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General mechanism for modulating immunoglobulin effector function

来自 Semantic Scholar

阅读量:

46

作者:

P SondermannA PinceticJ MaamaryK LammensJV Ravetch

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摘要:

Immunoglobulins recognize and clear microbial pathogens and toxins through the coupling of variable region specificity to Fc-triggered cellular activation. These proinflammatory activities are regulated, thus avoiding the pathogenic sequelae of uncontrolled inflammation by modulating the composition of the Fc-linked glycan. Upon sialylation, the affinities for Fc gamma receptors are reduced, whereas those for alternative cellular receptors, such as dendritic cell-specific intercellular adhesion molecule-3-grabbing nonintegrin (DC-SIGN)/CD23, are increased. We demonstrate that sialylation induces significant structural alterations in the C gamma 2 domain and propose a model that explains the observed changes in ligand specificity and biological activity. By analogy to related complexes formed by IgE and its evolutionarily related Fc receptors, we conclude that this mechanism is general for the modulation of antibody-triggered immune responses, characterized by a shift between an "open" activating conformation and a "closed" anti-inflammatory state of antibody Fc fragments. This common mechanism has been targeted by pathogens to avoid host defense and offers targets for therapeutic intervention in allergic and autoimmune disorders.

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关键词:

FC-EPSILON-RI HUMAN-IGG-FC ANTIINFLAMMATORY ACTIVITY DC-SIGN CRYSTAL-STRUCTURE CD23 GLYCOSYLATION BINDING FRAGMENT REVEALS

DOI:

10.1073/pnas.1307864110

被引量:

145

年份:

2013

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