Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial

OBJECTIVES: Maternal nutrition can alter the offspring epigenome at birth. We sought to examine epigenome-wide DNA methylation (DNAme) from a subset of Guatemalan mother-infant dyads from the Women First Preconception Maternal Nutrition Trial (WF). Women were randomized to either: Arm 1) women consu...

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Autores principales: Borengasser, Sarah, Murphy, Jessica, Null, Megan, Jambal, Purevsuren, Jones, Kenneth, Yang, Ivana, Friedman, Jacob, Waldrop, Stephanie, Gilley, Stephanie, Saint-Cyr, Martine, MacKenzie, Ian Arriaga, Kemp, Jennifer, Westcott, Jamie, Garces, Ana, Figueroa, Lester, Greally, John, Hambidge, K Michael, Hendricks, Audrey, Krebs, Nancy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Maternal, Perinatal and Pediatric Nutrition
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9193948/
http://dx.doi.org/10.1093/cdn/nzac061.009
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author Borengasser, Sarah
Murphy, Jessica
Null, Megan
Jambal, Purevsuren
Jones, Kenneth
Yang, Ivana
Friedman, Jacob
Waldrop, Stephanie
Gilley, Stephanie
Saint-Cyr, Martine
MacKenzie, Ian Arriaga
Kemp, Jennifer
Westcott, Jamie
Garces, Ana
Figueroa, Lester
Greally, John
Hambidge, K Michael
Hendricks, Audrey
Krebs, Nancy
author_facet Borengasser, Sarah
Murphy, Jessica
Null, Megan
Jambal, Purevsuren
Jones, Kenneth
Yang, Ivana
Friedman, Jacob
Waldrop, Stephanie
Gilley, Stephanie
Saint-Cyr, Martine
MacKenzie, Ian Arriaga
Kemp, Jennifer
Westcott, Jamie
Garces, Ana
Figueroa, Lester
Greally, John
Hambidge, K Michael
Hendricks, Audrey
Krebs, Nancy
author_sort Borengasser, Sarah
collection PubMed
description OBJECTIVES: Maternal nutrition can alter the offspring epigenome at birth. We sought to examine epigenome-wide DNA methylation (DNAme) from a subset of Guatemalan mother-infant dyads from the Women First Preconception Maternal Nutrition Trial (WF). Women were randomized to either: Arm 1) women consumed a daily maternal nutrition supplement (MNS) ≥ 3 months prior to conception until delivery; Arm 2) women consumed the same MNS starting at 12 weeks gestation until delivery; or Arm 3) no MNS. We tested if infant DNAme from amnion tissue at birth (N = 99) was associated with: 1) timing of exposure to maternal MNS; 2) pre-pregnancy body mass index (ppBMI); and 3) the interaction of maternal MNS and ppBMI. METHODS: Bisulfite-converted DNAme libraries were constructed using Roche NimbleGen SeqCap Epi CpGiant probes and were sequenced via 2 × 150 paired end reads. We assessed the relationship between Arm, ppBMI, and Arm x ppBMI interaction on CpG methylation. All statistical models adjusted for multiple testing using false discovery rate (FDR) and controlled for maternal age, infant sex, exposure to smoke, infant genetics, and cellular heterogeneity. Gene set enrichment analyses were performed via Enrichr. RESULTS: We identified 480 CpGs associated with Arm, 4 CpGs associated with ppBMI, and 22 CpGs associated with the interaction of Arm x ppBMI (FDR < 0.05). Further, we found that DNAme was changed between Arms (1 vs 2, 1 vs 3). There were 300 CpGs that were different between Arms 1 and 2 and 159 CpGs that were different between Arms 1 and 3 that annotated to genes and passed FDR < 0.05. These results suggest preconception consumption of maternal MNS elicits different epigenetic responses as compared to MNS commencing during gestation or not at all. In addition, CpGs that annotated to genes were enriched in pathways associated with growth, development, and metabolism that included circadian rhythm, TCA cycle, Wnt signaling, and melatonin metabolism. CONCLUSIONS: Our findings indicate that maternal MNS was robustly associated with amnion DNAme at birth. More specifically, preconception MNS resulted in DNAme changes that differed from the other Arms in biologically relevant pathways suggesting timing of maternal nutrition impacts the fetal epigenome. Future studies will examine DNAme associated with birth outcomes. FUNDING SOURCES: Bill & Melinda Gates Foundation and NIH NICHD/ODS.
