eLife (Dec 2019)

Repressive H3K9me2 protects lifespan against the transgenerational burden of COMPASS activity in C. elegans

  • Teresa Wei-sy Lee,
  • Heidi Shira David,
  • Amanda Kathryn Engstrom,
  • Brandon Scott Carpenter,
  • David John Katz

DOI
https://doi.org/10.7554/eLife.48498
Journal volume & issue
Vol. 8

Abstract

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In Caenorhabditis elegans, mutations in WDR-5 and other components of the COMPASS H3K4 methyltransferase complex extend lifespan and enable its inheritance. Here, we show that wdr-5 mutant longevity is itself a transgenerational trait that corresponds with a global enrichment of the heterochromatin factor H3K9me2 over twenty generations. In addition, we find that the transgenerational aspects of wdr-5 mutant longevity require the H3K9me2 methyltransferase MET-2, and can be recapitulated by removal of the putative H3K9me2 demethylase JHDM-1. Finally, we show that the transgenerational acquisition of longevity in jhdm-1 mutants is associated with accumulating genomic H3K9me2 that is inherited by their long-lived wild-type descendants at a subset of loci. These results suggest that heterochromatin facilitates the transgenerational establishment and inheritance of a complex trait. Based on these results, we propose that transcription-coupled H3K4me via COMPASS limits lifespan by encroaching upon domains of heterochromatin in the genome.

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