Tumour necrosis factor microsatellites in reactive arthritis.

J Tuokko, S Koskinen, P Westman, U Yli-Kerttula, A Toivanen, J Ilonen
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引用次数: 29

Abstract

The purpose was to study tumour necrosis factor (TNF)-a, -b and -c microsatellites as potential new susceptibility markers for reactive arthritis (ReA). Fifty-nine patients typed for HLA-B27 were studied for frequencies of TNF microsatellite alleles and compared with allele frequencies determined from 285 random haplotypes and 46 healthy HLA-B27-positive controls. TNFa, -b and -c microsatellite sequences were amplified by the polymerase chain reaction, and the size of the product was defined by an automated sequencer. The frequencies of TNFa6 and -c1 alleles were found to be increased in patients with ReA, whereas TNFa11 and -c2 frequencies were decreased as compared to control haplotypes. The increase in the c1 allele in patients with ReA independently from HLA-B27 suggests that it might be a new susceptibility marker for the disease. The association of ReA with other alleles was due to a linkage disequilibrium with HLA-B27.

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反应性关节炎中的肿瘤坏死因子微卫星。
目的是研究肿瘤坏死因子(TNF)-a、-b和-c微卫星作为反应性关节炎(ReA)潜在的新易感标志物。研究了59例HLA-B27分型患者的TNF微卫星等位基因频率,并与285个随机单倍型和46个健康HLA-B27阳性对照的等位基因频率进行了比较。通过聚合酶链反应扩增TNFa, -b和-c微卫星序列,并用自动测序仪确定产物的大小。与对照单倍型相比,ReA患者的TNFa6和-c1等位基因频率增加,而TNFa11和-c2等位基因频率降低。在独立于HLA-B27的ReA患者中c1等位基因的增加表明它可能是该疾病的新的易感标志物。ReA与其他等位基因的关联是由于与HLA-B27的连锁不平衡。
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