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Significant Impact of Single N-Glycan Residues on the Biological Activity of Fc-based Antibody-like Fragments
被引:23
作者:

Jez, Jakub
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Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Antes, Bernhard
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F Star Biotechnol Forsch, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Castilho, Alexandra
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机构:
Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Kainer, Manuela
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F Star Biotechnol Forsch, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Wiederkum, Susanne
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F Star Biotechnol Forsch, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Grass, Josephine
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Univ Nat Resources & Life Sci BOKU Wien, Dept Chem, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Rueker, Florian
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Univ Nat Resources & Life Sci BOKU Wien, Dept Biotechnol, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Woisetschlaeger, Max
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F Star Biotechnol Forsch, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria

Steinkellner, Herta
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h-index: 0
机构:
Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria
机构:
[1] Univ Nat Resources & Life Sci BOKU Wien, Dept Appl Genet & Cell Biol, A-1190 Vienna, Austria
[2] Univ Nat Resources & Life Sci BOKU Wien, Dept Chem, A-1190 Vienna, Austria
[3] Univ Nat Resources & Life Sci BOKU Wien, Dept Biotechnol, A-1190 Vienna, Austria
[4] F Star Biotechnol Forsch, A-1190 Vienna, Austria
基金:
奥地利科学基金会;
关键词:
HIGH-AFFINITY BINDING;
MONOCLONAL-ANTIBODIES;
GAMMA-RIII;
GLYCOSYLATION PATTERN;
DEVELOPMENT TRENDS;
CARBOHYDRATE;
TRANSFECTION;
EXPRESSION;
VACCINES;
RECEPTOR;
D O I:
10.1074/jbc.M112.360701
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
Recent studies have demonstrated that IgG-Fc fragments (Fcabs) can be engineered to form antigen-binding sites with antibody properties. Thus they may serve as an attractive alternative to conventional antibodies in therapeutic applications. The critical influence of Fc glycosylation on effector functions of IgGs is well documented; however, whether this applies to Fcabs is not known. Here we used human cells, wild type, and glycoengineered plants to generate four different glycoforms of H10-03-6, an Fcab with engineered HER2/neu-binding sites. Plant-derived H10-03-6 differed in the presence/absence of single oligosaccharide residues, i.e., core fucose and xylose, and terminal galactose. All of the glycoforms had similar binding to HER2/neu expressed on human tumor cells. By contrast, glycoforms that lacked core oligosaccharide modifications (i.e., core alpha 1,3-fucose and beta 1,2-xylose) showed significantly enhanced binding to the Fc gamma receptor IIIa, irrespective of whether plant or human expression systems were used. Consistent with this finding, plant-derived H10-03-6 glycoforms lacking core N-glycan residues mediated higher antibody-dependent cellular cytotoxicity against human tumor cells. No alteration in gamma-receptor binding and antibody-dependent cellular cytotoxicity activity was observed upon decoration of N-glycans by terminal galactose. The results point to a significant impact of distinct N-glycan residues on effector functions of Fcabs. Moreover, the outcomes imply that the effector functions mediated by H10-03-6 can be optimized by altering the N-glycosylation profile. Biasing vaccine-induced immune responses toward optimal Fc glycosylation patterns could result in improved vaccine efficacy.
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收藏
页码:24313 / 24319
页数:7
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