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血清可溶性白细胞介素-5 受体 α 水平升高先于儿童特应性皮炎的发生。

Increased serum-soluble interleukin-5 receptor alpha level precedes the development of eczema in children.

机构信息

The University of Manchester, University Hospital of South Manchester NHS Foundation Trust, Manchester, UK.

出版信息

Pediatr Allergy Immunol. 2010 Nov;21(7):1052-8. doi: 10.1111/j.1399-3038.2010.01077.x. Epub 2010 Aug 23.

DOI:10.1111/j.1399-3038.2010.01077.x
PMID:20735756
Abstract

Interleukin-5 receptor α-subunit expression may be implicated in the development of allergic diseases. In a population-based birth cohort, we investigated the relationship between IL-5Rα and the development of allergic phenotypes in childhood, using soluble IL-5Rα (s-IL-5Rα) as a marker. Children (n = 510) were followed from birth and assessed at age 3, 5 and 8. Based on the onset and resolution of symptoms, we assigned children into the following wheeze and eczema phenotypes: never, transient, persistent, intermittent and late-onset. Specific IgE to common allergens, s-IL-5Rα (ELISA) and urinary eosinophilic protein X (U-EPX) levels was measured at age 5. s-IL-5Rα was significantly higher among atopic compared to non-atopic children (pg/ml, geometric means [95% CI], 152.4 [126.0-184.5] vs. 103.4 [94.0-113.9], p < 0.0001). While we found no association between s-IL-5Rα and current eczema at age 5, there was a significant association between eczema phenotypes and s-IL-5Rα (multiple anova model adjusted for gender and atopy, F = 2.56, p = 0.04). After adjustment for multiple comparisons, we found that children with late-onset eczema had significantly higher s-IL-5Rα compared to those who have never had eczema (mean difference [95% CI], 2.41 [1.03-5.62], p = 0.04) and those with intermittent eczema (2.63 [1.08-6.41], p = 0.02), with no difference between children who have never had eczema and other eczema phenotypes. We found no such association for wheeze phenotypes. There was a weak correlation between s-IL-5Rα and U-EPX (r = 0.16, p < 0.0001). Increased serum s-IL-5Rα level at age 5 was associated with contemporaneous atopic sensitization and with subsequent development of eczema by age 8.

摘要

白细胞介素-5 受体 α 亚单位的表达可能与过敏性疾病的发展有关。在一项基于人群的出生队列研究中,我们使用可溶性白细胞介素-5 受体 α(s-IL-5Rα)作为标志物,研究了 IL-5Rα 与儿童期过敏性表型发展之间的关系。从出生开始,对 510 名儿童进行随访,并在 3、5 和 8 岁时进行评估。根据症状的发生和缓解,我们将儿童分为以下喘息和湿疹表型:从未有过、短暂、持续、间歇性和迟发性。在 5 岁时测量了常见过敏原的特异性 IgE、s-IL-5Rα(ELISA)和尿嗜酸性蛋白 X(U-EPX)水平。与非特应性儿童相比,特应性儿童的 s-IL-5Rα 水平明显更高(pg/ml,几何均数[95%CI],152.4[126.0-184.5]与 103.4[94.0-113.9],p<0.0001)。虽然我们没有发现 s-IL-5Rα 与 5 岁时当前湿疹之间存在关联,但湿疹表型与 s-IL-5Rα 之间存在显著关联(多变量方差分析模型调整性别和特应性,F=2.56,p=0.04)。在进行多次比较调整后,我们发现迟发性湿疹患儿的 s-IL-5Rα 明显高于从未有过湿疹的患儿(平均差异[95%CI],2.41[1.03-5.62],p=0.04)和间歇性湿疹患儿(2.63[1.08-6.41],p=0.02),但从未有过湿疹的患儿与其他湿疹表型患儿之间无差异。我们没有发现喘息表型有这种关联。s-IL-5Rα 与 U-EPX 之间存在弱相关性(r=0.16,p<0.0001)。5 岁时血清 s-IL-5Rα 水平升高与同期特应性致敏以及 8 岁时发展为湿疹有关。

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