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Krumsiek, J. ; Suhre, K. ; Evans, A.M.* ; Mitchell, M.W.* ; Mohney, R.P.* ; Milburn, M.V.* ; Wägele, B. ; Römisch-Margl, W. ; Illig, T. ; Adamski, J. ; Gieger, C. ; Theis, F.J. ; Kastenmüller, G.

Mining the unknown: A systems approach to metabolite identification combining genetic and metabolic information.

PLoS Genet. 8:e1003005 (2012)
Verlagsversion PDF DOI PMC
Open Access Gold
Creative Commons Lizenzvertrag
Recent genome-wide association studies (GWAS) with metabolomics data linked genetic variation in the human genome to differences in individual metabolite levels. A strong relevance of this metabolic individuality for biomedical and pharmaceutical research has been reported. However, a considerable amount of the molecules currently quantified by modern metabolomics techniques are chemically unidentified. The identification of these "unknown metabolites" is still a demanding and intricate task, limiting their usability as functional markers of metabolic processes. As a consequence, previous GWAS largely ignored unknown metabolites as metabolic traits for the analysis. Here we present a systems-level approach that combines genome-wide association analysis and Gaussian graphical modeling with metabolomics to predict the identity of the unknown metabolites. We apply our method to original data of 517 metabolic traits, of which 225 are unknowns, and genotyping information on 655,658 genetic variants, measured in 1,768 human blood samples. We report previously undescribed genotype-metabotype associations for six distinct gene loci (SLC22A2, COMT, CYP3A5, CYP2C18, GBA3, UGT3A1) and one locus not related to any known gene (rs12413935). Overlaying the inferred genetic associations, metabolic networks, and knowledge-based pathway information, we derive testable hypotheses on the biochemical identities of 106 unknown metabolites. As a proof of principle, we experimentally confirm nine concrete predictions. We demonstrate the benefit of our method for the functional interpretation of previous metabolomics biomarker studies on liver detoxification, hypertension, and insulin resistance. Our approach is generic in nature and can be directly transferred to metabolomics data from different experimental platforms.
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Publikationstyp Artikel: Journalartikel
Dokumenttyp Wissenschaftlicher Artikel
Korrespondenzautor
Schlagwörter GENOME-WIDE ASSOCIATION; CHRONIC KIDNEY-DISEASE; BILIRUBIN LEVELS; RECONSTRUCTION; VARIANTS; BIOLOGY; COMMON; LOCUS; ACID; TOOL
ISSN (print) / ISBN 1553-7390
e-ISSN 1553-7404
Zeitschrift PLoS Genetics
Quellenangaben Band: 8, Heft: 10, Seiten: , Artikelnummer: e1003005 Supplement: ,
Verlag Public Library of Science (PLoS)
Nichtpatentliteratur Publikationen
Begutachtungsstatus Peer reviewed