NMR metabolomics-guided DNA methylation mortality predictors

BBMRI Consortium

doi:10.1016/j.ebiom.2024.105279

NMR metabolomics-guided DNA methylation mortality predictors

BBMRI Consortium

Mailman School of Public Health

Résultat de recherche › examen par les pairs

Résumé

Background: ¹H-NMR metabolomics and DNA methylation in blood are widely known biomarkers predicting age-related physiological decline and mortality yet exert mutually independent mortality and frailty signals. Methods: Leveraging multi-omics data in four Dutch population studies (N = 5238, ∼40% of which male) we investigated whether the mortality signal captured by ¹H-NMR metabolomics could guide the construction of DNA methylation-based mortality predictors. Findings: We trained DNA methylation-based surrogates for 64 metabolomic analytes and found that analytes marking inflammation, fluid balance, or HDL/VLDL metabolism could be accurately reconstructed using DNA-methylation assays. Interestingly, a previously reported multi-analyte score indicating mortality risk (MetaboHealth) could also be accurately reconstructed. Sixteen of our derived surrogates, including the MetaboHealth surrogate, showed significant associations with mortality, independent of relevant covariates. Interpretation: The addition of our metabolic analyte-derived surrogates to the well-established epigenetic clock GrimAge demonstrates that our surrogates potentially represent valuable mortality signal. Funding: BBMRI-NL, X-omics, VOILA, Medical Delta, NWO, ERC.

Langue d'origine	English
Numéro d'article	105279
Journal	eBioMedicine
Volume	107
DOI	https://doi.org/10.1016/j.ebiom.2024.105279
Statut de publication	Published - sept. 2024

ASJC Scopus Subject Areas

General Biochemistry,Genetics and Molecular Biology

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10.1016/j.ebiom.2024.105279

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@article{4cfcd5a738ff4161bcdee3e6c387f1aa,

title = "NMR metabolomics-guided DNA methylation mortality predictors",

abstract = "Background: 1H-NMR metabolomics and DNA methylation in blood are widely known biomarkers predicting age-related physiological decline and mortality yet exert mutually independent mortality and frailty signals. Methods: Leveraging multi-omics data in four Dutch population studies (N = 5238, ∼40% of which male) we investigated whether the mortality signal captured by 1H-NMR metabolomics could guide the construction of DNA methylation-based mortality predictors. Findings: We trained DNA methylation-based surrogates for 64 metabolomic analytes and found that analytes marking inflammation, fluid balance, or HDL/VLDL metabolism could be accurately reconstructed using DNA-methylation assays. Interestingly, a previously reported multi-analyte score indicating mortality risk (MetaboHealth) could also be accurately reconstructed. Sixteen of our derived surrogates, including the MetaboHealth surrogate, showed significant associations with mortality, independent of relevant covariates. Interpretation: The addition of our metabolic analyte-derived surrogates to the well-established epigenetic clock GrimAge demonstrates that our surrogates potentially represent valuable mortality signal. Funding: BBMRI-NL, X-omics, VOILA, Medical Delta, NWO, ERC.",

author = "{BBMRI Consortium} and Daniele Bizzarri and Reinders, {Marcel J.T.} and Lieke Kuiper and Marian Beekman and Joris Deelen and {van Meurs}, {Joyce B.J.} and {van Dongen}, Jenny and Ren{\'e} Pool and Boomsma, {Dorret I.} and Mohsen Ghanbari and Lude Franke and Geleijnse, {J. M.} and E. Boersma and {van Spil}, {W. E.} and {van Greevenbroek}, {M. M.J.} and Stehouwer, {C. D.A.} and {van der Kallen}, {C. J.H.} and Arts, {I. C.W.} and F. Rutters and Beulens, {J. W.J.} and M. Muilwijk and Elders, {P. J.M.} and {'t Hart}, {L. M.} and M. Ghanbari and Ikram, {M. A.} and Netea, {M. G.} and M. Kloppenburg and Ramos, {Y. F.M.} and N. Bomer and I. Meulenbelt and K. Stronks and Snijder, {M. B.} and Zwinderman, {A. H.} and Heijmans, {B. T.} and Lumey, {L. H.} and C. Wijmenga and J. Fu and A. Zhernakova and J. Deelen and Mooijaart, {S. P.} and M. Beekman and Slagboom, {P. E.} and Onderwater, {G. L.J.} and {van den Maagdenberg}, {A. M.J.M.} and Terwindt, {G. M.} and C. Thesing and M. Bot and Penninx, {B. W.J.H.} and S. Trompet and Jukema, {J. W.}",

note = "Publisher Copyright: {\textcopyright} 2024 The Authors",

year = "2024",

month = sep,

doi = "10.1016/j.ebiom.2024.105279",

language = "English",

volume = "107",

journal = "eBioMedicine",

issn = "2352-3964",

publisher = "Elsevier BV",

}

TY - JOUR

T1 - NMR metabolomics-guided DNA methylation mortality predictors

AU - BBMRI Consortium

AU - Bizzarri, Daniele

AU - Reinders, Marcel J.T.

