首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Linkage analysis of Dermatophagoides pteronyssinus-specific IgE responsiveness with polymorphic markers on chromosome 6p21 (HLA-D region) in Caucasian families by the transmission/disequilibrium test. Collaborative Study on the Genetics of Asthma (CS
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Linkage analysis of Dermatophagoides pteronyssinus-specific IgE responsiveness with polymorphic markers on chromosome 6p21 (HLA-D region) in Caucasian families by the transmission/disequilibrium test. Collaborative Study on the Genetics of Asthma (CS

机译:通过传播/不平衡测试,分析白种人家庭中6D21号染色体(HLA-D区)多态性标记与Dermatophagoides pteronyssinus特异性IgE反应性的联系。哮喘遗传学的合作研究

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BACKGROUND: Recently, we have obtained evidence for linkage between Der p 1-specific IgE antibodies and markers on chromosome 6p21 (HLA-D region) in a genome-wide screening in Caucasian families recruited as a part of the Collaborative Study on the Genetics of Asthma (CSGA). OBJECTIVE: Specific IgE antibodies toward different Dermatophagoides pteronyssinus (Der p) polypeptides were detected by immunoblotting analysis, and the transmission/disequilibrium test (TDT) was performed between specific IgE responsiveness toward each different Der p polypeptide and markers on chromosome 6p21 to better clarify the genetic contribution of HLA-D genes. METHODS: We studied 299 individuals in 45 Caucasian families participating in the CSGA. Serum samples from 137 individuals that showed elevated specific IgE antibodies toward the Der p crude allergen (> -0.5 log IU/mL) by ACCESS immunoassay were subjected to immunoblotting analysis. TDT was conducted between the presence of specific IgE antibodies toward each of 12 different Der p polypeptides and 4 polymorphic markers on chromosome 6p21. RESULTS: The 196-bp allele of D6S1281 and the 104-bp allele of DQCAR showed significant excess transmission to specific IgE responders toward a particular Der p polypeptide (120 kd, 55 kd, 45 kd, or 37 kd). In contrast, the 200-bp allele of D6S1281 and the 204-bp allele of D6S291 showed significantly decreased transmission to specific IgE responders toward a particular Der p polypeptide (120 kd, 90 kd, 52 kd, or 45 kd). Deviation from the expected 50% transmission in heterozygous parents was statistically significant after correcting for multiple comparisons. CONCLUSION: This study supported our previous findings that genes on chromosome 6p21 (HLA-D region) may influence the expression of Der p-specific IgE responsiveness in this Caucasian population. Our results, however, reveal the complexity of genetic regulations of Der p-specific IgE responsiveness by HLA-D genes, suggesting the strong influence of non-HLA loci and perhaps environmental factors for the development of Der p-specific IgE responsiveness.
机译:背景:最近,我们获得了证据,证明在白人家庭的全基因组筛查中,Der p 1特异性IgE抗体与6p21染色体(HLA-D区)上的标记之间存在连锁关系,该研究被招募为高加索人遗传学合作研究的一部分哮喘(CSGA)。目的:通过免疫印迹法检测针对不同的Dermatophagoides Pteronyssinus(Der p)多肽的特异性IgE抗体,并在针对每种不同的Der p多肽的特异性IgE反应性与6p21染色体上的标记之间进行传输/不平衡测试(TDT)。 HLA-D基因的遗传贡献。方法:我们研究了参加CSGA的45个白种人家庭中的299个人。通过ACCESS免疫测定对来自137位个体的血清样品进行了免疫印迹分析,这些样品显示出针对Der p粗致敏原的特异性IgE抗体升高(> -0.5 log IU / mL)。在针对12种不同Der p多肽中的每一种的特异性IgE抗体与6p21染色体上的4种多态性标记之间存在TDT。结果:D6S1281的196 bp等位基因和DQCAR的104 bp等位基因显示了对特定IgE应答者向特定Der p多肽(120 kd,55 kd,45 kd或37 kd)的显着过量传递。相比之下,D6S1281的200 bp等位基因和D6S291的204 bp等位基因显示了对特定IgE应答剂向特定Der p多肽(120 kd,90 kd,52 kd或45 kd)的传递显着降低。校正多个比较后,杂合父母体中预期的50%传播率的差异具有统计学意义。结论:这项研究支持我们先前的发现,即6p21染色体(HLA-D区)上的基因可能影响该白种人人群中Der p特异性IgE反应性的表达。然而,我们的结果揭示了HLA-D基因对Der p特异性IgE响应能力的遗传调控的复杂性,这表明非HLA基因座以及环境因素对Der p特异性IgE响应能力发展的强大影响。

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