Assessing the effect of childbearing on blood DNA methylation through comparison of parous and nulliparous females
Assessing the effect of childbearing on blood DNA methylation through comparison of parous and nulliparous females
Background
Pregnancy and childbirth have been connected to modified risk of a wide variety of conditions in later life, including neurodegenerative disorders and cancers. The presence, extent, and direction of the effect that childbearing status has on decreasing or increasing the risk of these conditions differs depending on the disease.
The mechanisms by which pregnancy and childbirth modify the risk of diseases are still unknown. DNA methylation (DNAm) alterations that occur during pregnancy and persist after childbirth may help us understand this phenomenon.
Results
Blood DNAm was available from 89 women (28 parous; 61 nulliparous) at ages 18 and 26 years in the Isle of Wight birth cohort; no significant differences in the population characteristics were present between the analyzed population and the full cohort. We performed an epigenome-wide association study on 389,355 CpGs and identified 184 CpGs to be significantly differentially methylated between parous and nulliparous women after adjusting for confounders and multiple testing. Of these CpGs, 105 had regression coefficients in the same direction in an independent Mexico City based ELEMENT cohort, of which 13 were significant (replication P < 0.05). These 13 CpGs were associated with 16 unique genes. DNAm levels tracked with gene expression in 3 of the replicated genes, one of which (TM2D3) was differentially expressed in parous vs nulliparous women. Gene disease association analysis identified a network
of parous-associated diseases.
Conclusions
Our results suggest that pregnancy and childbirth lead to DNAm changes in parous women and these changes persist at least 6 months and up to 8 years postpartum. Parous-related CpG sites may play a role in how childbearing status modifies risk of later life diseases in women. Further studies are needed to explore the linkage
and mechanism.
Chen, Su
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Johs, Miranda
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Karmaus, Wilfried
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Holloway, John
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Kheirkhah Rahimabad, Parnian
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Goodrich, Jaclyn M.
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Peterson, Karen E.
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Dolinoy, Dana C.
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Arshad, S. Hasan
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Ewart, Susan
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10 April 2024
Chen, Su
f162e4ea-8a5d-4541-ae08-f785f819b949
Johs, Miranda
d22775f2-68f8-4e13-8ae1-04d29296a522
Karmaus, Wilfried
08ec79ca-9652-4d0d-a84f-51502364800d
Holloway, John
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Kheirkhah Rahimabad, Parnian
21d644dd-81f0-4d00-85d5-42c789476bdf
Goodrich, Jaclyn M.
7e5bd267-8c8f-48b7-863b-25efcd7b16b7
Peterson, Karen E.
d2627ae5-e0fc-4011-a5b1-15aed2779706
Dolinoy, Dana C.
8520047f-f7c5-4456-9385-11d39d9c9ae1
Arshad, S. Hasan
917e246d-2e60-472f-8d30-94b01ef28958
Ewart, Susan
2472c7b8-5b16-4666-a351-86d838927665
Chen, Su, Johs, Miranda, Karmaus, Wilfried, Holloway, John, Kheirkhah Rahimabad, Parnian, Goodrich, Jaclyn M., Peterson, Karen E., Dolinoy, Dana C., Arshad, S. Hasan and Ewart, Susan
(2024)
Assessing the effect of childbearing on blood DNA methylation through comparison of parous and nulliparous females.
Epigenetics Communications, 4 (2), [2].
(doi:10.1186/s43682-024-00025-9).
Abstract
Background
Pregnancy and childbirth have been connected to modified risk of a wide variety of conditions in later life, including neurodegenerative disorders and cancers. The presence, extent, and direction of the effect that childbearing status has on decreasing or increasing the risk of these conditions differs depending on the disease.
The mechanisms by which pregnancy and childbirth modify the risk of diseases are still unknown. DNA methylation (DNAm) alterations that occur during pregnancy and persist after childbirth may help us understand this phenomenon.
Results
Blood DNAm was available from 89 women (28 parous; 61 nulliparous) at ages 18 and 26 years in the Isle of Wight birth cohort; no significant differences in the population characteristics were present between the analyzed population and the full cohort. We performed an epigenome-wide association study on 389,355 CpGs and identified 184 CpGs to be significantly differentially methylated between parous and nulliparous women after adjusting for confounders and multiple testing. Of these CpGs, 105 had regression coefficients in the same direction in an independent Mexico City based ELEMENT cohort, of which 13 were significant (replication P < 0.05). These 13 CpGs were associated with 16 unique genes. DNAm levels tracked with gene expression in 3 of the replicated genes, one of which (TM2D3) was differentially expressed in parous vs nulliparous women. Gene disease association analysis identified a network
of parous-associated diseases.
Conclusions
Our results suggest that pregnancy and childbirth lead to DNAm changes in parous women and these changes persist at least 6 months and up to 8 years postpartum. Parous-related CpG sites may play a role in how childbearing status modifies risk of later life diseases in women. Further studies are needed to explore the linkage
and mechanism.
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More information
Accepted/In Press date: 28 March 2024
e-pub ahead of print date: 10 April 2024
Published date: 10 April 2024
Identifiers
Local EPrints ID: 509626
URI: http://eprints.soton.ac.uk/id/eprint/509626
ISSN: 2730-7034
PURE UUID: 2a832500-4325-4b30-a929-1af8cb3dab25
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Date deposited: 26 Feb 2026 18:04
Last modified: 28 Feb 2026 02:35
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Contributors
Author:
Su Chen
Author:
Miranda Johs
Author:
Wilfried Karmaus
Author:
Parnian Kheirkhah Rahimabad
Author:
Jaclyn M. Goodrich
Author:
Karen E. Peterson
Author:
Dana C. Dolinoy
Author:
Susan Ewart
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