AI Article Synopsis

  • Nucleosome positioning maps reveal that Transcription Start Sites (TSSs) are characterized by a lack of nucleosomes, surrounded by well-positioned nucleosomes in various organisms.
  • In mouse liver, most genes contain a notable nucleosome with the histone variant H2A.Z in their promoter regions, and clustering of genes is observed based on H2A.Z's distance from the TSS.
  • Genes lacking H2A.Z show lower expression, while those with H2A.Z closer to the TSS exhibit higher expression levels, indicating that TSS accessibility and H2A.Z proximity influence gene expression.

Article Abstract

Nucleosome positioning maps of several organisms have shown that Transcription Start Sites (TSSs) are marked by nucleosome depleted regions flanked by strongly positioned nucleosomes. Using genome-wide nucleosome maps and histone variant occupancy in the mouse liver, we show that the majority of genes were associated with a single prominent H2A.Z containing nucleosome in their promoter region. We classified genes into clusters depending on the proximity of H2A.Z to the TSS. The genes with no detectable H2A.Z showed lowest expression level, whereas H2A.Z was positioned closer to the TSS of genes with higher expression levels. We confirmed this relation between the proximity of H2A.Z and expression level in the brain. The proximity of histone variant H2A.Z, but not H3.3 to the TSS, over seven consecutive nucleosomes, was correlated with expression. Further, a nucleosome was positioned over the TSS of silenced genes while it was displaced to expose the TSS in highly expressed genes. Our results suggest that gene expression levels in vivo are determined by accessibility of the TSS and proximity of H2A.Z.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3467062PMC
http://dx.doi.org/10.1093/nar/gks665DOI Listing

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