DeMeo D L, Lange C, Silverman E K, Senter J M, Drazen J M, Barth M J, Laird N, Weiss S T
Channing Laboratory, Brigham and Women's Hospital, Boston, Massachusetts 02115, USA.
Genet Epidemiol. 2002 Nov;23(4):335-48. doi: 10.1002/gepi.10182.
Interleukin 13 (IL-13) has been demonstrated to have a crucial role in animal models of allergy and asthma. In human case-control genetic-association studies, the Arg130Gln polymorphism has been associated with elevated total serum IgE and an asthma diagnosis in atopic and nonatopic individuals (Graves et al. [2000] J. Allergy Clin. Immunol. 105:506-513; Heinzmann et al. [2000] Hum. Mol. Genet. 9:549-559). To apply family-based association methods, we obtained DNA samples from 685 asthmatic children from 640 sibships and their parents in the Childhood Asthma Management Program (CAMP). Six hundred and sixty-six asthmatic children had complete phenotypic information and were used for this analysis. We performed quantitative association analysis using the transmission disequilibrium test (TDT) on 22 individual phenotypes and 5 grouped phenotypes relating to allergy, airway responsiveness, pulmonary function, bronchodilator responsiveness, and asthma severity, using genotypes at the Arg130Gln polymorphism of the IL-13 gene. A positive association was obtained between Arg130Gln and a grouped phenotype of allergy (consisting of the individual phenotypes of eosinophils, IgE, and positive skin tests), using FBAT-GEE, a multivariate extension of the family-based association test (Lange et al. [2002] Biostatistics 1:1-15). The three phenotypes were then evaluated individually and revealed a significant association between total eosinophil count and the Arg130Gln locus; there was a trend for association between total IgE and the Arg130Gln polymorphism. The Arg130Gln polymorphism is associated with an elevated eosinophil count as well as with a grouped allergy phenotype, in children with mild to moderate asthma. No evidence for association was found between Arg130Gln and airway responsiveness, asthma diagnosis, or asthma severity.
白细胞介素13(IL - 13)已被证明在过敏和哮喘的动物模型中起关键作用。在人类病例对照基因关联研究中,Arg130Gln多态性与特应性和非特应性个体的血清总IgE升高及哮喘诊断相关(Graves等人[2000年]《变态反应与临床免疫学杂志》105:506 - 513;Heinzmann等人[2000年]《人类分子遗传学》9:549 - 559)。为了应用基于家系的关联方法,我们从儿童哮喘管理项目(CAMP)中640个同胞对的685名哮喘儿童及其父母那里获取了DNA样本。666名哮喘儿童有完整的表型信息并用于该分析。我们使用IL - 13基因Arg130Gln多态性的基因型,对22种个体表型和5种与过敏、气道反应性、肺功能、支气管扩张剂反应性及哮喘严重程度相关的分组表型进行传递不平衡检验(TDT),进行定量关联分析。使用基于家系关联检验的多变量扩展方法FBAT - GEE(Lange等人[2002年]《生物统计学》1:1 - 15),在Arg130Gln与一种过敏分组表型(由嗜酸性粒细胞、IgE和阳性皮肤试验的个体表型组成)之间获得了正相关。然后分别评估这三种表型,发现嗜酸性粒细胞总数与Arg130Gln位点之间存在显著关联;总IgE与Arg130Gln多态性之间存在关联趋势。在轻度至中度哮喘儿童中,Arg130Gln多态性与嗜酸性粒细胞计数升高以及过敏分组表型相关。未发现Arg130Gln与气道反应性、哮喘诊断或哮喘严重程度之间存在关联证据。