AI Article Synopsis

  • The amount of noncoding DNA increases with organism complexity, with humans having about 99% noncoding DNA, much of which produces noncoding RNA (ncRNA).
  • Noncoding transcription from intergenic regions in the human HOXA cluster is linked to the activity of nearby HOXA genes and is influenced by retinoic acid, aligning with the activation pattern of the cluster.
  • The activation of these noncoding transcripts is associated with changes in histone modifications and a decrease in repressive interactions, suggesting that noncoding transcription plays a crucial role in activating and maintaining HOX clusters.

Article Abstract

The ratio of noncoding to protein coding DNA rises with the complexity of the organism, culminating in nearly 99% of nonprotein coding DNA in humans. Nevertheless, a large portion of these regions is transcribed, creating the alleged paradox that noncoding RNA (ncRNA) represents the largest output of the human genome. Such a complex scenario may include epigenetic mechanisms where ncRNAs would be involved in chromatin regulation. We have investigated the intergenic, noncoding transcriptomes of mammalian HOX clusters. We show that "opposite strand transcription" from the intergenic spacer regions in the human HOXA cluster correlates with the activity state of adjacent HOXA genes. This noncoding transcription is regulated by the retinoic acid morphogen and follows the colinear activation pattern of the cluster. Opening of the cluster at sites of activation of intergenic transcripts is accompanied by changes in histone modifications and a loss of interaction with Polycomb group (PcG) repressive complexes. We propose that noncoding transcription is of fundamental importance for the opening and maintenance of the active state of HOX clusters.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1781374PMC
http://dx.doi.org/10.1261/rna.266707DOI Listing

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