Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study

Ikenna C. Eze; Ayoung Jeong; Emmanuel Schaffner; Faisal I Rezwan; Akram Ghantous; Maria Foraster; Danielle Vienneau; Florian Kronenberg; Zdenko Herceg; Paolo Vineis; Mark Brink; Jean-Marc Wunderli; Christian Schindler; Christian Cajochen; Martin Roosli; John W. Holloway; Medea Imboden; Nicole Probst-Hensch

doi:10.1289/EHP6174

Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study

Ikenna C. Eze^*, Ayoung Jeong, Emmanuel Schaffner, Faisal I Rezwan, Akram Ghantous, Maria Foraster, Danielle Vienneau, Florian Kronenberg, Zdenko Herceg, Paolo Vineis, Mark Brink, Jean-Marc Wunderli, Christian Schindler, Christian Cajochen, Martin Roosli, John W. Holloway, Medea Imboden, Nicole Probst-Hensch

^*Corresponding author for this work

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

71 Citations (Scopus)

Abstract

Background:
Few epigenome-wide association studies (EWAS) on air pollutants exist, and none have been done on transportation noise exposures, which also contribute to environmental burden of disease.

Objective:
We performed mutually independent EWAS on transportation noise and air pollution exposures.

Methods:
We used data from two time points of the Swiss Cohort Study on Air Pollution and Lung and Heart Diseases in Adults (SAPALDIA) from 1,389 participants contributing 2,542 observations. We applied multiexposure linear mixed-effects regressions with participant-level random intercept to identify significant Cytosine-phosphate-Guanine (CpG) sites and differentially methylated regions (DMRs) in relation to 1-y average aircraft, railway, and road traffic day-evening-night noise (Lden); nitrogen dioxide (NO₂); and particulate matter (PM) with aerodynamic diameter <2.5μm (PM_2.5). We performed candidate (CpG-based; cross-systemic phenotypes, combined into “allostatic load”) and agnostic (DMR-based) pathway enrichment tests, and replicated previously reported air pollution EWAS signals.

Results:
We found no statistically significant CpGs at false discovery rate <0.05. However, 14, 48, 183, 8, and 71 DMRs independently associated with aircraft, railway, and road traffic Lden; NO₂; and PM_2.5, respectively, with minimally overlapping signals. Transportation Lden and air pollutants tendentially associated with decreased and increased methylation, respectively. We observed significant enrichment of candidate DNA methylation related to C-reactive protein and body mass index (aircraft, road traffic Lden, and PM_2.5), renal function and “allostatic load” (all exposures). Agnostic functional networks related to cellular immunity, gene expression, cell growth/proliferation, cardiovascular, auditory, embryonic, and neurological systems development were enriched. We replicated increased methylation in cg08500171 (NO₂) and decreased methylation in cg17629796 (PM_2.5).

Conclusions:
Mutually independent DNA methylation was associated with source-specific transportation noise and air pollution exposures, with distinct and shared enrichments for pathways related to inflammation, cellular development, and immune responses. These findings contribute in clarifying the pathways linking these exposures and age-related diseases but need further confirmation in the context of mediation analyses. https://doi.org/10.1289/EHP6174

Original language	English
Article number	067003
Journal	Environmental Health Perspectives
Volume	128
Issue number	6
DOIs	https://doi.org/10.1289/EHP6174
Publication status	Published - 01 Jun 2020
Externally published	Yes

Keywords

Adult
Air Pollutants
Air Pollution/statistics & numerical data
Aircraft
Cohort Studies
DNA
DNA Methylation/physiology
Environmental Exposure/statistics & numerical data
Female
Humans
Linear Models
Male
Middle Aged
Nitrogen Dioxide
Noise, Transportation/statistics & numerical data
Particulate Matter

UN SDGs

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

Access to Document

10.1289/EHP6174

Permanent link

Persistent link

Cite this

Eze, I. C., Jeong, A., Schaffner, E., Rezwan, F. I., Ghantous, A., Foraster, M., Vienneau, D., Kronenberg, F., Herceg, Z., Vineis, P., Brink, M., Wunderli, J.-M., Schindler, C., Cajochen, C., Roosli, M., Holloway, J. W., Imboden, M., & Probst-Hensch, N. (2020). Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study. Environmental Health Perspectives, 128(6), Article 067003. https://doi.org/10.1289/EHP6174