AU - Kuiper, Lieke

AU - Beekman, Marian

AU - Deelen, Joris

AU - van Meurs, Joyce B.J.

AU - van Dongen, Jenny

AU - Pool, René

AU - Boomsma, Dorret I.

AU - Ghanbari, Mohsen

AU - Franke, Lude

AU - Geleijnse, J. M.

AU - Boersma, E.

AU - van Spil, W. E.

AU - van Greevenbroek, M. M.J.

AU - Stehouwer, C. D.A.

AU - van der Kallen, C. J.H.

AU - Arts, I. C.W.

AU - Rutters, F.

AU - Beulens, J. W.J.

AU - Muilwijk, M.

AU - Elders, P. J.M.

AU - 't Hart, L. M.

AU - Ghanbari, M.

AU - Ikram, M. A.

AU - Netea, M. G.

AU - Kloppenburg, M.

AU - Ramos, Y. F.M.

AU - Bomer, N.

AU - Meulenbelt, I.

AU - Stronks, K.

AU - Snijder, M. B.

AU - Zwinderman, A. H.

AU - Heijmans, B. T.

AU - Lumey, L. H.

AU - Wijmenga, C.

AU - Fu, J.

AU - Zhernakova, A.

AU - Deelen, J.

AU - Mooijaart, S. P.

AU - Beekman, M.

AU - Slagboom, P. E.

AU - Onderwater, G. L.J.

AU - van den Maagdenberg, A. M.J.M.

AU - Terwindt, G. M.

AU - Thesing, C.

AU - Bot, M.

AU - Penninx, B. W.J.H.

AU - Trompet, S.

AU - Jukema, J. W.

PY - 2024/9

Y1 - 2024/9

N2 - Background: 1H-NMR metabolomics and DNA methylation in blood are widely known biomarkers predicting age-related physiological decline and mortality yet exert mutually independent mortality and frailty signals. Methods: Leveraging multi-omics data in four Dutch population studies (N = 5238, ∼40% of which male) we investigated whether the mortality signal captured by 1H-NMR metabolomics could guide the construction of DNA methylation-based mortality predictors. Findings: We trained DNA methylation-based surrogates for 64 metabolomic analytes and found that analytes marking inflammation, fluid balance, or HDL/VLDL metabolism could be accurately reconstructed using DNA-methylation assays. Interestingly, a previously reported multi-analyte score indicating mortality risk (MetaboHealth) could also be accurately reconstructed. Sixteen of our derived surrogates, including the MetaboHealth surrogate, showed significant associations with mortality, independent of relevant covariates. Interpretation: The addition of our metabolic analyte-derived surrogates to the well-established epigenetic clock GrimAge demonstrates that our surrogates potentially represent valuable mortality signal. Funding: BBMRI-NL, X-omics, VOILA, Medical Delta, NWO, ERC.

AB - Background: 1H-NMR metabolomics and DNA methylation in blood are widely known biomarkers predicting age-related physiological decline and mortality yet exert mutually independent mortality and frailty signals. Methods: Leveraging multi-omics data in four Dutch population studies (N = 5238, ∼40% of which male) we investigated whether the mortality signal captured by 1H-NMR metabolomics could guide the construction of DNA methylation-based mortality predictors. Findings: We trained DNA methylation-based surrogates for 64 metabolomic analytes and found that analytes marking inflammation, fluid balance, or HDL/VLDL metabolism could be accurately reconstructed using DNA-methylation assays. Interestingly, a previously reported multi-analyte score indicating mortality risk (MetaboHealth) could also be accurately reconstructed. Sixteen of our derived surrogates, including the MetaboHealth surrogate, showed significant associations with mortality, independent of relevant covariates. Interpretation: The addition of our metabolic analyte-derived surrogates to the well-established epigenetic clock GrimAge demonstrates that our surrogates potentially represent valuable mortality signal. Funding: BBMRI-NL, X-omics, VOILA, Medical Delta, NWO, ERC.

UR - http://www.scopus.com/inward/record.url?scp=85201444255&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85201444255&partnerID=8YFLogxK

U2 - 10.1016/j.ebiom.2024.105279

DO - 10.1016/j.ebiom.2024.105279

M3 - Article

C2 - 39154540

AN - SCOPUS:85201444255

SN - 2352-3964

VL - 107

JO - eBioMedicine

JF - eBioMedicine

M1 - 105279

ER -

NMR metabolomics-guided DNA methylation mortality predictors

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