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Gene Expression

DNA Methylation Profile of the Mouse Skeletal α-Actin Promoter during Development and Differentiation

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Pages 164-172 | Received 04 Aug 1998, Accepted 17 Sep 1998, Published online: 28 Mar 2023
 

Abstract

Genomic levels of DNA methylation undergo widespread alterations in early embryonic development. However, changes in embryonic methylation have proven difficult to study at the level of single-copy genes due to the small amount of tissue available for assay. This study provides the first detailed analysis of the methylation state of a tissue-specific gene through early development and differentiation. Using bisulfite sequencing, we mapped the methylation profile of the tissue-specific mouse skeletal α-actin promoter at all stages of development, from gametes to postimplantation embryos. We show that the α-actin promoter, which is fully methylated in the sperm and essentially unmethylated in the oocyte, undergoes a general demethylation from morula to blastocyst stages, although the blastula is not completely demethylated. Remethylation of the α-actin promoter occurs after implantation in a stochastic pattern, with some molecules being extensively methylated and others sparsely methylated. Moreover, we demonstrate that tissue-specific expression of the skeletal α-actin gene in the adult mouse does not correlate with the methylation state of the promoter, as we find a similar low level of methylation in both expressing and one of the two nonexpressing tissues tested. However, a subset of CpG sites within the skeletal α-actin promoter are preferentially methylated in liver, a nonexpressing tissue.

ACKNOWLEDGMENTS

We thank Louise McDonald and Graham Kay, Queensland Institute of Medical Research, and Daniel Cass, New Children’s Hospital, Westmead, New South Wales, Australia, for assistance in obtaining mouse embryos used in this work. We also thank Marianne Frommer and Peter Molloy for critical reading of the manuscript.

P.W. is supported by an APRA scholarship.

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