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      Altered placental DNA methylation patterns associated with maternal smoking: current perspectives

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      Author(s): ,
      Publication date PMC-release:
      Journal: Advances in genomics and genetics
      Keywords: pregnancy, epigenetics, prenatal, placenta, tobacco

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          Abstract

          The developmental origins of health and disease hypothesis states that adverse early life exposures can have lasting, detrimental effects on lifelong health. Exposure to maternal cigarette smoking during pregnancy is associated with morbidity and mortality in offspring, including increased risks for miscarriage, stillbirth, low birth weight, preterm birth, asthma, obesity, altered neurobehavior, and other conditions. Maternal cigarette smoking during pregnancy interferes with placental growth and functioning, and it has been proposed that this may occur through the disruption of normal and necessary placental epigenetic patterns. Epigenome-wide association studies have identified a number of differentially methylated placental genes that are associated with maternal smoking during pregnancy, including RUNX3, PURA, GTF2H2, GCA, GPR135, and HKR1. The placental methylation status of RUNX3 and NR3C1 has also been linked to adverse infant outcomes, including preterm birth and low birth weight, respectively. Candidate gene analyses have also found maternal smoking-associated placental methylation differences in the NR3C1, CYP1A1, HTR2A, and HSD11B2 genes, as well as in the repetitive elements LINE-1 and AluYb8. The differential methylation patterns of several genes have been confirmed to also exhibit altered gene expression patterns, including CYP1A1, CYP19A1, NR3C1, and HTR2A. Placental methylation patterns associated with maternal smoking during pregnancy may be largely gene-specific and tissue-specific and, to a lesser degree, involve global changes. It is important for future research to investigate the mechanistic roles that these differentially methylated genes may play in mediating the association between maternal smoking during pregnancy and disease in later life, as well as to elucidate the potential influence of emerging tobacco product use during pregnancy, including the use of electronic cigarettes, on placental epigenetics.

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          Most cited references139

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          Epigenome-wide association studies for common human diseases.

          Vardhman Rakyan, Thomas A. Down, David Balding (2011)
          Despite the success of genome-wide association studies (GWASs) in identifying loci associated with common diseases, a substantial proportion of the causality remains unexplained. Recent advances in genomic technologies have placed us in a position to initiate large-scale studies of human disease-associated epigenetic variation, specifically variation in DNA methylation. Such epigenome-wide association studies (EWASs) present novel opportunities but also create new challenges that are not encountered in GWASs. We discuss EWAS design, cohort and sample selections, statistical significance and power, confounding factors and follow-up studies. We also discuss how integration of EWASs with GWASs can help to dissect complex GWAS haplotypes for functional analysis.
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            In utero programming of chronic disease.

            D. J. Barker (1998)
            1. Many human fetuses have to adapt to a limited supply of nutrients. In doing so they permanently change their structure and metabolism. 2. These 'programmed' changes may be the origins of a number of diseases in later life, including coronary heart disease and the related disorders stroke, diabetes and hypertension. 3. This review examines the evidence linking these diseases to fetal undernutrition and provides an overview of previous studies in this area.
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              DNA methylation and cancer.

              Marta Kulis, Manel Esteller (2010)
              DNA methylation is one of the most intensely studied epigenetic modifications in mammals. In normal cells, it assures the proper regulation of gene expression and stable gene silencing. DNA methylation is associated with histone modifications and the interplay of these epigenetic modifications is crucial to regulate the functioning of the genome by changing chromatin architecture. The covalent addition of a methyl group occurs generally in cytosine within CpG dinucleotides which are concentrated in large clusters called CpG islands. DNA methyltransferases are responsible for establishing and maintenance of methylation pattern. It is commonly known that inactivation of certain tumor-suppressor genes occurs as a consequence of hypermethylation within the promoter regions and a numerous studies have demonstrated a broad range of genes silenced by DNA methylation in different cancer types. On the other hand, global hypomethylation, inducing genomic instability, also contributes to cell transformation. Apart from DNA methylation alterations in promoter regions and repetitive DNA sequences, this phenomenon is associated also with regulation of expression of noncoding RNAs such as microRNAs that may play role in tumor suppression. DNA methylation seems to be promising in putative translational use in patients and hypermethylated promoters may serve as biomarkers. Moreover, unlike genetic alterations, DNA methylation is reversible what makes it extremely interesting for therapy approaches. The importance of DNA methylation alterations in tumorigenesis encourages us to decode the human epigenome. Different DNA methylome mapping techniques are indispensable to realize this project in the future. Copyright © 2010 Elsevier Inc. All rights reserved.
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                Author and article information

                Journal
                Journal ID (nlm-journal-id): 101586945
                Journal ID (pubmed-jr-id): 40443
                Journal ID (nlm-ta): Adv Genomics Genet
                Journal ID (iso-abbrev): Adv Genomics Genet
                Title: Advances in genomics and genetics
                ISSN (Electronic): 1179-9870
                Publication date Nihms-submitted: 16 June 2015
                Publication date (Print): 7 May 2015
                Publication date PMC-release: 19 July 2015
                Volume: 2015
                Issue: 5
                Pages: 205-214
                Affiliations
                Penn State Tobacco Center of Regulatory Science, College of Medicine, Department of Public Health Sciences, Hershey, PA, USA
                Author notes
                Correspondence: Jennifer ZJ Maccani Tobacco Center of Regulatory Science, Public Health Sciences Department, Suite PSHCi T3425, 500 University Drive, PO Box 850, Hershey, PA 17033-0850, USA, Tel +1 717 531 0003 ext 289575, Fax +1 717 531 0480, jmaccani@ 123456phs.psu.edu
                Article
                Manuscript ID: NIHMS700129
                DOI: 10.2147/AGG.S61518
                PMC ID: 4507353
                PubMed ID: 26203295
                SO-VID: f7faffde-77d7-490e-aaa0-ae79a75d3d3d
                Copyright © © 2015 Maccani and Maccani.
                License:

                This work is published by Dove Medical Press Limited, and licensed under Creative Commons Attribution – Non Commercial (unported, v3.0) License. The full terms of the License are available at http://creativecommons.org/licenses/by-nc/3.0/. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed. Permissions beyond the scope of the License are administered by Dove Medical Press Limited.

                Information on how to request permission may be found at: http://www.dovepress.com/permissions.php

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                Subject: Article

                Keywords: pregnancy,epigenetics,prenatal,placenta,tobacco
                Data availability:
                Keywords: pregnancy, epigenetics, prenatal, placenta, tobacco

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