Genome-wide association analysis in Primary sclerosing cholangitis and ulcerative colitis identifies risk loci atGPR35andTCF4

全基因组关联研究 原发性硬化性胆管炎 优势比 溃疡性结肠炎 单核苷酸多态性 遗传关联 炎症性肠病 生物 遗传学 内科学 基因型 医学 疾病 基因
作者
David Ellinghaus,Trine Folseraas,Kristian Holm,Eva Ellinghaus,Espen Melum,Tobias Balschun,Jon K. Laerdahl,Alexey Shiryaev,Daniel Gotthardt,Tobias J. Weismüller,Christoph Schramm,Michael Wittig,Annika Bergquist,Einar S. Björnsson,Hanns–Ulrich Marschall,Morten Vatn,Andreas Teufel,Christian Rust,Christian Gieger,H‐Erich Wichmann
出处
期刊:Hepatology [Lippincott Williams & Wilkins]
卷期号:58 (3): 1074-1083 被引量:188
标识
DOI:10.1002/hep.25977
摘要

Approximately 60%-80% of patients with primary sclerosing cholangitis (PSC) have concurrent ulcerative colitis (UC). Previous genome-wide association studies (GWAS) in PSC have detected a number of susceptibility loci that also show associations in UC and other immune-mediated diseases. We aimed to systematically compare genetic associations in PSC with genotype data in UC patients with the aim of detecting new susceptibility loci for PSC. We performed combined analyses of GWAS for PSC and UC comprising 392 PSC cases, 987 UC cases, and 2,977 controls and followed up top association signals in an additional 1,012 PSC cases, 4,444 UC cases, and 11,659 controls. We discovered novel genome-wide significant associations with PSC at 2q37 [rs3749171 at G-protein-coupled receptor 35 ( GPR35 ); P = 3.0 × 10 −9 in the overall study population, combined odds ratio [OR] and 95% confidence interval [CI] of 1.39 (1.24-1.55)] and at 18q21 [rs1452787 at transcription factor 4 ( TCF4 ); P = 2.61 × 10 −8 , OR (95% CI) = 0.75 (0.68-0.83)]. In addition, several suggestive PSC associations were detected. The GPR35 rs3749171 is a missense single nucleotide polymorphism resulting in a shift from threonine to methionine. Structural modeling showed that rs3749171 is located in the third transmembrane helix of GPR35 and could possibly alter efficiency of signaling through the GPR35 receptor. Conclusion : By refining the analysis of a PSC GWAS by parallel assessments in a UC GWAS, we were able to detect two novel risk loci at genome-wide significance levels. GPR35 shows associations in both UC and PSC, whereas TCF4 represents a PSC risk locus not associated with UC. Both loci may represent previously unexplored aspects of PSC pathogenesis. (HEPATOLOGY 2013;58:1074–1083)
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