Mitchell S A, Grove J, Spurkland A, Boberg K M, Fleming K A, Day C P, Schrumpf E, Chapman R W
Department of Gastroenterology, Oxford Radcliffe Hospital, Oxford, UK.
Gut. 2001 Aug;49(2):288-94. doi: 10.1136/gut.49.2.288.
Primary sclerosing cholangitis (PSC) is a chronic cholestatic liver disease of unknown aetiology. Abnormalities in immune regulation and genetic associations suggest that PSC is an immune mediated disease. Several polymorphisms within the tumour necrosis factor alpha (TNF-alpha) and interleukin 10 (IL-10) promoter genes have been described which influence expression of these cytokines. This study examines the possible association between polymorphisms at the -308 and -627 positions in the TNF-alpha and IL-10 promoter genes, respectively, and susceptibility to PSC.
TNF-alpha -308 genotypes were studied by polymerase chain reaction (PCR) in 160 PSC patients from Norway and the UK compared with 145 ethnically matched controls. IL-10 -627 genotypes were studied by PCR in 90 PSC patients compared with 84 ethnically matched controls.
A total of 16% of Norwegian PSC patients and 12% of British PSC patients were homozygous for the TNF2 allele compared with 3% and 6% of respective controls. The TNF2 allele was present in 60% of PSC patients versus 30% of controls (OR(combined data)=3.2 (95% confidence intervals (CI) 1.8--4.5); p(corr)=10(-5)). The association between the TNF2 allele and susceptibility to PSC was independent of the presence of concurrent inflammatory bowel disease (IBD) in the PSC patients; 61% of PSC patients without IBD had TNF2 compared with 30% of controls (OR(combined data)=3.2 (95% CI 1.2--9.0); p(corr)=0.006 ). There was no difference in the -627 IL-10 polymorphism distributions between patients and controls in either population. The increase in TNF2 allele in PSC patients only occurs in the presence of DRB10301 (DR3) and B8. In the combined population data, DRB10301 showed a stronger association with susceptibility to PSC than both the TNF2 and B8 alleles (OR(combined data)=3.8, p(corr)=10(-6) v OR(combined data)=3.2, p(corr)=10(-5) v OR(combined data )=3.41, p(corr)=10(-4), respectively).
This study identified a significant association between possession of the TNF2 allele, a G-->A substitution at position -308 in the TNF-alpha promoter, and susceptibility to PSC. This association was secondary to the association of PSC with the A1-B8-DRB10301-DQA10501-DQB1*0201 haplotype. No association was found between the IL-10 -627 promoter polymorphism and PSC.
原发性硬化性胆管炎(PSC)是一种病因不明的慢性胆汁淤积性肝病。免疫调节异常和基因关联提示PSC是一种免疫介导的疾病。肿瘤坏死因子α(TNF-α)和白细胞介素10(IL-10)启动子基因内的几种多态性已被描述,它们会影响这些细胞因子的表达。本研究探讨TNF-α和IL-10启动子基因分别在-308和-627位置的多态性与PSC易感性之间的可能关联。
通过聚合酶链反应(PCR)研究了来自挪威和英国的160例PSC患者的TNF-α -308基因型,并与145例种族匹配的对照进行比较。通过PCR研究了90例PSC患者的IL-10 -627基因型,并与84例种族匹配的对照进行比较。
挪威PSC患者中16%以及英国PSC患者中12%为TNF2等位基因纯合子,而各自对照中这一比例分别为3%和6%。TNF2等位基因在60%的PSC患者中存在,而对照中为30%(合并数据的比值比(OR)=3.2(95%置信区间(CI)1.8 - 4.5);校正p值=10^(-5))。TNF2等位基因与PSC易感性之间的关联独立于PSC患者中同时存在的炎症性肠病(IBD);61%无IBD的PSC患者有TNF2,而对照中为30%(合并数据的OR = 3.2(95% CI 1.2 - 9.0);校正p值=0.006)。在这两个人群中,患者和对照之间的-627 IL-10多态性分布没有差异。PSC患者中TNF2等位基因的增加仅在存在DRB10301(DR3)和B8时出现。在合并人群数据中,DRB10301与PSC易感性的关联比TNF2和B8等位基因都更强(合并数据的OR分别为=3.8,校正p值=10^(-6) 对比 合并数据的OR = 3.2,校正p值=10^(-5) 对比 合并数据的OR = 3.41,校正p值=10^(-4))。
本研究发现TNF2等位基因(TNF-α启动子-308位置的G→A替换)的携带与PSC易感性之间存在显著关联。这种关联是PSC与A1 - B8 - DRB10301 - DQA10501 - DQB1*0201单倍型关联的继发结果。未发现IL-10 -627启动子多态性与PSC之间存在关联。