Myosin IXB variant increases the risk of celiac disease and points toward a primary intestinal barrier defect |
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| Authors: | Monsuur Alienke J de Bakker Paul I W Alizadeh Behrooz Z Zhernakova Alexandra Bevova Marianna R Strengman Eric Franke Lude van't Slot Ruben van Belzen Martine J Lavrijsen Ineke C M Diosdado Begoña Daly Mark J Mulder Chris J J Mearin M Luisa Meijer Jos W R Meijer Gerrit A van Oort Erica Wapenaar Martin C Koeleman Bobby P C Wijmenga Cisca |
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| Affiliation: | Complex Genetics Section, DBG-Department of Medical Genetics, University Medical Center Utrecht, Universiteitsweg 100, 3584 CG Utrecht, the Netherlands. |
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| Abstract: | Celiac disease is probably the best-understood immune-related disorder. The disease presents in the small intestine and results from the interplay between multiple genes and gluten, the triggering environmental factor. Although HLA class II genes explain 40% of the heritable risk, non-HLA genes accounting for most of the familial clustering have not yet been identified. Here we report significant and replicable association (P = 2.1 x 10(-6)) to a common variant located in intron 28 of the gene myosin IXB (MYO9B), which encodes an unconventional myosin molecule that has a role in actin remodeling of epithelial enterocytes. Individuals homozygous with respect to the at-risk allele have a 2.3-times higher risk of celiac disease (P = 1.55 x 10(-5)). This result is suggestive of a primary impairment of the intestinal barrier in the etiology of celiac disease, which may explain why immunogenic gluten peptides are able to pass through the epithelial barrier. |
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