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Epigenetic memory at embryonic enhancers identified in DNA methylation maps from adult mouse tissues

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TLDR
By mapping base-resolution methylomes in adult mouse tissues at shallow coverage, this work identifies 302,864 tissue-specific differentially methylated regions (tsDMRs) and estimates that >6.7% of the mouse genome is variably methylated, and suggests that epigenetic memory of embryonic development may be retained in adult tissues.
Abstract
Mammalian development requires cytosine methylation, a heritable epigenetic mark of cellular memory believed to maintain a cell's unique gene expression pattern. However, it remains unclear how dynamic DNA methylation relates to cell type-specific gene expression and animal development. Here, by mapping base-resolution methylomes in 17 adult mouse tissues at shallow coverage, we identify 302,864 tissue-specific differentially methylated regions (tsDMRs) and estimate that >6.7% of the mouse genome is variably methylated. Supporting a prominent role for DNA methylation in gene regulation, most tsDMRs occur at distal cis-regulatory elements. Unexpectedly, some tsDMRs mark enhancers that are dormant in adult tissues but active in embryonic development. These 'vestigial' enhancers are hypomethylated and lack active histone modifications in adult tissues but nevertheless exhibit activity during embryonic development. Our results provide new insights into the role of DNA methylation at tissue-specific enhancers and suggest that epigenetic memory of embryonic development may be retained in adult tissues.

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Potential of adipose-derived stem cells in muscular regenerative therapies.

TL;DR: This review will summarize the use of ASCs in muscle regenerative approaches, which have been successfully differentiated in vitro to osteogenic, chondrogenic, neurogenic and myogenic lineages and hold promise for a range of therapeutic applications.
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DNA methylation at the crossroads of gene and environment interactions.

TL;DR: This work uses the developmental origins of adult disease hypothesis to understand environmental epigenomics and highlights recent evidence that suggests that genomic regions that are absent from genome assemblies may be unappreciated hotspots for environmental modulation of the epigenetic state.
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Decoding neural transcriptomes and epigenomes via high-throughput sequencing

TL;DR: The complexity of the nervous system is discussed, then various applications of NGS are introduced with practical considerations and basic principles underlying various NGS technologies are described.
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Epigenetic regulation in the inner ear and its potential roles in development, protection, and regeneration.

TL;DR: This review highlights emerging paradigms for epigenetic modifications related to inner ear development, and how epigenetics may have a significant role in hearing loss, protection, and regeneration.
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Epigenetics: a new way to look at kidney diseases

TL;DR: Recent advances in the area of epigenetics--specifically in cytosine modifications--and its application in the field of nephrology are discussed.
References
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Simple Combinations of Lineage-Determining Transcription Factors Prime cis-Regulatory Elements Required for Macrophage and B Cell Identities

TL;DR: It is demonstrated in macrophages and B cells that collaborative interactions of the common factor PU.1 with small sets of macrophage- or B cell lineage-determining transcription factors establish cell-specific binding sites that are associated with the majority of promoter-distal H3K4me1-marked genomic regions.
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DNA methylation patterns and epigenetic memory

TL;DR: The heritability of methylation states and the secondary nature of the decision to invite or exclude methylation support the idea that DNA methylation is adapted for a specific cellular memory function in development.
Journal ArticleDOI

Topological domains in mammalian genomes identified by analysis of chromatin interactions

TL;DR: It is found that the boundaries of topological domains are enriched for the insulator binding protein CTCF, housekeeping genes, transfer RNAs and short interspersed element (SINE) retrotransposons, indicating that these factors may have a role in establishing the topological domain structure of the genome.
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