Association of NKG2D gene variants with susceptibility and severity of rheumatoid arthritis

C. Mariaselvam, C. Mariaselvam, R. Tamouza, Rajagopal Krishnamoorthy, Dominique Charron, Durga Prasanna Misra, Vikramraj K Jain, V. S. Negi
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引用次数: 20

Abstract

NKG2D (KLRK1) is a C‐type lectin receptor present on natural killer (NK) cells, γδ, CD8+ and CD4+ T cells. Upon ligand binding, NKG2D mediates activatory and co‐stimulatory signals to NK cells and activated CD4+ T cells, respectively. Polymorphisms in NKG2D predispose to infectious diseases, cancer, transplantation and autoimmune disorders. We studied the influence of this NK receptor polymorphism on predisposition to and modification of the disease phenotype in patients with rheumatoid arthritis (RA). Eight different single nucleotide polymorphisms (SNP) in the NKG2 gene were genotyped in 236 patients with RA and 187 controls using Taqman 5' nuclease assays. NKG2D genotype/allele frequency did not differ between patients and controls. Subgroup analysis showed that the frequency of A allele of NKG2D9 and T allele of NKG2D10 was significantly higher in patients with deformities (a marker of severe disease) [11 versus 5%, Pc = 0·03, odds ratio (OR) = 2·44, 95% confidence interval (CI) = 1·09‐5·98 and 10 versus 4%, Pc = 0·04, OR = 2·45, 95% CI = 1·05‐6·39, respectively], while the frequency of alleles G of NKG2D9 and A of NKG2D10 was greater in patients without deformities (Pc = 0·03, OR = 0·41, 95% CI = 0·17‐0·91 and Pc = 0·04, OR = 0·41, 95% CI = 0·16‐0·96). Similar trends of association were observed with deforming phenotype of RA in female patients and deforming young onset RA subgroups. Haplotype analysis revealed that the frequency of haplotype G‐C‐A‐G‐A‐T‐C‐C was higher in patients than in controls (12 versus 8%, P = 0·04, OR = 1·61, 95% CI = 1·01‐2·55), suggesting that it may predispose to RA. Our study suggests that the NKG2D gene polymorphisms may modify the risk of development and severity of RA.
NKG2D基因变异与类风湿关节炎易感性和严重程度的关系
NKG2D (KLRK1)是一种C型凝集素受体,存在于自然杀伤细胞(NK)、γδ、CD8+和CD4+ T细胞上。在配体结合后,NKG2D分别介导NK细胞和活化CD4+ T细胞的激活和共刺激信号。NKG2D的多态性易导致传染病、癌症、移植和自身免疫性疾病。我们研究了这种NK受体多态性对类风湿关节炎(RA)患者的易感性和疾病表型改变的影响。采用Taqman 5′核酸酶测定方法,对236例RA患者和187例对照患者的NKG2基因进行了8种不同的单核苷酸多态性(SNP)分型。NKG2D基因型/等位基因频率在患者和对照组之间没有差异。亚组分析显示,一个等位基因的频率NKG2D10 NKG2D9和T等位基因的患者明显高于畸形(严重疾病的一个标志)(11 5%,电脑= 0·03,比值比(或)= 2·44岁的95%可信区间(CI) = 1·09年5·98和10 4%,个人电脑= 0·04或45 = 2·95% CI = 1·05年还是6·39岁,分别),而G等位基因的频率NKG2D9和NKG2D10更大的患者没有畸形(电脑= 0·03,或= 0·41岁,95% CI = 0·17 0·91和Pc = 0·04,Or = 0.41, 95% ci = 0.16‐0.96)。在女性患者和年轻发病的变形型RA亚组中,观察到类似的关联趋势。单倍型分析显示,患者中G‐C‐A‐G‐A‐T‐C‐C的单倍型频率高于对照组(12%比8%,P = 0.04, OR = 1.61, 95% CI = 1.01‐2.55),提示其可能易患RA。我们的研究提示NKG2D基因多态性可能改变RA的发展风险和严重程度。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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