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Title: Impact of vitamin D depletion during development on mouse sperm DNA methylation.

Authors: Xue, Jing; Gharaibeh, Raad Z; Pietryk, Edward W; Brouwer, Cory; Tarantino, Lisa M; Valdar, William; Ideraabdullah, Folami Y

Published In Epigenetics, (2018)

Abstract: Suboptimal environmental conditions during development can substantially alter the epigenome. Stable environmentally-induced changes to the germline epigenome, in particular, have important implications for the health of the next generation. We showed previously that developmental vitamin D depletion (DVD) resulted in loss of DNA methylation at several imprinted loci over two generations. Here, we assessed the impact of DVD on genome-wide methylation in mouse sperm in order to characterize the number, extent and distribution of methylation changes in response to DVD and to find genes that may be susceptible to this prevalent environmental perturbation. We detected 15,827 loci that were differentially methylated in DVD mouse sperm vs. controls. Most epimutations (69%) were loss of methylation, and the extent of methylation change and number of CpGs affected in a region were associated with genic location and baseline methylation state. Methylation response to DVD at validated loci was only detected in offspring that exhibited a phenotypic response to DVD (increased body and testes weight) suggesting the two types of responses are linked, though a causal relationship is unclear. Epimutations localized to regions enriched for developmental and metabolic genes and pathway analyses showed enrichment for Cadherin, Wnt, PDGF and Integrin signaling pathways. These findings show for the first time that vitamin D status during development leads to substantial DNA methylation changes across the sperm genome and that locus susceptibility is linked to genomic and epigenomic context.

PubMed ID: 30239288 Exiting the NIEHS site

MeSH Terms: Animals; CpG Islands; DNA Methylation*; Male; Mice; Spermatozoa/growth & development; Spermatozoa/metabolism*; Vitamin D Deficiency/genetics*

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