Literature DB >> 21855548

Combined Fc-protein- and Fc-glyco-engineering of scFv-Fc fusion proteins synergistically enhances CD16a binding but does not further enhance NK-cell mediated ADCC.

Roland Repp1, Christian Kellner, Anja Muskulus, Matthias Staudinger, Sahar Mohseni Nodehi, Pia Glorius, Dalia Akramiene, Michael Dechant, Georg H Fey, Patrick H C van Berkel, Jan G J van de Winkel, Paul W H I Parren, Thomas Valerius, Martin Gramatzki, Matthias Peipp.   

Abstract

Protein- or glyco-engineering of antibody molecules can be used to enhance Fc-mediated effector functions. ScFv-Fc fusion proteins (scFv-Fc) represent interesting antibody derivatives due to their relatively simple design and increased tissue penetration. Here, the impact of protein- and glyco-engineering on ADCC potency of a panel of human IgG1-based scFv-Fc was tested. Three matched sets of scFv-Fc variants targeting CD7, CD20 or HLA class II and optimized for CD16a binding by mutagenesis, lack of core-fucose, or their combination, were generated and functionally tested in comparison to the corresponding wild type scFv-Fc. Antigen binding activity was not compromised by altered glycosylation or Fc mutagenesis, whereas Fc binding to CD16a was significantly enhanced in the order: non-core fucosylated/Fc-mutated double-engineered≫Fc-mutated≥non-core-fucosylated>wild-type IgG1-Fc. All engineered variants triggered potent ADCC with up to 100-fold reduced EC50 values compared to non-engineered variants. Interestingly, double-engineered variants were similarly effective in triggering ADCC compared to single-engineered variants irrespective of their 1 log greater CD16a binding affinity. Thus, these data demonstrate that protein- and glyco-engineering enhances NK-cell mediated ADCC of scFv-Fc similarly and show that enhancing CD16a affinity beyond a certain threshold does not result in a further increase of NK-cell mediated ADCC.
Copyright © 2011 Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 21855548     DOI: 10.1016/j.jim.2011.08.003

Source DB:  PubMed          Journal:  J Immunol Methods        ISSN: 0022-1759            Impact factor:   2.303


  15 in total

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2.  Enhancing natural killer cell-mediated lysis of lymphoma cells by combining therapeutic antibodies with CD20-specific immunoligands engaging NKG2D or NKp30.

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3.  Asymmetrical Fc engineering greatly enhances antibody-dependent cellular cytotoxicity (ADCC) effector function and stability of the modified antibodies.

Authors:  Zhi Liu; Kannan Gunasekaran; Wei Wang; Vladimir Razinkov; Laura Sekirov; Esther Leng; Heather Sweet; Ian Foltz; Monique Howard; Anne-Marie Rousseau; Carl Kozlosky; William Fanslow; Wei Yan
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4.  The Development and Characterization of an scFv-Fc Fusion-Based Gene Therapy to Reduce the Psychostimulant Effects of Methamphetamine Abuse.

Authors:  Charles E Hay; Laura E Ewing; Michael D Hambuchen; Shannon M Zintner; Juliana C Small; Chris T Bolden; William E Fantegrossi; Paris Margaritis; S Michael Owens; Eric C Peterson
Journal:  J Pharmacol Exp Ther       Date:  2020-04-03       Impact factor: 4.030

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

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6.  An Fc Double-Engineered CD20 Antibody with Enhanced Ability to Trigger Complement-Dependent Cytotoxicity and Antibody-Dependent Cell-Mediated Cytotoxicity.

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Review 8.  Engineering broadly neutralizing antibodies for HIV prevention and therapy.

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Journal:  Adv Drug Deliv Rev       Date:  2016-01-29       Impact factor: 15.470

9.  Human anti-CCR4 minibody gene transfer for the treatment of cutaneous T-cell lymphoma.

Authors:  Thomas Han; Ussama M Abdel-Motal; De-Kuan Chang; Jianhua Sui; Asli Muvaffak; James Campbell; Quan Zhu; Thomas S Kupper; Wayne A Marasco
Journal:  PLoS One       Date:  2012-09-04       Impact factor: 3.240

10.  The use of epidermal growth factor receptor monoclonal antibodies in squamous cell carcinoma of the head and neck.

Authors:  Jeffery S Russell; A Dimitrios Colevas
Journal:  Chemother Res Pract       Date:  2012-09-13
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