芬兰和匈牙利人群染色体5q31-q33上CELIAC2位点的精细定位。

L L E Koskinen, E Einarsdottir, I R Korponay-Szabo, K Kurppa, K Kaukinen, P Sistonen, Z Pocsai, G Széles, R Adány, M Mäki, J Kere, P Saavalainen
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引用次数: 15

摘要

乳糜泻是小肠的一种慢性炎症,在遗传易感的个体中由于摄入饮食中的麸质而引起。乳糜泻的唯一确认和功能特征的遗传危险因素是主要组织相容性复合体(MHC) II类位点(CELIAC1)上的DQ2或DQ8异源二聚体。这些基因对疾病的发生是必要的,但单独是不够的。全基因组连锁扫描提示染色体5q31-q33 (CELIAC2)是乳糜泻的重要危险位点。该区域也与其他炎症性疾病有关,尽管目前还没有发现明确的基因关联。在目前的研究中,在匈牙利人群中筛选了11个乳糜泻候选基因座进行遗传连锁。由于CELIAC2位点显示出最强的连锁证据,因此选择该位点进行随访。从CELIAC2位点中选择了17个候选基因,并使用芬兰和匈牙利大家族材料中的48个单倍型标记单核苷酸多态性(snp)进行基因分型。其中的一个子集,在15个基因中标记了40个snp,在芬兰和匈牙利的一组独立病例和对照中进行了基因分型。我们证实了该地区与乳糜泻的联系,并报告了芬兰和匈牙利人群的强烈联系。关联分析显示,整个地区存在适度关联。这些关联发现在病例对照数据集中没有得到重复。我们的研究强烈支持CELIAC2基因座在乳糜泻中的作用,但它也强调需要在该区域进行更强大的研究设计,以定位真正的疾病风险变异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Fine mapping of the CELIAC2 locus on chromosome 5q31-q33 in the Finnish and Hungarian populations.

Celiac disease is a chronic inflammation of the small intestine, arising in genetically predisposed individuals as a result of ingestion of dietary gluten. The only confirmed and functionally characterised genetic risk factors for celiac disease are the DQ2 or DQ8 heterodimers at the major histocompatibility complex (MHC) class II locus (CELIAC1). These genes are necessary but alone not sufficient for disease onset. Genome-wide linkage scans have suggested chromosome 5q31-q33 (CELIAC2) as an important risk locus for celiac disease. This region has also been associated to other inflammatory disorders, although as yet, no clear gene associations have been found. In the current study, 11 celiac disease candidate loci were screened for genetic linkage in the Hungarian population. As the CELIAC2 locus showed the strongest evidence for linkage, this locus was selected for follow-up. Seventeen candidate genes were selected from the CELIAC2 locus, and genotyped using 48 haplotype tagging single nucleotide polymorphisms (SNPs) in large Finnish and Hungarian family materials. A subset of these, 40 tagging SNPs in 15 genes, were genotyped in an independent set of Finnish and Hungarian cases and controls. We confirmed linkage of this region with celiac disease and report strong linkage in both the Finnish and Hungarian populations. The association analysis showed modest associations throughout the whole region. These association findings were not replicated in the case-control datasets. Our study strongly supports the role of the CELIAC2 locus in celiac disease, but it also highlights the need for a more powerful study design in the region, to locate the true disease risk variants.

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Tissue antigens
Tissue antigens 医学-病理学
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