INSERM, U946, Paris, France.
Eur J Hum Genet. 2010 Jun;18(6):700-6. doi: 10.1038/ejhg.2009.224. Epub 2010 Jan 13.
Asthma is caused by a heterogeneous combination of environmental and genetic factors. In the context of GA2LEN (Global Allergy and Asthma European Network), we carried out meta-analyses of almost all genome-wide linkage screens conducted to date in 20 independent populations from different ethnic origins (>or=3024 families with >or=10 027 subjects) for asthma, atopic asthma, bronchial hyper-responsiveness and five atopy-related traits (total immunoglobulin E level, positive skin test response (SPT) to at least one allergen or to House Dust Mite, quantitative score of SPT (SPTQ) and eosinophils (EOS)). We used the genome scan meta-analysis method to assess evidence for linkage within bins of traditionally 30-cM width, and explored the manner in which these results were affected by bin definition. Meta-analyses were conducted in all studies and repeated in families of European ancestry. Genome-wide evidence for linkage was detected for asthma in two regions (2p21-p14 and 6p21) in European families ascertained through two asthmatic sibs. With regard to atopy phenotypes, four regions reached genome-wide significance: 3p25.3-q24 in all families for SPT and three other regions in European families (2q32-q34 for EOS, 5q23-q33 for SPTQ and 17q12-q24 for SPT). Tests of heterogeneity showed consistent evidence of linkage of SPTQ to 3p11-3q21, whereas between-study heterogeneity was detected for asthma in 2p22-p13 and 6p21, and for atopic asthma in 1q23-q25. This large-scale meta-analysis provides an important resource of information that can be used to prioritize further fine-mapping studies and also be integrated with genome-wide association studies to increase power and better interpret the outcomes of these studies.
哮喘是由环境和遗传因素的异质组合引起的。在 GA2LEN(全球过敏和哮喘欧洲网络)的背景下,我们对来自不同种族起源的 20 个独立群体进行的几乎所有全基因组连锁扫描进行了荟萃分析(>或=3024 个家庭,每个家庭>或=10027 名受试者),这些群体的研究对象为哮喘、特应性哮喘、支气管高反应性和五个特应性相关特征(总免疫球蛋白 E 水平、对至少一种过敏原或屋尘螨的阳性皮肤试验反应(SPT)、SPT 的定量评分(SPTQ)和嗜酸性粒细胞(EOS))。我们使用基因组扫描荟萃分析方法评估了在传统 30-cM 宽度的范围内进行连锁的证据,并探索了这种结果受 bin 定义影响的方式。在所有研究中进行了荟萃分析,并在欧洲血统的家族中重复进行了荟萃分析。在通过两个哮喘同胞确定的欧洲家族中,哮喘的两个区域(2p21-p14 和 6p21)检测到全基因组连锁证据。关于特应性表型,四个区域达到了全基因组显著性:所有家族的 3p25.3-q24 区域的 SPT 和欧洲家族的另外三个区域(2q32-q34 区域的 EOS、5q23-q33 区域的 SPTQ 和 17q12-q24 区域的 SPT)。异质性检验显示,3p11-3q21 与 SPTQ 的连锁具有一致性证据,而在 2p22-p13 和 6p21 区域检测到哮喘之间的异质性,在 1q23-q25 区域检测到特应性哮喘之间的异质性。这项大规模的荟萃分析提供了一个重要的信息资源,可以用于优先进行进一步的精细映射研究,也可以与全基因组关联研究相结合,以提高功率并更好地解释这些研究的结果。