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食物过敏:病理生理学和诊断的新进展。

Food allergy: recent advances in pathophysiology and diagnosis.

机构信息

Gastroentérologie pédiatrique ambulatoire, Allergie alimentaire et Explorations fonctionnelles digestives, Hôpital Necker-Enfants Malades, 149 rue de Sèvres, Paris, France.

出版信息

Ann Nutr Metab. 2011;59 Suppl 1:8-18. doi: 10.1159/000334145. Epub 2011 Dec 21.

Abstract

Approximately 5% of young children and 3-4% of adults exhibit adverse immune responses to foods in westernized countries, with a tendency to increase. The pathophysiology of food allergy (FA) relies on immune reactions triggered by epitopes, i.e. small amino-acid sequences able to bind to antibodies or cells. Some food allergens share specific physicochemical characteristics that allow them to resist digestion, thus enhancing allergenicity. These allergens encounter specialized dendritic cell populations in the gut, which leads to T-cell priming. In case of IgE-mediated allergy, this process triggers the production of allergen-specific IgE by B cells. Tissue-resident reactive cells, including mast cells, then bind IgE, and allergic reactions are elicited when these cells, with adjacent IgE molecules bound to their surface, are re-exposed to allergen. Allergic reactions occurring in the absence of detectable IgE are labeled non-IgE mediated. The abrogation of oral tolerance which leads to FA is likely favored by genetic disposition and environmental factors (e.g. increased hygiene or enhanced allergenicity of some foods). For an accurate diagnosis, complete medical history, laboratory tests and, in most cases, an oral food challenge are needed. Noticeably, the detection of food-specific IgE (sensitization) does not necessarily indicate clinical allergy. Novel diagnostic methods currently under study focus on the immune responses to specific food proteins or epitopes of specific proteins. Food-induced allergic reactions represent a large array of symptoms involving the skin and gastrointestinal and respiratory systems. They can be attributed to IgE-mediated and non-IgE-mediated (cellular) mechanisms and thus differ in their nature, severity and outcome. Outcome also differs according to allergens.

摘要

在西化国家,约 5%的幼儿和 3-4%的成年人表现出对食物的不良免疫反应,且呈上升趋势。食物过敏(FA)的病理生理学依赖于由表位引发的免疫反应,即能够与抗体或细胞结合的小氨基酸序列。一些食物过敏原具有特定的物理化学特性,使其能够抵抗消化,从而增强其致敏性。这些过敏原在肠道中遇到专门的树突状细胞群,导致 T 细胞启动。在 IgE 介导的过敏反应中,这个过程会触发 B 细胞产生过敏原特异性 IgE。组织驻留的反应性细胞,包括肥大细胞,然后结合 IgE,当这些细胞再次暴露于过敏原时,与表面结合的相邻 IgE 分子结合,引发过敏反应。在没有检测到 IgE 的情况下发生的过敏反应被标记为非 IgE 介导。导致 FA 的口服耐受中断可能由遗传倾向和环境因素(例如增加卫生或某些食物的致敏性)促进。为了进行准确诊断,需要完整的病史、实验室检查,在大多数情况下,还需要进行口服食物挑战。值得注意的是,食物特异性 IgE(致敏)的检测不一定表明存在临床过敏。目前正在研究的新型诊断方法侧重于针对特定食物蛋白或特定蛋白的表位的免疫反应。食物引起的过敏反应表现为涉及皮肤、胃肠道和呼吸系统的多种症状。它们可能归因于 IgE 介导和非 IgE 介导(细胞)机制,因此在性质、严重程度和结果上有所不同。结果也因过敏原而异。

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