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Understanding Fc Receptor Involvement in Inflammatory Diseases: From Mechanisms to New Therapeutic Tools

机译:了解Fc受体参与炎性疾病:从机制到新的治疗工具

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摘要

Fc receptors (FcRs) belong to the ITAM-associated receptor family. FcRs control the humoral and innate immunity which are essential for appropriate responses to infections and prevention of chronic inflammation or auto-immune diseases. Following their crosslinking by immune complexes, FcRs play various roles such as modulation of the immune response by released cytokines or of phagocytosis. Here, we review FcR involvement in pathologies leading notably to altered intracellular signaling with functionally relevant consequences to the host, and targeting of Fc receptors as therapeutic approaches. Special emphasis will be given to some FcRs, such as the FcαRI, the FcγRIIA and the FcγRIIIA, which behave like the ancient god Janus depending on the ITAM motif to inhibit or activate immune responses depending on their targeting by monomeric/dimeric immunoglobulins or by immune complexes. This ITAM duality has been recently defined as inhibitory or activating ITAM (ITAMi or ITAMa) which are controlled by Src family kinases. Involvement of various ITAM-bearing FcRs observed during infectious or autoimmune diseases is associated with allelic variants, changes in ligand binding ability responsible for host defense perturbation. During auto-immune diseases such as rheumatoid arthritis, lupus or immune thrombocytopenia, the autoantibodies and immune complexes lead to inflammation through FcR aggregation. We will discuss the role of FcRs in autoimmune diseases, and focus on novel approaches to target FcRs for resolution of antibody-mediated autoimmunity. We will finally also discuss the down-regulation of FcR functionality as a therapeutic approach for autoimmune diseases.
机译:Fc受体(FcR)属于ITAM相关受体家族。 FcR控制体液和先天免疫,这对于对感染的适当反应以及预防慢性炎症或自身免疫性疾病至关重要。在通过免疫复合物交联后,FcR发挥各种作用,例如通过释放的细胞因子或吞噬作用调节免疫应答。在这里,我们审查FcR参与病理导致明显改变细胞内信号转导功能相关的结果到主机,并针对Fc受体作为治疗手段的病理。将特别强调某些FcR,例如FcαRI,FcγRIIA和FcγRIIIA,它们的行为像古代神Janus一样,取决于ITAM主题抑制或激活免疫应答,具体取决于它们对单体/二聚体免疫球蛋白或免疫的靶向作用。复合体。最近将这种ITAM对偶性定义为受Src家族激酶控制的抑制性或激活ITAM(ITAMi或ITAMa)。在传染性或自身免疫性疾病中观察到的各种携带ITAM的FcR的参与与等位基因变体,配体结合能力的变化引起宿主防御微扰有关。在诸如类风湿性关节炎,狼疮或免疫性血小板减少症等自身免疫疾病期间,自身抗体和免疫复合物通过FcR聚集导致炎症。我们将讨论FcR在自身免疫性疾病中的作用,并着重于靶向FcR的新方法来解决抗体介导的自身免疫。最后,我们还将讨论FcR功能的下调作为自身免疫性疾病的治疗方法。

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