The Cord Blood Insulin and Mitochondrial DNA Content Related Methylome

Brigitte Reimann; Bram G. Janssen; Rossella Alfano; Akram Ghantous; Almudena Espin-Perez; Theo M. de Kok; Nelly D. Saenen; Bianca Cox; Oliver Robinson; Marc Chadeau-Hyam; Joris Penders; Zdenko Herceg; Paolo Vineis; Tim S. Nawrot; Michelle Plusquin

doi:10.3389/fgene.2019.00325

The Cord Blood Insulin and Mitochondrial DNA Content Related Methylome

Brigitte Reimann, Bram G. Janssen, Rossella Alfano, Akram Ghantous, Almudena Espin-Perez, Theo M. de Kok, Nelly D. Saenen, Bianca Cox, Oliver Robinson, Marc Chadeau-Hyam, Joris Penders, Zdenko Herceg, Paolo Vineis, Tim S. Nawrot, Michelle Plusquin^*

^*Corresponding author for this work

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

Abstract

Mitochondrial dysfunction seems to play a key role in the etiology of insulin resistance. At birth, a link has already been established between mitochondrial DNA (mtDNA) content and insulin levels in cord blood. In this study, we explore shared epigenetic mechanisms of the association between mtDNA content and insulin levels, supporting the developmental origins of this link. First, the association between cord blood insulin and mtDNA content in 882 newborns of the ENVIRONAGE birth cohort was assessed. Cord blood mtDNA content was established via qPCR, while cord blood levels of insulin were determined using electrochemiluminescence immunoassays. Then the cord blood DNA methylome and transcriptome were determined in 179 newborns, using the human 450K methylation Illumina and Agilent Whole Human Genome 8 x 60 K microarrays, respectively. Subsequently, we performed an epigenome-wide association study (EWAS) adjusted for different maternal and neonatal variables. Afterward, we focused on the 20 strongest associations based on p-values to assign transcriptomic correlates and allocate corresponding pathways employing the R packages ReactomePA and RDAVIDWebService. On the regional level, we examined differential methylation using the DMRcate and Bumphunter packages in R. Cord blood mtDNA content and insulin were significantly correlated (r = 0.074, p = 0.028), still showing a trend after additional adjustment for maternal and neonatal variables (p = 0.062). We found an overlap of 33 pathways which were in common between the association with cord blood mtDNA content and insulin levels, including pathways of neurodevelopment, histone modification, cytochromes P450 (CYP)-metabolism, and biological aging. We further identified a DMR annotated to Repulsive Guidance Molecule BMP Co-Receptor A (RGMA) linked to cord blood insulin as well as mtDNA content. Metabolic variation in early life represented by neonatal insulin levels and mtDNA content might reflect or accommodate alterations in neurodevelopment, histone modification, CYP-metabolism, and aging, indicating etiological origins in epigenetic programming. Variation in metabolic hormones at birth, reflected by molecular changes, might via these alterations predispose children to metabolic diseases later in life. The results of this study may provide important markers for following targeted studies.

Original language	English
Article number	325
Pages (from-to)	1-15
Number of pages	15
Journal	Frontiers in Genetics
Volume	10
Issue number	APR
DOIs	https://doi.org/10.3389/fgene.2019.00325
Publication status	Published - 12 Apr 2019

Keywords

insulin
mitochondrial DNA content
epigenome-wide methylation
cord blood insulin levels
mitochondrial dysfunction
differentially methylated regions
DMRs
ENVIRONAGE
REPULSIVE GUIDANCE MOLECULE
GENE-BODY METHYLATION
POSTTRANSCRIPTIONAL REGULATION
CYTOCHROME-P450 2E1
CELLULAR SENESCENCE
DOPAMINE AGONIST
AIR-POLLUTION
RESISTANCE
EXPOSURE
DISEASE

