eLife (Mar 2018)

Efficient termination of nuclear lncRNA transcription promotes mitochondrial genome maintenance

  • Dorine Jeanne Mariëtte du Mee,
  • Maxim Ivanov,
  • Joseph Paul Parker,
  • Stephen Buratowski,
  • Sebastian Marquardt

DOI
https://doi.org/10.7554/eLife.31989
Journal volume & issue
Vol. 7

Abstract

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Most DNA in the genomes of higher organisms does not code for proteins. RNA Polymerase II (Pol II) transcribes non-coding DNA into long non-coding RNAs (lncRNAs), but biological roles of lncRNA are unclear. We find that mutations in the yeast lncRNA CUT60 result in poor growth. Defective termination of CUT60 transcription causes read-through transcription across the ATP16 gene promoter. Read-through transcription localizes chromatin signatures associated with Pol II elongation to the ATP16 promoter. The act of Pol II elongation across this promoter represses functional ATP16 expression by a Transcriptional Interference (TI) mechanism. Atp16p function in the mitochondrial ATP-synthase complex promotes mitochondrial DNA stability. ATP16 repression by TI through inefficient termination of CUT60 therefore triggers mitochondrial genome loss. Our results expand the functional and mechanistic implications of non-coding DNA in eukaryotes by highlighting termination of nuclear lncRNA transcription as mechanism to stabilize an organellar genome.

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