Identification of ST3AGL4, MFHAS1, CSNK2A2 and CD226 as loci associated with systemic lupus erythematosus (SLE) and evaluation of SLE genetics in drug repositioning

全基因组关联研究 基因座(遗传学) 遗传关联 医学 遗传学 药物重新定位 基因 药品 生物信息学 生物 单核苷酸多态性 基因型 药理学
作者
Yongfei Wang,Yan Zhang,Zhengwei Zhu,Ting-You Wang,David Morris,Jiangshan Jane Shen,Huoru Zhang,Hai‐Feng Pan,Jing Yang,Sen Yang,Dong‐Qing Ye,Timothy J. Vyse,Yong Cui,Xuejun Zhang,Yujun Sheng,YL Lau,Wanling Yang
出处
期刊:Annals of the Rheumatic Diseases [BMJ]
卷期号:77 (7): 1078-1084 被引量:38
标识
DOI:10.1136/annrheumdis-2018-213093
摘要

Objectives Systemic lupus erythematosus (SLE) is a prototype autoimmune disease with a strong genetic component in its pathogenesis. Through genome-wide association studies (GWAS), we recently identified 10 novel loci associated with SLE and uncovered a number of suggestive loci requiring further validation. This study aimed to validate those loci in independent cohorts and evaluate the role of SLE genetics in drug repositioning. Methods We conducted GWAS and replication studies involving 12 280 SLE cases and 18 828 controls, and performed fine-mapping analyses to identify likely causal variants within the newly identified loci. We further scanned drug target databases to evaluate the role of SLE genetics in drug repositioning. Results We identified three novel loci that surpassed genome-wide significance, including ST3AGL4 (rs13238909, p meta =4.40E-08), MFHAS1 (rs2428, p meta =1.17E-08) and CSNK2A2 (rs2731783, p meta =1.08E-09). We also confirmed the association of CD226 locus with SLE (rs763361, p meta =2.45E-08). Fine-mapping and functional analyses indicated that the putative causal variants in CSNK2A2 locus reside in an enhancer and are associated with expression of CSNK2A2 in B-lymphocytes, suggesting a potential mechanism of association. In addition, we demonstrated that SLE risk genes were more likely to be interacting proteins with targets of approved SLE drugs (OR=2.41, p=1.50E-03) which supports the role of genetic studies to repurpose drugs approved for other diseases for the treatment of SLE. Conclusion This study identified three novel loci associated with SLE and demonstrated the role of SLE GWAS findings in drug repositioning.
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