Access to Document

10.3389/fgene.2019.00325Licence: CC BY

Cite this

Reimann, B., Janssen, B. G., Alfano, R., Ghantous, A., Espin-Perez, A., de Kok, T. M., Saenen, N. D., Cox, B., Robinson, O., Chadeau-Hyam, M., Penders, J., Herceg, Z., Vineis, P., Nawrot, T. S., & Plusquin, M. (2019). The Cord Blood Insulin and Mitochondrial DNA Content Related Methylome. Frontiers in Genetics, 10(APR), 1-15. Article 325. https://doi.org/10.3389/fgene.2019.00325

@article{5a6a9610b56e40c2a7dc83ecaf2aabd5,

title = "The Cord Blood Insulin and Mitochondrial DNA Content Related Methylome",

abstract = "Mitochondrial dysfunction seems to play a key role in the etiology of insulin resistance. At birth, a link has already been established between mitochondrial DNA (mtDNA) content and insulin levels in cord blood. In this study, we explore shared epigenetic mechanisms of the association between mtDNA content and insulin levels, supporting the developmental origins of this link. First, the association between cord blood insulin and mtDNA content in 882 newborns of the ENVIRONAGE birth cohort was assessed. Cord blood mtDNA content was established via qPCR, while cord blood levels of insulin were determined using electrochemiluminescence immunoassays. Then the cord blood DNA methylome and transcriptome were determined in 179 newborns, using the human 450K methylation Illumina and Agilent Whole Human Genome 8 x 60 K microarrays, respectively. Subsequently, we performed an epigenome-wide association study (EWAS) adjusted for different maternal and neonatal variables. Afterward, we focused on the 20 strongest associations based on p-values to assign transcriptomic correlates and allocate corresponding pathways employing the R packages ReactomePA and RDAVIDWebService. On the regional level, we examined differential methylation using the DMRcate and Bumphunter packages in R. Cord blood mtDNA content and insulin were significantly correlated (r = 0.074, p = 0.028), still showing a trend after additional adjustment for maternal and neonatal variables (p = 0.062). We found an overlap of 33 pathways which were in common between the association with cord blood mtDNA content and insulin levels, including pathways of neurodevelopment, histone modification, cytochromes P450 (CYP)-metabolism, and biological aging. We further identified a DMR annotated to Repulsive Guidance Molecule BMP Co-Receptor A (RGMA) linked to cord blood insulin as well as mtDNA content. Metabolic variation in early life represented by neonatal insulin levels and mtDNA content might reflect or accommodate alterations in neurodevelopment, histone modification, CYP-metabolism, and aging, indicating etiological origins in epigenetic programming. Variation in metabolic hormones at birth, reflected by molecular changes, might via these alterations predispose children to metabolic diseases later in life. The results of this study may provide important markers for following targeted studies.",

keywords = "insulin, mitochondrial DNA content, epigenome-wide methylation, cord blood insulin levels, mitochondrial dysfunction, differentially methylated regions, DMRs, ENVIRONAGE, REPULSIVE GUIDANCE MOLECULE, GENE-BODY METHYLATION, POSTTRANSCRIPTIONAL REGULATION, CYTOCHROME-P450 2E1, CELLULAR SENESCENCE, DOPAMINE AGONIST, AIR-POLLUTION, RESISTANCE, EXPOSURE, DISEASE",

author = "Brigitte Reimann and Janssen, {Bram G.} and Rossella Alfano and Akram Ghantous and Almudena Espin-Perez and {de Kok}, {Theo M.} and Saenen, {Nelly D.} and Bianca Cox and Oliver Robinson and Marc Chadeau-Hyam and Joris Penders and Zdenko Herceg and Paolo Vineis and Nawrot, {Tim S.} and Michelle Plusquin",

