Increasing FcγRIIa affinity of an FcγRIII-optimized anti-EGFR antibody restores neutrophil-mediated cytotoxicity

Antibody-dependent cell-mediated cytotoxicity (ADCC) has been suggested as an essential mechanism for the in vivo activity of cetuximab, an epidermal growth factor receptor (EGFR)-targeting therapeutic antibody. Thus, enhancing the affinity of human IgG1 antibodies to natural killer (NK) cell-expres...

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Bibliographic Details
Published in:mAbs 2014-03, Vol.6 (2), p.409-421
Main Authors: Derer, Stefanie, Glorius, Pia, Schlaeth, Martin, Lohse, Stefan, Klausz, Katja, Muchhal, Umesh, Desjarlais, John R, Humpe, Andreas, Valerius, Thomas, Peipp, Matthias
Format: Article
Language:English
Subjects:
ADCC
Antibodies, Monoclonal, Humanized - genetics
Antibodies, Monoclonal, Humanized - metabolism
Antibody Affinity - genetics
Antibody-Dependent Cell Cytotoxicity - genetics
Cells, Cultured
Cetuximab
Cytotoxicity, Immunologic - genetics
EGFR
Eosinophils - immunology
ErbB Receptors - immunology
Fc-engineering
FcγRIIa
FcγRIII
FcγRIIIb
Glycosylation
Hemoglobinuria, Paroxysmal - immunology
Hemoglobinuria, Paroxysmal - therapy
Humans
Immunoglobulin Fc Fragments - genetics
Immunoglobulin G - genetics
Immunoglobulin G - metabolism
Immunotherapy - methods
Immunotherapy - trends
Neutrophils - immunology
PMN
Polymorphism, Genetic
Protein Engineering
Receptors, IgG - genetics
Receptors, IgG - immunology
Receptors, IgG - metabolism
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Summary:Antibody-dependent cell-mediated cytotoxicity (ADCC) has been suggested as an essential mechanism for the in vivo activity of cetuximab, an epidermal growth factor receptor (EGFR)-targeting therapeutic antibody. Thus, enhancing the affinity of human IgG1 antibodies to natural killer (NK) cell-expressed FcγRIIIa by glyco- or protein-engineering of their Fc portion has been demonstrated to improve NK cell-mediated ADCC and to represent a promising strategy to improve antibody therapy. However, human polymorphonuclear (PMN) effector cells express the highly homologous FcγRIIIb isoform, which is described to be ineffective in triggering ADCC. Here, non-fucosylated or protein-engineered anti-EGFR antibodies with optimized FcγRIIIa affinities demonstrated the expected benefit in NK cell-mediated ADCC, but did not mediate ADCC by PMN, which could be restored by FcγRIIIb blockade. Furthermore, eosinophils and PMN from paroxysmal nocturnal hemoglobinuria patients that expressed no or low levels of FcγRIIIb mediated effective ADCC with FcγRIII-optimized anti-EGFR antibody. Additional experiments with double FcγRIIa/FcγRIII-optimized constructs demonstrated enhanced PMN-mediated ADCC compared with single FcγRIII-optimized antibody. In conclusion, our data demonstrate that FcγRIIIb engagement impairs PMN-mediated ADCC activity of FcγRIII-optimized anti-EGFR antibodies, while further optimization of FcγRIIa binding significantly restores PMN recruitment.
ISSN:1942-0862
1942-0870
1942-0870
1942-0862
DOI:10.4161/mabs.27457