Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity

OBJECTIVE: Fixed genomic variation explains only a small proportion of the risk of adiposity. In animal models, maternal diet alters offspring body composition, accompanied by epigenetic changes in metabolic control genes. Little is known about whether such processes operate in humans. RESEARCH DESI...

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Autores principales: Godfrey, Keith M., Sheppard, Allan, Gluckman, Peter D., Lillycrop, Karen A., Burdge, Graham C., McLean, Cameron, Rodford, Joanne, Slater-Jefferies, Joanne L., Garratt, Emma, Crozier, Sarah R., Emerald, B. Starling, Gale, Catharine R., Inskip, Hazel M., Cooper, Cyrus, Hanson, Mark A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2011
Materias:
Obesity Studies
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3115550/
https://www.ncbi.nlm.nih.gov/pubmed/21471513
http://dx.doi.org/10.2337/db10-0979
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author Godfrey, Keith M.
Sheppard, Allan
Gluckman, Peter D.
Lillycrop, Karen A.
Burdge, Graham C.
McLean, Cameron
Rodford, Joanne
Slater-Jefferies, Joanne L.
Garratt, Emma
Crozier, Sarah R.
Emerald, B. Starling
Gale, Catharine R.
Inskip, Hazel M.
Cooper, Cyrus
Hanson, Mark A.
author_facet Godfrey, Keith M.
Sheppard, Allan
Gluckman, Peter D.
Lillycrop, Karen A.
Burdge, Graham C.
McLean, Cameron
Rodford, Joanne
Slater-Jefferies, Joanne L.
Garratt, Emma
Crozier, Sarah R.
Emerald, B. Starling
Gale, Catharine R.
Inskip, Hazel M.
Cooper, Cyrus
Hanson, Mark A.
author_sort Godfrey, Keith M.
collection PubMed
description OBJECTIVE: Fixed genomic variation explains only a small proportion of the risk of adiposity. In animal models, maternal diet alters offspring body composition, accompanied by epigenetic changes in metabolic control genes. Little is known about whether such processes operate in humans. RESEARCH DESIGN AND METHODS: Using Sequenom MassARRAY we measured the methylation status of 68 CpGs 5′ from five candidate genes in umbilical cord tissue DNA from healthy neonates. Methylation varied greatly at particular CpGs: for 31 CpGs with median methylation ≥5% and a 5–95% range ≥10%, we related methylation status to maternal pregnancy diet and to child’s adiposity at age 9 years. Replication was sought in a second independent cohort. RESULTS: In cohort 1, retinoid X receptor-α (RXRA) chr9:136355885+ and endothelial nitric oxide synthase (eNOS) chr7:150315553+ methylation had independent associations with sex-adjusted childhood fat mass (exponentiated regression coefficient [β] 17% per SD change in methylation [95% CI 4–31], P = 0.009, n = 64, and β = 20% [9–32], P < 0.001, n = 66, respectively) and %fat mass (β = 10% [1–19], P = 0.023, n = 64 and β =12% [4–20], P = 0.002, n = 66, respectively). Regression analyses including sex and neonatal epigenetic marks explained >25% of the variance in childhood adiposity. Higher methylation of RXRA chr9:136355885+, but not of eNOS chr7:150315553+, was associated with lower maternal carbohydrate intake in early pregnancy, previously linked with higher neonatal adiposity in this population. In cohort 2, cord eNOS chr7:150315553+ methylation showed no association with adiposity, but RXRA chr9:136355885+ methylation showed similar associations with fat mass and %fat mass (β = 6% [2–10] and β = 4% [1–7], respectively, both P = 0.002, n = 239). CONCLUSIONS: Our findings suggest a substantial component of metabolic disease risk has a prenatal developmental basis. Perinatal epigenetic analysis may have utility in identifying individual vulnerability to later obesity and metabolic disease.
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spelling pubmed-31155502011-11-01 Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity Godfrey, Keith M. Sheppard, Allan Gluckman, Peter D. Lillycrop, Karen A. Burdge, Graham C. McLean, Cameron Rodford, Joanne Slater-Jefferies, Joanne L. Garratt, Emma Crozier, Sarah R. Emerald, B. Starling Gale, Catharine R. Inskip, Hazel M. Cooper, Cyrus Hanson, Mark A. Diabetes Obesity Studies OBJECTIVE: Fixed genomic variation explains only a small proportion of the risk of adiposity. In animal models, maternal diet alters offspring body composition, accompanied by epigenetic changes in metabolic control genes. Little is known about whether such processes operate in humans. RESEARCH DESIGN AND METHODS: Using Sequenom MassARRAY we measured the methylation status of 68 CpGs 5′ from five candidate genes in umbilical cord tissue DNA from healthy neonates. Methylation varied greatly at particular CpGs: for 31 CpGs with median methylation ≥5% and a 5–95% range ≥10%, we related methylation status to maternal pregnancy diet and to child’s adiposity at age 9 years. Replication was sought in a second independent cohort. RESULTS: In cohort 1, retinoid X receptor-α (RXRA) chr9:136355885+ and endothelial nitric oxide synthase (eNOS) chr7:150315553+ methylation had independent associations with sex-adjusted childhood fat mass (exponentiated regression coefficient [β] 17% per SD change in methylation [95% CI 4–31], P = 0.009, n = 64, and β = 20% [9–32], P < 0.001, n = 66, respectively) and %fat mass (β = 10% [1–19], P = 0.023, n = 64 and β =12% [4–20], P = 0.002, n = 66, respectively). Regression analyses including sex and neonatal epigenetic marks explained >25% of the variance in childhood adiposity. Higher methylation of RXRA chr9:136355885+, but not of eNOS chr7:150315553+, was associated with lower maternal carbohydrate intake in early pregnancy, previously linked with higher neonatal adiposity in this population. In cohort 2, cord eNOS chr7:150315553+ methylation showed no association with adiposity, but RXRA chr9:136355885+ methylation showed similar associations with fat mass and %fat mass (β = 6% [2–10] and β = 4% [1–7], respectively, both P = 0.002, n = 239). CONCLUSIONS: Our findings suggest a substantial component of metabolic disease risk has a prenatal developmental basis. Perinatal epigenetic analysis may have utility in identifying individual vulnerability to later obesity and metabolic disease. American Diabetes Association 2011-05 2011-04-23 /pmc/articles/PMC3115550/ /pubmed/21471513 http://dx.doi.org/10.2337/db10-0979 Text en © 2011 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.
spellingShingle Obesity Studies
Godfrey, Keith M.
Sheppard, Allan
Gluckman, Peter D.
Lillycrop, Karen A.
Burdge, Graham C.
McLean, Cameron
Rodford, Joanne
Slater-Jefferies, Joanne L.
Garratt, Emma
Crozier, Sarah R.
Emerald, B. Starling
Gale, Catharine R.
Inskip, Hazel M.
Cooper, Cyrus
Hanson, Mark A.
Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity
title Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity
title_full Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity
title_fullStr Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity
title_full_unstemmed Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity
title_short Epigenetic Gene Promoter Methylation at Birth Is Associated With Child’s Later Adiposity
title_sort epigenetic gene promoter methylation at birth is associated with child’s later adiposity
topic Obesity Studies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3115550/
https://www.ncbi.nlm.nih.gov/pubmed/21471513
http://dx.doi.org/10.2337/db10-0979
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