PLoS Genetics (Jun 2021)

An enhancer screen identifies new suppressors of small-RNA-mediated epigenetic gene silencing.

  • Yukiko Shimada,
  • Sarah H Carl,
  • Merle Skribbe,
  • Valentin Flury,
  • Tahsin Kuzdere,
  • Georg Kempf,
  • Marc Bühler

DOI
https://doi.org/10.1371/journal.pgen.1009645
Journal volume & issue
Vol. 17, no. 6
p. e1009645

Abstract

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Small non-protein coding RNAs are involved in pathways that control the genome at the level of chromatin. In Schizosaccharomyces pombe, small interfering RNAs (siRNAs) are required for the faithful propagation of heterochromatin that is found at peri-centromeric repeats. In contrast to repetitive DNA, protein-coding genes are refractory to siRNA-mediated heterochromatin formation, unless siRNAs are expressed in mutant cells. Here we report the identification of 20 novel mutant alleles that enable de novo formation of heterochromatin at a euchromatic protein-coding gene by using trans-acting siRNAs as triggers. For example, a single amino acid substitution in the pre-mRNA cleavage factor Yth1 enables siRNAs to trigger silent chromatin formation with unparalleled efficiency. Our results are consistent with a kinetic nascent transcript processing model for the inhibition of small-RNA-directed de novo formation of heterochromatin and lay a foundation for further mechanistic dissection of cellular activities that counteract epigenetic gene silencing.