Fcgamma受体在关节炎病理中的复杂作用。

Springer seminars in immunopathology Pub Date : 2006-12-01 Epub Date: 2006-10-17 DOI:10.1007/s00281-006-0049-9
Peter Boross, J Sjef Verbeek
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引用次数: 25

摘要

IgG类自身抗体及其形成的免疫复合物在类风湿关节炎(RA)的病理中起着核心作用。IgG Fc部分的受体FcgammaR是IgG免疫复合物发挥作用的主要效应机制之一。FcgammaR家族的不同成员表现出广泛的结构同源性,导致配体特异性和信号转导的冗余。此外,IgG免疫复合物启动效应机制也可由补体系统介导。这种强冗余和高度复杂性阻碍了抗体效应途径的直接体内分析。在过去的十年中,通过基因靶向已经产生了缺乏不同FcgammaR组合的小鼠。这些基因敲除小鼠提供了很好的工具来确定不同的FcgammaR对IgG效应途径的具体贡献,在体内小鼠模型中建立关节炎。本综述将讨论分析FcgammaR家族不同成员在小鼠关节炎模型中的作用的研究结果及其对我们理解人类疾病的意义。
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The complex role of Fcgamma receptors in the pathology of arthritis.

Autoantibodies of the IgG class and the immune complexes they form are central players in the pathology of rheumatoid arthritis (RA). Receptors for the Fc part of IgG, FcgammaR constitute one of the main effector mechanisms through which IgG immune complexes exert their action. The different members of the FcgammaR family exhibit extensive structural homology leading to redundancy in ligand specificity and signal transduction. Moreover, the initiation of effector mechanisms by IgG immune complexes can also be mediated by the complement system. This strong redundancy and high degree of complexity hampers a direct in vivo analysis of antibody effector pathways. Over the last decade, mice deficient for different combinations of FcgammaR have been generated by gene targeting. These knockout mice provide excellent tools to define the specific contribution of the different FcgammaR to IgG effector pathways in well-established in vivo mouse models for arthritis. This review will discuss the results of the studies that analyze the role of the different members of the FcgammaR family in murine arthritis models and their implications for our understanding of the human disease.

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The discovery of immunostimulatory DNA sequence Cellular aspects of vasculitis — T cell-mediated aspects The complex role of Fcgamma receptors in the pathology of arthritis. IgA and IgA-specific receptors in human disease: structural and functional insights into pathogenesis and therapeutic potential. IgG transport across mucosal barriers by neonatal Fc receptor for IgG and mucosal immunity.
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