一项全基因组关联研究提示原发性抗磷脂综合征的新易感位点

Desire Casares-Marfil, Manuel Martinez-Bueno, Maria Orietta Borghi, Guillermo Pons-Estel, PRECISESADS Clinical Consortium, Guillermo Reales, Yu Zuo, Gerard Espinosa, Timothy R.D.J. Radstake, Lucas L. van den Hoogen, Chris Wallace, Joel Guthridge, Judith James, Ricard Cervera, Pier Luigi Luigi Meroni, Javier Martín, Jason Knight, Marta Alarcon-Riquelme, Amr H Sawalha
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摘要

目的:原发性抗磷脂综合征(PAPS)是一种罕见的自身免疫性疾病,其特征是存在抗磷脂抗体,并发生血栓形成事件和妊娠并发症。我们的研究旨在确定与PAPS相关的新的遗传易感位点。方法:我们进行了一项全基因组关联研究,包括5485名欧洲血统个体(482名受影响个体)。从大约700万个变异的荟萃分析中评估了重要的和具有启发性的独立变异,以进行功能和生物过程富集。还评估了不同人群中PAPS的遗传风险变异性。采用层次聚类、马氏距离和Dirichlet过程混合不确定聚类方法来评估PAPS与其他免疫介导疾病之间的遗传相似性。结果:我们揭示了在HLA- dra附近的HLA II类区域和STAT4中的一个调控位点与PAPS的遗传关联,具有全基因组水平的显著性。另外还发现了34个提示PAPS的遗传易感性位点。HLAⅱ类位点疾病风险等位基因与HLA- drb6、HLA- drb9、HLA- dpb2、HLA- dqa2和HLA- dqb2过表达相关,与PAPS与HLA- drb1 *1302的关联无关。功能分析强调了paps相关基因座中的免疫和神经系统相关通路。与其他免疫介导疾病的比较显示,与视神经脊髓炎、系统性硬化症和干燥综合征有密切的遗传关系,提示STAT4、TNPO3和BLK的共定位因果变异。结论:本研究对PAPS进行了全面、大规模的遗传分析,为这一罕见疾病的遗传基础和病理生理提供了新的认识。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A genome-wide association study suggests new susceptibility loci for primary antiphospholipid syndrome
Objectives: Primary antiphospholipid syndrome (PAPS) is a rare autoimmune disease characterized by the presence of antiphospholipid antibodies and the occurrence of thrombotic events and pregnancy complications. Our study aimed to identify novel genetic susceptibility loci associated with PAPS. Methods: We performed a genome-wide association study comprising 5,485 individuals (482 affected individuals) of European ancestry. Significant and suggestive independent variants from a meta-analysis of approximately 7 million variants were evaluated for functional and biological process enrichment. The genetic risk variability for PAPS in different populations was also assessed. Hierarchical clustering, Mahalanobis distance, and Dirichlet Process Mixtures with uncertainty clustering methods were used to assess genetic similarities between PAPS and other immune-mediated diseases. Results: We revealed genetic associations with PAPS in a regulatory locus within the HLA class II region near HLA-DRA and in STAT4 with a genome-wide level of significance. 34 additional suggestive genetic susceptibility loci for PAPS were also identified. The disease risk allele in the HLA class II locus is associated with overexpression of HLA-DRB6, HLA-DRB9, HLA-DPB2, HLA-DQA2 and HLA-DQB2, and is independent of the association between PAPS and HLA-DRB1*1302. Functional analyses highlighted immune and nervous system related pathways in PAPS-associated loci. The comparison with other immune-mediated diseases revealed a close genetic relatedness to neuromyelitis optica, systemic sclerosis, and Sjogren syndrome, suggesting colocalized causal variations close to STAT4, TNPO3, and BLK. Conclusions: This study represents a comprehensive large-scale genetic analysis for PAPS and provides new insights into the genetic basis and pathophysiology of this rare disease.
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