Genome-Wide Association Study for Alcohol-Related Cirrhosis Identifies Risk Loci in MARC1 and HNRNPUL1

被引:51
|
作者
Innes, Hamish [1 ,2 ,3 ]
Buch, Stephan [4 ]
Hutchinson, Sharon [1 ,3 ]
Guha, Indra Neil [5 ,6 ]
Morling, Joanne R. [2 ,5 ,6 ]
Barnes, Eleanor [7 ,8 ]
Irving, Will [5 ,6 ]
Forrest, Ewan [9 ]
Pedergnana, Vincent [10 ]
Goldberg, David [1 ,3 ]
Aspinall, Esther [1 ,3 ]
Barclay, Stephan [9 ]
Hayes, Peter C. [11 ]
Dillon, John [12 ]
Nischalke, Hans Dieter [13 ]
Lutz, Philipp [13 ]
Spengler, Ulrich [13 ]
Fischer, Janett [14 ]
Berg, Thomas [14 ]
Brosch, Mario [4 ]
Eyer, Florian [15 ]
Datz, Christian [16 ]
Mueller, Sebastian [17 ,18 ]
Peccerella, Teresa [17 ,18 ]
Deltenre, Pierre [19 ]
Marot, Astrid [19 ]
Soyka, Michael [20 ,21 ]
McQuillin, Andrew [22 ]
Morgan, Marsha Y. [23 ]
Hampe, Jochen [4 ]
Stickel, Felix [24 ]
机构
[1] Glasgow Caledonian Univ, Sch Hlth & Life Sci, Glasgow, Lanark, Scotland
[2] Univ Nottingham, Div Epidemiol & Publ Hlth, Nottingham, England
[3] Hlth Protect Scotland, Glasgow, Lanark, Scotland
[4] Tech Univ Dresden, Univ Hosp Dresden, Med Dept 1, Dresden, Germany
[5] Nottingham Univ Hosp Natl Hlth Serv Trust, Natl Inst Hlth Res Nottingham Biomed Res Ctr, Nottingham, England
[6] Univ Nottingham, Natl Inst Hlth Res Nottingham Biomed Res Ctr, Nottingham, England
[7] Univ Oxford, Peter Medawar Bldg Pathogen Res, Nuffield Dept Med, Oxford, England
[8] Univ Oxford, Oxford Natl Inst Hlth Res Biomed Res Ctr, Nuffield Dept Med, Oxford, England
[9] Glasgow Royal Infirm, Glasgow, Lanark, Scotland
[10] UM, UMR CNRS 5290, UR IRD 224, Lab Malad Infect & Vecteurs Ecol Genet Evolut & C, Montpellier, France
[11] Royal Infirm Edinburgh NHS Trust, Edinburgh, Midlothian, Scotland
[12] Univ Dundee, Sch Med, Dundee, Scotland
[13] Univ Bonn, Dept Internal Med 1, Bonn, Germany
[14] Leipzig Univ Med Ctr, Dept Med 2, Div Hepatol, Leipzig, Germany
[15] Tech Univ Munich, Dept Clin Toxicol, Klinikum Rechts Isar, Munich, Germany
[16] Teaching Hosp Paracelsus Private Med Univ Salzbur, Hosp Oberndorf, Dept Internal Med, Oberndorf, Austria
[17] Salem Med Ctr Univ Hosp Heidelberg, Dept Internal Med, Heidelberg, Germany
[18] Salem Med Ctr Univ Hosp Heidelberg, Ctr Alcohol Res, Heidelberg, Germany
[19] Univ Lausanne, Ctr Hosp Univ Vaudois, Div Gastroenterol & Hepatol, Lausanne, Switzerland
[20] Univ Munich, Psychiat Hosp, Munich, Switzerland
[21] Meiringen Hosp, Dept Psychiat, Meiringen, Switzerland
[22] UCL, Div Psychiat, Mol Psychiat Lab, London, England
[23] UCL, Univ Coll London Inst Liver & Digest Hlth, Div Med, Royal Free Campus, London, England
[24] Univ Hosp Zurich, Dept Gastroenterol & Hepatol, Zurich, Switzerland
来源
GASTROENTEROLOGY | 2020年 / 159卷 / 04期
基金
英国医学研究理事会; 瑞士国家科学基金会;
关键词
Biomarker; Hepatic Fibrogenesis; Prognostic Factor; SNP; LIVER-DISEASE; GENETIC PREDISPOSITION; END-POINTS; BETA; EXPRESSION; MORTALITY; DIAGNOSIS; BURDEN; PNPLA3; UK;
D O I
10.1053/j.gastro.2020.06.014
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
BACKGROUND AND AIMS: Little is known about genetic factors that affect development of alcohol-related cirrhosis. We performed a genome-wide association study (GWAS) of samples from the United Kingdom Biobank (UKB) to identify polymorphisms associated with risk of alcohol-related liver disease. METHODS: We performed a GWAS of 35,839 participants in the UKB with high intake of alcohol against markers of hepatic fibrosis (FIB-4, APRI, and Forns index scores) and hepatocellular injury (levels of aminotransferases). Loci identified in the discovery analysis were tested for their association with alcohol-related cirrhosis in 3 separate European cohorts (phase 1 validation cohort; n=2545). Variants associated with alcohol-related cirrhosis in the validation at a false discovery rate of less than 20% were then directly genotyped in 2 additional European validation cohorts (phase 2 validation, n=2068). RESULTS: In the GWAS of the discovery cohort, we identified 50 independent risk loci with genome-wide significance (P < 5 x 10(-8)). Nine of these loci were significantly associated with alcohol-related cirrhosis in the phase 1 validation cohort; 6 of these 9 loci were significantly associated with alcohol-related cirrhosis in phase 2 validation cohort, at a false discovery rate below 5%. The loci included variants in the mitochondrial amidoxime reducing component 1 gene (MARC1) and the heterogeneous nuclear ribonucleoprotein U like 1 gene (HNRNPUL1). After we adjusted for age, sex, body mass index, and type-2 diabetes in the phase 2 validation cohort, the minor A allele of MARC1:rs2642438 was associated with reduced risk of alcohol-related cirrhosis (adjusted odds ratio, 0.76; P=.0027); conversely, the minor C allele of HNRNPUL1:rs15052 was associated with an increased risk of alcohol-related cirrhosis (adjusted odds ratio, 1.30; P=.020). CONCLUSIONS: In a GWAS of samples from the UKB, we identified and validated (in 5 European cohorts) single-nucleotide polymorphisms that affect risk of alcohol-related cirrhosis in opposite directions: the minor A allele in MARC1:rs2642438 decreases risk, whereas the minor C allele in HNRNPUL1:rs15052 increases risk.
引用
收藏
页码:1276 / +
页数:21
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