@article{b5b911ba98454100a80ebf7a9e0a95d7,

title = "Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study",

abstract = "Background:Few epigenome-wide association studies (EWAS) on air pollutants exist, and none have been done on transportation noise exposures, which also contribute to environmental burden of disease.Objective:We performed mutually independent EWAS on transportation noise and air pollution exposures.Methods:We used data from two time points of the Swiss Cohort Study on Air Pollution and Lung and Heart Diseases in Adults (SAPALDIA) from 1,389 participants contributing 2,542 observations. We applied multiexposure linear mixed-effects regressions with participant-level random intercept to identify significant Cytosine-phosphate-Guanine (CpG) sites and differentially methylated regions (DMRs) in relation to 1-y average aircraft, railway, and road traffic day-evening-night noise (Lden); nitrogen dioxide (NO2); and particulate matter (PM) with aerodynamic diameter <2.5μm (PM2.5). We performed candidate (CpG-based; cross-systemic phenotypes, combined into “allostatic load”) and agnostic (DMR-based) pathway enrichment tests, and replicated previously reported air pollution EWAS signals.Results:We found no statistically significant CpGs at false discovery rate <0.05. However, 14, 48, 183, 8, and 71 DMRs independently associated with aircraft, railway, and road traffic Lden; NO2; and PM2.5, respectively, with minimally overlapping signals. Transportation Lden and air pollutants tendentially associated with decreased and increased methylation, respectively. We observed significant enrichment of candidate DNA methylation related to C-reactive protein and body mass index (aircraft, road traffic Lden, and PM2.5), renal function and “allostatic load” (all exposures). Agnostic functional networks related to cellular immunity, gene expression, cell growth/proliferation, cardiovascular, auditory, embryonic, and neurological systems development were enriched. We replicated increased methylation in cg08500171 (NO2) and decreased methylation in cg17629796 (PM2.5).Conclusions:Mutually independent DNA methylation was associated with source-specific transportation noise and air pollution exposures, with distinct and shared enrichments for pathways related to inflammation, cellular development, and immune responses. These findings contribute in clarifying the pathways linking these exposures and age-related diseases but need further confirmation in the context of mediation analyses. https://doi.org/10.1289/EHP6174",

keywords = "Adult, Air Pollutants, Air Pollution/statistics \& numerical data, Aircraft, Cohort Studies, DNA, DNA Methylation/physiology, Environmental Exposure/statistics \& numerical data, Female, Humans, Linear Models, Male, Middle Aged, Nitrogen Dioxide, Noise, Transportation/statistics \& numerical data, Particulate Matter",

author = "Eze, \{Ikenna C.\} and Ayoung Jeong and Emmanuel Schaffner and Rezwan, \{Faisal I\} and Akram Ghantous and Maria Foraster and Danielle Vienneau and Florian Kronenberg and Zdenko Herceg and Paolo Vineis and Mark Brink and Jean-Marc Wunderli and Christian Schindler and Christian Cajochen and Martin Roosli and Holloway, \{John W.\} and Medea Imboden and Nicole Probst-Hensch",

