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食物过敏的启动机制:依赖于皮肤屏障突变和环境变应原的共刺激。

Mechanism for initiation of food allergy: Dependence on skin barrier mutations and environmental allergen costimulation.

机构信息

Allergy-Immunology Division, Northwestern University Feinberg School of Medicine, Chicago, Ill.

Department of Pediatrics, HB Wells Center for Pediatric Research, Indiana University School of Medicine, Indianapolis, Ind.

出版信息

J Allergy Clin Immunol. 2018 May;141(5):1711-1725.e9. doi: 10.1016/j.jaci.2018.02.003. Epub 2018 Feb 15.

DOI:10.1016/j.jaci.2018.02.003
PMID:29454836
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5938139/
Abstract

BACKGROUND

Mechanisms for the development of food allergy in neonates are unknown but clearly linked in patient populations to a genetic predisposition to skin barrier defects. Whether skin barrier defects contribute functionally to development of food allergy is unknown.

OBJECTIVE

The purpose of the study was to determine whether skin barrier mutations, which are primarily heterozygous in patient populations, contribute to the development of food allergy.

METHODS

Mice heterozygous for the filaggrin (Flg) and Tmem79 mutations were skin sensitized with environmental and food allergens. After sensitization, mice received oral challenge with food allergen, and then inflammation, inflammatory mediators, and anaphylaxis were measured.

RESULTS

We define development of inflammation, inflammatory mediators, and food allergen-induced anaphylaxis in neonatal mice with skin barrier mutations after brief concurrent cutaneous exposure to food and environmental allergens. Moreover, neonates of allergic mothers have increased responses to suboptimal sensitization with food allergens. Importantly, responses to food allergens by these neonatal mice were dependent on genetic defects in skin barrier function and on exposure to environmental allergens. ST2 blockade during skin sensitization inhibited the development of anaphylaxis, antigen-specific IgE, and inflammatory mediators. Neonatal anaphylactic responses and antigen-specific IgE were also inhibited by oral pre-exposure to food allergen, but interestingly, this was blunted by concurrent pre-exposure of the skin to environmental allergen.

CONCLUSION

These studies uncover mechanisms for food allergy sensitization and anaphylaxis in neonatal mice that are consistent with features of human early-life exposures and genetics in patients with clinical food allergy and demonstrate that changes in barrier function drive development of anaphylaxis to food allergen.

摘要

背景

新生儿食物过敏的发展机制尚不清楚,但在患者群体中显然与皮肤屏障缺陷的遗传易感性有关。皮肤屏障缺陷是否会对食物过敏的发展产生功能上的影响尚不清楚。

目的

本研究旨在确定皮肤屏障突变(在患者群体中主要为杂合子)是否会促进食物过敏的发展。

方法

皮肤屏障突变的 Flg 和 Tmem79 杂合子小鼠经环境和食物过敏原致敏。致敏后,用食物过敏原对小鼠进行口服挑战,然后测量炎症、炎症介质和过敏反应。

结果

我们定义了皮肤屏障突变的新生鼠在短暂同时接触食物和环境过敏原后,发展为炎症、炎症介质和食物过敏原诱导的过敏反应。此外,有过敏史母亲的新生儿对食物过敏原的低剂量致敏反应增强。重要的是,这些新生鼠对食物过敏原的反应依赖于皮肤屏障功能的遗传缺陷和环境过敏原的暴露。在皮肤致敏期间阻断 ST2 可抑制过敏反应、抗原特异性 IgE 和炎症介质的产生。食物过敏原的口服预暴露也抑制了新生鼠的过敏反应和抗原特异性 IgE,但有趣的是,这种抑制作用会被皮肤同时暴露于环境过敏原所减弱。

结论

这些研究揭示了新生鼠食物过敏致敏和过敏反应的机制,与人类早期生活暴露和具有临床食物过敏的患者的遗传特征一致,并表明屏障功能的改变会导致对食物过敏原的过敏反应。

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