PLoS Genetics (Feb 2009)

Genome-wide analysis of factors affecting transcription elongation and DNA repair: a new role for PAF and Ccr4-not in transcription-coupled repair.

  • Hélène Gaillard,
  • Cristina Tous,
  • Javier Botet,
  • Cristina González-Aguilera,
  • Maria José Quintero,
  • Laia Viladevall,
  • María L García-Rubio,
  • Alfonso Rodríguez-Gil,
  • Antonio Marín,
  • Joaquín Ariño,
  • José Luis Revuelta,
  • Sebastián Chávez,
  • Andrés Aguilera

DOI
https://doi.org/10.1371/journal.pgen.1000364
Journal volume & issue
Vol. 5, no. 2
p. e1000364

Abstract

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RNA polymerases frequently deal with a number of obstacles during transcription elongation that need to be removed for transcription resumption. One important type of hindrance consists of DNA lesions, which are removed by transcription-coupled repair (TC-NER), a specific sub-pathway of nucleotide excision repair. To improve our knowledge of transcription elongation and its coupling to TC-NER, we used the yeast library of non-essential knock-out mutations to screen for genes conferring resistance to the transcription-elongation inhibitor mycophenolic acid and the DNA-damaging agent 4-nitroquinoline-N-oxide. Our data provide evidence that subunits of the SAGA and Ccr4-Not complexes, Mediator, Bre1, Bur2, and Fun12 affect transcription elongation to different extents. Given the dependency of TC-NER on RNA Polymerase II transcription and the fact that the few proteins known to be involved in TC-NER are related to transcription, we performed an in-depth TC-NER analysis of a selection of mutants. We found that mutants of the PAF and Ccr4-Not complexes are impaired in TC-NER. This study provides evidence that PAF and Ccr4-Not are required for efficient TC-NER in yeast, unraveling a novel function for these transcription complexes and opening new perspectives for the understanding of TC-NER and its functional interconnection with transcription elongation.