In Planta Glycan Engineering and Functional Activities of IgE Antibodies

Montero-Morales, Laura; Maresch, Daniel; Crescioli, Silvia; Castilho, Alexandra; Ilieva, Kristina M.; Mele, Silvia; Karagiannis, Sophia N.; Altmann, Friedrich; Steinkellner, Herta

doi:10.3389/fbioe.2019.00242

Cited by 18 publications

(15 citation statements)

References 41 publications

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“…The column was equilibrated with 1.5 CV running buffer (1xPBS, 200 mM NaCl, pH 7.4) before loading the sample. All steps took place at a flow rate of 0.8 mL/min ( Montero-Morales et al, 2019 ). The fractions corresponding to the monomeric peak collected and concentrated with Amicon centrifugal filters, MWCO 10,000 kDa (Merck Millipore).…”

Section: Methodsmentioning

confidence: 99%

Expression Profiling and Glycan Engineering of IgG Subclass 1–4 in Nicotiana benthamiana

Kallolimath

Hackl

Gahn

et al. 2020

Front. Bioeng. Biotechnol.

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IgG, the main serum immunoglobulin isotype, exists in four subclasses which selectively appear with distinctive glycosylation profiles. However, very little is known about the biological consequences mainly due to the difficulties in the generation of distinct IgG subtypes with targeted glycosylation. Here, we show a comprehensive expression and glycan modulation profiling of IgG variants in planta that are identical in their antigen binding domain but differ in their subclass appearance. While IgG1, 2, and 4 exhibit similar expression levels and purification yields, IgG3 is generated only at low levels due to the in planta degradation of the heavy chain. All IgG subtypes are produced with four distinct N-glycosylation profiles, differing in sugar residues previously shown to impact IgG activities, i.e., galactosylation, sialylation and core fucosylation. Affinity purified IgG variants are shown to be fully assembled to heterodimers but display different biochemical/physical features. All subtypes are equally well amenable to targeted glycosylation, except sialylated IgG4 which frequently accumulates substantial fractions of unusual oligo-mannosidic structures. IgG variants show significant differences in aggregate formation and endotoxin contamination which are eliminated by additional polishing steps (size exclusion chromatography, endotoxin removal treatments). Collectively we demonstrate the generation of 16 IgG variants at high purity and large glycan homogeneity which constitute an excellent toolbox to further study the biological impact of the two main Fc features, subclass and glycosylation.

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Section: Methodsmentioning

confidence: 99%

Expression Profiling and Glycan Engineering of IgG Subclass 1–4 in Nicotiana benthamiana

Kallolimath

Hackl

Gahn

et al. 2020

Front. Bioeng. Biotechnol.

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“…While recombinant IgGs are currently most widely used as therapeutic antibodies to combat infections or diseases, alternative antibody formats are gaining attention as potential biopharmaceuticals due to their specific structural properties and binding to different immune receptors (Loos et al, 2014;Brandsma et al, 2019;Montero-Morales et al, 2019). Polymeric antibody formats have a higher valency of antigen-binding sites which has several advantages compared to monomeric antibodies.…”

Section: Introductionmentioning

confidence: 99%

“…These non-human residues are potentially immunogenic and numerous strategies have been employed to prevent their attachment to N-glycans (Montero-Morales and Steinkellner, 2018). These efforts resulted in the formation of human-like N-glycan structures on recombinant glycoproteins including different immunoglobulin classes (Strasser et al, 2008;Loos et al, 2014;Göritzer et al, 2017;Montero-Morales et al, 2019) and showed that plants tolerate extensive engineering of their glycan structures. Different plant expression systems have been used to produce monomeric, dimeric or secretory IgA variants (Ma et al, 1995;Karnoup et al, 2005;Juarez et al, 2013;Virdi et al, 2013;Paul et al, 2014;Westerhof et al, 2014Westerhof et al, , 2015Dicker et al, 2016;Göritzer et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

