爱沙尼亚青少年特发性关节炎遗传易感性因素的关联分析。
Association analysis of juvenile idiopathic arthritis genetic susceptibility factors in Estonian patients.
机构信息
Estonian Genome Center, Institute of Genomics, University of Tartu, Riia 23B, 51010, Tartu, Estonia.
Institute of Dentistry, University of Tartu, Tartu, Estonia.
出版信息
Clin Rheumatol. 2021 Oct;40(10):4157-4165. doi: 10.1007/s10067-021-05756-x. Epub 2021 Jun 8.
BACKGROUND
Juvenile idiopathic arthritis (JIA) is the most common chronic rheumatic condition of childhood. Genetic association studies have revealed several JIA susceptibility loci with the strongest effect size observed in the human leukocyte antigen (HLA) region. Genome-wide association studies have augmented the number of JIA-associated loci, particularly for non-HLA genes. The aim of this study was to identify new associations at non-HLA loci predisposing to the risk of JIA development in Estonian patients.
METHODS
We performed genome-wide association analyses in an entire JIA case-control sample (All-JIA) and in a case-control sample for oligoarticular JIA, the most prevalent JIA subtype. The entire cohort was genotyped using the Illumina HumanOmniExpress BeadChip arrays. After imputation, 16,583,468 variants were analyzed in 263 cases and 6956 controls.
RESULTS
We demonstrated nominal evidence of association for 12 novel non-HLA loci not previously implicated in JIA predisposition. We replicated known JIA associations in CLEC16A and VCTN1 regions in the oligoarticular JIA sample. The strongest associations in the All-JIA analysis were identified at PRKG1 (P = 2,54 × 10), LTBP1 (P = 9,45 × 10), and ELMO1 (P = 1,05 × 10). In the oligoarticular JIA analysis, the strongest associations were identified at NFIA (P = 5,05 × 10), LTBP1 (P = 9,95 × 10), MX1 (P = 1,65 × 10), and CD200R1 (P = 2,59 × 10).
CONCLUSION
This study increases the number of known JIA risk loci and provides additional evidence for the existence of overlapping genetic risk loci between JIA and other autoimmune diseases, particularly rheumatoid arthritis. The reported loci are involved in molecular pathways of immunological relevance and likely represent genomic regions that confer susceptibility to JIA in Estonian patients. Key Points • Juvenile idiopathic arthritis (JIA) is the most common childhood rheumatic disease with heterogeneous presentation and genetic predisposition. • Present genome-wide association study for Estonian JIA patients is first of its kind in Northern and Northeastern Europe. • The results of the present study increase the knowledge about JIA risk loci replicating some previously described associations, so adding weight to their relevance and describing novel loci. • The study provides additional evidence for the existence of overlapping genetic risk loci between JIA and other autoimmune diseases, particularly rheumatoid arthritis.
背景
幼年特发性关节炎(JIA)是儿童中最常见的慢性风湿性疾病。遗传关联研究已经揭示了几个 JIA 易感基因座,其中最强的效应大小在人类白细胞抗原(HLA)区域观察到。全基因组关联研究增加了 JIA 相关基因座的数量,特别是非 HLA 基因。本研究的目的是在爱沙尼亚患者中确定新的非 HLA 基因座,这些基因座易患 JIA 发展的风险。
方法
我们对整个 JIA 病例对照样本(All-JIA)和寡关节 JIA 病例对照样本(最常见的 JIA 亚型)进行了全基因组关联分析。整个队列使用 Illumina HumanOmniExpress BeadChip 阵列进行基因分型。在进行 imputation 后,在 263 例病例和 6956 例对照中分析了 16583468 个变体。
结果
我们证明了 12 个以前未涉及 JIA 易感性的新非 HLA 基因座存在名义上的关联。我们在寡关节 JIA 样本中复制了已知的 JIA 关联CLEC16A 和 VCTN1 区域。在 All-JIA 分析中最强的关联位于 PRKG1(P=2.54×10)、LTBP1(P=9.45×10)和 ELMO1(P=1.05×10)。在寡关节 JIA 分析中,最强的关联位于 NFIA(P=5.05×10)、LTBP1(P=9.95×10)、MX1(P=1.65×10)和 CD200R1(P=2.59×10)。
结论
本研究增加了已知的 JIA 风险基因座的数量,并为 JIA 和其他自身免疫性疾病(特别是类风湿关节炎)之间存在重叠的遗传风险基因座提供了额外的证据。报告的基因座参与了免疫相关的分子途径,并且可能代表了赋予爱沙尼亚患者 JIA 易感性的基因组区域。
关键点
幼年特发性关节炎(JIA)是儿童中最常见的风湿性疾病,具有异质性表现和遗传易感性。
这是首次在北欧和东北欧进行的针对爱沙尼亚 JIA 患者的全基因组关联研究。
本研究结果复制了一些以前描述的关联,增加了 JIA 风险基因座的知识,从而增加了它们的相关性,并描述了新的基因座。
该研究为 JIA 和其他自身免疫性疾病(特别是类风湿关节炎)之间存在重叠的遗传风险基因座提供了额外的证据。
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