Section of Molecular Pathology and Human Genetics, Department of Internal Medicine, School of Medicine, University of Crete, Heraklion 71003, Greece.
4th Department of Internal Medicine, Hippocratio Hospital, Aristotle University of Thessaloniki, Thessaloniki 54124, Greece.
Mol Med Rep. 2017 Dec;16(6):8793-8798. doi: 10.3892/mmr.2017.7733. Epub 2017 Oct 5.
Juvenile idiopathic arthritis (JIA) is an autoimmune disease that is characterized by persistent chronic arthritis and affected by genetic and environmental factors. Different genetic variations have been reported as risk factors for JIA. However, given that many results could not be replicated in individuals of different ancestral origin, it was assumed that heterogeneous genetic factors are involved in this disease. In the present study, we analyzed three single nucleotide polymorphisms (SNPs), namely PTPRC (rs10919563), TYK2 (rs34536443) and PRKCQ (rs4750316), which were found to be associated with JIA in previous studies. We also investigated whether the intron‑4 located 27‑bp VNTR of endothelial nitric oxide synthase (eNOS), is associated with risk for JIA in Greece. In total, 125 JIA patients and 221 healthy controls from northern Greece were included in the study as a sample set. Samples were then analyzed, and genotyped for the three SNPs with TaqMan primer‑probe sets, using a Real‑Time PCR platform (ViiA™ 7 Real‑Time PCR system), while eNOS VNTR polymorphism was genotyped by PCR. Statistical analysis was performed using a GraphPad Prism statistical program. The χ2 test was used to examine differences of genotype and allele frequencies between patients and controls. Statistical significance was defined by using the two‑tailed P<0.05 test. Bioinformatics analysis was conducted by using BlastP, Pymol, Maestro and Desmond. In the case‑control association study performed, eNOS only was found to be associated with JIA. Genotype a/a and allele 'a' were found in a higher frequency in JIA patients than in controls [p<0.0001, odds ratio (OR)=0.15, 95% confidence intervals (CI): 0.065‑0.37; and p<0.0001, OR=0.34, 95% CI: 0.23‑0.49, respectively]. No associations with JIA were detected for TYK2, PTPRC or PRKCQ. Aiming to investigate the structural consequences and the structure/function relationships accompanying the Pro1104 to Ala (rs34536443) mutation on TYK2 protein, bioinformatics analysis was performed. Combining three‑dimensional (3D)‑modeling and molecular dynamics simulations we identified changes in structural flexibility, affecting the functionality of the kinase domain of TYK2. To the best of our knowledge, this is the first time that eNOS VNTR polymorphism is associated with susceptibility to JIA, suggesting a differential role of allele 'a' in various complex diseases. The current data emphasize the importance of comparative studies in populations of a different ancestral background towards the clarification of the role of specific alleles in the development of JIA.
幼年特发性关节炎(JIA)是一种自身免疫性疾病,其特征为持续性慢性关节炎,并受遗传和环境因素影响。已有报道称,不同的遗传变异是 JIA 的风险因素。然而,鉴于许多结果在不同祖源的个体中无法复制,因此假设该疾病涉及异质遗传因素。在本研究中,我们分析了三个单核苷酸多态性(SNP),即 PTPRC(rs10919563)、TYK2(rs34536443)和 PRKCQ(rs4750316),这些 SNP 先前被报道与 JIA 相关。我们还研究了内皮型一氧化氮合酶(eNOS)内含子 4 27-bpVNTR 是否与希腊 JIA 患者的患病风险相关。本研究共纳入了来自希腊北部的 125 名 JIA 患者和 221 名健康对照作为样本。使用 TaqMan 引物-探针试剂盒通过实时 PCR 平台(ViiA™ 7 实时 PCR 系统)分析了三个 SNP 的基因型,并通过 PCR 分析了 eNOSVNTR 多态性。使用 GraphPad Prism 统计程序进行统计分析。卡方检验用于检验患者和对照组之间基因型和等位基因频率的差异。采用双侧 P<0.05 检验定义统计学意义。使用 BlastP、Pymol、Maestro 和 Desmond 进行生物信息学分析。在进行的病例对照关联研究中,仅发现 eNOS 与 JIA 相关。与对照组相比,JIA 患者中基因型 a/a 和等位基因 'a' 的频率更高[P<0.0001,优势比(OR)=0.15,95%置信区间(CI):0.065-0.37;P<0.0001,OR=0.34,95%CI:0.23-0.49]。未发现 TYK2、PTPRC 或 PRKCQ 与 JIA 相关。为了研究 TYK2 蛋白上 Pro1104 到 Ala(rs34536443)突变所伴随的结构后果和结构/功能关系,我们进行了生物信息学分析。通过结合三维(3D)建模和分子动力学模拟,我们发现了结构灵活性的变化,影响了 TYK2 激酶结构域的功能。据我们所知,这是首次发现 eNOSVNTR 多态性与 JIA 易感性相关,表明等位基因 'a' 在各种复杂疾病中的作用不同。目前的数据强调了在不同祖源背景的人群中进行比较研究的重要性,以阐明特定等位基因在 JIA 发展中的作用。
