Literature DB >> 27994062

Engineering an IgG Scaffold Lacking Effector Function with Optimized Developability.

Frederick W Jacobsen1, Riki Stevenson2, Cynthia Li2, Hossein Salimi-Moosavi2, Ling Liu2, Jie Wen2, Quanzhou Luo2, Kristine Daris2, Lynette Buck2, Sterling Miller2, Shu-Yin Ho2, Wei Wang2, Qing Chen2, Kenneth Walker2, Jette Wypych2, Linda Narhi2, Kannan Gunasekaran3.   

Abstract

IgG isotypes can differentially bind to Fcγ receptors and complement, making the selection of which isotype to pursue for development of a particular therapeutic antibody important in determining the safety and efficacy of the drug. IgG2 and IgG4 isotypes have significantly lower binding affinity to Fcγ receptors. Recent evidence suggests that the IgG2 isotype is not completely devoid of effector function, whereas the IgG4 isotype can undergo in vivo Fab arm exchange leading to bispecific antibody and off-target effects. Here an attempt was made to engineer an IgG1-based scaffold lacking effector function but with stability equivalent to that of the parent IgG1. Care was taken to ensure that both stability and lack of effector function was achieved with a minimum number of mutations. Among the Asn297 mutants that result in lack of glycosylation and thus loss of effector function, we demonstrate that the N297G variant has better stability and developability compared with the N297Q or N297A variants. To further improve the stability of N297G, we introduced a novel engineered disulfide bond at a solvent inaccessible location in the CH2 domain. The resulting scaffold has stability greater than or equivalent to that of the parental IgG1 scaffold. Extensive biophysical analyses and pharmacokinetic (PK) studies in mouse, rat, and monkey further confirmed the developability of this unique scaffold, and suggest that it could be used for all Fc containing therapeutics (e.g. antibodies, bispecific antibodies, and Fc fusions) requiring lack of effector function or elimination of binding to Fcγ receptors.
© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  Fc receptor; aglycosylated IgG; antibody developability; antibody engineering; antibody-dependent cellular cytotoxicity; complement-dependent cytotoxicity; disulfide engineering; drug development; immunoglobulin G (IgG); protein stability

Mesh:

Substances:

Year:  2016        PMID: 27994062      PMCID: PMC5290958          DOI: 10.1074/jbc.M116.748525

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  38 in total

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8.  Studies of aglycosylated chimeric mouse-human IgG. Role of carbohydrate in the structure and effector functions mediated by the human IgG constant region.

Authors:  M H Tao; S L Morrison
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9.  Biological Characterization of a Stable Effector Functionless (SEFL) Monoclonal Antibody Scaffold in Vitro.

Authors:  Ling Liu; Frederick W Jacobsen; Nancy Everds; Yao Zhuang; Yan Bin Yu; Nianyu Li; Darcey Clark; Mai Phuong Nguyen; Madeline Fort; Padma Narayanan; Kei Kim; Riki Stevenson; Linda Narhi; Kannan Gunasekaran; Jeanine L Bussiere
Journal:  J Biol Chem       Date:  2016-12-19       Impact factor: 5.157

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2.  Engineering a human IgG2 antibody stable at low pH.

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3.  Plasma Pharmacokinetics of High-Affinity Transferrin Receptor Antibody-Erythropoietin Fusion Protein is a Function of Effector Attenuation in Mice.

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4.  Eliminating Fc N-Linked Glycosylation and Its Impact on Dosing Consideration for a Transferrin Receptor Antibody-Erythropoietin Fusion Protein in Mice.

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5.  Comprehensive elucidation of the structural and functional roles of engineered disulfide bonds in antibody Fc fragment.

Authors:  Fang Zeng; Chunpeng Yang; Xinyu Gao; Xuan Li; Zhe Zhang; Rui Gong
Journal:  J Biol Chem       Date:  2018-10-16       Impact factor: 5.157

6.  Biological Characterization of a Stable Effector Functionless (SEFL) Monoclonal Antibody Scaffold in Vitro.

Authors:  Ling Liu; Frederick W Jacobsen; Nancy Everds; Yao Zhuang; Yan Bin Yu; Nianyu Li; Darcey Clark; Mai Phuong Nguyen; Madeline Fort; Padma Narayanan; Kei Kim; Riki Stevenson; Linda Narhi; Kannan Gunasekaran; Jeanine L Bussiere
Journal:  J Biol Chem       Date:  2016-12-19       Impact factor: 5.157

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