Intragenic CpG islands play important roles in bivalent chromatin assembly of developmental genes

CpG, 5′-C-phosphate-G-3′, islands (CGIs) have long been known for their association with enhancers, silencers, and promoters, and for their epigenetic signatures. They are maintained in embryonic stem cells (ESCs) in a poised but inactive state via the formation of bivalent chromatin containing both...

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Published inProceedings of the National Academy of Sciences - PNAS Vol. 114; no. 10; pp. E1885 - E1894
Main Authors Lee, Sun-Min, Lee, Jungwoo, Noh, Kyung-Min, Choi, Won-Young, Jeon, Sejin, Oh, Goo Taeg, Kim-Ha, Jeongsil, Jin, Yoonhee, Cho, Seung-Woo, Kim, Young-Joon
Format Journal Article
LanguageEnglish
Published United States National Academy of Sciences 07.03.2017
SeriesPNAS Plus
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Summary:CpG, 5′-C-phosphate-G-3′, islands (CGIs) have long been known for their association with enhancers, silencers, and promoters, and for their epigenetic signatures. They are maintained in embryonic stem cells (ESCs) in a poised but inactive state via the formation of bivalent chromatin containing both active and repressive marks. CGIs also occur within coding sequences, where their functional role has remained obscure. Intragenic CGIs (iCGIs) are largely absent from housekeeping genes, but they are found in all genes associated with organ development and cell lineage control. In this paper, we investigated the epigenetic status of iCGIs and found that they too reside in bivalent chromatin in ESCs. Cell type-specific DNA methylation of iCGIs in differentiated cells was linked to the loss of both the H3K4me3 and H3K27me3 marks, and disruption of physical interaction with promoter regions, resulting in transcriptional activation of key regulators of differentiation such as PAXs, HOXs, and WNTs. The differential epigenetic modification of iCGIs appears to be mediated by cell type-specific transcription factors distinct from those bound by promoter, and these transcription factors may be involved in the hypermethylation of iCGIs upon cell differentiation. iCGIs thus play a key role in the cell type-specific regulation of transcription.
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Edited by Roger D. Kornberg, Stanford University School of Medicine, Stanford, CA, and approved January 31, 2017 (received for review August 9, 2016)
Author contributions: S.-M.L. and Y.-J.K. designed research; S.-M.L., J.L., K.-M.N., S.J., and G.T.O. performed research; K.-M.N., Y.J., and S.-W.C. contributed new reagents/analytic tools; S.-M.L., J.L., and W.-Y.C. analyzed data; and S.-M.L., J.K.-H., and Y.-J.K. wrote the paper.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.1613300114