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      Decoding the Human Immunoglobulin G-Glycan Repertoire Reveals a Spectrum of Fc-Receptor- and Complement-Mediated-Effector Activities

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          Abstract

          Glycosylation of the immunoglobulin G (IgG)-Fc tail is required for binding to Fc-gamma receptors (FcγRs) and complement-component C1q. A variety of IgG1-glycoforms is detected in human sera. Several groups have found global or antigen-specific skewing of IgG glycosylation, for example in autoimmune diseases, viral infections, and alloimmune reactions. The IgG glycoprofiles seem to correlate with disease outcome. Additionally, IgG-glycan composition contributes significantly to Ig-based therapies, as for example IVIg in autoimmune diseases and therapeutic antibodies for cancer treatment. The effect of the different glycan modifications, especially of fucosylation, has been studied before. However, the contribution of the 20 individual IgG glycoforms, in which the combined effect of all 4 modifications, to the IgG function has never been investigated. Here, we combined six glyco-engineering methods to generate all 20 major human IgG1-glycoforms and screened their functional capacity for FcγR and complement activity. Bisection had no effect on FcγR or C1q-binding, and sialylation had no- or little effect on FcγR binding. We confirmed that hypo-fucosylation of IgG1 increased binding to FcγRIIIa and FcγRIIIb by ~17-fold, but in addition we showed that this effect could be further increased to ~40-fold for FcγRIIIa upon simultaneous hypo-fucosylation and hyper-galactosylation, resulting in enhanced NK cell-mediated antibody-dependent cellular cytotoxicity. Moreover, elevated galactosylation and sialylation significantly increased (independent of fucosylation) C1q-binding, downstream complement deposition, and cytotoxicity. In conclusion, fucosylation and galactosylation are primary mediators of functional changes in IgG for FcγR- and complement-mediated effector functions, respectively, with galactose having an auxiliary role for FcγRIII-mediated functions. This knowledge could be used not only for glycan profiling of clinically important (antigen-specific) IgG but also to optimize therapeutic antibody applications.

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          Specificity and affinity of human Fcgamma receptors and their polymorphic variants for human IgG subclasses.

          Pierre Bruhns, Bruno Iannascoli, Patrick England (2009)
          Distinct genes encode 6 human receptors for IgG (hFcgammaRs), 3 of which have 2 or 3 polymorphic variants. The specificity and affinity of individual hFcgammaRs for the 4 human IgG subclasses is unknown. This information is critical for antibody-based immunotherapy which has been increasingly used in the clinics. We investigated the binding of polyclonal and monoclonal IgG1, IgG2, IgG3, and IgG4 to FcgammaRI; FcgammaRIIA, IIB, and IIC; FcgammaRIIIA and IIIB; and all known polymorphic variants. Wild-type and low-fucosylated IgG1 anti-CD20 and anti-RhD mAbs were also examined. We found that (1) IgG1 and IgG3 bind to all hFcgammaRs; (2) IgG2 bind not only to FcgammaRIIA(H131), but also, with a lower affinity, to FcgammaRIIA(R131) and FcgammaRIIIA(V158); (3) IgG4 bind to FcgammaRI, FcgammaRIIA, IIB and IIC and FcgammaRIIIA(V158); and (4) the inhibitory receptor FcgammaRIIB has a lower affinity for IgG1, IgG2, and IgG3 than all other hFcgammaRs. We also identified parameters that determine the specificity and affinity of hFcgammaRs for IgG subclasses. These results document how hFcgammaR specificity and affinity may account for the biological activities of antibodies. They therefore highlight the role of specific hFcgammaRs in the therapeutic and pathogenic effects of antibodies in disease.
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            Unique carbohydrate-carbohydrate interactions are required for high affinity binding between FcgammaRIII and antibodies lacking core fucose.

            Claudia Ferrara, Sandra Grau, Christiane Jäger (2011)
            Antibody-mediated cellular cytotoxicity (ADCC), a key immune effector mechanism, relies on the binding of antigen-antibody complexes to Fcγ receptors expressed on immune cells. Antibodies lacking core fucosylation show a large increase in affinity for FcγRIIIa leading to an improved receptor-mediated effector function. Although afucosylated IgGs exist naturally, a next generation of recombinant therapeutic, glycoenginereed antibodies is currently being developed to exploit this finding. In this study, the crystal structures of a glycosylated Fcγ receptor complexed with either afucosylated or fucosylated Fc were determined allowing a detailed, molecular understanding of the regulatory role of Fc-oligosaccharide core fucosylation in improving ADCC. The structures reveal a unique type of interface consisting of carbohydrate-carbohydrate interactions between glycans of the receptor and the afucosylated Fc. In contrast, in the complex structure with fucosylated Fc, these contacts are weakened or nonexistent, explaining the decreased affinity for the receptor. These findings allow us to understand the higher efficacy of therapeutic antibodies lacking the core fucose and also suggest a unique mechanism by which the immune system can regulate antibody-mediated effector functions.
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              Copy number polymorphism in Fcgr3 predisposes to glomerulonephritis in rats and humans.

