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接触性皮炎的独特分子特征及其治疗意义。

The Unique Molecular Signatures of Contact Dermatitis and Implications for Treatment.

机构信息

Department of Dermatology and the Laboratory of Inflammatory Skin Diseases, Icahn School of Medicine at Mount Sinai Medical Center, 5 E. 98th Street, New York, NY, 10029, USA.

出版信息

Clin Rev Allergy Immunol. 2019 Feb;56(1):1-8. doi: 10.1007/s12016-018-8685-0.

Abstract

Irritant contact dermatitis (ICD) and allergic contact dermatitis (ACD) are common skin disorders that are characterized by inflammation, oozing, crusting, and pruritus. Atopic dermatitis (AD) is an inflammatory skin disease characterized by immune and barrier abnormalities and is additionally a risk factor for acquiring ICD and ACD. New work on allergic sensitization to common allergens (e.g., nickel and fragrance) in human skin has shown that different allergens have distinct molecular fingerprinting. For example, nickel promotes strong Th1/Th17 polarization, whereas fragrance allergy causes Th2/Th22 skewing, which is similar to the phenotype of AD. While ACD has previously been considered to be constant across all allergens, largely based on mouse models involving strong sensitizers, these new data suggest that ACD differs mechanistically according to allergen. Further, ACD in the setting of concurrent AD shows a different and attenuated phenotype as compared to healthy individuals with ACD, which influences the way AD patients respond to vaccination and other treatment modalities. As in contact sensitization, skin challenged by food patch testing shows that common food allergens (e.g., peanut and barley) also cause distinct immune polarizations in the skin. Additionally, house dust mite reactions in human skin have been profiled to show unique Th2, Th9, and Th17/22 activation as compared to controls, which are similar to the phenotype of psoriasis and contact responses to nickel. Given this information, ACD patients should be treated based on their unique allergen polarity. Refined understanding of the molecular behavior of contact dermatitis and related diseases translates to improved methods of inducing tolerance in sensitized allergic patients, such as with targeted drug therapy and epicutaneous immunotherapy.

摘要

刺激性接触性皮炎(ICD)和过敏性接触性皮炎(ACD)是常见的皮肤疾病,其特征为炎症、渗出、结痂和瘙痒。特应性皮炎(AD)是一种炎症性皮肤病,其特征为免疫和屏障异常,并且是获得 ICD 和 ACD 的一个风险因素。关于常见变应原(如镍和香料)在人类皮肤中的过敏致敏的新研究表明,不同的变应原具有不同的分子指纹。例如,镍促进强烈的 Th1/Th17 极化,而香料过敏导致 Th2/Th22 偏倚,类似于 AD 的表型。虽然 ACD 以前被认为在所有变应原中都是恒定的,主要基于涉及强敏化剂的小鼠模型,但这些新数据表明 ACD 根据变应原在机制上有所不同。此外,在同时患有 AD 的情况下,ACD 表现出与健康个体的 ACD 不同且减弱的表型,这影响了 AD 患者对疫苗接种和其他治疗方式的反应方式。与接触致敏一样,通过食物斑贴试验刺激的皮肤表明,常见的食物变应原(如花生和大麦)也会在皮肤中引起不同的免疫极化。此外,与对照相比,人类皮肤中的屋尘螨反应已被描绘为显示出独特的 Th2、Th9 和 Th17/22 激活,类似于银屑病和对镍的接触反应。有了这些信息,ACD 患者应该根据其独特的变应原极性进行治疗。对接触性皮炎和相关疾病的分子行为的更深入理解转化为改善致敏过敏患者的耐受诱导方法,例如靶向药物治疗和经皮免疫疗法。

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