Article ID Journal Published Year Pages File Type
2041079 Cell Reports 2015 13 Pages PDF
Abstract

•DNA methylation directly affects mRNA alternative splicing•Methylation-affected exons display distinct genetic and epigenetic signatures•HP1 mediates DNA methylation’s effect on splicing by recruiting splicing factors•HP1 enhances or silences inclusion depending on its relative binding position

SummaryThe global impact of DNA methylation on alternative splicing is largely unknown. Using a genome-wide approach in wild-type and methylation-deficient embryonic stem cells, we found that DNA methylation can either enhance or silence exon recognition and affects the splicing of more than 20% of alternative exons. These exons are characterized by distinct genetic and epigenetic signatures. Alternative splicing regulation of a subset of these exons can be explained by heterochromatin protein 1 (HP1), which silences or enhances exon recognition in a position-dependent manner. We constructed an experimental system using site-specific targeting of a methylated/unmethylated gene and demonstrate a direct causal relationship between DNA methylation and alternative splicing. HP1 regulates this gene’s alternative splicing in a methylation-dependent manner by recruiting splicing factors to its methylated form. Our results demonstrate DNA methylation’s significant global influence on mRNA splicing and identify a specific mechanism of splicing regulation mediated by HP1.

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Life Sciences Agricultural and Biological Sciences Agricultural and Biological Sciences (General)
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