Efficient N-Glycosylation of the Heavy Chain Tailpiece Promotes the Formation of Plant-Produced Dimeric IgA

et al. 2020

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Production of monomeric IgA in mammalian cells and plant expression systems such as Nicotiana benthamiana is well-established and can be achieved by co-expression of the corresponding light and heavy chains. In contrast, the assembly of dimeric IgA requires the additional expression of the joining chain and remains challenging especially in plant-based systems. Here, we examined factors affecting the assembly and expression of HER2 binding dimeric IgA1 and IgA2m(2) variants transiently produced in N. benthamiana. While co-expression of the joining chain resulted in efficient formation of dimeric IgAs in HEK293F cells, a mixture of monomeric, dimeric and tetrameric variants was detected in plants. Mass-spectrometric analysis of site-specific glycosylation revealed that the N-glycan profile differed between monomeric and dimeric IgAs in the plant expression system. Co-expression of a single-subunit oligosaccharyltransferase from the protozoan Leishmania major in N. benthamiana increased the N-glycosylation occupancy at the C-terminal heavy chain tailpiece and changed the ratio of monomeric to dimeric IgAs. Our data demonstrate that N-glycosylation engineering is a suitable strategy to promote the formation of dimeric IgA variants in plants.

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“…Sialylated therapeutic N-glycoproteins are predominantly produced in eukaryotic expression systems such as plants (Montero-Morales et al, 2019) and mammalian cell lines, particularly Chinese hamster ovary (CHO) cells and human embryonic kidney (HEK) cells, even though these platforms are associated with incomplete glycosylation and low efficiency of sialylation (Thi Sam et al, 2018). Engineering approaches to resolve these limitations have included simultaneous overexpression of human beta-galactoside α-2,6 sialyltransferase I and UDP-GlcNAc 2-epimerase/ManNAc kinase, resulting in yields of sialylated N-glycoprotein increased more than 7-fold compared to the wild-type (Thi Sam et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

An Engineered Pathway for Production of Terminally Sialylated N-glycoproteins in the Periplasm of Escherichia coli

Zhu

Ruan

et al. 2020

Front. Bioeng. Biotechnol.

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Terminally sialylated N-glycoproteins are of great interest in therapeutic applications. Due to the inability of prokaryotes to carry out this post-translational modification, they are currently predominantly produced in eukaryotic host cells. In this study, we report a synthetic pathway to produce a terminally sialylated N-glycoprotein in the periplasm of Escherichia coli, mimicking the sialylated moiety (Neu5Ac-α-2,6-Gal-β-1,4-GlcNAc-) of human glycans. A sialylated pentasaccharide, Neu5Ac-α-2,6-Gal-β-1,4-GlcNAc-β-1,3-Gal-β-1,3-GlcNAc-, was synthesized through the activity of co-expressed glycosyltransferases LsgCDEF from Haemophilus influenzae, Campylobacter jejuni NeuBCA enzymes, and Photobacterium leiognathi α-2,6sialyltransferase in an engineered E. coli strain which produces CMP-Neu5Ac. C. jejuni oligosaccharyltransferase PglB was used to transfer the terminally sialylated glycan onto a glyco-recognition sequence in the tenth type III cell adhesion module of human fibronectin. Sialylation of the target protein was confirmed by lectin blotting and mass spectrometry. This proof-of-concept study demonstrates the successful production of terminally sialylated, homogeneous N-glycoproteins with α-2,6-linkages in the periplasm of E. coli and will facilitate the construction of E. coli strains capable of producing terminally sialylated N-glycoproteins in high yield.

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In Planta Glycan Engineering and Functional Activities of IgE Antibodies

Cited by 18 publications

References 41 publications

Expression Profiling and Glycan Engineering of IgG Subclass 1–4 in Nicotiana benthamiana

Expression Profiling and Glycan Engineering of IgG Subclass 1–4 in Nicotiana benthamiana

Efficient N-Glycosylation of the Heavy Chain Tailpiece Promotes the Formation of Plant-Produced Dimeric IgA

An Engineered Pathway for Production of Terminally Sialylated N-glycoproteins in the Periplasm of Escherichia coli

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