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spelling pubmed-91939482022-06-14 Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial Borengasser, Sarah Murphy, Jessica Null, Megan Jambal, Purevsuren Jones, Kenneth Yang, Ivana Friedman, Jacob Waldrop, Stephanie Gilley, Stephanie Saint-Cyr, Martine MacKenzie, Ian Arriaga Kemp, Jennifer Westcott, Jamie Garces, Ana Figueroa, Lester Greally, John Hambidge, K Michael Hendricks, Audrey Krebs, Nancy Curr Dev Nutr Maternal, Perinatal and Pediatric Nutrition OBJECTIVES: Maternal nutrition can alter the offspring epigenome at birth. We sought to examine epigenome-wide DNA methylation (DNAme) from a subset of Guatemalan mother-infant dyads from the Women First Preconception Maternal Nutrition Trial (WF). Women were randomized to either: Arm 1) women consumed a daily maternal nutrition supplement (MNS) ≥ 3 months prior to conception until delivery; Arm 2) women consumed the same MNS starting at 12 weeks gestation until delivery; or Arm 3) no MNS. We tested if infant DNAme from amnion tissue at birth (N = 99) was associated with: 1) timing of exposure to maternal MNS; 2) pre-pregnancy body mass index (ppBMI); and 3) the interaction of maternal MNS and ppBMI. METHODS: Bisulfite-converted DNAme libraries were constructed using Roche NimbleGen SeqCap Epi CpGiant probes and were sequenced via 2 × 150 paired end reads. We assessed the relationship between Arm, ppBMI, and Arm x ppBMI interaction on CpG methylation. All statistical models adjusted for multiple testing using false discovery rate (FDR) and controlled for maternal age, infant sex, exposure to smoke, infant genetics, and cellular heterogeneity. Gene set enrichment analyses were performed via Enrichr. RESULTS: We identified 480 CpGs associated with Arm, 4 CpGs associated with ppBMI, and 22 CpGs associated with the interaction of Arm x ppBMI (FDR < 0.05). Further, we found that DNAme was changed between Arms (1 vs 2, 1 vs 3). There were 300 CpGs that were different between Arms 1 and 2 and 159 CpGs that were different between Arms 1 and 3 that annotated to genes and passed FDR < 0.05. These results suggest preconception consumption of maternal MNS elicits different epigenetic responses as compared to MNS commencing during gestation or not at all. In addition, CpGs that annotated to genes were enriched in pathways associated with growth, development, and metabolism that included circadian rhythm, TCA cycle, Wnt signaling, and melatonin metabolism. CONCLUSIONS: Our findings indicate that maternal MNS was robustly associated with amnion DNAme at birth. More specifically, preconception MNS resulted in DNAme changes that differed from the other Arms in biologically relevant pathways suggesting timing of maternal nutrition impacts the fetal epigenome. Future studies will examine DNAme associated with birth outcomes. FUNDING SOURCES: Bill & Melinda Gates Foundation and NIH NICHD/ODS. Oxford University Press 2022-06-14 /pmc/articles/PMC9193948/ http://dx.doi.org/10.1093/cdn/nzac061.009 Text en © The Author 2022. Published by Oxford University Press on behalf of The International Society for Human and Animal Mycology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Maternal, Perinatal and Pediatric Nutrition
Borengasser, Sarah
Murphy, Jessica
Null, Megan
Jambal, Purevsuren
Jones, Kenneth
Yang, Ivana
Friedman, Jacob
Waldrop, Stephanie
Gilley, Stephanie
Saint-Cyr, Martine
MacKenzie, Ian Arriaga
Kemp, Jennifer
Westcott, Jamie
Garces, Ana
Figueroa, Lester
Greally, John
Hambidge, K Michael
Hendricks, Audrey
Krebs, Nancy
Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial
title Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial
title_full Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial
title_fullStr Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial
title_full_unstemmed Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial
title_short Role of a Preconception Maternal Nutrition Supplement and Pre-pregnancy BMI on Amnion DNA Methylation at Birth in Guatemalan Mother-Infant Dyads: The Women First Trial
title_sort role of a preconception maternal nutrition supplement and pre-pregnancy bmi on amnion dna methylation at birth in guatemalan mother-infant dyads: the women first trial
topic Maternal, Perinatal and Pediatric Nutrition
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9193948/
http://dx.doi.org/10.1093/cdn/nzac061.009
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