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Article

Chromosome-Wide Analysis of Parental Allele-Specific Chromatin and DNA Methylation

, , , , , , & show all
Pages 1757-1770 | Received 17 Aug 2010, Accepted 04 Feb 2011, Published online: 20 Mar 2023
 

Abstract

To reveal the extent of domain-wide epigenetic features at imprinted gene clusters, we performed a high-resolution allele-specific chromatin analysis of over 100 megabases along the maternally or paternally duplicated distal chromosome 7 (Chr7) and Chr15 in mouse embryo fibroblasts (MEFs). We found that reciprocal allele-specific features are limited to imprinted genes and their differentially methylated regions (DMRs), whereas broad local enrichment of H3K27me3 (BLOC) is a domain-wide feature at imprinted clusters. We uncovered novel allele-specific features of BLOCs. A maternally biased BLOC was found along the H19-Igf2 domain. A paternal allele-specific gap was found along Kcnq1ot1, interrupting a biallelic BLOC in the Kcnq1-Cdkn1c domain. We report novel allele-specific chromatin marks at the Peg13 and Slc38a4 DMRs, Cdkn1c upstream region, and Inpp5f_v2 DMR and paternal allele-specific CTCF binding at the Peg13 DMR. Additionally, we derived an imprinted gene predictor algorithm based on our allele-specific chromatin mapping data. The binary predictor H3K9ac and CTCF or H3K4me3 in one allele and H3K9me3 in the reciprocal allele, using a sliding-window approach, recognized with precision the parental allele specificity of known imprinted genes, H19, Igf2, Igf2as, Cdkn1c, Kcnq1ot1, and Inpp5f_v2 on Chr7 and Peg13 and Slc38a4 on Chr15. Chromatin features, therefore, can unequivocally identify genes with imprinted expression.

View publisher note:
Articles of Significant Interest Selected from This Issue by the Editors

Supplemental material for this article may be found at http://dx.doi.org/10.1128/MCB.00961-10.

ACKNOWLEDGMENTS

We thank Diana Tran and Guillermo Rivas for performing the allele-specific RNA quantitation and Mai Dang, summer student, for technical assistance.

This work was supported by a Public Health Service grant (GM064378) from the National Institute of General Medicine to P.E.S.

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