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• W2897747202 endingPage "442" @default.
• W2897747202 startingPage "433" @default.
• W2897747202 abstract "As a complex and common post-translational modification, N-linked glycosylation affects a recombinant glycoprotein's biological activity and efficacy. For example, the α1,6-fucosylation significantly affects antibody-dependent cellular cytotoxicity and α2,6-sialylation is critical for antibody anti-inflammatory activity. Terminal sialylation is important for a glycoprotein's circulatory half-life. Chinese hamster ovary (CHO) cells are currently the predominant recombinant protein production platform, and, in this review, the characteristics of CHO glycosylation are summarized. Moreover, recent and current metabolic engineering strategies for tailoring glycoprotein fucosylation and sialylation in CHO cells, intensely investigated in the past decades, are described. One approach for reducing α1,6-fucosylation is through inhibiting fucosyltransferase (FUT8) expression by knockdown and knockout methods. Another approach to modulate fucosylation is through inhibition of multiple genes in the fucosylation biosynthesis pathway or through chemical inhibitors. To modulate antibody sialylation of the fragment crystallizable region, expressions of sialyltransferase and galactotransferase individually or together with amino acid mutations can affect antibody glycoforms and further influence antibody effector functions. The inhibition of sialidase expression and chemical supplementations are also effective and complementary approaches to improve the sialylation levels on recombinant glycoproteins. The engineering of CHO cells or protein sequence to control glycoforms to produce more homogenous glycans is an emerging topic. For modulating the glycosylation metabolic pathways, the interplay of multiple glyco-gene knockouts and knockins and the combination of multiple approaches, including genetic manipulation, protein engineering and chemical supplementation, are detailed in order to achieve specific glycan profiles on recombinant glycoproteins for superior biological function and effectiveness." @default.
• W2897747202 created "2018-10-26" @default.
• W2897747202 creator A5000044234 @default.
• W2897747202 creator A5014510444 @default.
• W2897747202 date "2018-10-18" @default.
• W2897747202 modified "2023-09-27" @default.
• W2897747202 title "Metabolic engineering of CHO cells to prepare glycoproteins" @default.
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• W2897747202 doi "https://doi.org/10.1042/etls20180056" @default.
• W2897747202 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/33525787" @default.
• W2897747202 hasPublicationYear "2018" @default.
• W2897747202 type Work @default.

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