note = "Funding Information: The ENVIRONAGE birth cohort is supported by grants from the European Research Council (Grant No. ERC-2012-StG310898), the Flemish Scientific Fund (FWO, Grant No. 1516112N/G.0873.11.N.10), and the STOP project (Grant No. 774548-H2020). The laboratory analysis of epigenome-wide DNA methylation was carried out within the scope of the European Commission Seventh Framework program grant EXPOsOMICS (Grant No. 308610-FP7 to PV, ZH, and AG). ZH and AG and the Epigenetics Group at IARC are supported by grants from the Institut National du Cancer (INCa, Plan Cancer-EVA-INSERM, France). BR was financially supported by the University Research Fund (Bijzonder Onderzoeksfonds Universiteit Hasselt). Publisher Copyright: Copyright {\textcopyright} 2019 Reimann, Janssen, Alfano, Ghantous, Esp{\'i}n-P{\'e}rez, de Kok, Saenen, Cox, Robinson, Chadeau-Hyam, Penders, Herceg, Vineis, Nawrot and Plusquin.",

year = "2019",

month = apr,

day = "12",

doi = "10.3389/fgene.2019.00325",

language = "English",

volume = "10",

pages = "1--15",

journal = "Frontiers in Genetics",

issn = "1664-8021",

publisher = "Frontiers Media SA",

number = "APR",

}

TY - JOUR

T1 - The Cord Blood Insulin and Mitochondrial DNA Content Related Methylome

AU - Reimann, Brigitte

AU - Janssen, Bram G.

AU - Alfano, Rossella

AU - Ghantous, Akram

AU - Espin-Perez, Almudena

AU - de Kok, Theo M.

AU - Saenen, Nelly D.

AU - Cox, Bianca

AU - Robinson, Oliver

AU - Chadeau-Hyam, Marc

AU - Penders, Joris

AU - Herceg, Zdenko

AU - Vineis, Paolo

AU - Nawrot, Tim S.

AU - Plusquin, Michelle

N1 - Funding Information: The ENVIRONAGE birth cohort is supported by grants from the European Research Council (Grant No. ERC-2012-StG310898), the Flemish Scientific Fund (FWO, Grant No. 1516112N/G.0873.11.N.10), and the STOP project (Grant No. 774548-H2020). The laboratory analysis of epigenome-wide DNA methylation was carried out within the scope of the European Commission Seventh Framework program grant EXPOsOMICS (Grant No. 308610-FP7 to PV, ZH, and AG). ZH and AG and the Epigenetics Group at IARC are supported by grants from the Institut National du Cancer (INCa, Plan Cancer-EVA-INSERM, France). BR was financially supported by the University Research Fund (Bijzonder Onderzoeksfonds Universiteit Hasselt). Publisher Copyright: Copyright © 2019 Reimann, Janssen, Alfano, Ghantous, Espín-Pérez, de Kok, Saenen, Cox, Robinson, Chadeau-Hyam, Penders, Herceg, Vineis, Nawrot and Plusquin.

PY - 2019/4/12

Y1 - 2019/4/12

N2 - Mitochondrial dysfunction seems to play a key role in the etiology of insulin resistance. At birth, a link has already been established between mitochondrial DNA (mtDNA) content and insulin levels in cord blood. In this study, we explore shared epigenetic mechanisms of the association between mtDNA content and insulin levels, supporting the developmental origins of this link. First, the association between cord blood insulin and mtDNA content in 882 newborns of the ENVIRONAGE birth cohort was assessed. Cord blood mtDNA content was established via qPCR, while cord blood levels of insulin were determined using electrochemiluminescence immunoassays. Then the cord blood DNA methylome and transcriptome were determined in 179 newborns, using the human 450K methylation Illumina and Agilent Whole Human Genome 8 x 60 K microarrays, respectively. Subsequently, we performed an epigenome-wide association study (EWAS) adjusted for different maternal and neonatal variables. Afterward, we focused on the 20 strongest associations based on p-values to assign transcriptomic correlates and allocate corresponding pathways employing the R packages ReactomePA and RDAVIDWebService. On the regional level, we examined differential methylation using the DMRcate and Bumphunter packages in R. Cord blood mtDNA content and insulin were significantly correlated (r = 0.074, p = 0.028), still showing a trend after additional adjustment for maternal and neonatal variables (p = 0.062). We found an overlap of 33 pathways which were in common between the association with cord blood mtDNA content and insulin levels, including pathways of neurodevelopment, histone modification, cytochromes P450 (CYP)-metabolism, and biological aging. We further identified a DMR annotated to Repulsive Guidance Molecule BMP Co-Receptor A (RGMA) linked to cord blood insulin as well as mtDNA content. Metabolic variation in early life represented by neonatal insulin levels and mtDNA content might reflect or accommodate alterations in neurodevelopment, histone modification, CYP-metabolism, and aging, indicating etiological origins in epigenetic programming. Variation in metabolic hormones at birth, reflected by molecular changes, might via these alterations predispose children to metabolic diseases later in life. The results of this study may provide important markers for following targeted studies.

