Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome

BACKGROUND: Obesity and its associated diseases are major health problems characterized by extensive metabolic disturbances. Understanding the causal connections between these phenotypes and variation in metabolite levels can uncover relevant biology and inform novel intervention strategies. Recent...

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Autores principales: Hsu, Yu-Han H., Astley, Christina M., Cole, Joanne B., Vedantam, Sailaja, Mercader, Josep M., Metspalu, Andres, Fischer, Krista, Fortney, Kristen, Morgen, Eric K., Gonzalez, Clicerio, Gonzalez, Maria E., Esko, Tonu, Hirschhorn, Joel N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7332400/
https://www.ncbi.nlm.nih.gov/pubmed/32467615
http://dx.doi.org/10.1038/s41366-020-0603-x
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author Hsu, Yu-Han H.
Astley, Christina M.
Cole, Joanne B.
Vedantam, Sailaja
Mercader, Josep M.
Metspalu, Andres
Fischer, Krista
Fortney, Kristen
Morgen, Eric K.
Gonzalez, Clicerio
Gonzalez, Maria E.
Esko, Tonu
Hirschhorn, Joel N.
author_facet Hsu, Yu-Han H.
Astley, Christina M.
Cole, Joanne B.
Vedantam, Sailaja
Mercader, Josep M.
Metspalu, Andres
Fischer, Krista
Fortney, Kristen
Morgen, Eric K.
Gonzalez, Clicerio
Gonzalez, Maria E.
Esko, Tonu
Hirschhorn, Joel N.
author_sort Hsu, Yu-Han H.
collection PubMed
description BACKGROUND: Obesity and its associated diseases are major health problems characterized by extensive metabolic disturbances. Understanding the causal connections between these phenotypes and variation in metabolite levels can uncover relevant biology and inform novel intervention strategies. Recent studies have combined metabolite profiling with genetic instrumental variable (IV) analysis (Mendelian randomization) to infer the direction of causality between metabolites and obesity, but often omitted a large portion of untargeted profiling data consisting of unknown, unidentified metabolite signals. METHODS: We expanded upon previous research by identifying body mass index (BMI)-associated metabolites in multiple untargeted metabolomics datasets, and then performing bidirectional IV analysis to classify metabolites based on their inferred causal relationships with BMI. Meta-analysis and pathway analysis of both known and unknown metabolites across datasets were enabled by our recently developed bioinformatics suite, PAIRUP-MS. RESULTS: We identified 10 known metabolites that are more likely to be causes (e.g. alpha-hydroxybutyrate) or effects (e.g. valine) of BMI, or may have more complex bidirectional cause-effect relationships with BMI (e.g. glycine). Importantly, we also identified about 5 times more unknown than known metabolites in each of these three categories. Pathway analysis incorporating both known and unknown metabolites prioritized 40 enriched (p < 0.05) metabolite sets for the cause versus effect groups, providing further support that these two metabolite groups are linked to obesity via distinct biological mechanisms. CONCLUSIONS: These findings demonstrate the potential utility of our approach to uncover causal connections with obesity from untargeted metabolomics datasets. Combining genetically informed causal inference with the ability to map unknown metabolites across datasets provides a path to jointly analyze many untargeted datasets with obesity or other phenotypes. This approach, applied to larger datasets with genotype and untargeted metabolite data, should generate sufficient power for robust discovery and replication of causal biological connections between metabolites and various human diseases.
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spelling pubmed-73324002020-11-28 Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome Hsu, Yu-Han H. Astley, Christina M. Cole, Joanne B. Vedantam, Sailaja Mercader, Josep M. Metspalu, Andres Fischer, Krista Fortney, Kristen Morgen, Eric K. Gonzalez, Clicerio Gonzalez, Maria E. Esko, Tonu Hirschhorn, Joel N. Int J Obes (Lond) Article BACKGROUND: Obesity and its associated diseases are major health problems characterized by extensive metabolic disturbances. Understanding the causal connections between these phenotypes and variation in metabolite levels can uncover relevant biology and inform novel intervention strategies. Recent studies have combined metabolite profiling with genetic instrumental variable (IV) analysis (Mendelian randomization) to infer the direction of causality between metabolites and obesity, but often omitted a large portion of untargeted profiling data consisting of unknown, unidentified metabolite signals. METHODS: We expanded upon previous research by identifying body mass index (BMI)-associated metabolites in multiple untargeted metabolomics datasets, and then performing bidirectional IV analysis to classify metabolites based on their inferred causal relationships with BMI. Meta-analysis and pathway analysis of both known and unknown metabolites across datasets were enabled by our recently developed bioinformatics suite, PAIRUP-MS. RESULTS: We identified 10 known metabolites that are more likely to be causes (e.g. alpha-hydroxybutyrate) or effects (e.g. valine) of BMI, or may have more complex bidirectional cause-effect relationships with BMI (e.g. glycine). Importantly, we also identified about 5 times more unknown than known metabolites in each of these three categories. Pathway analysis incorporating both known and unknown metabolites prioritized 40 enriched (p < 0.05) metabolite sets for the cause versus effect groups, providing further support that these two metabolite groups are linked to obesity via distinct biological mechanisms. CONCLUSIONS: These findings demonstrate the potential utility of our approach to uncover causal connections with obesity from untargeted metabolomics datasets. Combining genetically informed causal inference with the ability to map unknown metabolites across datasets provides a path to jointly analyze many untargeted datasets with obesity or other phenotypes. This approach, applied to larger datasets with genotype and untargeted metabolite data, should generate sufficient power for robust discovery and replication of causal biological connections between metabolites and various human diseases. 2020-05-28 2020-07 /pmc/articles/PMC7332400/ /pubmed/32467615 http://dx.doi.org/10.1038/s41366-020-0603-x Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Hsu, Yu-Han H.
Astley, Christina M.
Cole, Joanne B.
Vedantam, Sailaja
Mercader, Josep M.
Metspalu, Andres
Fischer, Krista
Fortney, Kristen
Morgen, Eric K.
Gonzalez, Clicerio
Gonzalez, Maria E.
Esko, Tonu
Hirschhorn, Joel N.
Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
title Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
title_full Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
title_fullStr Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
title_full_unstemmed Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
title_short Integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
title_sort integrating untargeted metabolomics, genetically informed causal inference, and pathway enrichment to define the obesity metabolome
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7332400/
https://www.ncbi.nlm.nih.gov/pubmed/32467615
http://dx.doi.org/10.1038/s41366-020-0603-x
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