4.8 Article

Chemoenzymatic Glycoengineering of Intact IgG Antibodies for Gain of Functions

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JOURNAL OF THE AMERICAN CHEMICAL SOCIETY
卷 134, 期 29, 页码 12308-12318

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AMER CHEMICAL SOC
DOI: 10.1021/ja3051266

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  1. National Institutes of Health (NIH) [GM096973, GM080374]

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The fine structures of Fc N-glycans can modulate the effector functions of IgG antibodies. It has been demonstrated that lack of the core fucose on the Fc N-glycans leads to drastic enhancement of antibody-dependent cellular cytotoxicity (ADCC), while terminal alpha 2,6-sialylation of Fc glycan plays a critical role for the anti-inflammatory activity of human intravenous immunoglobulin (IVIG). We describe in this paper a highly efficient chemoenzymatic method for site selective Fc glycoengineering of intact monoclonal antibody and WIG. Two new glycosynthase mutants (EndoS-D233A and D233Q) were generated by site directed mutagenesis of EndoS (an endoglycosidase from Streptococcus pyogenes) and were found to be capable of efficiently transferring predefined N-glycans from corresponding glycan oxazolines to the Fc-deglycosylated intact,IgGs without product hydrolysis. As a model study, rituximab (a therapeutic monoclonal antibody) was successfully transformed from mixtures of G0F, G1F, and G2F glycoforms to well-defined homogeneous glycoforms, including a fully sialylated (S2G2F) glycoform that may gain anti-inflammatory activity, a nonfucosylated G2 glycoform that showed significantly enhanced Fc gamma IIIa receptor binding activity, and an azido-tagged glycoform that can be further transformed into other glycoforms. We also found that EndoS could selectively remove the Fc N-glycans in the presence of FAB glycosylation. This finding, coupled with the remarkable transglycosylation activity of the EndoS glycosynthase mutants, permitted a highly selective glycoengineering of the WIG's Fc glycans into a fully sialylated Fc glycoform, which may possess significantly enhanced anti-inflammatory activity. The glycoengineering approach described here provides a general platform to modulate the effector functions of IgG antibodies, enabling the optimization of therapeutic efficacy and gain of new functions of monoclonal antibodies and WIG.

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