Genome-Wide Association Study of Metabolic Traits Reveals Novel Gene-Metabolite-Disease Links

被引:69
|
作者
Rueedi, Rico [1 ,2 ]
Ledda, Mirko [3 ]
Nicholls, Andrew W. [4 ]
Salek, Reza M. [5 ,6 ,7 ]
Marques-Vidal, Pedro [8 ]
Morya, Edgard [9 ,10 ,11 ]
Sameshima, Koichi [12 ]
Montoliu, Ivan [13 ]
Da Silva, Laeticia [13 ]
Collino, Sebastiano [13 ]
Martin, Francois-Pierre [13 ]
Rezzi, Serge [13 ]
Steinbeck, Christoph [5 ]
Waterworth, Dawn M. [14 ]
Waeber, Gerard [15 ]
Vollenweider, Peter [15 ]
Beckmann, Jacques S. [1 ,2 ,16 ]
Le Coutre, Johannes [3 ,17 ]
Mooser, Vincent [18 ]
Bergmann, Sven [1 ,2 ]
Genick, Ulrich K. [3 ]
Kutalik, Zoltan [1 ,2 ,8 ]
机构
[1] Univ Lausanne, Dept Med Genet, Lausanne, Switzerland
[2] Swiss Inst Bioinformat, Lausanne, Switzerland
[3] Nestle Res Ctr, Dept Food Consumer Interact, CH-1000 Lausanne, Switzerland
[4] GlaxoSmithKline R&D, Invest Preclin Toxicol, Ware, Herts, England
[5] European Bioinformat Inst, Cambridge, England
[6] Univ Cambridge, Dept Biochem, Cambridge CB2 1QW, England
[7] Univ Cambridge, Cambridge Syst Biol Ctr, Cambridge CB2 1QW, England
[8] Univ Lausanne, CHUV, Inst Social & Prevent Med IUMSP, Lausanne, Switzerland
[9] Alberto Santos Dumont Res Support Assoc, Senson Lab, Sao Paulo, Brazil
[10] Libanes Hosp, IEP Sirio, Sao Paulo, Brazil
[11] Edmond & Lily Safra Int Inst Neurosci Natal, Natal, RN, Brazil
[12] Univ Sao Paulo, Fac Med, Dept Radiol & Oncol, Sao Paulo, Brazil
[13] Nestle Res Ctr, Dept Bioanalyt Sci, CH-1000 Lausanne, Switzerland
[14] GlaxoSmithKline, Med Genet, Philadelphia, PA USA
[15] CHU Vaudois, Dept Med, Lausanne, Switzerland
[16] CHU Vaudois, Serv Med Genet, Lausanne, Switzerland
[17] Univ Tokyo, Org Interdisciplinary Res Projects, Bunkyo Ku, Tokyo, Japan
[18] CHU Vaudois, Dept Med, Lausanne, Switzerland
来源
PLOS GENETICS | 2014年 / 10卷 / 02期
基金
瑞士国家科学基金会;
关键词
MENDELIAN RANDOMIZATION; CROHN DISEASE; MOUSE MODEL; LOCI; POLYMORPHISM; PHENOTYPES;
D O I
10.1371/journal.pgen.1004132
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Author Summary The concentrations of small molecules known as metabolites, are subject to tight regulation in all organisms. Collectively, the metabolite concentrations make up the metabolome, which differs amongst individuals as a function of their environment and genetic makeup. In our study, we have further developed an untargeted approach to identify genetic factors affecting human metabolism. In this approach, we first identify all genetic variants that correlate with any of the measured metabolome features in a large set of individuals. For these variants, we then compute a profile of significance for association with all features, generating a signature that facilitates the expert or computational identification of the metabolite whose concentration is most likely affected by the genetic variant at hand. Our study replicated many of the previously reported genetically driven variations in human metabolism and revealed two new striking examples of genetic variations with a sizeable effect on the urine metabolome. Interestingly, in these two gene-metabolite pairs both the gene and the affected metabolite are related to human diseases - Crohn's disease in the first case, and kidney disease in the second. This highlights the connection between genetic predispositions, affected metabolites, and human health. Metabolic traits are molecular phenotypes that can drive clinical phenotypes and may predict disease progression. Here, we report results from a metabolome- and genome-wide association study on H-1-NMR urine metabolic profiles. The study was conducted within an untargeted approach, employing a novel method for compound identification. From our discovery cohort of 835 Caucasian individuals who participated in the CoLaus study, we identified 139 suggestively significant (P<5x10(-8)) and independent associations between single nucleotide polymorphisms (SNP) and metabolome features. Fifty-six of these associations replicated in the TasteSensomics cohort, comprising 601 individuals from Sao Paulo of vastly diverse ethnic background. They correspond to eleven gene-metabolite associations, six of which had been previously identified in the urine metabolome and three in the serum metabolome. Our key novel findings are the associations of two SNPs with NMR spectral signatures pointing to fucose (rs492602, P = 6.9x10(-44)) and lysine (rs8101881, P = 1.2x10(-33)), respectively. Fine-mapping of the first locus pinpointed the FUT2 gene, which encodes a fucosyltransferase enzyme and has previously been associated with Crohn's disease. This implicates fucose as a potential prognostic disease marker, for which there is already published evidence from a mouse model. The second SNP lies within the SLC7A9 gene, rare mutations of which have been linked to severe kidney damage. The replication of previous associations and our new discoveries demonstrate the potential of untargeted metabolomics GWAS to robustly identify molecular disease markers.
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页数:10
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