University of Chicago Pritzker School of Medicine, Chicago, IL 60637, USA.
Arthritis Res Ther. 2010;12(4):R151. doi: 10.1186/ar3101. Epub 2010 Jul 26.
Systemic lupus erythematosus (SLE) is a highly heterogeneous disorder, characterized by differences in autoantibody profile, serum cytokines, and clinical manifestations. SLE-associated autoantibodies and high serum interferon alpha (IFN-α) are important heritable phenotypes in SLE which are correlated with each other, and play a role in disease pathogenesis. These two heritable risk factors are shared between ancestral backgrounds. The aim of the study was to detect genetic factors associated with autoantibody profiles and serum IFN-α in SLE.
We undertook a case-case genome-wide association study of SLE patients stratified by ancestry and extremes of phenotype in serology and serum IFN-α. Single nucleotide polymorphisms (SNPs) in seven loci were selected for follow-up in a large independent cohort of 538 SLE patients and 522 controls using a multi-step screening approach based on novel metrics and expert database review. The seven loci were: leucine-rich repeat containing 20 (LRRC20); protein phosphatase 1 H (PPM1H); lysophosphatidic acid receptor 1 (LPAR1); ankyrin repeat and sterile alpha motif domain 1A (ANKS1A); protein tyrosine phosphatase, receptor type M (PTPRM); ephrin A5 (EFNA5); and V-set and immunoglobulin domain containing 2 (VSIG2).
SNPs in the LRRC20, PPM1H, LPAR1, ANKS1A, and VSIG2 loci each demonstrated strong association with a particular serologic profile (all odds ratios > 2.2 and P < 3.5 × 10-4). Each of these serologic profiles was associated with increased serum IFN-α. SNPs in both PTPRM and LRRC20 were associated with increased serum IFN-α independent of serologic profile (P = 2.2 × 10-6 and P = 2.6 × 10-3 respectively). None of the SNPs were strongly associated with SLE in case-control analysis, suggesting that the major impact of these variants will be upon subphenotypes in SLE.
This study demonstrates the power of using serologic and cytokine subphenotypes to elucidate genetic factors involved in complex autoimmune disease. The distinct associations observed emphasize the heterogeneity of molecular pathogenesis in SLE, and the need for stratification by subphenotypes in genetic studies. We hypothesize that these genetic variants play a role in disease manifestations and severity in SLE.
系统性红斑狼疮(SLE)是一种高度异质性疾病,其特征在于自身抗体谱、血清细胞因子和临床表现的差异。SLE 相关自身抗体和高血清干扰素 α(IFN-α)是 SLE 中重要的遗传表型,它们相互关联,并在疾病发病机制中发挥作用。这两个遗传危险因素在祖先背景之间是共享的。本研究旨在检测与 SLE 患者自身抗体谱和血清 IFN-α相关的遗传因素。
我们对按祖裔和血清学和血清 IFN-α极端表型分层的 SLE 患者进行了病例-病例全基因组关联研究。基于新的指标和专家数据库审查,对七个候选基因座中的单核苷酸多态性(SNP)进行了多步筛选,在一个包含 538 名 SLE 患者和 522 名对照的大型独立队列中进行了后续检测。七个候选基因座分别是:富含亮氨酸重复序列 20(LRRC20);蛋白磷酸酶 1H(PPM1H);溶血磷脂酸受体 1(LPAR1);锚蛋白重复和无菌α基序域 1A(ANKS1A);蛋白酪氨酸磷酸酶,受体型 M(PTPRM);表皮生长因子 A5(EFNA5);和 V 集和免疫球蛋白域包含 2(VSIG2)。
LRRC20、PPM1H、LPAR1、ANKS1A 和 VSIG2 基因座中的 SNP 均与特定的血清学特征强烈相关(所有比值比均>2.2,P<3.5×10-4)。这些血清学特征中的每一个都与血清 IFN-α的增加有关。PTPRM 和 LRRC20 中的 SNP 与血清 IFN-α的增加独立相关,而与血清学特征无关(P=2.2×10-6 和 P=2.6×10-3)。在病例对照分析中,没有 SNP 与 SLE 强烈相关,这表明这些变体的主要影响将是 SLE 中的亚表型。
本研究表明,使用血清学和细胞因子亚表型来阐明复杂自身免疫性疾病中涉及的遗传因素具有强大的作用。观察到的独特关联强调了 SLE 中分子发病机制的异质性,以及在遗传研究中按亚表型分层的必要性。我们假设这些遗传变异在 SLE 的临床表现和严重程度中发挥作用。
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