note = "Funding Information: SAPALDIA is also supported by the Swiss Federal Office for the Environment; Federal Office of Public Health; the Federal Office of Roads and Transport; the canton{\textquoteright}s government of Aargau, Basel-Stadt, Basel-Land, Geneva, Luzern, Ticino, Valais, and Z{\"u}rich; the Swiss Lung League; the canton{\textquoteright}s Lung League of Basel Stadt/Basel Landschaft, Geneva, Ticino, Valais, Graub{\"u}nden and Zurich, Stiftung ehemals B{\"u}ndner Heilst{\"a}tten, SUVA, Freiwillige Akademische Gesellschaft; UBS Wealth Foundation; Talecris Biotherapeutics GmbH; Abbott Diagnostics; European Commission 018996 (GABRIEL); and Wellcome Trust WT 084703MA. MF. has received support of the Beatriu de Pin{\'o}s postdoctoral programme of the Government of Catalonia{\textquoteright}s Secretariat for Universities and Research of the Ministry of Economy and Knowledge. Funding Information: This work was supported by the Swiss National Science Foundation, SNF-SAPALDIA (grant numbers 33CS30-148470/1, 33CSCO-134276/1, 33CSCO-108796, 324730\_135673, 3247BO-104283, 3247BO-104288, 3247BO-104284, 3247-065896, 3100-059302, 3200-052720, 3200-042532, 4026-028099, PMPDP3\_129021/1, PMPDP3\_141671/1); SNF-SiRENE (grant number CRSII3\_147635); the European Commission Horizon 2020 research and innovation programme (ALEC study; grant number 633212); grant FP7 of the European Commission ?Enhanced exposure 36 assessment and-omic profiling for high priority environmental exposures in Europe? (EXPOsOMICS study; grant number 308610). SAPALDIA is also supported by the Swiss Federal Office for the Environment; Federal Office of Public Health; the Federal Office of Roads and Transport; the canton?s government of Aargau, Basel-Stadt, Basel-Land, Geneva, Luzern, Ticino, Valais, and Z?rich; the Swiss Lung League; the canton?s Lung League of Basel Stadt/Basel Landschaft, Geneva, Ticino, Valais, Graub?nden and Zurich, Stiftung ehemals B?ndner Heilst?tten, SUVA, Freiwillige Akademische Gesellschaft; UBS Wealth Foundation; Talecris Biotherapeutics GmbH; Abbott Diagnostics; European Commission 018996 (GABRIEL); and Wellcome Trust WT 084703MA. MF. has received support of the Beatriu de Pin?s postdoctoral programme of the Government of Catalonia?s Secretariat for Universities and Research of the Ministry of Economy and Knowledge. Where authors are identified as personnel of the International Agency for Research on Cancer/World Health Organization (WHO), the authors alone are responsible for the views expressed in this article, and they do not necessarily represent the decisions, policy, or views of the International Agency for Research on Cancer/WHO. Funding Information: This work was supported by the Swiss National Science Foundation, SNF-SAPALDIA (grant numbers 33CS30-148470/1, 33CSCO-134276/1, 33CSCO-108796, 324730\_135673, 3247BO-104283, 3247BO-104288, 3247BO-104284, 3247-065896, 3100-059302, 3200-052720, 3200-042532, 4026-028099, PMPDP3\_129021/1, PMPDP3\_141671/1); SNF-SiRENE (grant number CRSII3\_147635); the European Commission Horizon 2020 research and innovation programme (ALEC study; grant number 633212); grant FP7 of the European Commission “Enhanced exposure 36 assessment and -omic profiling for high priority environmental exposures in Europe” (EXPOsOMICS study; grant number 308610). Publisher Copyright: {\textcopyright} 2020, Public Health Services, US Dept of Health and Human Services. All rights reserved.",

year = "2020",

month = jun,

day = "1",

doi = "10.1289/EHP6174",

language = "English",

volume = "128",

journal = "Environmental Health Perspectives",

publisher = "National Institute of Environmental Health Sciences",

number = "6",

}

Eze, IC, Jeong, A, Schaffner, E, Rezwan, FI, Ghantous, A, Foraster, M, Vienneau, D, Kronenberg, F, Herceg, Z, Vineis, P, Brink, M, Wunderli, J-M, Schindler, C, Cajochen, C, Roosli, M, Holloway, JW, Imboden, M & Probst-Hensch, N 2020, 'Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study', Environmental Health Perspectives, vol. 128, no. 6, 067003. https://doi.org/10.1289/EHP6174

TY - JOUR

T1 - Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study

AU - Eze, Ikenna C.

AU - Jeong, Ayoung

AU - Schaffner, Emmanuel

AU - Rezwan, Faisal I

AU - Ghantous, Akram

AU - Foraster, Maria

AU - Vienneau, Danielle

AU - Kronenberg, Florian

AU - Herceg, Zdenko

AU - Vineis, Paolo

AU - Brink, Mark

AU - Wunderli, Jean-Marc

AU - Schindler, Christian

AU - Cajochen, Christian

AU - Roosli, Martin

AU - Holloway, John W.

