克罗恩病(CD)中肿瘤坏死因子(TNF)基因多态性:对疾病行为的影响?
Tumour necrosis factor (TNF) gene polymorphism in Crohn's disease (CD): influence on disease behaviour?
作者信息
Louis E, Peeters M, Franchimont D, Seidel L, Fontaine F, Demolin G, Croes F, Dupont P, Davin L, Omri S, Rutgeerts P, Belaiche J
机构信息
Department of Gastroenterology, University Hospital of Liège, Belgium.
出版信息
Clin Exp Immunol. 2000 Jan;119(1):64-8. doi: 10.1046/j.1365-2249.2000.01106.x.
Crohn's disease (CD) is a multifactorial disease with genetic heterogeneity. TNF-alpha plays a key role in the development of the mucosal lesions. The aim of our work was to study a single base pair polymorphism located in the promoter region of TNF gene, in a large population of CD patients with well defined phenotypes. One hundred and ninety-three patients with CD and 98 ethnically matched controls were studied. The -308 single base pair polymorphism of TNF gene was studied using an allele-specific polymerase chain reaction. Genotype and allelic frequencies were compared between patients and controls and between subgroups of patients defined by sex, age at diagnosis, familial history, location of disease, type of disease, extra-intestinal manifestations, and response to steroid treatment. In 29 patients a measure of TNF-alpha production by colonic biopsies was performed. The frequency of the allele TNF2 as well as the proportion of carriers of the allele TNF2 were slightly but not significantly lower in CD than in controls (11.9% versus 14.8% and 21.5% versus 27.6%, respectively). A more prominent difference in frequencies of allele TNF2 and in proportions of TNF2 carriers was found when comparing subgroups of patients. The frequency of allele TNF2 was significantly higher in steroid-dependent than in non-steroid-dependent disease (28.1% versus 10.3%; Delta = 17.8%, 95% confidence interval (CI) = 6.3-29.5%, P = 0.0027) and tended to be higher in colonic than in small bowel disease and in fistulizing than in stricturing disease. Furthermore, TNF2 carriers tended to be more frequent in patients with steroid-dependent than non-steroid-dependent disease (43.8% versus 19.3%; Delta = 24.5%, 95% CI = 3.6-45.4%, P = 0.022), in patients with fistulizing than stricturing disease (26.5% versus 9.6%; Delta = 16.9%, 95% CI = 1. 1-32.6%, P = 0.036), and in patients with colonic than small bowel disease (26.5% versus 11.1%; Delta = 15.4%, 95% CI = -0.8-31.6%, P = 0.063). Finally, patients carrying at least one copy of allele 2 were found to produce slightly more TNF-alpha at the colonic level. The -308 TNF gene polymorphism may have a slight influence on the behaviour of CD. The carriage of allele 2 may favour steroid-dependent disease and to a lesser extent fistulizing and colonic disease, possibly secondary to a more intense TNF-alpha-driven inflammatory reaction at the mucosal level.
克罗恩病(CD)是一种具有遗传异质性的多因素疾病。肿瘤坏死因子-α(TNF-α)在黏膜病变的发生发展中起关键作用。我们研究的目的是在一大群具有明确表型的CD患者中,研究位于TNF基因启动子区域的单碱基对多态性。研究了193例CD患者和98例种族匹配的对照。采用等位基因特异性聚合酶链反应研究TNF基因的-308单碱基对多态性。比较了患者与对照之间以及按性别、诊断时年龄、家族史、疾病部位、疾病类型、肠外表现和对类固醇治疗反应定义的患者亚组之间的基因型和等位基因频率。对29例患者进行了结肠活检中TNF-α产生量的测定。CD患者中TNF2等位基因的频率以及TNF2等位基因携带者的比例略低于对照,但差异无统计学意义(分别为11.9%对14.8%和21.5%对27.6%)。比较患者亚组时,发现TNF2等位基因频率和TNF2携带者比例存在更显著差异。依赖类固醇的疾病中TNF2等位基因频率显著高于非依赖类固醇的疾病(28.1%对10.3%;差值=17.8%,95%置信区间(CI)=6.3-29.5%,P=0.0027),结肠疾病中TNF2等位基因频率倾向于高于小肠疾病,瘘管形成性疾病中TNF2等位基因频率倾向于高于狭窄性疾病。此外,依赖类固醇的疾病患者中TNF2携带者往往比非依赖类固醇的疾病患者更常见(43.8%对19.3%;差值=24.5%,95%CI=3.6-45.4%,P=0.022),瘘管形成性疾病患者中TNF2携带者比狭窄性疾病患者更常见(26.5%对9.6%;差值=16.9%,95%CI=1.1-32.6%,P=0.036),结肠疾病患者中TNF2携带者比小肠疾病患者更常见(26.5%对11.1%;差值=15.4%,95%CI=-0.8-31.6%,P=0.063)。最后,发现携带至少一个2等位基因拷贝的患者在结肠水平产生的TNF-α略多。-308 TNF基因多态性可能对CD的病情有轻微影响。2等位基因的携带可能有利于依赖类固醇的疾病,在较小程度上有利于瘘管形成性和结肠疾病,这可能继发于黏膜水平更强烈的TNF-α驱动的炎症反应。
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