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Coeliac disease-associated polymorphisms influence thymic gene expression

机译:腹腔疾病相关的多态性影响胸腺基因表达

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Significant associations between coeliac disease (CD) and single nucleotide polymorphisms (SNPs) distributed over 40 genetic regions have been established. The majority of these SNPs are non-coding and 20 SNPs were, by expression quantitative trait loci (eQTL) analysis, found to harbour cis regulatory potential in peripheral blood mononuclear cells (PBMC). Almost all regions contain genes with an immunological relevant function, of which many act in the same biological pathways. One such pathway is T-cell development in the thymus, a pathway previously not explored in CD pathogenesis. The aim of our study was to explore the regulatory potential of the CD-associated SNPs (n=50) by eQTL analysis in thymic tissue from 42 subjects. In total, 43 nominal significant (P<0.05) eQTLs were found within 24 CD-associated chromosomal regions, corresponding to 27 expression-altering SNPs (eSNPs) and 40 probes (eProbes) that represents 39 unique genes (eGenes). Nine significant probe-SNP pairs (corresponding to 8 eSNPs and 7 eGenes) overlapped with previous findings in PBMC (rs12727642-PARK7, rs296547-DDX59, rs917997-IL18RAP, rs842647-AHSA2, rs13003464-AHSA2, rs6974491-ELMO1, rs2074404-NSF (two independent probes) and rs2298428-UBE2L3). When compared across more tissues, we found that 14 eQTLs could represent potentially novel thymus-specific eQTLs. This implies that CD risk polymorphisms could affect gene regulation in thymus.
机译:腹腔疾病(CD)和分布在40个遗传区域中的单核苷酸多态性(SNP)之间已建立了重要的联系。这些SNP中的大多数是非编码的,通过表达定量性状位点(eQTL)分析,发现20个SNP在外周血单核细胞(PBMC)中具有顺式调节潜力。几乎所有区域都包含具有免疫相关功能的基因,其中许多在相同的生物途径中起作用。这样的途径之一是胸腺中的T细胞发育,这是CD发病机理中以前未曾探索过的途径。我们研究的目的是通过eQTL分析探索42位受试者胸腺组织中CD相关SNP(n = 50)的调节潜力。总共在24个CD相关染色体区域内发现了43个名义上显着(P <0.05)的eQTL,对应于27个表达改变SNP(eSNPs)和40个代表39个独特基因(eGenes)的探针。九个重要的探针SNP对(对应于8个eSNP和7个eGene)与先前在PBMC中的发现重叠(rs12727642-PARK7,rs296547-DDX59,rs917997-IL18RAP,rs842647-AHSA2,rs13003464-AHSA2,rs6974491-ELMO1,(rs2074404-NS两个独立的探针)和rs2298428-UBE2L3)。当在更多组织中进行比较时,我们发现14个eQTL可能代表潜在的新型胸腺特异性eQTL。这表明CD风险多态性可能影响胸腺的基因调控。

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