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C反应蛋白介导的吞噬作用以及通过免疫球蛋白G高亲和力受体(FcγRI)的磷脂酶D信号传导。

C-reactive protein-mediated phagocytosis and phospholipase D signalling through the high-affinity receptor for immunoglobulin G (FcgammaRI).

作者信息

Bodman-Smith Katherine B, Melendez Alirio J, Campbell Ian, Harrison Patrick T, Allen Janet M, Raynes John G

机构信息

Immunology Unit, Department of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine, Keppel Street, London, WC1E 7HT, UK.

出版信息

Immunology. 2002 Oct;107(2):252-60. doi: 10.1046/j.1365-2567.2002.01481.x.

Abstract

C-reactive protein (CRP) is the prototypic acute-phase protein in man which performs innate immune functions. CRP-mediated phagocytosis may be indirect, through activation of complement and complement receptors, or direct, through receptors for the Fc portion of immunoglobulin G (IgG; FcgammaRs) or even a putative CRP-specific receptor. No strong evidence has been shown to indicate which receptors may be responsible for phagocytosis or signalling responses. Using BIAcore technology, we confirm that CRP binds directly to the extracellular portion of FcgammaRI with a threefold higher affinity than IgG (KD = 0.81 x 10-9 m). Binding is Ca2+ dependent and is inhibited by IgG1 but not by phosphorylcholine (PC). CRP opsonization (using CRP concentrations within the normal human serum range) of PC-conjugated sheep erythrocytes increased phagocytosis of these particles by COS-7 cells transfected with FcgammaRI-II chimaera or FcgammaRI/gamma-chain. Interferon-gamma-treated U937 cells, which signal through FcgammaRI to activate phospholipase D (PLD) in response to cross-linked IgG, were also activated by CRP without any requirement for further cross-linking. These studies indicate that CRP is capable of binding to and cross-linking FcgammaRI thereby resulting in PLD activation and increased phagocytosis. Uptake by FcgammaRI has been reported to promote various acquired immune responses suggesting that CRP could act in a similar way.

摘要

C反应蛋白(CRP)是人体中的典型急性期蛋白,具有天然免疫功能。CRP介导的吞噬作用可能是间接的,通过补体和补体受体的激活,也可能是直接的,通过免疫球蛋白G(IgG)Fc段的受体(FcγRs),甚至是一种假定的CRP特异性受体。尚无有力证据表明哪些受体可能负责吞噬作用或信号反应。利用BIAcore技术,我们证实CRP直接与FcγRI的细胞外部分结合,其亲和力比IgG高3倍(KD = 0.81×10-9 m)。结合依赖于Ca2+,并被IgG1抑制,但不被磷酸胆碱(PC)抑制。用正常人血清范围内的CRP浓度对PC偶联的绵羊红细胞进行调理,可增加转染了FcγRI-II嵌合体或FcγRI/γ链的COS-7细胞对这些颗粒的吞噬作用。干扰素-γ处理的U937细胞通过FcγRI发出信号,在交联IgG时激活磷脂酶D(PLD),它也可被CRP激活,而无需进一步交联。这些研究表明,CRP能够与FcγRI结合并使其交联,从而导致PLD激活和吞噬作用增强。据报道,FcγRI的摄取可促进各种获得性免疫反应,这表明CRP可能以类似方式发挥作用。

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