胰腺表达定量性状基因座（eQTLs）与酒精性和新型非酒精性慢性胰腺炎全基因组关联研究（GWAS）风险位点的共定位分析提示了潜在的致病机制。

Colocalization analysis of pancreas eQTLs with risk loci from alcoholic and novel non-alcoholic chronic pancreatitis GWAS suggests potential disease causing mechanisms.

作者信息

Schmidt Andreas W, Kühnapfel Andreas, Kirsten Holger, Grallert Harald, Hellerbrand Claus, Kiefer Falk, Mann Karl, Mueller Sebastian, Nöthen Markus M, Peters Annette, Ridinger Monika, Frank Josef, Rietschel Marcella, Soranzo Nicole, Soyka Michael, Wodarz Norbert, Malerba Giovanni, Gambaro Giovanni, Gieger Christian, Scholz Markus, Krug Sebastian, Michl Patrick, Ewers Maren, Witt Heiko, Laumen Helmut, Rosendahl Jonas

机构信息

Department of Internal Medicine I, Martin-Luther-University Halle-Wittenberg, Halle, Saale, Germany; Else Kröner-Fresenius-Zentrum für Ernährungsmedizin (EKFZ), Paediatric Nutritional Medicine, Technische Universität München (TUM), Freising, Germany.

Institute for Medical Informatics, Statistics and Epidemiology, University of Leipzig, Leipzig, Germany; LIFE- Leipzig Research Center for Civilization Diseases, University of Leipzig, Leipzig, Germany.

出版信息

Pancreatology. 2022 May;22(4):449-456. doi: 10.1016/j.pan.2022.03.007. Epub 2022 Mar 11.

DOI:10.1016/j.pan.2022.03.007

PMID:35331647

Abstract

BACKGROUND

Previous genome-wide association studies (GWAS) identified genome-wide significant risk loci in chronic pancreatitis and investigated underlying disease causing mechanisms by simple overlaps with expression quantitative trait loci (eQTLs), a procedure which may often result in false positive conclusions.

METHODS

We conducted a GWAS in 584 non-alcoholic chronic pancreatitis (NACP) patients and 6040 healthy controls. Next, we applied Bayesian colocalization analysis of identified genome-wide significant risk loci from both, our recently published alcoholic chronic pancreatitis (ACP) and the novel NACP dataset, with pancreas eQTLs from the GTEx V8 European cohort to prioritize candidate causal genes and extracted credible sets of shared causal variants.

RESULTS

Variants at the CTRC (p = 1.22 × 10) and SPINK1 (p = 6.59 × 10) risk loci reached genome-wide significance in NACP. CTRC risk variants colocalized with CTRC eQTLs in ACP (PP4 = 0.99, PP4/PP3 = 95.51) and NACP (PP4 = 0.99, PP4/PP3 = 95.46). For both diseases, the 95% credible set of shared causal variants consisted of rs497078 and rs545634. CLDN2-MORC4 risk variants colocalized with CLDN2 eQTLs in ACP (PP4 = 0.98, PP4/PP3 = 42.20) and NACP (PP4 = 0.67, PP4/PP3 = 7.18), probably driven by the shared causal variant rs12688220.

CONCLUSIONS

A shared causal CTRC risk variant might unfold its pathogenic effect in ACP and NACP by reducing CTRC expression, while the CLDN2-MORC4 shared causal variant rs12688220 may modify ACP and NACP risk by increasing CLDN2 expression.

摘要

背景

既往全基因组关联研究（GWAS）在慢性胰腺炎中鉴定出全基因组显著风险位点，并通过与表达数量性状位点（eQTL）进行简单重叠来研究潜在的致病机制，该过程往往会得出假阳性结论。

方法

我们对584例非酒精性慢性胰腺炎（NACP）患者和6040例健康对照进行了GWAS。接下来，我们对最近发表的酒精性慢性胰腺炎（ACP）和新的NACP数据集中鉴定出的全基因组显著风险位点，与GTEx V8欧洲队列的胰腺eQTL进行贝叶斯共定位分析，以确定候选因果基因的优先级，并提取共享因果变异的可信集。

结果

CTRC（p = 1.22×10）和SPINK1（p = 6.59×10）风险位点的变异在NACP中达到全基因组显著性。CTRC风险变异在ACP（PP4 = 0.99, PP4/PP3 = 95.51）和NACP（PP4 = 0.99, PP4/PP3 = 95.46）中与CTRC eQTL共定位。对于这两种疾病，共享因果变异的95%可信集由rs497078和rs545634组成。CLDN2-MORC4风险变异在ACP（PP4 = 0.98, PP4/PP3 = 42.20）和NACP（PP4 = 0.67, PP4/PP3 = 7.18）中与CLDN2 eQTL共定位，可能由共享因果变异rs12688220驱动。