AU - Imboden, Medea

AU - Probst-Hensch, Nicole

N1 - Funding Information: SAPALDIA is also supported by the Swiss Federal Office for the Environment; Federal Office of Public Health; the Federal Office of Roads and Transport; the canton’s government of Aargau, Basel-Stadt, Basel-Land, Geneva, Luzern, Ticino, Valais, and Zürich; the Swiss Lung League; the canton’s Lung League of Basel Stadt/Basel Landschaft, Geneva, Ticino, Valais, Graubünden and Zurich, Stiftung ehemals Bündner Heilstätten, SUVA, Freiwillige Akademische Gesellschaft; UBS Wealth Foundation; Talecris Biotherapeutics GmbH; Abbott Diagnostics; European Commission 018996 (GABRIEL); and Wellcome Trust WT 084703MA. MF. has received support of the Beatriu de Pinós postdoctoral programme of the Government of Catalonia’s Secretariat for Universities and Research of the Ministry of Economy and Knowledge. Funding Information: This work was supported by the Swiss National Science Foundation, SNF-SAPALDIA (grant numbers 33CS30-148470/1, 33CSCO-134276/1, 33CSCO-108796, 324730_135673, 3247BO-104283, 3247BO-104288, 3247BO-104284, 3247-065896, 3100-059302, 3200-052720, 3200-042532, 4026-028099, PMPDP3_129021/1, PMPDP3_141671/1); SNF-SiRENE (grant number CRSII3_147635); the European Commission Horizon 2020 research and innovation programme (ALEC study; grant number 633212); grant FP7 of the European Commission ?Enhanced exposure 36 assessment and-omic profiling for high priority environmental exposures in Europe? (EXPOsOMICS study; grant number 308610). SAPALDIA is also supported by the Swiss Federal Office for the Environment; Federal Office of Public Health; the Federal Office of Roads and Transport; the canton?s government of Aargau, Basel-Stadt, Basel-Land, Geneva, Luzern, Ticino, Valais, and Z?rich; the Swiss Lung League; the canton?s Lung League of Basel Stadt/Basel Landschaft, Geneva, Ticino, Valais, Graub?nden and Zurich, Stiftung ehemals B?ndner Heilst?tten, SUVA, Freiwillige Akademische Gesellschaft; UBS Wealth Foundation; Talecris Biotherapeutics GmbH; Abbott Diagnostics; European Commission 018996 (GABRIEL); and Wellcome Trust WT 084703MA. MF. has received support of the Beatriu de Pin?s postdoctoral programme of the Government of Catalonia?s Secretariat for Universities and Research of the Ministry of Economy and Knowledge. Where authors are identified as personnel of the International Agency for Research on Cancer/World Health Organization (WHO), the authors alone are responsible for the views expressed in this article, and they do not necessarily represent the decisions, policy, or views of the International Agency for Research on Cancer/WHO. Funding Information: This work was supported by the Swiss National Science Foundation, SNF-SAPALDIA (grant numbers 33CS30-148470/1, 33CSCO-134276/1, 33CSCO-108796, 324730_135673, 3247BO-104283, 3247BO-104288, 3247BO-104284, 3247-065896, 3100-059302, 3200-052720, 3200-042532, 4026-028099, PMPDP3_129021/1, PMPDP3_141671/1); SNF-SiRENE (grant number CRSII3_147635); the European Commission Horizon 2020 research and innovation programme (ALEC study; grant number 633212); grant FP7 of the European Commission “Enhanced exposure 36 assessment and -omic profiling for high priority environmental exposures in Europe” (EXPOsOMICS study; grant number 308610). Publisher Copyright: © 2020, Public Health Services, US Dept of Health and Human Services. All rights reserved.

