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儿童哮喘:通过细胞因子进行新型表型分型,并通过致敏谱和临床特征进行验证。

Childhood asthma: Novel endotyping by cytokines, validated through sensitization profiles and clinical characteristics.

机构信息

Department of Pulmonary and Allergy, Dr. von Hauner Children's Hospital, LMU University of Munich, Munich, Germany.

Dr. von Hauner Children's Hospital, LMU University of Munich, Munich, Germany.

出版信息

Clin Exp Allergy. 2021 May;51(5):654-665. doi: 10.1111/cea.13858. Epub 2021 Mar 14.

Abstract

BACKGROUND

Specific allergy sensitization pattern, using "component-resolved diagnosis" (CRD), is a central component of allergy and asthma in childhood. Besides this, allergic asthma has been characterized by a Th2-shifted endotype with elevation of classical Th2 cytokines. Recently, other endotypes with distinct mechanisms focusing on cytokine regulation evolved, yet those pathways are still not well understood.

OBJECTIVE

(a) To define reproducible immunological endotypes using cytokine expression in an asthma cohort and (b) to characterize their sensitization profile and clinical phenotype.

METHODS

Supernatants from PBMCs of 234 children (median age 10 years) of an asthma cohort were analysed for cytokine expressions. The children were split into a training (n = 49) and validation (n = 185) group. The training group was used to identify immunological endotypes by clustering cytokine expressions, which were then assessed regarding clinical characteristics and specific IgE of recombinant allergen components. Next, our findings were validated in the validation group.

RESULTS

We identified novel endotypes based on primarily unstimulated cytokine expression. One endotype showed an IFN-γ/Interleukin (IL)-17/IL-5 predominance, a different sensitization pattern (high in birch/apple; p < .01), and inferior lung function (p < .01). A second endotype grouped young children with food allergy and reduced lung function. Our findings were reproducible in the validation group.

CONCLUSION AND CLINICAL RELEVANCE

We identified two novel clinical asthma endotypes via cytokine expression pattern with distinct sensitization patterns. These novel findings are critical for clinical guidance and open avenues for identifying underlying mechanisms and more patient-specific therapies.

摘要

背景

使用“成分分辨诊断”(CRD)的特定过敏致敏模式是儿童过敏和哮喘的核心组成部分。除此之外,过敏性哮喘的特征是 Th2 偏移表型,伴有经典 Th2 细胞因子的升高。最近,出现了其他具有不同机制的特征性表型,这些机制集中在细胞因子调节上,但这些途径仍未得到很好的理解。

目的

(a)使用哮喘队列中的细胞因子表达定义可重复的免疫学表型,(b)描述其致敏特征和临床表型。

方法

分析 234 名哮喘队列儿童(中位数年龄 10 岁)的 PBMC 上清液中的细胞因子表达。将儿童分为训练组(n=49)和验证组(n=185)。使用训练组通过聚类细胞因子表达来识别免疫学表型,然后评估其与临床特征和重组过敏原成分的特异性 IgE 的相关性。接下来,在验证组中验证我们的发现。

结果

我们基于主要未刺激的细胞因子表达确定了新的表型。一种表型表现出 IFN-γ/白细胞介素(IL)-17/IL-5 优势,具有不同的致敏模式(桦树/苹果高;p<0.01),肺功能较差(p<0.01)。第二种表型将具有食物过敏和肺功能降低的幼儿分组。我们的发现在验证组中具有可重复性。

结论和临床意义

我们通过细胞因子表达模式识别出两种新的临床哮喘表型,具有不同的致敏模式。这些新发现对临床指导至关重要,并为识别潜在机制和更具患者特异性的治疗方法开辟了途径。

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