Production of non-fucosylated antibodies by co-expression of heterologous GDP-6-deoxy-D-lyxo-4-hexulose reductase

Horsten, Hans Henning von; Ogorek, Christiane; Blanchard, Véronique; Demmler, Christian; Giese, Christoph; Winkler, Karsten; Kaup, Matthias; Berger, Markus; Jordan, Ingo; Sandig, Volker

doi:10.1093/glycob/cwq109

Cited by 95 publications

(86 citation statements)

References 45 publications

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“…GDP-rhamnose is a common component of bacterial cell surface glycans. Heterologous expression of bacterial RMD in the cytosol of CHO cells allowed the GDP-fucose de novo pathway to be efficiently bypassed and afucosylated IgG antibodies to be produced 88 . The dead-end product GDP-rhamnose is likely to inhibit the activity of GMD as a competitive inhibitor.…”

Section: Strategies To Produce Afucosylated Antibodiesmentioning

confidence: 99%

The “less-is-more” in therapeutic antibodies: Afucosylated anti-cancer antibodies with enhanced antibody-dependent cellular cytotoxicity

Pereira

Chan

Lin

et al. 2018

mAbs

254

211

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Therapeutic monoclonal antibodies are the fastest growing class of biological therapeutics for the treatment of various cancers and inflammatory disorders. In cancer immunotherapy, some IgG1 antibodies rely on the Fc-mediated immune effector function, antibody-dependent cellular cytotoxicity (ADCC), as the major mode of action to deplete tumor cells. It is well-known that this effector function is modulated by the N-linked glycosylation in the Fc region of the antibody. In particular, absence of core fucose on the Fc N-glycan has been shown to increase IgG1 Fc binding affinity to the FcγRIIIa present on immune effector cells such as natural killer cells and lead to enhanced ADCC activity. As such, various strategies have focused on producing afucosylated antibodies to improve therapeutic efficacy. This review discusses the relevance of antibody core fucosylation to ADCC, different strategies to produce afucosylated antibodies, and an update of afucosylated antibody drugs currently undergoing clinical trials as well as those that have been approved.

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Section: Strategies To Produce Afucosylated Antibodiesmentioning

confidence: 99%

The “less-is-more” in therapeutic antibodies: Afucosylated anti-cancer antibodies with enhanced antibody-dependent cellular cytotoxicity

Pereira

Chan

Lin

et al. 2018

mAbs

254

211

View full text Add to dashboard Cite

show abstract

“…18,25 The therapeutic anticancer potential of antibodies with decreased fucosylation, however, has been well recognized, and their power is currently being harnessed in clinical trials. 18,[20][21][22][23][24][26][27][28][29][30] In whites, the main antibodies causing FNAIT are the anti-human platelet antigen (HPA) 1a antibodies, found in ;85% of the cases and in ;1:1500 pregnancies. [31][32][33] The HPA-1a epitope resides in the GPIIIa protein of the GPIIb/IIIa complex and is missing in individuals with a single nucleotide polymorphism resulting in an L to P change at position 33 in the mature protein.…”

Section: Introductionmentioning

confidence: 99%

A prominent lack of IgG1-Fc fucosylation of platelet alloantibodies in pregnancy

Kapur¹,

Kustiawan

Vestrheim

et al. 2014

Blood

188

285

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“…Knock-out of endogenous fucosyl transferase resulted in the desired alterations in glycan profile (Lee et al 1989;Yamane-Ohnuki et al 2004). Using a prokaryotic enzyme to divert the metabolic flux from the synthesis of GDP-L-fucose to GDP-D-rhaborthmnose reduced the GDP-L-fucose substrate pool for the fucosylation reaction and led to reduced fucosylation (von Horsten et al 2010). However, it is worth noting that glycosylation pathway is very complex.…”

Section: Host Cells and Engineering Host Cellsmentioning

confidence: 99%

Cell line development for biomanufacturing processes: recent advances and an outlook

et al. 2015

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At the core of a biomanufacturing process for recombinant proteins is the production cell line. It influences the productivity and product quality. Its characteristics also dictate process development, as the process is optimized to complement the producing cell to achieve the target productivity and quality. Advances in the past decade, from vector design to cell line screening, have greatly expanded our capability to attain producing cell lines with certain desired traits. Increasing availability of genomic and transcriptomic resources for industrially important cell lines coupled with advances in genome editing technology have opened new avenues for cell line development. These developments are poised to help biosimilar manufacturing, which requires targeting pre-defined product quality attributes, e.g., glycoform, to match the innovator's range. This review summarizes recent advances and discusses future possibilities in this area.

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Production of non-fucosylated antibodies by co-expression of heterologous GDP-6-deoxy-D-lyxo-4-hexulose reductase

Cited by 95 publications

References 45 publications

The “less-is-more” in therapeutic antibodies: Afucosylated anti-cancer antibodies with enhanced antibody-dependent cellular cytotoxicity

The “less-is-more” in therapeutic antibodies: Afucosylated anti-cancer antibodies with enhanced antibody-dependent cellular cytotoxicity

A prominent lack of IgG1-Fc fucosylation of platelet alloantibodies in pregnancy

Cell line development for biomanufacturing processes: recent advances and an outlook

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