| Literature DB >> 31485074 |
Stephanie P DiTroia1,2,3, Michelle Percharde1,2,4,5, Marie-Justine Guerquin6, Estelle Wall1,2, Evelyne Collignon7, Kevin T Ebata1,2, Kathryn Mesh1,2, Swetha Mahesula8, Michalis Agathocleous8, Diana J Laird1,2, Gabriel Livera6, Miguel Ramalho-Santos9,10,11.
Abstract
Development is often assumed to be hardwired in the genome, but several lines of evidence indicate that it is susceptible to environmental modulation with potential long-term consequences, including in mammals1,2. The embryonic germline is of particular interest because of the potential for intergenerational epigenetic effects. The mammalian germline undergoes extensive DNA demethylation3-7 that occurs in large part by passive dilution of methylation over successive cell divisions, accompanied by active DNA demethylation by TET enzymes3,8-10. TET activity has been shown to be modulated by nutrients and metabolites, such as vitamin C11-15. Here we show that maternal vitamin C is required for proper DNA demethylation and the development of female fetal germ cells in a mouse model. Maternal vitamin C deficiency does not affect overall embryonic development but leads to reduced numbers of germ cells, delayed meiosis and reduced fecundity in adult offspring. The transcriptome of germ cells from vitamin-C-deficient embryos is remarkably similar to that of embryos carrying a null mutation in Tet1. Vitamin C deficiency leads to an aberrant DNA methylation profile that includes incomplete demethylation of key regulators of meiosis and transposable elements. These findings reveal that deficiency in vitamin C during gestation partially recapitulates loss of TET1, and provide a potential intergenerational mechanism for adjusting fecundity to environmental conditions.Entities:
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Year: 2019 PMID: 31485074 DOI: 10.1038/s41586-019-1536-1
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962