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与青少年类风湿性关节炎相关的NRAMP1和D2S1471基因座的多态性。

Polymorphism at NRAMP1 and D2S1471 loci associated with juvenile rheumatoid arthritis.

作者信息

Sanjeevi C B, Miller E N, Dabadghao P, Rumba I, Shtauvere A, Denisova A, Clayton D, Blackwell J M

机构信息

University of Cambridge School of Clinical Medicine, UK.

出版信息

Arthritis Rheum. 2000 Jun;43(6):1397-404. doi: 10.1002/1529-0131(200006)43:6<1397::AID-ANR25>3.0.CO;2-6.

Abstract

OBJECTIVE

To examine the role of NRAMP1 in susceptibility to juvenile rheumatoid arthritis (JRA).

METHODS

DNA from 119 JRA patients (72 pauciarticular, 47 polyarticular) and 111 healthy controls from Latvia was genotyped for a functional repeat polymorphism in the promoter of NRAMP1 and a linked (<150 kb) microsatellite D2S1471. The findings were compared with those from HLA-DQ alleles typed previously. Chi-square analyses were performed using the Mantel-Haenszel test and stratification according to pure Latvian or pure Russian descent. Haplotype analysis was performed using the Associate program to implement the expectation-maximization algorithm based on the gene-counting technique.

RESULTS

Allele 3 at NRAMP1 conferred increased risk (odds ratios [ORs] 2.26, 2.31, and 2.19; P = 0.0006, 0.003, and 0.019) of disease in the JRA, pauciarticular, and polyarticular patient groups, respectively. Allele 2 conferred protection (OR 0.44, 0.43, and 0.46). Alleles at D2S1471 that conferred susceptibility (6 and 12) or protection (11) did so only when on a haplotype with alleles 3 or 2, respectively, at NRAMP1. Allele 3 at NRAMP1 was additive with HLA-DQ7 for susceptibility (OR 3.71, 3.71, and 4.02), and allele 2 at NRAMP1 was additive with HLA-DQ5 for protection (OR 0.19, 0.08, and 0.12).

CONCLUSION

The NRAMP1 allele conferring susceptibility to JRA drives high levels of NRAMP1 expression, while the allele associated with protection drives low levels. These 2 alleles are inversely associated with susceptibility to infectious disease, consistent with their maintenance in populations through balancing selection.

摘要

目的

研究天然抗性相关巨噬蛋白1(NRAMP1)在青少年类风湿性关节炎(JRA)易感性中的作用。

方法

对来自拉脱维亚的119例JRA患者(72例少关节型、47例多关节型)和111例健康对照者的DNA进行基因分型,检测NRAMP1启动子区的功能性重复多态性以及一个连锁的(<150 kb)微卫星D2S1471。将研究结果与之前检测的HLA - DQ等位基因的结果进行比较。采用Mantel - Haenszel检验和根据纯拉脱维亚或纯俄罗斯血统进行分层的卡方分析。使用Associate程序基于基因计数技术实施期望最大化算法进行单倍型分析。

结果

NRAMP1基因的3号等位基因分别使JRA患者组、少关节型患者组和多关节型患者组的疾病风险增加(比值比[OR]分别为2.26、2.31和2.19;P = 0.0006、0.003和0.019)。2号等位基因具有保护作用(OR分别为0.44、0.43和0.46)。D2S1471的6号和12号等位基因分别赋予易感性,11号等位基因赋予保护性,且只有当它们与NRAMP1基因的3号或2号等位基因处于同一单倍型时才会如此。NRAMP1基因的3号等位基因与HLA - DQ7在易感性方面具有累加效应(OR分别为3.71、3.71和4.02),而NRAMP1基因的2号等位基因与HLA - DQ5在保护性方面具有累加效应(OR分别为0.19、0.08和0.12)。

结论

赋予JRA易感性的NRAMP1等位基因驱动高水平的NRAMP1表达,而与保护作用相关的等位基因驱动低水平表达。这两个等位基因与传染病易感性呈负相关,这与其通过平衡选择在人群中得以维持一致。

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