AB - Mitochondrial dysfunction seems to play a key role in the etiology of insulin resistance. At birth, a link has already been established between mitochondrial DNA (mtDNA) content and insulin levels in cord blood. In this study, we explore shared epigenetic mechanisms of the association between mtDNA content and insulin levels, supporting the developmental origins of this link. First, the association between cord blood insulin and mtDNA content in 882 newborns of the ENVIRONAGE birth cohort was assessed. Cord blood mtDNA content was established via qPCR, while cord blood levels of insulin were determined using electrochemiluminescence immunoassays. Then the cord blood DNA methylome and transcriptome were determined in 179 newborns, using the human 450K methylation Illumina and Agilent Whole Human Genome 8 x 60 K microarrays, respectively. Subsequently, we performed an epigenome-wide association study (EWAS) adjusted for different maternal and neonatal variables. Afterward, we focused on the 20 strongest associations based on p-values to assign transcriptomic correlates and allocate corresponding pathways employing the R packages ReactomePA and RDAVIDWebService. On the regional level, we examined differential methylation using the DMRcate and Bumphunter packages in R. Cord blood mtDNA content and insulin were significantly correlated (r = 0.074, p = 0.028), still showing a trend after additional adjustment for maternal and neonatal variables (p = 0.062). We found an overlap of 33 pathways which were in common between the association with cord blood mtDNA content and insulin levels, including pathways of neurodevelopment, histone modification, cytochromes P450 (CYP)-metabolism, and biological aging. We further identified a DMR annotated to Repulsive Guidance Molecule BMP Co-Receptor A (RGMA) linked to cord blood insulin as well as mtDNA content. Metabolic variation in early life represented by neonatal insulin levels and mtDNA content might reflect or accommodate alterations in neurodevelopment, histone modification, CYP-metabolism, and aging, indicating etiological origins in epigenetic programming. Variation in metabolic hormones at birth, reflected by molecular changes, might via these alterations predispose children to metabolic diseases later in life. The results of this study may provide important markers for following targeted studies.

KW - insulin

KW - mitochondrial DNA content

KW - epigenome-wide methylation

KW - cord blood insulin levels

KW - mitochondrial dysfunction

KW - differentially methylated regions

KW - DMRs

KW - ENVIRONAGE

KW - REPULSIVE GUIDANCE MOLECULE

KW - GENE-BODY METHYLATION

KW - POSTTRANSCRIPTIONAL REGULATION

KW - CYTOCHROME-P450 2E1

KW - CELLULAR SENESCENCE

KW - DOPAMINE AGONIST

KW - AIR-POLLUTION

KW - RESISTANCE

KW - EXPOSURE

KW - DISEASE

U2 - 10.3389/fgene.2019.00325

DO - 10.3389/fgene.2019.00325

M3 - Article

C2 - 31031804

SN - 1664-8021

VL - 10

SP - 1

EP - 15

JO - Frontiers in Genetics

JF - Frontiers in Genetics

IS - APR

M1 - 325

ER -

The Cord Blood Insulin and Mitochondrial DNA Content Related Methylome

Abstract

Keywords

Access to Document

Fingerprint

Cite this