AI Article Synopsis

  • The study identifies the gene Sfmbt2 as an imprinted gene in the proximal region of murine chromosome 2, expressing from the paternal allele in early embryos and extraembryonic tissues.
  • Sfmbt2 and a non-coding antisense transcript were found to be the only imprinted genes in a 3.9 Mb region, while rat Sfmbt2 also shows imprinting, but other mammals like cows and pigs do not.
  • The researchers suggest that the presence of a block of miRNAs in the Sfmbt2 gene may be linked to its imprinting, highlighting potential evolutionary changes in imprinting mechanisms across different species.

Article Abstract

Background: The proximal region of murine Chr 2 has long been known to harbour one or more imprinted genes from classic genetic studies involving reciprocal translocations. No imprinted gene had been identified from this region until our study demonstrated that the PcG gene Sfmbt2 is expressed from the paternally inherited allele in early embryos and extraembryonic tissues. Imprinted genes generally reside in clusters near elements termed Imprinting Control Regions (ICRs), suggesting that Sfmbt2 might represent an anchor for a new imprinted domain.

Results: We analyzed allelic expression of approximately 20 genes within a 3.9 Mb domain and found that Sfmbt2 and an overlapping non-coding antisense transcript are the only imprinted genes in this region. These transcripts represent a very narrow imprinted gene locus. We also demonstrate that rat Sfmbt2 is imprinted in extraembryonic tissues. An interesting feature of both mouse and rat Sfmbt2 genes is the presence of a large block of miRNAs in intron 10. Other mammals, including the bovine, lack this block of miRNAs. Consistent with this association, we show that human and bovine Sfmbt2 are biallelic. Other evidence indicates that pig Sfmbt2 is also not imprinted. Further strengthening the argument for recent evolution of Sfmbt2 is our demonstration that a more distant muroid rodent, Peromyscus also lacks imprinting and the block of miRNAs.

Conclusions: These observations are consistent with the hypothesis that the block of miRNAs are driving imprinting at this locus. Our results are discussed in the context of ncRNAs at other imprinted loci. Accession numbers for Peromyscus cDNA and intron 10 genomic DNA are [Genbank:HQ416417 and Genbank:HQ416418], respectively.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3110154PMC
http://dx.doi.org/10.1186/1471-2164-12-204DOI Listing

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