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调节免疫球蛋白效应功能的一般机制。

General mechanism for modulating immunoglobulin effector function.

机构信息

SuppreMol GmbH, 82152 Martinsried, Germany.

出版信息

Proc Natl Acad Sci U S A. 2013 Jun 11;110(24):9868-72. doi: 10.1073/pnas.1307864110. Epub 2013 May 22.

Abstract

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 Fcγ 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 Cγ2 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.

摘要

免疫球蛋白通过可变区特异性与 Fc 触发的细胞激活偶联来识别和清除微生物病原体和毒素。这些促炎活性受到调节,从而通过调节 Fc 连接聚糖的组成来避免不受控制的炎症的致病后果。唾液酸化后,与 Fcγ 受体的亲和力降低,而与替代细胞受体(如树突状细胞特异性细胞间黏附分子 3 抓取非整联蛋白 (DC-SIGN)/CD23)的亲和力增加。我们证明唾液酸化诱导 Cγ2 结构域发生显著结构改变,并提出了一个解释观察到的配体特异性和生物学活性变化的模型。通过与 IgE 及其进化相关的 Fc 受体形成的相关复合物进行类比,我们得出结论,这种机制是调节抗体触发的免疫反应的通用机制,其特征是抗体 Fc 片段在“开放”激活构象和“封闭”抗炎状态之间发生转变。这种共同的机制已被病原体利用来逃避宿主防御,并为过敏和自身免疫性疾病的治疗干预提供了目标。

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