Variation in histone configurations correlates with gene expression across nine inbred strains of mice

Author:

Tyler Anna L.ORCID,Spruce Catrina,Kursawe Romy,Haber Annat,Ball Robyn L.,Pitman Wendy A.,Fine Alexander D.,Raghupathy Narayanan,Walker Michael,Philip Vivek M.,Baker Christopher L.ORCID,Mahoney J. Matthew,Churchill Gary A.,Trowbridge Jennifer J.,Stitzel Michael L.,Paigen Kenneth,Petkov Petko M.,Carter Gregory W.ORCID

Abstract

The Diversity Outbred (DO) mice and their inbred founders are widely used models of human disease. However, although the genetic diversity of these mice has been well documented, their epigenetic diversity has not. Epigenetic modifications, such as histone modifications and DNA methylation, are important regulators of gene expression and, as such, are a critical mechanistic link between genotype and phenotype. Therefore, creating a map of epigenetic modifications in the DO mice and their founders is an important step toward understanding mechanisms of gene regulation and the link to disease in this widely used resource. To this end, we performed a strain survey of epigenetic modifications in hepatocytes of the DO founders. We surveyed four histone modifications (H3K4me1, H3K4me3, H3K27me3, and H3K27ac), as well as DNA methylation. We used ChromHMM to identify 14 chromatin states, each of which represents a distinct combination of the four histone modifications. We found that the epigenetic landscape is highly variable across the DO founders and is associated with variation in gene expression across strains. We found that epigenetic state imputed into a population of DO mice recapitulated the association with gene expression seen in the founders, suggesting that both histone modifications and DNA methylation are highly heritable mechanisms of gene expression regulation. We illustrate how DO gene expression can be aligned with inbred epigenetic states to identify putativecis-regulatory regions. Finally, we provide a data resource that documents strain-specific variation in the chromatin state and DNA methylation in hepatocytes across nine widely used strains of laboratory mice.

Funder

The Jackson Laboratory Director's Innovation Fund

National Institutes of Health

Publisher

Cold Spring Harbor Laboratory

Subject

Genetics (clinical),Genetics

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