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Automated pathway and reaction prediction facilitates in silico identification of unknown metabolites in human cohort studies

Quell, Jan D. ; Römisch-Margl, Werner ; Colombo, Marco ; Krumsiek, Jan ; Evans, Anne M. ; Mohney, Robert ; Salomaa, Veikko ; De Faire, Ulf ; Groop, Leif C. LU and Agakov, Felix , et al. (2017) In Journal of Chromatography B: Analytical Technologies in the Biomedical and Life Sciences 1071. p.58-67
Abstract

Identification of metabolites in non-targeted metabolomics continues to be a bottleneck in metabolomics studies in large human cohorts. Unidentified metabolites frequently emerge in the results of association studies linking metabolite levels to, for example, clinical phenotypes. For further analyses these unknown metabolites must be identified. Current approaches utilize chemical information, such as spectral details and fragmentation characteristics to determine components of unknown metabolites. Here, we propose a systems biology model exploiting the internal correlation structure of metabolite levels in combination with existing biochemical and genetic information to characterize properties of unknown molecules.Levels of 758... (More)

Identification of metabolites in non-targeted metabolomics continues to be a bottleneck in metabolomics studies in large human cohorts. Unidentified metabolites frequently emerge in the results of association studies linking metabolite levels to, for example, clinical phenotypes. For further analyses these unknown metabolites must be identified. Current approaches utilize chemical information, such as spectral details and fragmentation characteristics to determine components of unknown metabolites. Here, we propose a systems biology model exploiting the internal correlation structure of metabolite levels in combination with existing biochemical and genetic information to characterize properties of unknown molecules.Levels of 758 metabolites (439 known, 319 unknown) in human blood samples of 2279 subjects were measured using a non-targeted metabolomics platform (LC-MS and GC-MS). We reconstructed the structure of biochemical pathways that are imprinted in these metabolomics data by building an empirical network model based on 1040 significant partial correlations between metabolites. We further added associations of these metabolites to 134 genes from genome-wide association studies as well as reactions and functional relations to genes from the public database Recon 2 to the network model. From the local neighborhood in the network, we were able to predict the pathway annotation of 180 unknown metabolites. Furthermore, we classified 100 pairs of known and unknown and 45 pairs of unknown metabolites to 21 types of reactions based on their mass differences. As a proof of concept, we then looked further into the special case of predicted dehydrogenation reactions leading us to the selection of 39 candidate molecules for 5 unknown metabolites. Finally, we could verify 2 of those candidates by applying LC-MS analyses of commercially available candidate substances. The formerly unknown metabolites X-13891 and X-13069 were shown to be 2-dodecendioic acid and 9-tetradecenoic acid, respectively.Our data-driven approach based on measured metabolite levels and genetic associations as well as information from public resources can be used alone or together with methods utilizing spectral patterns as a complementary, automated and powerful method to characterize unknown metabolites.

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organization
publishing date
type
Contribution to journal
publication status
published
subject
keywords
Biochemical pathway prediction, Metabolic network reconstruction, Metabolite identification, Non-targeted metabolomics, Reaction prediction
in
Journal of Chromatography B: Analytical Technologies in the Biomedical and Life Sciences
volume
1071
pages
58 - 67
publisher
Elsevier
external identifiers
  • scopus:85018979296
  • pmid:28479069
ISSN
1570-0232
DOI
10.1016/j.jchromb.2017.04.002
language
English
LU publication?
yes
id
3217e453-75f4-46a7-beb9-a233a19f5d80
date added to LUP
2017-06-07 13:43:11
date last changed
2024-05-12 15:11:00
@article{3217e453-75f4-46a7-beb9-a233a19f5d80,
  abstract     = {{<p>Identification of metabolites in non-targeted metabolomics continues to be a bottleneck in metabolomics studies in large human cohorts. Unidentified metabolites frequently emerge in the results of association studies linking metabolite levels to, for example, clinical phenotypes. For further analyses these unknown metabolites must be identified. Current approaches utilize chemical information, such as spectral details and fragmentation characteristics to determine components of unknown metabolites. Here, we propose a systems biology model exploiting the internal correlation structure of metabolite levels in combination with existing biochemical and genetic information to characterize properties of unknown molecules.Levels of 758 metabolites (439 known, 319 unknown) in human blood samples of 2279 subjects were measured using a non-targeted metabolomics platform (LC-MS and GC-MS). We reconstructed the structure of biochemical pathways that are imprinted in these metabolomics data by building an empirical network model based on 1040 significant partial correlations between metabolites. We further added associations of these metabolites to 134 genes from genome-wide association studies as well as reactions and functional relations to genes from the public database Recon 2 to the network model. From the local neighborhood in the network, we were able to predict the pathway annotation of 180 unknown metabolites. Furthermore, we classified 100 pairs of known and unknown and 45 pairs of unknown metabolites to 21 types of reactions based on their mass differences. As a proof of concept, we then looked further into the special case of predicted dehydrogenation reactions leading us to the selection of 39 candidate molecules for 5 unknown metabolites. Finally, we could verify 2 of those candidates by applying LC-MS analyses of commercially available candidate substances. The formerly unknown metabolites X-13891 and X-13069 were shown to be 2-dodecendioic acid and 9-tetradecenoic acid, respectively.Our data-driven approach based on measured metabolite levels and genetic associations as well as information from public resources can be used alone or together with methods utilizing spectral patterns as a complementary, automated and powerful method to characterize unknown metabolites.</p>}},
  author       = {{Quell, Jan D. and Römisch-Margl, Werner and Colombo, Marco and Krumsiek, Jan and Evans, Anne M. and Mohney, Robert and Salomaa, Veikko and De Faire, Ulf and Groop, Leif C. and Agakov, Felix and Looker, Helen C. and McKeigue, Paul M. and Colhoun, Helen M. and Kastenmüller, Gabi}},
  issn         = {{1570-0232}},
  keywords     = {{Biochemical pathway prediction; Metabolic network reconstruction; Metabolite identification; Non-targeted metabolomics; Reaction prediction}},
  language     = {{eng}},
  month        = {{04}},
  pages        = {{58--67}},
  publisher    = {{Elsevier}},
  series       = {{Journal of Chromatography B: Analytical Technologies in the Biomedical and Life Sciences}},
  title        = {{Automated pathway and reaction prediction facilitates in silico identification of unknown metabolites in human cohort studies}},
  url          = {{http://dx.doi.org/10.1016/j.jchromb.2017.04.002}},
  doi          = {{10.1016/j.jchromb.2017.04.002}},
  volume       = {{1071}},
  year         = {{2017}},
}