PY - 2020/6/1

Y1 - 2020/6/1

N2 - Background:Few epigenome-wide association studies (EWAS) on air pollutants exist, and none have been done on transportation noise exposures, which also contribute to environmental burden of disease.Objective:We performed mutually independent EWAS on transportation noise and air pollution exposures.Methods:We used data from two time points of the Swiss Cohort Study on Air Pollution and Lung and Heart Diseases in Adults (SAPALDIA) from 1,389 participants contributing 2,542 observations. We applied multiexposure linear mixed-effects regressions with participant-level random intercept to identify significant Cytosine-phosphate-Guanine (CpG) sites and differentially methylated regions (DMRs) in relation to 1-y average aircraft, railway, and road traffic day-evening-night noise (Lden); nitrogen dioxide (NO2); and particulate matter (PM) with aerodynamic diameter <2.5μm (PM2.5). We performed candidate (CpG-based; cross-systemic phenotypes, combined into “allostatic load”) and agnostic (DMR-based) pathway enrichment tests, and replicated previously reported air pollution EWAS signals.Results:We found no statistically significant CpGs at false discovery rate <0.05. However, 14, 48, 183, 8, and 71 DMRs independently associated with aircraft, railway, and road traffic Lden; NO2; and PM2.5, respectively, with minimally overlapping signals. Transportation Lden and air pollutants tendentially associated with decreased and increased methylation, respectively. We observed significant enrichment of candidate DNA methylation related to C-reactive protein and body mass index (aircraft, road traffic Lden, and PM2.5), renal function and “allostatic load” (all exposures). Agnostic functional networks related to cellular immunity, gene expression, cell growth/proliferation, cardiovascular, auditory, embryonic, and neurological systems development were enriched. We replicated increased methylation in cg08500171 (NO2) and decreased methylation in cg17629796 (PM2.5).Conclusions:Mutually independent DNA methylation was associated with source-specific transportation noise and air pollution exposures, with distinct and shared enrichments for pathways related to inflammation, cellular development, and immune responses. These findings contribute in clarifying the pathways linking these exposures and age-related diseases but need further confirmation in the context of mediation analyses. https://doi.org/10.1289/EHP6174

AB - Background:Few epigenome-wide association studies (EWAS) on air pollutants exist, and none have been done on transportation noise exposures, which also contribute to environmental burden of disease.Objective:We performed mutually independent EWAS on transportation noise and air pollution exposures.Methods:We used data from two time points of the Swiss Cohort Study on Air Pollution and Lung and Heart Diseases in Adults (SAPALDIA) from 1,389 participants contributing 2,542 observations. We applied multiexposure linear mixed-effects regressions with participant-level random intercept to identify significant Cytosine-phosphate-Guanine (CpG) sites and differentially methylated regions (DMRs) in relation to 1-y average aircraft, railway, and road traffic day-evening-night noise (Lden); nitrogen dioxide (NO2); and particulate matter (PM) with aerodynamic diameter <2.5μm (PM2.5). We performed candidate (CpG-based; cross-systemic phenotypes, combined into “allostatic load”) and agnostic (DMR-based) pathway enrichment tests, and replicated previously reported air pollution EWAS signals.Results:We found no statistically significant CpGs at false discovery rate <0.05. However, 14, 48, 183, 8, and 71 DMRs independently associated with aircraft, railway, and road traffic Lden; NO2; and PM2.5, respectively, with minimally overlapping signals. Transportation Lden and air pollutants tendentially associated with decreased and increased methylation, respectively. We observed significant enrichment of candidate DNA methylation related to C-reactive protein and body mass index (aircraft, road traffic Lden, and PM2.5), renal function and “allostatic load” (all exposures). Agnostic functional networks related to cellular immunity, gene expression, cell growth/proliferation, cardiovascular, auditory, embryonic, and neurological systems development were enriched. We replicated increased methylation in cg08500171 (NO2) and decreased methylation in cg17629796 (PM2.5).Conclusions:Mutually independent DNA methylation was associated with source-specific transportation noise and air pollution exposures, with distinct and shared enrichments for pathways related to inflammation, cellular development, and immune responses. These findings contribute in clarifying the pathways linking these exposures and age-related diseases but need further confirmation in the context of mediation analyses. https://doi.org/10.1289/EHP6174

KW - Adult

KW - Air Pollutants

KW - Air Pollution/statistics & numerical data

KW - Aircraft

KW - Cohort Studies

KW - DNA

KW - DNA Methylation/physiology

KW - Environmental Exposure/statistics & numerical data

KW - Female

KW - Humans

KW - Linear Models

KW - Male

KW - Middle Aged

KW - Nitrogen Dioxide

KW - Noise, Transportation/statistics & numerical data

KW - Particulate Matter

UR - http://www.scopus.com/inward/record.url?scp=85085909871&partnerID=8YFLogxK

U2 - 10.1289/EHP6174

DO - 10.1289/EHP6174

M3 - Article

C2 - 32484729

VL - 128

JO - Environmental Health Perspectives

JF - Environmental Health Perspectives

IS - 6

M1 - 067003

ER -

Genome-wide DNA methylation in peripheral blood, and long-term exposure to source-specific transportation noise and air pollution, the SAPALDIA study

Abstract

Keywords

UN SDGs

Access to Document

Permanent link

Other files and links

Fingerprint

Cite this