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Resequencing of positional candidates identifies low frequency IL23R coding variants protecting against inflammatory bowel disease
Authors:Momozawa Yukihide  Mni Myriam  Nakamura Kayo  Coppieters Wouter  Almer Sven  Amininejad Leila  Cleynen Isabelle  Colombel Jean-Frédéric  de Rijk Peter  Dewit Olivier  Finkel Yigael  Gassull Miquel A  Goossens Dirk  Laukens Debby  Lémann Marc  Libioulle Cécile  O'Morain Colm  Reenaers Catherine  Rutgeerts Paul  Tysk Curt  Zelenika Diana  Lathrop Mark  Del-Favero Jurgen  Hugot Jean-Pierre  de Vos Martine  Franchimont Denis  Vermeire Severine  Louis Edouard  Georges Michel
Institution:Unit of Animal Genomics, Groupe Interdisciplinaire de Génoprotéomique Appliquée (GIGA-R) and Faculty of Veterinary Medicine, University of Liège (B34), Liège, Belgium.
Abstract:Genome-wide association studies (GWAS) have identified dozens of risk loci for many complex disorders, including Crohn's disease. However, common disease-associated SNPs explain at most ~20% of the genetic variance for Crohn's disease. Several factors may account for this unexplained heritability, including rare risk variants not adequately tagged thus far in GWAS. That rare susceptibility variants indeed contribute to variation in multifactorial phenotypes has been demonstrated for colorectal cancer, plasma high-density lipoprotein cholesterol levels, blood pressure, type 1 diabetes, hypertriglyceridemia and, in the case of Crohn's disease, for NOD2 (refs. 14,15). Here we describe the use of high-throughput resequencing of DNA pools to search for rare coding variants influencing susceptibility to Crohn's disease in 63 GWAS-identified positional candidate genes. We identify low frequency coding variants conferring protection against inflammatory bowel disease in IL23R, but we conclude that rare coding variants in positional candidates do not make a large contribution to inherited predisposition to Crohn's disease.
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