MEG3 long noncoding RNA regulates the TGF-β pathway genes through formation of RNA–DNA triplex structures

نویسندگان

  • Tanmoy Mondal
  • Santhilal Subhash
  • Roshan Vaid
  • Stefan Enroth
  • Sireesha Uday
  • Björn Reinius
  • Sanhita Mitra
  • Arif Mohammed
  • Alva Rani James
  • Emily Hoberg
  • Aristidis Moustakas
  • Ulf Gyllensten
  • Steven J.M. Jones
  • Claes M Gustafsson
  • Andrew H Sims
  • Fredrik Westerlund
  • Eduardo Gorab
  • Chandrasekhar Kanduri
چکیده

Long noncoding RNAs (lncRNAs) regulate gene expression by association with chromatin, but how they target chromatin remains poorly understood. We have used chromatin RNA immunoprecipitation-coupled high-throughput sequencing to identify 276 lncRNAs enriched in repressive chromatin from breast cancer cells. Using one of the chromatin-interacting lncRNAs, MEG3, we explore the mechanisms by which lncRNAs target chromatin. Here we show that MEG3 and EZH2 share common target genes, including the TGF-β pathway genes. Genome-wide mapping of MEG3 binding sites reveals that MEG3 modulates the activity of TGF-β genes by binding to distal regulatory elements. MEG3 binding sites have GA-rich sequences, which guide MEG3 to the chromatin through RNA-DNA triplex formation. We have found that RNA-DNA triplex structures are widespread and are present over the MEG3 binding sites associated with the TGF-β pathway genes. Our findings suggest that RNA-DNA triplex formation could be a general characteristic of target gene recognition by the chromatin-interacting lncRNAs.

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MEG3 long noncoding RNA regulates the TGF-b pathway genes through formation of RNA–DNA triplex structures

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2015