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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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Journal ArticleDOI

Guide Positioning Sequencing identifies aberrant DNA methylation patterns that alter cell identity and tumor-immune surveillance networks

TL;DR: Using GPS, it is shown that aberrant DNA methylation is associated with altering cell identity and immune surveillance networks, which may contribute to tumorigenesis and metastasis, and is demonstrated that GPS is a powerful tool with improved accuracy and efficiency over WGBS in simultaneously detecting genome-wideDNA methylation and genomic variation.
Journal ArticleDOI

FASTmC: A Suite of Predictive Models for Nonreference-Based Estimations of DNA Methylation.

TL;DR: A suite of predictive models are described, coined FASTmC, for nonreference, cost-effective exploration and comparative analysis of context-specific DNA methylation levels, which make high-resolution time course or developmental and large diversity studies practical regardless of species, genome size, and availability of a reference genome.
Journal ArticleDOI

A long non-coding RNA, BC048612 and a microRNA, miR-203 coordinate the gene expression of neuronal growth regulator 1 (NEGR1) adhesion protein.

TL;DR: The long non-coding RNA, BC048612, and microRNA-203 were determined to be positive and negative regulators of Negr1 gene expression respectively and have a direct effect on NEGR1 protein levels and neurite length, thus highlighting the importance of the regulatory non-Coding RNAs in modulating Negr 1 gene expression for precise neuronal development.
Journal ArticleDOI

Enhancer, epigenetics, and human disease.

TL;DR: The advances in the transcriptional enhancer field hold great promise in linking developmental or disease phenotypes to genetic variants and promoting precision medicine.
Posted ContentDOI

Genome-scale oscillations in DNA methylation during exit from pluripotency

TL;DR: It is shown that during this phase, coexpression of enzymes required for DNA methylation turnover, DNMT3s and TETs, promotes cell-to-cell variability in this epigenetic mark, indicating that dynamic changes inDNA methylation might influence early cell fate decisions.
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Journal ArticleDOI

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