Genomic properties of variably methylated retrotransposons in mouse

Author:

Elmer Jessica L.,Hay Amir D.,Kessler Noah J.,Bertozzi Tessa M.,Ainscough Eve A. C.,Ferguson-Smith Anne C.ORCID

Abstract

AbstractBackgroundTransposable elements (TEs) are enriched in cytosine methylation, preventing their mobility within the genome. We previously identified a genome-wide repertoire of candidate intracisternal A particle (IAP) TEs in mice that exhibit inter-individual variability in this methylation (VM-IAPs) with implications for genome function.ResultsHere we validate these metastable epialleles and discover a novel class that exhibit tissue specificity (tsVM-IAPs) in addition to those with uniform methylation in all tissues (constitutive- or cVM-IAPs); both types have the potential to regulate genes incis. Screening for variable methylation at other TEs shows that this phenomenon is largely limited to IAPs, which are amongst the youngest and most active endogenous retroviruses. We identify sequences enriched within cVM-IAPs, but determine that these are not sufficient to confer epigenetic variability. CTCF is enriched at VM-IAPs with binding inversely correlated with DNA methylation. We uncover dynamic physical interactions between cVM-IAPs with low methylation ranges and other genomic loci, suggesting that VM-IAPs have the potential for long-range regulation.ConclusionOur findings indicate that a recently evolved interplay between genetic sequence, CTCF binding, and DNA methylation at young TEs can result in inter-individual variability in transcriptional outcomes with implications for phenotypic variation.

Funder

Medical Research Council

Biotechnology and Biological Sciences Research Council

Wellcome Trust

Publisher

Springer Science and Business Media LLC

Subject

Molecular Biology

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