              Timothy J. Aitman, Rong Dong, Timothy Vyse (2006)
              Identification of the genes underlying complex phenotypes and the definition of the evolutionary forces that have shaped eukaryotic genomes are among the current challenges in molecular genetics. Variation in gene copy number is increasingly recognized as a source of inter-individual differences in genome sequence and has been proposed as a driving force for genome evolution and phenotypic variation. Here we show that copy number variation of the orthologous rat and human Fcgr3 genes is a determinant of susceptibility to immunologically mediated glomerulonephritis. Positional cloning identified loss of the newly described, rat-specific Fcgr3 paralogue, Fcgr3-related sequence (Fcgr3-rs), as a determinant of macrophage overactivity and glomerulonephritis in Wistar Kyoto rats. In humans, low copy number of FCGR3B, an orthologue of rat Fcgr3, was associated with glomerulonephritis in the autoimmune disease systemic lupus erythematosus. The finding that gene copy number polymorphism predisposes to immunologically mediated renal disease in two mammalian species provides direct evidence for the importance of genome plasticity in the evolution of genetically complex phenotypes, including susceptibility to common human disease.
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                Author and article information

                Contributors
                Gillian Dekkers: URI : http://frontiersin.org/people/u/181191
                Louise Treffers: URI : http://frontiersin.org/people/u/457160
                Arthur E. H. Bentlage: URI : http://frontiersin.org/people/u/454817
                Suzanne N. Lissenberg-Thunnissen: URI : http://frontiersin.org/people/u/455226
                Theo Rispens: URI : http://frontiersin.org/people/u/188621
                Gestur Vidarsson: URI : http://frontiersin.org/people/u/88709
                Journal
                Journal ID (nlm-ta): Front Immunol
                Journal ID (iso-abbrev): Front Immunol
                Journal ID (publisher-id): Front. Immunol.
                Title: Frontiers in Immunology
                Publisher: Frontiers Media S.A.
                ISSN (Electronic): 1664-3224
                Publication date (Electronic): 02 August 2017
                Publication date Collection: 2017
                Volume: 8
                Electronic Location Identifier: 877
                Affiliations
                [1] 1Sanquin Research and Landsteiner Laboratory, Department Experimental Immunohematology, Academic Medical Centre, University of Amsterdam , Amsterdam, Netherlands
                [2] 2Sanquin Research and Landsteiner Laboratory, Department Blood Cell Research, Academic Medical Centre, University of Amsterdam , Amsterdam, Netherlands
                [3] 3Center for Proteomics and Metabolomics, Leiden University Medical Center , Leiden, Netherlands
                [4] 4Sanquin Research and Landsteiner Laboratory, Department Immunopathology, Academic Medical Centre, University of Amsterdam , Amsterdam, Netherlands
                [5] 5Sanquin Reagents , Amsterdam, Netherlands
                Author notes

                Edited by: José Mordoh, Fundación Instituto Leloir, Argentina

                Reviewed by: Raffael Nachbagauer, Icahn School of Medicine at Mount Sinai, United States; Johannes S. Gach, University of California, Irvine, United States

                *Correspondence: Gestur Vidarsson, g.vidarsson@ 123456sanquin.nl

                Specialty section: This article was submitted to Vaccines and Molecular Therapeutics, a section of the journal Frontiers in Immunology

                Article
                DOI: 10.3389/fimmu.2017.00877
                PMC ID: 5539844
                PubMed ID: 28824618
                SO-VID: 41f08442-6b20-4654-ad0f-db756853995b
                Copyright © Copyright © 2017 Dekkers, Treffers, Plomp, Bentlage, de Boer, Koeleman, Lissenberg-Thunnissen, Visser, Brouwer, Mok, Matlung, van den Berg, van Esch, Kuijpers, Wouters, Rispens, Wuhrer and Vidarsson.
                License:

                This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

                History
                Date received : 08 May 2017
                Date accepted : 10 July 2017
                Page count
                Figures: 6, Tables: 2, Equations: 0, References: 67, Pages: 15, Words: 9518
                Funding
                Funded by: Process Development Plasma Products
                Award ID: 12-001
                Categories
                Subject: Immunology
                Subject: Original Research

                ScienceOpen disciplines: Immunology
                Keywords: immunoglobulin g glycosylation,fc gamma receptor,antibody-dependent cellular cytotoxicity,complement,antibody effector functions
                Data availability:
                ScienceOpen disciplines: Immunology
                Keywords: immunoglobulin g glycosylation, fc gamma receptor, antibody-dependent cellular cytotoxicity, complement, antibody effector functions

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