NMR metabolomics-guided DNA methylation mortality predictors

Daniele Bizzarri; Marcel J. T. Reinders; Lieke Kuiper; Marian Beekman; Joris Deelen; Joyce B. J. van Meurs; Jenny van Dongen; René Pool; Dorret I. Boomsma; Mohsen Ghanbari; BBMRI Consortium

doi:10.1016/j.ebiom.2024.105279

NMR metabolomics-guided DNA methylation mortality predictors

Daniele Bizzarri
, Marcel J. T. Reinders
, Lieke Kuiper
, Marian Beekman
, Joris Deelen
, Joyce B. J. van Meurs
, Jenny van Dongen
, René Pool
, Dorret I. Boomsma
, Mohsen Ghanbari
, BBMRI Consortium

Leiden University
Delft University of Technology
Erasmus University Rotterdam
National Institute of Public Health and the Environment
Max Planck Institute for Biology of Ageing
University of Cologne
Vrije Universiteit Amsterdam
Amsterdam UMC
University of Groningen

Research output: Contribution to journal › Article › Academic › peer-review

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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.

Original language	English
Article number	105279
Journal	EBioMedicine
Volume	107
DOIs	https://doi.org/10.1016/j.ebiom.2024.105279
Publication status	Published - 1 Sept 2024

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Ageing biomarkers
DNA methylation predictors
Epidemiology
Epigenetic clock
Metabolic risk score
NMR metabolomics

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10.1016/j.ebiom.2024.105279

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@article{f132c2335d23411f9a5dd1192447859e,

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.",

keywords = "Ageing biomarkers, DNA methylation predictors, Epidemiology, Epigenetic clock, Metabolic risk score, NMR metabolomics",

author = "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 \{BBMRI Consortium\} 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.\} and N. Sattar and \{van der Horst\}, \{I. C. C.\} and \{van der Harst\}, P. and C. So-Osman and \{van Hilten\}, \{J. A.\} and Nelissen, \{R. G. H. H.\} and H{\"o}fer, \{I. E.\} and Asselbergs, \{F. W.\} and P. Scheltens and Teunissen, \{C. E.\} and \{van der Flier\}, \{W. M.\} and \{van Dongen\}, J. and R. Pool and Willemsen, \{A. H. M.\} and Boomsma, \{D. I.\} and Suchiman, \{H. E. D.\} and \{Barkey Wolf\}, \{J. J. H.\} and D. Cats and H. Mei and M. Slofstra and M. Swertz and Reinders, \{M. J. T.\} and \{van den Akker\}, \{E. B.\} and Slagboom, \{Pieternella E.\} and \{van den Akker\}, \{Erik B.\}",

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

year = "2024",

month = sep,

day = "1",

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

language = "English",

volume = "107",

journal = "EBioMedicine",

issn = "2352-3964",

publisher = "Elsevier B.V.",

}

TY - JOUR

T1 - NMR metabolomics-guided DNA methylation mortality predictors

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 - BBMRI Consortium

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.

AU - Sattar, N.

AU - van der Horst, I. C. C.

AU - van der Harst, P.

AU - So-Osman, C.

AU - van Hilten, J. A.

AU - Nelissen, R. G. H. H.

AU - Höfer, I. E.

AU - Asselbergs, F. W.

AU - Scheltens, P.

AU - Teunissen, C. E.

AU - van der Flier, W. M.

AU - van Dongen, J.

AU - Pool, R.

AU - Willemsen, A. H. M.

AU - Boomsma, D. I.

AU - Suchiman, H. E. D.

AU - Barkey Wolf, J. J. H.

AU - Cats, D.

AU - Mei, H.

AU - Slofstra, M.

AU - Swertz, M.

AU - Reinders, M. J. T.

AU - van den Akker, E. B.

AU - Slagboom, Pieternella E.

AU - van den Akker, Erik B.

PY - 2024/9/1

Y1 - 2024/9/1

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.

KW - Ageing biomarkers

KW - DNA methylation predictors

KW - Epidemiology

KW - Epigenetic clock

KW - Metabolic risk score

KW - NMR metabolomics

UR - https://www.scopus.com/pages/publications/85201444255

U2 - 10.1016/j.ebiom.2024.105279

DO - 10.1016/j.ebiom.2024.105279

M3 - Article

C2 - 39154540

SN - 2352-3964

VL - 107

JO - EBioMedicine

JF - EBioMedicine

M1 - 105279

ER -

NMR metabolomics-guided DNA methylation mortality predictors

Abstract

UN SDGs

Keywords

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