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The R30Q DLG5 variant is not associated with celiac disease or inflammatory bowel disease in the Spanish population.

机译:R30Q DLG5变体与西班牙人群的乳糜泻或炎症性肠病无关。

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摘要

Alterations in intestinal epithelial permeability could underlie inflammatory bowel disease (IBD) and celiac disease (CeD) etiology, as supported by previous association studies. One related gene, DLG5 [discs, large homologue 5 (Drosophila)], has been associated with IBD in several populations and with CeD in the Dutch population. We tried to confirm the involvement of DLG5 in CeD performing a case-control study (725 CeD patients and 803 controls) by analysing the R30Q variant (rs1248696). Genetic frequencies did not significantly differ between groups (P > 0.80) and the meta-analysis with the Dutch data did not show any association. Additionally, we evaluated the effect of R30Q in IBD risk (858 patients), as discordant results were previously obtained. No association was detected. Our study does not support the effect of the R30Q DLG5 variant in CeD or IBD predisposition in the Spanish population.
机译:如先前的关联研究所支持,肠上皮通透性的改变可能是炎症性肠病(IBD)和腹腔疾病(CeD)病因的基础。一种相关基因DLG5 [discs,大同系物5(Drosophila)],在几个人群中与IBD相关,在荷兰人群中与CeD相关。我们试图通过分析R30Q变异体(rs1248696)来确认DLG5是否参与了CeD的病例对照研究(725名CeD患者和803名对照)。两组之间的遗传频率没有显着差异(P> 0.80),并且基于荷兰数据的荟萃分析未显示任何相关性。另外,由于先前获得了不一致的结果,我们评估了R30Q对IBD风险的影响(858例患者)。未检测到关联。我们的研究不支持R30Q DLG5变体对西班牙人群中CeD或IBD易感性的影响。

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