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Whole genome bisulfite sequencing reveals a sparse, but robust pattern of DNA methylation in the Dictyostelium discoideum genome

Jacob L. Steenwyk, James St. Denis, Jacqueline M. Dresch, Denis A. Larochelle, Robert A. Drewell
doi: https://doi.org/10.1101/166033
Jacob L. Steenwyk
1 Biology Department, Clark University, 950 Main Street, Worcester, MA 01610
3 Department of Biological Sciences, Vanderbilt University, Box 351634 Station B, Nashville, TN 37235
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James St. Denis
1 Biology Department, Clark University, 950 Main Street, Worcester, MA 01610
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Jacqueline M. Dresch
2 Department of Mathematics and Computer Science, Clark University, 950 Main Street, Worcester, MA 01610
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Denis A. Larochelle
1 Biology Department, Clark University, 950 Main Street, Worcester, MA 01610
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Robert A. Drewell
1 Biology Department, Clark University, 950 Main Street, Worcester, MA 01610
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Abstract

DNA methylation, the addition of a methyl (CH3) group to a cytosine residue, is an evolutionarily conserved epigenetic mark involved in a number of different biological functions in eukaryotes, including transcriptional regulation, chromatin structural organization, cellular differentiation and development. In the slime mold Dictyostelium, previous studies have shown the existence of a DNA methyltransferase (DNMA) belonging to the DNMT2 family, but the extent and function of 5-methyl-cytosine in the genome is unclear. Here we present the whole genome DNA methylation profile of Dictyostelium discoideum using deep coverage, replicate sequencing of bisulfite converted gDNA extracted from post-starvation cells. We find an overall very low level of DNA methylation, occurring at only 462 out of the ~7.5 million (0.006%) cytosines in the genome. Despite this sparse profile, significant methylation can be detected at 51 of these sites in replicate experiments, suggesting they are robust targets for DNA methylation. These 5-methyl-cytosines are associated with a broad range of protein-coding genes, tRNA-encoding genes and retrotransposable elements. Our data provides evidence of a minimal, but functional, methylome in Dictyostelium, thereby making Dictyostelium a candidate model organism to further investigate the evolutionary function of DNA methylation.

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Posted July 20, 2017.
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Whole genome bisulfite sequencing reveals a sparse, but robust pattern of DNA methylation in the Dictyostelium discoideum genome
Jacob L. Steenwyk, James St. Denis, Jacqueline M. Dresch, Denis A. Larochelle, Robert A. Drewell
bioRxiv 166033; doi: https://doi.org/10.1101/166033
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Whole genome bisulfite sequencing reveals a sparse, but robust pattern of DNA methylation in the Dictyostelium discoideum genome
Jacob L. Steenwyk, James St. Denis, Jacqueline M. Dresch, Denis A. Larochelle, Robert A. Drewell
bioRxiv 166033; doi: https://doi.org/10.1101/166033

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