Association of celiac disease genes with inflammatory bowel disease in Finnish and Swedish patients

被引:0
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作者
A S Parmar
M Lappalainen
P Paavola-Sakki
L Halme
M Färkkilä
U Turunen
K Kontula
A Aromaa
V Salomaa
L Peltonen
J Halfvarson
L Törkvist
M D'Amato
P Saavalainen
E Einarsdottir
机构
[1] Research Program for Molecular Medicine,Department of Medical Genetics
[2] University of Helsinki,Department of Medicine
[3] Haartman Institute,Department of Gastroenterology
[4] Biomedicum Helsinki,Department of Surgery
[5] University of Helsinki,Department of Medicine
[6] Helsinki University Hospital,Department of Clinical Science
[7] Helsinki University Hospital,Department of Biosciences and Nutrition
[8] Helsinki University Hospital,undefined
[9] National Institute for Health and Welfare,undefined
[10] Institute for Molecular Medicine Finland,undefined
[11] Wellcome Trust Sanger Institute,undefined
[12] School of Health and Medical Sciences,undefined
[13] Örebro University,undefined
[14] Intervention and Technology,undefined
[15] Karolinska Institutet,undefined
[16] Karolinska Institutet,undefined
来源
Genes & Immunity | 2012年 / 13卷
关键词
celiac disease; Crohn's disease; ulcerative colitis; association;
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摘要
Some genetic loci may affect susceptibility to multiple immune system-related diseases. In the current study, we investigated whether the known susceptibility loci for celiac disease (CelD) also associate with Crohn's disease (CD) and/or ulcerative colitis (UC), the two main forms of inflammatory bowel disease (IBD), in Finnish patients. A total of 45 genetic markers were genotyped in a Finnish data set comprising 699 IBD patients and 2482 controls. Single-marker association with IBD and its subphenotypes was tested. A meta-analysis with a Swedish UC data set was also performed. A total of 12 single-nucleotide polymorphisms associated with CD and/or UC (P<0.05). In the subphenotype analysis, rs6974491-ELMO1 (P=0.0002, odds ratio (OR): 2.20) and rs2298428-UBE2L3 (P=5.44 × 10−5, OR: 2.59) associated with pediatric UC and CD, respectively. In the meta-analysis, rs4819388-ICOSLG (P=0.00042, OR: 0.79) associated with UC. In the subphenotype meta-analysis, rs1738074-TAGAP (P=7.40 × 10−5, OR: 0.61), rs6974491-ELMO1 (P=0.00052, OR: 1.73) and rs4819388-ICOSLG (P=0.00019, OR: 0.75) associated with familial UC, pediatric UC and sporadic UC, respectively. Multiple CelD risk loci also confer susceptibility for CD and/or UC in the Finnish and Swedish populations. Certain genetic risk variants may furthermore predispose an individual for developing a particular disease phenotype.
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页码:474 / 480
页数:6
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