Gestational arsenic exposure induces site-specific DNA hypomethylation in active retrotransposon subfamilies in offspring sperm in mice

Keiko Nohara; Kazuhiko Nakabayashi; Kazuyuki Okamura; Takehiro Suzuki; Shigekatsu Suzuki; Kenichiro Hata

doi:10.1186/s13072-020-00375-3

Epigenetics & Chromatin (Dec 2020)

Gestational arsenic exposure induces site-specific DNA hypomethylation in active retrotransposon subfamilies in offspring sperm in mice

Keiko Nohara,
Kazuhiko Nakabayashi,
Kazuyuki Okamura,
Takehiro Suzuki,
Shigekatsu Suzuki,
Kenichiro Hata

Affiliations

Keiko Nohara: Center for Health and Environmental Risk Research, National Institute for Environmental Studies
Kazuhiko Nakabayashi: Department of Maternal-Fetal Biology, National Center for Child Health and Development
Kazuyuki Okamura: Center for Health and Environmental Risk Research, National Institute for Environmental Studies
Takehiro Suzuki: Center for Health and Environmental Risk Research, National Institute for Environmental Studies
Shigekatsu Suzuki: Center for Environmental Biology and Ecosystem Studies, National Institute for Environmental Studies
Kenichiro Hata: Department of Maternal-Fetal Biology, National Center for Child Health and Development

DOI: https://doi.org/10.1186/s13072-020-00375-3
Journal volume & issue: Vol. 13, no. 1
pp. 1 – 14

Abstract

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Abstract Background Environmental impacts on a fetus can disrupt germ cell development leading to epimutations in mature germ cells. Paternal inheritance of adverse health effects through sperm epigenomes, including DNA methylomes, has been recognized in human and animal studies. However, the impacts of gestational exposure to a variety of environmental factors on the germ cell epigenomes are not fully investigated. Arsenic, a naturally occurring contaminant, is one of the most concerning environmental chemicals, that is causing serious health problems, including an increase in cancer, in highly contaminated areas worldwide. We previously showed that gestational arsenic exposure of pregnant C3H mice paternally induces hepatic tumor increase in the second generation (F2). In the present study, we have investigated the F1 sperm DNA methylomes genome-widely by one-base resolution analysis using a reduced representation bisulfite sequencing (RRBS) method. Results We have clarified that gestational arsenic exposure increases hypomethylated cytosines in all the chromosomes and they are significantly overrepresented in the retrotransposon LINEs and LTRs, predominantly in the intergenic regions. Closer analyses of detailed annotated DNA sequences showed that hypomethylated cytosines are especially accumulated in the promoter regions of the active full-length L1MdA subfamily in LINEs, and 5′LTRs of the active IAPE subfamily in LTRs. This is the first report that has identified the specific positions of methylomes altered in the retrotransposon elements by environmental exposure, by genome-wide methylome analysis. Conclusion Lowered DNA methylation potentially enhances L1MdA retrotransposition and cryptic promoter activity of 5′LTR for coding genes and non-coding RNAs. The present study has illuminated the environmental impacts on sperm DNA methylome establishment that can lead to augmented retrotransposon activities in germ cells and can cause harmful effects in the following generation.

Published in Epigenetics & Chromatin

ISSN: 1756-8935 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General): Genetics
Website: https://epigeneticsandchromatin.biomedcentral.com/

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