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特应性皮炎患者对皮肤过敏原暴露反应的谜题。

The riddle of response to cutaneous allergen exposure in patients with atopic dermatitis.

机构信息

Division of Allergy and Immunology, Department of Pediatrics, Jaffe Food Allergy Research Institute, Icahn School of Medicine at Mount Sinai, New York, New York.

出版信息

Ann Allergy Asthma Immunol. 2024 Sep;133(3):244-251. doi: 10.1016/j.anai.2024.05.005. Epub 2024 May 11.

Abstract

The skin is the largest immunologic organ in the body and contains immune cells that play a role in both food allergen sensitization and desensitization. The dual allergen exposure hypothesis posits that sensitization to food allergens may occur with cutaneous exposure on inflamed skin, eg, atopic dermatitis, but early oral consumption generally leads to tolerance. However, only one-third of children with atopic dermatitis develop a food allergy, suggesting that there is a more complex mechanism for allergen sensitization. Emerging evidence suggests that the outcome of cutaneous allergen exposure is context-dependent and largely influenced by the state of the skin barrier with healthy skin promoting natural tolerance. Current research supports the ability to induce desensitization through repeated application of allergens to the skin, known as epicutaneous immunotherapy. Preclinical research with an occlusive patch has demonstrated a significantly reduced T-helper cell type 2-driven immunologic response when applied to intact, uninflamed skin and induction of a unique population of regulatory T cells that express a broader range of homing receptors, which may be able to maintain sustained protection. In clinical studies of children aged 1 through 11 years with a peanut allergy, epicutaneous immunotherapy with an occlusive patch led to significant desensitization with no major differences in efficacy or safety between children with and without atopic dermatitis. These data begin to answer the conundrum of how allergens that are applied to the skin can lead to both sensitization and desensitization, and future studies should enable us to optimize the power of the skin as a complex immunologic organ to treat allergic, autoimmune, and autoinflammatory disorders.

摘要

皮肤是人体最大的免疫器官,其中含有免疫细胞,在食物过敏原致敏和脱敏中发挥作用。双重过敏原暴露假说认为,食物过敏原的致敏可能发生在炎症皮肤的皮肤暴露中,例如特应性皮炎,但早期口服摄入通常会导致耐受。然而,只有三分之一的特应性皮炎儿童会发展为食物过敏,这表明过敏原致敏存在更复杂的机制。新出现的证据表明,皮肤过敏原暴露的结果取决于具体情况,并且在很大程度上受到皮肤屏障状态的影响,健康的皮肤促进自然耐受。目前的研究支持通过反复将过敏原应用于皮肤来诱导脱敏的能力,称为经皮免疫疗法。封闭贴剂的临床前研究表明,当应用于完整、非炎症的皮肤时,可显著降低辅助性 T 细胞 2 驱动的免疫反应,并诱导表达更广泛归巢受体的独特调节性 T 细胞群,这可能能够维持持续的保护。在对 1 至 11 岁患有花生过敏的儿童进行的临床研究中,经皮免疫疗法联合封闭贴剂可显著脱敏,患有和不患有特应性皮炎的儿童在疗效和安全性方面没有显著差异。这些数据开始解答过敏原应用于皮肤既能致敏又能脱敏的难题,未来的研究应该使我们能够优化皮肤作为复杂免疫器官的功能,以治疗过敏、自身免疫和自身炎症性疾病。

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