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首页> 外文期刊>Inflammatory bowel diseases >Association of polymorphisms in the interleukin-18 gene in patients with Crohn's disease depending on the CARD15/NOD2 genotype.
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Association of polymorphisms in the interleukin-18 gene in patients with Crohn's disease depending on the CARD15/NOD2 genotype.

机译:克罗恩病患者白介素18基因多态性的相关性取决于CARD15 / NOD2基因型。

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摘要

An increased expression of interleukin-18 (IL-18), a proinflammatory cytokine inducing interferon-gamma, has been found in Crohn's disease (CD). In the IL-18 gene, several partly functional relevant polymorphisms are known. This study sought to investigate associations of IL-18 polymorphisms in inflammatory bowel disease and CD according to CARD15/NOD2 mutation status and clinical phenotypes. METHODS: The IL-18 polymorphisms -607, -137, and the third position of codon 35 (c35/3) were genotyped in 210 patients with CD, 140 patients with ulcerative colitis, and 265 healthy controls using polymerase chain reaction and restriction fragment length polymorphism analysis. RESULTS: Frequencies of alleles and genotypes of the 3 polymorphisms and of the respective haplotypes and diplotypes displayed no significant differences between the whole groups of patients with CD and ulcerative colitis, respectively, compared with the controls. After stratification of patients with CD for CARD15/NOD2 status, significant associations of genotypes -137 CC (P = 0.018) and c35/3 CC (P = 0.010) and of the diplotype 2-2 (P = 0.018) were found in cases carrying CARD15/NOD2 mutations. Associations of genotypes -137 GG (P = 0.015) and c35/3 AA (P = 0.030) with colonic disease only in cases positive for CARD15/NOD2 mutations and of the genotype -607 AA (P = 0.007) with fistulas in cases negative for CARD15/NOD2 mutations were observed. CONCLUSIONS: In this study, significant differences of several genotypes and diplotypes within the IL-18 gene in CD depending on CARD15/NOD2 status have been found. In context with an increased expression of IL-18 in CD, it remains to be shown whether the expression of IL-18 is influenced by CARD15/NOD2 mutation status.
机译:已经在克罗恩病(CD)中发现了白细胞介素18(IL-18)(一种促炎细胞因子诱导的干扰素-γ)表达的增加。在IL-18基因中,已知几种部分功能相关的多态性。这项研究试图根据CARD15 / NOD2突变状态和临床表型研究炎症性肠病和CD中IL-18多态性的关联。方法:采用聚合酶链反应和限制性酶切片段技术对210例CD患者,140例溃​​疡性结肠炎患者和265例健康对照者的IL-18基因多态性-607,-137和第35位密码子(c35 / 3)进行基因分型。长度多态性分析。结果:3种多态性的等位基因和基因型的频率以及相应的单倍型和双倍型的频率与对照组相比,在整个CD和溃疡性结肠炎患者组中均无显着差异。在对CD患者进行CARD15 / NOD2状态分层后,发现病例中基因型-137 CC(P = 0.018)和c35 / 3 CC(P = 0.010)与双倍型2-2(P = 0.018)有显着关联。携带CARD15 / NOD2突变。基因型-137 GG(P = 0.015)和c35 / 3 AA(P = 0.030)仅在CARD15 / NOD2突变阳性的情况下与结肠疾病相关,基因型-607 AA(P = 0.007)在阴性的情况下与瘘管相关观察到CARD15 / NOD2突变。结论:在这项研究中,发现CD中IL-18基因内的几种基因型和双型显着不同,这取决于CARD15 / NOD2的状态。在CD中IL-18的表达增加的情况下,IL-18的表达是否受CARD15 / NOD2突变状态的影响尚待证实。

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