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人类补体介导的过敏反应研究。IgG亚类(IgG1和/或IgG4)在免疫复合物补体激活能力中的作用。

Study of complement-mediated anaphylaxis in humans. The role of IgG subclasses (IgG1 and/or IgG4) in the complement-activating capacity of immune complexes.

作者信息

Bergamaschini L, Santangelo T, Faricciotti A, Ciavarella N, Mannucci P M, Agostoni A

机构信息

Institute of Internal Medicine, University of Milan, Italy.

出版信息

J Immunol. 1996 Feb 1;156(3):1256-61.

PMID:8558005
Abstract

The role of Ig classes and subclasses in complement activation has been investigated both in vitro and in experimental animals, but not in humans. This study was conducted to determine the immunologic events of post-transfusion anaphylaxis in humans, and the effects of immune complexes of different IgG subclass compositions on complement activation. The ability of immune complexes containing mixed IgG1 and IgG4 or IgG4 Ab only to activate complement was investigated in two patients with von Willebrand's disease (a congenital bleeding disorder). This disease was complicated by precipitating IgG alloantibodies to von Willebrand factor (vWF), which triggered complement-mediated anaphylaxis after infusion of vWF-containing preparations. Complement activation was greater in the presence of mixed IgG1- and IgG4-vWF complexes than with IgG4-vWF alone. In one patient, the generation of large amounts of C4a, C3a, and terminal complement complexes following the formation of mixed IgG1- and IgG4-vWF was associated with life-threatening anaphylaxis. In this patient, IgG4 appeared to have no inhibitory effect on antigen-bound IgG1-mediated complement activation. In the other patient, formation of IgG4-vWF led to a lesser degree of complement activation and was associated with moderately severe anaphylaxis. Since neither patient showed any biochemical alterations indicating the involvement of mast cells or the contact phase of coagulation at any time, it is probable that the pathogenetic mechanism of the clinical syndrome was a direct effect of complement anaphylatoxins on vascular permeability and smooth muscle contraction. In both patients, IgG-vWF bound C4 and C3 (IgG4-vWF to a lesser extent than mixed IgG1- and IgG4-vWF), and this probably prevented serum sickness as a complication.

摘要

Ig类别和亚类在补体激活中的作用已在体外和实验动物中进行了研究,但尚未在人类中进行。本研究旨在确定人类输血后过敏反应的免疫事件,以及不同IgG亚类组成的免疫复合物对补体激活的影响。在两名患有血管性血友病(一种先天性出血性疾病)的患者中,研究了含有混合IgG1和IgG4或仅含IgG4抗体的免疫复合物激活补体的能力。这种疾病因针对血管性血友病因子(vWF)的IgG同种异体抗体沉淀而复杂化,这些抗体在输注含vWF的制剂后引发补体介导的过敏反应。与单独的IgG4-vWF相比,混合IgG1-和IgG4-vWF复合物存在时补体激活更强。在一名患者中,混合IgG1-和IgG4-vWF形成后大量C4a、C3a和末端补体复合物的产生与危及生命的过敏反应相关。在该患者中,IgG4似乎对抗原结合的IgG1介导的补体激活没有抑制作用。在另一名患者中,IgG4-vWF的形成导致补体激活程度较低,并与中度严重的过敏反应相关。由于两名患者在任何时候均未显示出任何表明肥大细胞参与或凝血接触相的生化改变,临床综合征的发病机制可能是补体过敏毒素对血管通透性和平滑肌收缩的直接作用。在两名患者中,IgG-vWF结合了C4和C3(IgG4-vWF的结合程度低于混合IgG1-和IgG4-vWF),这可能预防了血清病作为一种并发症。

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