Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context

Epigenetic control of gene transcription is critical for normal human development and cellular differentiation. While alterations of epigenetic marks such as DNA methylation have been linked to cancers and many other human diseases, interindividual epigenetic variations in normal tissues due to agin...

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Autores principales: Christensen, Brock C., Houseman, E. Andres, Marsit, Carmen J., Zheng, Shichun, Wrensch, Margaret R., Wiemels, Joseph L., Nelson, Heather H., Karagas, Margaret R., Padbury, James F., Bueno, Raphael, Sugarbaker, David J., Yeh, Ru-Fang, Wiencke, John K., Kelsey, Karl T.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2718614/
https://www.ncbi.nlm.nih.gov/pubmed/19680444
http://dx.doi.org/10.1371/journal.pgen.1000602
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author Christensen, Brock C.
Houseman, E. Andres
Marsit, Carmen J.
Zheng, Shichun
Wrensch, Margaret R.
Wiemels, Joseph L.
Nelson, Heather H.
Karagas, Margaret R.
Padbury, James F.
Bueno, Raphael
Sugarbaker, David J.
Yeh, Ru-Fang
Wiencke, John K.
Kelsey, Karl T.
author_facet Christensen, Brock C.
Houseman, E. Andres
Marsit, Carmen J.
Zheng, Shichun
Wrensch, Margaret R.
Wiemels, Joseph L.
Nelson, Heather H.
Karagas, Margaret R.
Padbury, James F.
Bueno, Raphael
Sugarbaker, David J.
Yeh, Ru-Fang
Wiencke, John K.
Kelsey, Karl T.
author_sort Christensen, Brock C.
collection PubMed
description Epigenetic control of gene transcription is critical for normal human development and cellular differentiation. While alterations of epigenetic marks such as DNA methylation have been linked to cancers and many other human diseases, interindividual epigenetic variations in normal tissues due to aging, environmental factors, or innate susceptibility are poorly characterized. The plasticity, tissue-specific nature, and variability of gene expression are related to epigenomic states that vary across individuals. Thus, population-based investigations are needed to further our understanding of the fundamental dynamics of normal individual epigenomes. We analyzed 217 non-pathologic human tissues from 10 anatomic sites at 1,413 autosomal CpG loci associated with 773 genes to investigate tissue-specific differences in DNA methylation and to discern how aging and exposures contribute to normal variation in methylation. Methylation profile classes derived from unsupervised modeling were significantly associated with age (P<0.0001) and were significant predictors of tissue origin (P<0.0001). In solid tissues (n = 119) we found striking, highly significant CpG island–dependent correlations between age and methylation; loci in CpG islands gained methylation with age, loci not in CpG islands lost methylation with age (P<0.001), and this pattern was consistent across tissues and in an analysis of blood-derived DNA. Our data clearly demonstrate age- and exposure-related differences in tissue-specific methylation and significant age-associated methylation patterns which are CpG island context-dependent. This work provides novel insight into the role of aging and the environment in susceptibility to diseases such as cancer and critically informs the field of epigenomics by providing evidence of epigenetic dysregulation by age-related methylation alterations. Collectively we reveal key issues to consider both in the construction of reference and disease-related epigenomes and in the interpretation of potentially pathologically important alterations.
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spelling pubmed-27186142009-08-14 Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context Christensen, Brock C. Houseman, E. Andres Marsit, Carmen J. Zheng, Shichun Wrensch, Margaret R. Wiemels, Joseph L. Nelson, Heather H. Karagas, Margaret R. Padbury, James F. Bueno, Raphael Sugarbaker, David J. Yeh, Ru-Fang Wiencke, John K. Kelsey, Karl T. PLoS Genet Research Article Epigenetic control of gene transcription is critical for normal human development and cellular differentiation. While alterations of epigenetic marks such as DNA methylation have been linked to cancers and many other human diseases, interindividual epigenetic variations in normal tissues due to aging, environmental factors, or innate susceptibility are poorly characterized. The plasticity, tissue-specific nature, and variability of gene expression are related to epigenomic states that vary across individuals. Thus, population-based investigations are needed to further our understanding of the fundamental dynamics of normal individual epigenomes. We analyzed 217 non-pathologic human tissues from 10 anatomic sites at 1,413 autosomal CpG loci associated with 773 genes to investigate tissue-specific differences in DNA methylation and to discern how aging and exposures contribute to normal variation in methylation. Methylation profile classes derived from unsupervised modeling were significantly associated with age (P<0.0001) and were significant predictors of tissue origin (P<0.0001). In solid tissues (n = 119) we found striking, highly significant CpG island–dependent correlations between age and methylation; loci in CpG islands gained methylation with age, loci not in CpG islands lost methylation with age (P<0.001), and this pattern was consistent across tissues and in an analysis of blood-derived DNA. Our data clearly demonstrate age- and exposure-related differences in tissue-specific methylation and significant age-associated methylation patterns which are CpG island context-dependent. This work provides novel insight into the role of aging and the environment in susceptibility to diseases such as cancer and critically informs the field of epigenomics by providing evidence of epigenetic dysregulation by age-related methylation alterations. Collectively we reveal key issues to consider both in the construction of reference and disease-related epigenomes and in the interpretation of potentially pathologically important alterations. Public Library of Science 2009-08-14 /pmc/articles/PMC2718614/ /pubmed/19680444 http://dx.doi.org/10.1371/journal.pgen.1000602 Text en Christensen et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Christensen, Brock C.
Houseman, E. Andres
Marsit, Carmen J.
Zheng, Shichun
Wrensch, Margaret R.
Wiemels, Joseph L.
Nelson, Heather H.
Karagas, Margaret R.
Padbury, James F.
Bueno, Raphael
Sugarbaker, David J.
Yeh, Ru-Fang
Wiencke, John K.
Kelsey, Karl T.
Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context
title Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context
title_full Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context
title_fullStr Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context
title_full_unstemmed Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context
title_short Aging and Environmental Exposures Alter Tissue-Specific DNA Methylation Dependent upon CpG Island Context
title_sort aging and environmental exposures alter tissue-specific dna methylation dependent upon cpg island context
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2718614/
https://www.ncbi.nlm.nih.gov/pubmed/19680444
http://dx.doi.org/10.1371/journal.pgen.1000602
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