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用于研究变应原及变应原特异性免疫球蛋白E和免疫球蛋白G的体外系统的开发:Fcepsilon受体I超交联是免疫球蛋白G依赖性增强I型过敏反应的一种可能新机制。

Development of an in vitro system for the study of allergens and allergen-specific immunoglobulin E and immunoglobulin G: Fcepsilon receptor I supercross-linking is a possible new mechanism of immunoglobulin G-dependent enhancement of type I allergic reactions.

作者信息

Sellge G, Laffer S, Mierke C, Vrtala S, Hoffmann M W, Klempnauer J, Manns M P, Valenta R, Bischoff S C

机构信息

Department of Gastroenterology, Hepatology and Endocrinology, Hannover, Germany.

出版信息

Clin Exp Allergy. 2005 Jun;35(6):774-81. doi: 10.1111/j.1365-2222.2005.02248.x.

DOI:10.1111/j.1365-2222.2005.02248.x
PMID:15969669
Abstract

BACKGROUND

IgE-dependent activation of mast cells (MCs) is a key pathomechanism of type I allergies. In contrast, allergen-specific IgG Abs are thought to attenuate immediate allergic reactions by blocking IgE binding and by cross-linking the inhibitory Fcgamma receptor IIB on MCs.

OBJECTIVES

To establish a defined in vitro system using human MCs to study the biological activity of allergens and to investigate the role of allergen-specific IgE and IgG.

METHODS

Purified human intestinal MCs sensitized with different forms of specific IgE Abs were triggered by monomeric and oligomeric forms of recombinant Bet v 1, the major birch pollen allergen, in the presence or absence of allergen-specific IgG Abs. Results MCs sensitized with an anti-Bet v 1 IgE mAb or sera obtained from birch pollen allergic patients released histamine and sulphidoleukotrienes after exposure to oligomeric Bet v 1. Monomeric Bet v 1 provoked mediator release only in MCs sensitized with patients sera but not in MCs sensitized with anti-Bet v 1 IgE mAb. Interestingly, MC activation could be induced by supercross-linking of monomeric Bet v 1 bound to monovalent IgE on MCs with a secondary allergen-specific IgG pAb. By using IgG F(ab')2 fragments we provide evidence that this effect is not a result of IgG binding to Fcgamma receptors.

CONCLUSION

This assay represents a new tool for the in vitro study of MC activation in response to natural and genetically modified allergens. Fcepsilon receptor I supercross-linking by allergen-specific IgG Abs provides a possible new mechanism of IgG-dependent enhancement of type I allergic reactions.

摘要

背景

肥大细胞(MCs)的IgE依赖性激活是I型过敏反应的关键发病机制。相比之下,过敏原特异性IgG抗体被认为可通过阻断IgE结合以及交联MCs上的抑制性Fcγ受体IIB来减轻速发型过敏反应。

目的

建立一个使用人MCs的特定体外系统,以研究过敏原的生物学活性,并探讨过敏原特异性IgE和IgG的作用。

方法

用不同形式的特异性IgE抗体致敏的纯化人肠道MCs,在存在或不存在过敏原特异性IgG抗体的情况下,由重组桦树花粉主要过敏原Bet v 1的单体和寡聚体形式触发。结果:用抗Bet v 1 IgE单克隆抗体或从桦树花粉过敏患者获得的血清致敏的MCs,在暴露于寡聚体Bet v 1后释放组胺和硫代白三烯。单体Bet v 1仅在患者血清致敏的MCs中引起介质释放,而在抗Bet v 1 IgE单克隆抗体致敏的MCs中则不会。有趣的是,通过用二级过敏原特异性IgG多克隆抗体对MCs上与单价IgE结合的单体Bet v 1进行超交联,可以诱导MC激活。通过使用IgG F(ab')2片段,我们提供证据表明这种效应不是IgG与Fcγ受体结合的结果。

结论

该检测方法代表了一种用于体外研究MCs对天然和转基因过敏原反应激活的新工具。过敏原特异性IgG抗体介导的Fcepsilon受体I超交联为IgG依赖性增强I型过敏反应提供了一种可能的新机制。

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