Undermethylation of structural gene sequences in extraembryonic lineages of the mouse |
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| Authors: | J Rossant J P Sanford V M Chapman G K Andrews |
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| Affiliation: | 2. North Florida Research and Education Center, University of Florida, Marianna 32446;3. Department of Animal and Dairy Science, University of Georgia, Tifton 31793;1. Department of Pharmacodynamics, College of Pharmacy, University of Florida, United States;2. Department of Physiology and Functional Genomics, College of Medicine, University of Florida, United States |
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| Abstract: | The first two lineages to differentiate in the mouse embryo are the trophectoderm and primitive endoderm, which give rise to various extraembryonic structures only. Previous work has shown that all derivatives of these two lineages share the property of undermethylation of repetitive DNA sequences, both satellite and dispersed. Here we show that this undermethylation is not a peculiarity of these repetitive elements but is also a feature of structural gene sequences within both lineages. alpha-Fetoprotein, albumin, and major urinary protein gene sequences all showed extensive undermethylation at MspI restriction sites in extraembryonic lineages, which did not correlate with their expression in these tissues. The same sequences were heavily methylated in embryonic tissues as early as 7.5 days of development. There are, therefore, major global differences in DNA methylation between the earliest cell lineages to be established in the mouse embryo. The significance of these differences for cellular commitment events remains to be elucidated. |
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