Abstract
Peg3 (paternally expressed gene 3) is an imprinted gene encoding a DNA-binding protein. This gene plays important roles in controlling fetal growth rates and nurturing behaviors. In the current study, a new mutant mouse model has been generated to further characterize the functions of this DNA-binding protein. Besides known phenotypes, this new mutant model also revealed potential roles of Peg3 in mammalian reproduction. Female heterozygotes produce a much smaller number of mature oocytes than the wild-type littermates, resulting in reduced litter sizes. According to genome-wide expression analyses, several placenta-specific gene families are de-repressed in the brain of Peg3 heterozygous embryos, including prolactin, cathepsin and carcinoembryonic antigen cell adhesion molecule (Ceacam) families. The observed de-repression is more pronounced in females than in males. The de-repression of several members of these gene families is observed even in the adult brain, suggesting potential defects in epigenetic setting of the placenta-specific gene families in the Peg3 mutants. Overall, these results indicate that Peg3 likely controls the transcription of several placenta-specific gene families, and further suggest that this predicted transcriptional control by Peg3 might be mediated through unknown epigenetic mechanisms.
Highlights
IntroductionPeg (paternally expressed gene 3) is an imprinted gene located in proximal mouse chromosome 7/human chromosome 19q13.4 [1,2,3]
Peg3 is an imprinted gene located in proximal mouse chromosome 7/human chromosome 19q13.4 [1,2,3]
Reintroducing PEG3 into primary cell lines derived from these cancer patients inhibited cell growth, demonstrating tumor suppressor activity
Summary
Peg (paternally expressed gene 3) is an imprinted gene located in proximal mouse chromosome 7/human chromosome 19q13.4 [1,2,3]. The genomic interval surrounding this gene is filled with lineage-specific Kruppel-type zinc finger genes [3]. According to earlier studies on a mutant mouse line targeting Peg, this gene is involved in controlling milk ‘letdown’ processes and nurturing behaviors in females [5],[6]. The imprinting of Peg is regulated through a 4-kb CpG island surrounding its 1st exon, termed the Peg3-DMR (Differentially Methylated Region) [9]. Reintroducing PEG3 into primary cell lines derived from these cancer patients inhibited cell growth, demonstrating tumor suppressor activity [17],[19]. PEG3 has been often regarded as a potential tumor suppressor in humans
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