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首页> 外文期刊>Clinical and experimental allergy : >A polymorphism of MS4A2 (-109T>C) encoding the beta-chain of the high-affinity immunoglobulin E receptor (FcepsilonR1beta) is associated with a susceptibility to aspirin-intolerant asthma.
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A polymorphism of MS4A2 (-109T>C) encoding the beta-chain of the high-affinity immunoglobulin E receptor (FcepsilonR1beta) is associated with a susceptibility to aspirin-intolerant asthma.

机译:编码高亲和力免疫球蛋白E受体(FcepsilonR1beta)β链的MS4A2(-109T> C)多态性与阿司匹林耐受性哮喘相关。

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The MS4A2 gene, the beta chain of the high-affinity receptor for immunoglobulin (Ig)E, has previously been linked to atopy and asthma. The beta-chain of FcepsilonR1 enhances receptor maturation and signal transduction capacity, leading to the release of proinflammatory mediators and cytokines that can exacerbate the symptom of asthma. This study was performed to evaluate whether two genetic polymorphisms of the FcepsilonR1beta gene (FcepsilonR1beta-109T>C and FcepsilonR1beta E237G) are associated with aspirin-intolerant asthma (AIA). The MS4A2 gene polymorphisms (FcepsilonR1beta-109T>C and FcepsilonR1beta E237G) were determined by SNP-ITtrade mark assays in patients with AIA (N=164), aspirin-tolerant asthma (ATA, N=144) and normal controls (NC, N=264) recruited from a Korean population. The genotype frequencies of FcepsilonR1beta-109T>C and E237G polymorphisms were not significantly associated with the pathogenesis of AIA. However, FcepsilonR1beta-109T>C polymorphism was significantly associated with the presence of specific IgE to Staphylococcal enterotoxin B (SEB); the number of subjects carrying both homozygous TT genotype of FcepsilonR1beta-109T>C and specific IgE to SEB was significantly higher in the AIA group when compared with the other control groups (P=0.01, odds ratio (OR)=7.723, 95% confidence interval (CI)=1.327-39.860 for AIA vs. ATA; P=0.02, OR=6.364, 95% CI=1.149 approximately 35.229 for AIA vs. NC). In addition, luciferase reporter assays also showed that the FcepsilonR1beta-109T allele was associated with higher promoter activity of MS4A2 in both RBL-2H3 and A549 cell lines. FcepsilonR1beta-109T>C polymorphism may increase expression of MS4A2 by mast cells, leading to enhanced release of proinflammatory mediators in the asthmatic airway, contributing to increased susceptibility to AIA.
机译:MS4A2基因是免疫球蛋白(Ig)E的高亲和力受体的β链,以前与特应性疾病和哮喘有关。 FcepsilonR1的β链增强受体成熟度和信号转导能力,导致促炎性介质和细胞因子的释放,从而加剧哮喘的症状。进行这项研究以评估FcepsilonR1beta基因的两个遗传多态性(FcepsilonR1beta-109T> C和FcepsilonR1beta E237G)是否与阿司匹林耐受性哮喘(AIA)相关。通过SNP-IT商标测定法在AIA(N = 164),阿司匹林耐受性哮喘(ATA,N = 144)和正常对照(NC,N)中确定MS4A2基因多态性(FcepsilonR1beta-109T> C和FcepsilonR1beta E237G) = 264)从韩国人口中招募。 FcepsilonR1beta-109T> C和E237G多态性的基因型频率与AIA的发病机制没有显着相关。然而,FcepsilonR1beta-109T> C多态性与葡萄球菌肠毒素B(SEB)特异性IgE的存在显着相关。与其他对照组相比,AIA组中携带FcepsilonR1beta-109T> C的纯合TT基因型和SEB特异性IgE的受试者数量显着高于其他对照组(P = 0.01,优势比(OR)= 7.723,95%置信度AIA与ATA的区间(CI)= 1.327-39.860; AIA与NC的区间分别为P = 0.02,OR = 6.364、95%CI = 1.149和35.229)。此外,荧光素酶报告基因测定还显示,FcepsilonR1beta-109T等位基因与RBL-2H3和A549细胞系中MS4A2的较高启动子活性相关。 FcepsilonR1beta-109T> C多态性可能会增加肥大细胞MS4A2的表达,从而导致哮喘气道中促炎性介质的释放增加,从而导致对AIA的敏感性增加。

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