Developmental methylation program and concerted expression of Stx11 in mouse tissues |
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Authors: | Geneviève Marcelin Catherine Diatloff-Zito Annie Nicole Jean-Jacques Robert |
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Affiliation: | 1. INSERM U781, Université René Descartes Paris, H?pital Necker Enfants Malades Clinique Maurice Lamy, 161 rue de Sèvres, 75743, Paris Cedex 15, France 2. Life Science Department, Centre National de la Recherche Scientifique (CNRS), Paris, France 3. Fédération de Pédiatrie, H?pital Necker Enfants Malades, Paris, France
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Abstract: | The human 6q24 region is involved in growth and development, transient neonatal diabetes (TND), cancer, and metabolic dysfunction. To further characterize this region, the developmental status of DNA methylation and expression of Zac1 and Stx11 genes located within the mouse 10A1 region ortholog of human 6q24 were determined. In mice, imprinted Zac1 and Stx11 were highly expressed at the end of fetal development but downregulated at 4 and 11 weeks in brain, pancreas, and heart. Postnatal Zac1 downregulation was independent from promoter methylation of the expressed allele, suggesting the mediation of age-dependent chromatin remodeling. Stx11 nonpromoter CpG island was methylated de novo from E18 to 1 year with tissue-specific kinetics. The high conservation in vertebrates of Stx11 CpG2 is suggestive of an important regulatory function in age-related regional epigenetic state and/or chromatin configuration. Stx11 alleles were unequally expressed in F1 mice tissues, reflecting the influence of cis-regulatory factors on its expression. These data suggest the presence of a methylation domain and a coordinated gene expression pattern in multiple tissues. Methylation variation and allelic regulation of expression may underlie genetic diversity and contribute to disease susceptibility at the 6q24 locus in humans. Electronic supplementary material The online version of this article (doi:) contains supplementary material, which is available to authorized users. |
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