在匈牙利克罗恩病患者中,NOD1基因E266K多态性与疾病易感性相关,但与疾病表型或NOD2/CARD15无关。
NOD1 gene E266K polymorphism is associated with disease susceptibility but not with disease phenotype or NOD2/CARD15 in Hungarian patients with Crohn's disease.
作者信息
Molnar T, Hofner P, Nagy F, Lakatos P L, Fischer S, Lakatos L, Kovacs A, Altorjay I, Papp M, Palatka K, Demeter P, Tulassay Z, Nyari T, Miheller P, Papp J, Mandi Y, Lonovics J
机构信息
1st Department of Medicine, University of Szeged, Faculty of Medicine, Szeged, Hungary.
出版信息
Dig Liver Dis. 2007 Dec;39(12):1064-70. doi: 10.1016/j.dld.2007.09.003. Epub 2007 Oct 26.
BACKGROUND
NOD1/CARD4, a member of the pattern-recognition receptor family, is a perfect candidate as a susceptibility gene for Crohn's disease. Since only limited and conflicting data are available on G796A polymorphisms in inflammatory bowel disease patients, we set out to study the effect of this polymorphism on the susceptibility and course of Crohn's disease in the Hungarian population.
METHODS
Four hundred thirty-four unrelated Crohn's disease patients (age at presentation: 28.6+/-9.6 years, female/male: 210/224, duration of Crohn's disease: 8.2+/-6.9 years) and 200 healthy subjects (blood donors) and 136 non-inflammatory bowel disease gastrointestinal controls with chronic gastritis were investigated. NOD1 G796A was detected by using polymerase chain reaction/restriction fragment length polymorphism. Detailed clinical phenotypes were determined by reviewing the medical charts.
RESULTS
The frequencies of the variant alleles of NOD1 G796A differed significantly between the Crohn's disease patients and both healthy (GG 49.5% vs. 67%; AG 41.5% vs. 28%; and AA 9.0% vs. 5.2%; p<0.0001) and non-inflammatory bowel disease controls with chronic gastritis. Carriage of the single nucleotide polymorphism of NOD1 G796A proved to be a highly significant risk factor for Crohn's disease compared to both healthy (p<0.0001, OR: 2.1, 95% CI: 1.5-2.9) and non-inflammatory bowel disease controls with chronic gastritis (p=0.008). Significant associations were not found between the different genotypes and the demographic data on the patients or the clinical characteristics of Crohn's disease. The different polymorphisms of pattern-recognition receptors (e.g. NOD2/CARD15 SNP8, SNP12 and SNP13 mutations, the TLR4 D299G polymorphism and NOD1 G796A) did not reveal a mutual basis.
CONCLUSIONS
Our results suggest that carriage of the NOD1 G796A mutation increases susceptibility for Crohn's disease in the Hungarian population.
背景
模式识别受体家族成员NOD1/CARD4是克罗恩病易感性基因的理想候选者。由于关于炎症性肠病患者中G796A多态性的数据有限且相互矛盾,我们着手研究该多态性对匈牙利人群中克罗恩病易感性和病程的影响。
方法
对434例无血缘关系的克罗恩病患者(就诊时年龄:28.6±9.6岁,女性/男性:210/224,克罗恩病病程:8.2±6.9年)、200例健康受试者(献血者)以及136例患有慢性胃炎的非炎症性肠病胃肠道对照进行了研究。采用聚合酶链反应/限制性片段长度多态性方法检测NOD1 G796A。通过查阅病历确定详细的临床表型。
结果
NOD1 G796A变异等位基因的频率在克罗恩病患者与健康人群(GG 49.5%对67%;AG 41.5%对28%;AA 9.0%对5.2%;p<0.0001)以及患有慢性胃炎的非炎症性肠病对照之间存在显著差异。与健康人群(p<0.0001,OR:2.1,95%CI:1.5 - 2.9)和患有慢性胃炎的非炎症性肠病对照(p = 0.008)相比,NOD1 G796A单核苷酸多态性的携带被证明是克罗恩病的一个高度显著的危险因素。在不同基因型与患者的人口统计学数据或克罗恩病的临床特征之间未发现显著关联。模式识别受体的不同多态性(如NOD2/CARD15 SNP8、SNP12和SNP13突变、TLR4 D299G多态性以及NOD1 G796A)未显示出共同基础。
结论
我们的结果表明,NOD1 G796A突变的携带增加了匈牙利人群中克罗恩病的易感性。
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