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特应性皮炎发病期的早期免疫学变化。

Early immunologic changes during the onset of atopic dermatitis.

机构信息

Department of Dermatology, Medical University of Vienna, Austria.

出版信息

Ann Allergy Asthma Immunol. 2019 Aug;123(2):152-157. doi: 10.1016/j.anai.2019.03.033. Epub 2019 Apr 4.

Abstract

OBJECTIVE

Atopic dermatitis (AD), which is commonly called eczema, is the most common chronic inflammatory skin disease. The pipeline of new targeted treatments is currently expanding, a development that is largely based on our increasing understanding of disease mechanisms. Mechanistic insights have long been based on long-standing adult AD. Recently, studies also investigated early pediatric AD at disease onset, and revealed several differences in barrier and immune properties when compared with long-standing adult AD. This review focuses on immunological changes very early in life that predispose to the development of AD, and summarizes characteristics of the molecular AD phenotype in this age group.

DATA SOURCES

Review of published literature.

STUDY SELECTIONS

Studies investigating human AD at disease onset in newborns, toddlers, and young children, in comparison with adults with long-standing disease.

RESULTS

Already in cord blood, increased Th2 and decreased Th1 levels were found to increase the risk of AD development. Both pediatric and adult AD share Th2/Th22 activation and defects in lipid barrier deposition and tight junction formation, but Th1 activation and epidermal differentiation complex defects are largely absent in pediatric AD.

CONCLUSION

Immune changes predisposing to AD development are present very early in life. During the first months of disease, AD shows various differences in immune and barrier properties from long-standing adult AD, which might necessitate tailored treatment approaches depending on the age of the patient.

摘要

目的

特应性皮炎(AD),通常称为湿疹,是最常见的慢性炎症性皮肤病。新的靶向治疗药物管线目前正在扩展,这在很大程度上是基于我们对疾病机制的认识不断加深。对发病机制的认识长期以来一直基于成人 AD。最近,研究还在发病早期对儿童 AD 进行了研究,与成人 AD 相比,在屏障和免疫特性方面发现了一些差异。这篇综述重点关注了易患 AD 发展的生命早期的免疫学变化,并总结了这一年龄组中 AD 分子表型的特征。

数据来源

已发表文献的综述。

研究选择

对新生儿、幼儿和儿童 AD 发病期的研究,并与长期患有成人 AD 的患者进行比较。

结果

在脐血中,已发现 Th2 增加和 Th1 减少会增加 AD 发病的风险。儿科 AD 和成人 AD 均存在 Th2/Th22 激活以及脂质屏障沉积和紧密连接形成缺陷,但在儿科 AD 中,Th1 激活和表皮分化复合物缺陷基本不存在。

结论

易患 AD 发展的免疫变化在生命早期就存在。在疾病的最初几个月,AD 在免疫和屏障特性方面与成人 AD 存在各种差异,这可能需要根据患者的年龄制定针对性的治疗方法。

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