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首页> 外文期刊>Human Molecular Genetics >Association of Eotaxin gene family with asthma and serum total IgE.
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Association of Eotaxin gene family with asthma and serum total IgE.

机译:趋化因子基因家族与哮喘和血清总IgE的关系。

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The Eotaxin gene family (Eotaxin1, Eotaxin2 and Eotaxin3) recruits and activates CCR3-bearing cells such as eosinophils, mast cells and Th2 lymphocytes that play a major role in allergic disorders. To date, the effect of polymorphisms of Eotaxin genes on asthma phenotypes has not been thoroughly examined. In our research, we sequenced whole regions of the Eotaxin gene family to identify polymorphisms, which may be involved in the development of asthma and total serum IgE. We have identified 37 SNPs in the Exotaxin gene family (Exotaxin1, 2 and 3), and 17 common polymorphic sites were selected for genotyping in our asthma cohort (n=721). Statistical analysis revealed that the EOT2+1265A>G G* allele showed significantly lower frequency in asthmatics than in normal healthy controls (0.14 versus 0.23, P=0.002), and that distribution of the EOT2+1265A>G G* allele-containing genotypes was also much lower in asthmatics (26.3 versus 40.8%, P=0.003). In addition, a non-synonymous SNP in Eotaxin1, EOT1+123Ala>Thr showed significant association with total serum IgE levels (P=0.002-0.02). The effect of EOT1+123Ala>Thr on total serum IgE appeared in a gene-dose-dependent manner. Our findings suggest that the development of asthma may be associated with EOT2+1265A>G polymorphisms, and the susceptibility to high IgE production may be attributed to the EOT1+123Ala>Thr polymorphism. Eotaxin variation/haplotype information identified in this study might provide valuable insights into strategies for the control of asthma.
机译:Eotaxin基因家族(Eotaxin1,Eotaxin2和Eotaxin3)募集并激活带有CCR3的细胞,如嗜酸性粒细胞,肥大细胞和Th2淋巴细胞,它们在过敏性疾病中起主要作用。迄今为止,尚未全面研究嗜酸细胞活化趋化因子基因多态性对哮喘表型的影响。在我们的研究中,我们对嗜酸细胞活化趋化因子基因家族的整个区域进行了测序,以鉴定多态性,这可能与哮喘的发生和血清总IgE的发生有关。我们已经确定了Exotaxin基因家族中的37个SNP(Exotaxin1、2和3),并选择了17个常见的多态性位点用于我们的哮喘队列的基因分型(n = 721)。统计分析显示,哮喘患者中EOT2 + 1265A> GG *等位基因的频率显着低于正常健康对照组(0.14比0.23,P = 0.002),并且EOT2 + 1265A> GG *等位基因的基因型分布也很正常。哮喘患者的发病率要低得多(26.3比40.8%,P = 0.003)。此外,Eotaxin1,EOT1 + 123Ala> Thr中的一个非同义SNP与总血清IgE水平显着相关(P = 0.002-0.02)。 EOT1 + 123Ala> Thr对总血清IgE的影响以基因剂量依赖性的方式出现。我们的发现表明哮喘的发展可能与EOT2 + 1265A> G多态性有关,对高IgE产生的敏感性可能归因于EOT1 + 123Ala> Thr多态性。在这项研究中鉴定的嗜酸性粒细胞趋化因子/单倍型信息可能为哮喘控制策略提供有价值的见解。

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