Donn Rachelle, Alourfi Zaynab, De Benedetti Fabrizio, Meazza Cristina, Zeggini Eleftheria, Lunt Mark, Stevens Adam, Shelley Emma, Lamb Rebecca, Ollier William E R, Thomson Wendy, Ray David
Epidemiology Unit, Arthritis Research Campaign, University of Manchester, Manchester, UK.
Arthritis Rheum. 2002 Sep;46(9):2402-9. doi: 10.1002/art.10492.
To determine if polymorphisms of the macrophage migration inhibitory factor (MIF) gene are associated with juvenile idiopathic arthritis (JIA).
Denaturing high-performance liquid chromatography was used to screen the MIF gene in 32 UK Caucasian controls and 88 UK Caucasian JIA patients. Ninety-two healthy UK Caucasian controls were then genotyped for each of the polymorphic positions identified. A panel of 526 UK Caucasian JIA patients and 259 UK Caucasian controls were subsequently genotyped for a single-nucleotide polymorphism (SNP) identified in the 5'-flanking region of the gene, using SNaPshot ddNTP primer extension and capillary electrophoresis. The functional significance of this polymorphism was also studied using luciferase-based reporter gene assays in human T lymphoblast and epithelial cell lines.
A tetranucleotide repeat CATT((5-7)) beginning at nucleotide position -794 and 3 SNPs at positions -173 (G to C), +254 (T to C), and +656 (C to G) of the MIF gene were identified. No JIA-specific mutations were found. Allele and genotype frequencies differed significantly between the controls and the JIA patients for the MIF-173 polymorphism. Individuals possessing a MIF-173C allele had an increased risk of JIA (34.8% versus 21.6%) (odds ratio 1.9, 95% confidence interval 1.4-2.7; P = 0.0002). Furthermore, the MIF-173 G and C variants resulted in altered expression of MIF in a cell type-specific manner. Serum levels of MIF were also significantly higher in individuals who carried a MIF-173*C allele (P = 0.04).
The -173-MIF*C allele confers increased risk of susceptibility to JIA. Our data suggest a cell type-specific regulation of MIF, which may be central to understanding its role in inflammation.
确定巨噬细胞移动抑制因子(MIF)基因多态性是否与青少年特发性关节炎(JIA)相关。
采用变性高效液相色谱法对32名英国白种人对照者和88名英国白种人JIA患者的MIF基因进行筛查。随后对92名健康英国白种人对照者在已确定的每个多态性位点进行基因分型。使用SNaPshot ddNTP引物延伸和毛细管电泳技术,对526名英国白种人JIA患者和259名英国白种人对照者针对该基因5'侧翼区域中鉴定出的一个单核苷酸多态性(SNP)进行基因分型。还利用基于荧光素酶的报告基因检测在人T淋巴母细胞和上皮细胞系中研究了这种多态性的功能意义。
在MIF基因中鉴定出一个始于核苷酸位置 -794的四核苷酸重复序列CATT((5 - 7))以及位于 -173(G到C)、 +254(T到C)和 +656(C到G)位置的3个SNP。未发现JIA特异性突变。MIF -173多态性在对照者和JIA患者之间的等位基因和基因型频率存在显著差异。携带MIF -173C等位基因的个体患JIA的风险增加(34.8%对21.6%)(优势比1.9,95%置信区间1.4 - 2.7;P = 0.0002)。此外,MIF -173G和C变体以细胞类型特异性方式导致MIF表达改变。携带MIF -173*C等位基因个体的血清MIF水平也显著更高(P = 0.04)。
-173 - MIF*C等位基因增加了患JIA的易感性风险。我们的数据表明MIF存在细胞类型特异性调节,这可能是理解其在炎症中作用的关键。
