Sýkora Josef, Subrt Ivan, Dìdek Petr, Siala Konrad, Schwarz Jan, Machalová Veronika, Varvarovská Jana, Pazdiora Petr, Pozler Oldrich, Stozický Frantisek
Department of Pediatrics, Charles University Hospital, Division of Gastroenterology, Pilsen, Czech Republic.
J Pediatr Gastroenterol Nutr. 2006 May;42(5):479-87. doi: 10.1097/01.mpg.0000221917.80887.9e.
Our pilot study aimed to determine the effect of tumor necrosis factor-alpha (TNF-alpha) 308 G-->A promoter single-nucleotide polymorphism in pediatric inflammatory bowel disease (IBD), its influence on inflammatory activity and the clinical manifestations.
We obtained genomic DNA from 164 subjects, 82 with long-standing IBD aged 8 to 18 years: 46 with Crohn disease (CD) and 36 with ulcerative colitis (UC). Eighty-two healthy children served as the control population. Genotyping was determined by using a restriction enzyme-based assay. TNF-alpha 308 G-->A polymorphism was assessed in terms of inflammatory (C-reactive protein [CRP]) and disease activity. The latter was assessed by the Pediatric Crohn's Disease Activity Index (PCDAI) and the Truelove index for CD and UC, respectively.
Significant differences in TNF-alpha 308 A polymorphism were found between the IBD group and controls (P < 0.05) and the UC group and controls (P < 0.001). No differences were noted between TNF-alpha 308 A polymorphism and clinical characteristics in UC. The frequency of the -308 A allele of TNF was not different in CD compared with that in the control group. The frequency of TNF-alpha 308 A genotype was significantly higher in CD patients with predominantly stenosing/penetrating disease compared with patients without complications (P < 0.001) and healthy controls (P < 0.01). In CD patients, those carrying TNF -308 A had a significant increase in CRP (P < 0.05) and the PCDAI (P < 0.05). In CD, CRP levels strongly correlated with the PCDAI (r = 0.6150, P < 0.001). In UC, significant differences among the mean levels of CRP (P < 0.05) and disease activity (P < 0.001) related to TNF-alpha 308 A polymorphism were found. Allele distribution (odds ratio, 12.9; CI, 1.18-140.81, P < 0.001) and CRP serum levels (odds ratio, 1.020; CI, 1.00-1.04, P < 0.001) were independently associated with CD complications.
Although not necessarily dictating IBD initiation, the TNF-alpha 308 A polymorphism may play a role in modifying the CD phenotype. The polymorphism may influence disease activity as well as more intense inflammatory activity in both forms of IBD and may modify the progression of chronic digestive tract inflammation.
我们的初步研究旨在确定肿瘤坏死因子-α(TNF-α)308G→A启动子单核苷酸多态性在儿童炎症性肠病(IBD)中的作用、其对炎症活动及临床表现的影响。
我们从164名受试者中获取基因组DNA,其中82名患有8至18岁的长期IBD:46名患有克罗恩病(CD),36名患有溃疡性结肠炎(UC)。82名健康儿童作为对照人群。采用基于限制性酶切分析的方法进行基因分型。从炎症(C反应蛋白[CRP])和疾病活动方面评估TNF-α 308G→A多态性。后者分别通过儿童克罗恩病活动指数(PCDAI)和针对CD及UC的特鲁洛夫指数进行评估。
在IBD组与对照组之间(P<0.05)以及UC组与对照组之间(P<0.001)发现TNF-α 308A多态性存在显著差异。在UC中,TNF-α 308A多态性与临床特征之间未发现差异。与对照组相比,CD中TNF -308A等位基因频率无差异。与无并发症患者(P<0.001)及健康对照(P<0.01)相比,以狭窄/穿透性疾病为主的CD患者中TNF-α 308A基因型频率显著更高。在CD患者中,携带TNF -308A的患者CRP(P<0.05)和PCDAI(P<0.05)显著升高。在CD中,CRP水平与PCDAI密切相关(r = 0.6150,P<0.001)。在UC中,发现与TNF-α 308A多态性相关的CRP平均水平(P<0.05)和疾病活动(P<0.001)存在显著差异。等位基因分布(优势比,12.9;CI,1.18 - 140.81,P<0.001)和CRP血清水平(优势比,1.020;CI,1.00 - 1.04,P<0.001)与CD并发症独立相关。
尽管TNF-α 308A多态性不一定决定IBD的发病,但它可能在改变CD表型中起作用。该多态性可能影响两种形式IBD的疾病活动以及更强烈的炎症活动,并可能改变慢性消化道炎症的进展。
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