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首页> 外文期刊>Frontiers in Endocrinology >Dissecting the Genetic Susceptibility to Graves’ Disease in a Cohort of Patients of Italian Origin
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Dissecting the Genetic Susceptibility to Graves’ Disease in a Cohort of Patients of Italian Origin

机译:剖析一批意大利裔患者对Graves病的遗传易感性

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Graves’ disease (GD) is an autoimmune oligogenic disorder with a strong hereditary component. Several GD susceptibility genes have been identified and confirmed during the last two decades. However, there are very few studies that evaluated susceptibility genes for GD in specific geographic subsets. Previously, we mapped a new locus on chromosome 3q that was unique to GD families of Italian origin. In the present study, we used association analysis of single-nucleotide polymorphism (SNPs) at the 3q locus in a cohort of GD patients of Italian origin in order to prioritize the best candidates among the known genes in this locus to choose the one(s) best supported by the association. DNA samples were genotyped using the Illumina GoldenGate genotyping assay analyzing 690 SNP in the linked 3q locus covering all 124 linkage disequilibrium blocks in this locus. Candidate non-HLA (human-leukocyte-antigen) genes previously reported to be associated with GD and/or other autoimmune disorders were analyzed separately. Three SNPs in the 3q locus showed a nominal association ( p ?
机译:格雷夫斯病(GD)是一种自身免疫性寡聚性疾病,具有很强的遗传成分。在过去的二十年中,已经鉴定并证实了几种GD敏感性基因。但是,很少有研究评估特定地理亚组中GD的易感基因。以前,我们在3q号染色体上绘制了一个新位点,该位点是意大利起源的GD家族独有的。在本研究中,我们对来自意大利的GD患者队列中的3q位点的单核苷酸多态性(SNP)进行关联分析,以便在该位点的已知基因中优先选择最佳候选者,以选择一个)得到协会的最佳支持。使用Illumina GoldenGate基因分型分析法对DNA样本进行基因分型,分析连接的3q基因座中的690个SNP,覆盖该基因座中的所有124个连锁不平衡区。先前报告与GD和/或其他自身免疫性疾病相关的候选非HLA(人类白细胞抗原)基因被单独分析。 3q基因座中的三个SNP显示出标称关联(p <0.05)(rs13097181,rs763313和rs6792646)。尽管无法通过多重比较校正进一步验证这些基因,但我们在已知具有GD相关基因的基因座上优先考虑候选基因,而不是进行假设检验。此外,我们发现与促甲状腺激素受体(TSHR)基因,细胞毒性T淋巴细胞抗原4(CTLA-4)基因和甲状腺球蛋白(TG)基因之间存在显着关联。总之,我们在3q染色体上鉴定了三个SNP,这些SNP可能在该区域映射了一个新的GD易感基因,这对意大利人来说是唯一的。此外,我们证实了TSHR,CTLA-4和TG基因在意大利人中与GD相关。我们的发现强调了种族和地理差异对GD遗传易感性的影响。

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