCHO-S™, we co-transfected galactosyltransferase and sialyltransferase genes along with the target genes, as well as supplemented the culture medium with glycan precursors. The authors have demonstrated that co-transfection of glycosyltransferases combined with medium addition of galactose and uridine led to increased sialylation content of N-glycans during transient ExpiCHO-S™ expression. These results have provided a scientific basis for developing a future transient CHO system with N-glycan compositions that are similar to those profiles obtained from stable CHO protein production systems.
© 2018 American Institute of Chemical Engineers Biotechnol. Prog., 35: e2724, 2019. © 2018 American Institute of Chemical Engineers.

Entities:  

Keywords:  Chinese hamster ovary cells; N-linked glycosylation and sialylation; antibody; therapeutic glycoproteins; transient and stable expression

Year:  2018        PMID: 30299005     DOI: 10.1002/btpr.2724

Source DB:  PubMed          Journal:  Biotechnol Prog        ISSN: 1520-6033


  7 in total

1.  Structure-function relationships of the soluble form of the antiaging protein Klotho have therapeutic implications for managing kidney disease.

Authors:  Xiaotian Zhong; Srinath Jagarlapudi; Yan Weng; Mellisa Ly; Jason C Rouse; Kim McClure; Tetsuya Ishino; Yan Zhang; Eric Sousa; Justin Cohen; Boriana Tzvetkova; Kaffa Cote; John J Scarcelli; Keith Johnson; Joe Palandra; James R Apgar; Suma Yaddanapudi; Romer A Gonzalez-Villalobos; Alan C Opsahl; Khetemenee Lam; Qing Yao; Weili Duan; Annette Sievers; Jing Zhou; Darren Ferguson; Aaron D'Antona; Richard Zollner; Hongli L Zhu; Ron Kriz; Laura Lin; Valerie Clerin
Journal:  J Biol Chem       Date:  2020-01-31       Impact factor: 5.157

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Review 4.  Cellular and Molecular Engineering of Glycan Sialylation in Heterologous Systems.

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5.  Multiplexed engineering glycosyltransferase genes in CHO cells via targeted integration for producing antibodies with diverse complex-type N-glycans.

Authors:  Ngan T B Nguyen; Jianer Lin; Shi Jie Tay; Jessna Yeo; Terry Nguyen-Khuong; Yuansheng Yang
Journal:  Sci Rep       Date:  2021-06-21       Impact factor: 4.379

6.  Transfection of glycoprotein encoding mRNA for swift evaluation of N-glycan engineering strategies.

Authors:  Nina Bydlinski; Michael T Coats; Daniel Maresch; Richard Strasser; Nicole Borth
Journal:  Biotechnol Prog       Date:  2020-03-13

7.  Genetic rearrangement during site specific integration event facilitates cell line development of a bispecific molecule.

Authors:  Barbara Tevelev; Himakshi Patel; Kathleen Shields; Wei Wei; Cecilia Cooley; Sam Zhang; Gabrielle Bitzas; Weili Duan; Lam Khetemenee; Ryan Jackobek; Aaron D'Antona; Annette Sievers; Amy King; Amy Tam; Yan Zhang; Eric Sousa; Justin Cohen; Lila Wroblewska; Jeffrey Marshall; Martha Jackson; John J Scarcelli
Journal:  Biotechnol Prog       Date:  2021-05-12
  7 in total

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