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在一项基于人群的白人成年队列研究中,STAT 6单倍型与血清IgE水平升高的关联。

Association of a STAT 6 haplotype with elevated serum IgE levels in a population based cohort of white adults.

作者信息

Weidinger S, Klopp N, Wagenpfeil S, Rümmler L, Schedel M, Kabesch M, Schäfer T, Darsow U, Jakob T, Behrendt H, Wichmann H E, Ring J, Illig T

机构信息

Department of Dermatology and Allergy, Technical University Munich, Biedersteiner St. 29, 80802 Munich, Germany.

出版信息

J Med Genet. 2004 Sep;41(9):658-63. doi: 10.1136/jmg.2004.020263.

Abstract

BACKGROUND

Several studies have shown linkage of chromosome 12q 13-24 with atopy related phenotypes. Among candidate genes in this region is STAT6 (signal transducer and activator of transcription), which is essential for Th2 cell differentiation, recruitment, and effector function.

METHODS

We evaluated six polymorphisms of STAT6 for evidence of associations with serum IgE levels and atopic diseases in a population based cross sectional cohort of 1407 German adults. Genotyping was performed using the matrix assisted laser desorption ionisation-time of flight mass spectrometry method. Haplotypes were estimated using the SAS/Genetics module, and population-derived IgE percentiles (50% IgE>53 kU/l, 66% IgE>99 kU/l and 90% IgE>307 kU/l) were modelled as outcome variables in haplotype trend regression analysis.

RESULTS

All polymorphisms were genotyped successfully. Haplotype reconstruction revealed 8/64 possible haplotypes, reaching estimated frequencies of 1% or more. One polymorphism in intron 2 (rs324011) showed a significant association with total serum IgE (p = 0.015). A STAT6 risk haplotype for elevated IgE showing odds ratios of 1.7 (p = 0.015) for IgE cut-off 100 kU/l, and 1.54 (p = 0.032), 1.6 (p = 0.025), and 2.54 (p = 0.007) for IgE percentiles 50%, 66%, and 90%, respectively was detected. The increased risk of this haplotype was confirmed by linear haplotype trend regression on log transformed IgE values (p = 0.007). Analysis further revealed a risk haplotype for specific sensitisation and a risk haplotype for asthma.

CONCLUSION

The data indicate that genetic variants within STAT6 contribute significantly to IgE regulation and manifestation of atopic diseases.

摘要

背景

多项研究表明,12号染色体13 - 24区域与特应性相关表型存在连锁关系。该区域的候选基因之一是STAT6(信号转导子和转录激活子),它对Th2细胞的分化、募集及效应功能至关重要。

方法

我们在一个由1407名德国成年人组成的基于人群的横断面队列中,评估了STAT6的6种多态性与血清IgE水平及特应性疾病之间的关联证据。采用基质辅助激光解吸电离飞行时间质谱法进行基因分型。使用SAS/Genetics模块估计单倍型,并将人群衍生的IgE百分位数(50% IgE>53 kU/l、66% IgE>99 kU/l和90% IgE>307 kU/l)作为单倍型趋势回归分析中的结果变量进行建模。

结果

所有多态性均成功进行了基因分型。单倍型重建显示有8/64种可能的单倍型,估计频率达到1%或更高。内含子2中的一个多态性(rs324011)与总血清IgE显著相关(p = 0.015)。检测到一种与IgE升高相关的STAT6风险单倍型,对于IgE临界值100 kU/l,优势比为1.7(p = 0.015),对于IgE百分位数50%、66%和90%,优势比分别为1.54(p = 0.032)、1.6(p = 0.025)和2.54(p = 0.007)。通过对对数转换后的IgE值进行线性单倍型趋势回归,证实了该单倍型风险增加(p = 0.007)。分析还揭示了一种与特异性致敏相关的风险单倍型和一种与哮喘相关的风险单倍型。

结论

数据表明,STAT6内的基因变异对IgE调节及特应性疾病的表现有显著贡献。

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