Cross-Phenotype GWAS Supports Shared Genetic Susceptibility to Systemic Sclerosis and Primary Biliary Cholangitis

Yiming Luo, Atlas Khan, Lili Liu, Cue Hyunkyu Lee, Gabriel J. Perreault, Sydney F. Pomenti, Pravitt Gourh, Krzysztof Kiryluk, Elana J. Bernstein
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Abstract

Objective An increased risk of primary biliary cholangitis (PBC) has been reported in patients with systemic sclerosis (SSc). Our study aims to investigate the shared genetic susceptibility between the two disorders and to define candidate causal genes using cross-phenotype GWAS meta-analysis. Methods We performed cross-phenotype GWAS meta-analysis and colocalization analysis for SSc and PBC. We performed both genome-wide and locus-based analysis, including tissue and pathway enrichment analyses, fine-mapping, colocalization analyses with expression quantitative trait loci (eQTL) and protein quantitative trait loci (pQTL) datasets, and phenome-wide association studies (PheWAS). Finally, we used an integrative approach to prioritize candidate causal genes from the novel loci. Results We detected a strong genetic correlation between SSc and PBC (rg = 0.84, p = 1.7 x 10-6). In the cross-phenotype GWAS meta-analysis, we identified 44 non-HLA loci that reached genome-wide significance (p < 5 x 10-8). Evidence of shared causal variants between SSc and PBC was found for nine loci, five of which were novel. Integrating multiple sources of evidence, we prioritized CD40, ERAP1, PLD4, SPPL3, and CCDC113 as novel candidate causal genes. The CD40 risk locus colocalized with trans-pQTLs of multiple plasma proteins involved in B cell function. Conclusion Our study supports a strong shared genetic susceptibility between SSc and PBC. Through cross-phenotype analyses, we have prioritized several novel candidate causal genes and pathways for these disorders.
交叉表型 GWAS 证实系统性硬化症和原发性胆汁性胆管炎具有共同的遗传易感性
目的 据报道,系统性硬化症(SSc)患者患原发性胆汁性胆管炎(PBC)的风险增加。我们的研究旨在调查这两种疾病之间的共同遗传易感性,并通过跨表型 GWAS meta 分析确定候选致病基因。方法我们对 SSc 和 PBC 进行了跨表型 GWAS meta 分析和共定位分析。我们进行了全基因组分析和基于位点的分析,包括组织和通路富集分析、精细图谱分析、与表达定量性状位点(eQTL)和蛋白质定量性状位点(pQTL)数据集的共定位分析以及全表型关联研究(PheWAS)。最后,我们采用综合方法从新的基因座中筛选出候选因果基因。结果我们发现 SSc 和 PBC 之间存在很强的遗传相关性(rg = 0.84,p = 1.7 x 10-6)。在跨表型 GWAS 的荟萃分析中,我们确定了 44 个非 HLA 基因位点达到了全基因组显著性(p < 5 x 10-8)。在 9 个基因位点上发现了 SSc 和 PBC 之间共享因果变异的证据,其中 5 个是新发现的。综合多种证据来源,我们优先选择了 CD40、ERAP1、PLD4、SPPL3 和 CCDC113 作为新的候选致病基因。CD40 风险位点与涉及 B 细胞功能的多种血浆蛋白的反式-pQTLs 共同定位。结论我们的研究支持 SSc 和 PBC 之间存在很强的共同遗传易感性。通过交叉表型分析,我们优先确定了这两种疾病的几个新的候选致病基因和通路。
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