Cell Reports (Mar 2018)

Muscle-Specific Histone H3K36 Dimethyltransferase SET-18 Shortens Lifespan of Caenorhabditis elegans by Repressing daf-16a Expression

  • Liangping Su,
  • Hongyuan Li,
  • Cheng Huang,
  • Tingting Zhao,
  • Yongjun Zhang,
  • Xueqing Ba,
  • Zhongwei Li,
  • Yu Zhang,
  • Baiqu Huang,
  • Jun Lu,
  • Yanmei Zhao,
  • Xiaoxue Li

Journal volume & issue
Vol. 22, no. 10
pp. 2716 – 2729

Abstract

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Summary: Mounting evidence shows that histone methylation, a typical epigenetic mark, is crucial for gene expression regulation during aging. Decreased trimethylation of Lys 36 on histone H3 (H3K36me3) in worms and yeast is reported to shorten lifespan. The function of H3K36me2 in aging remains unclear. In this study, we identified Caenorhabditis elegans SET-18 as a histone H3K36 dimethyltransferase. SET-18 deletion extended lifespan and increased oxidative stress resistance, dependent on daf-16 activity in the insulin/IGF pathway. In set-18 mutants, transcription of daf-16 isoform a (daf-16a) was specifically upregulated. Accordingly, a decrease in H3K36me2 on daf-16a promoter was observed. Muscle-specific expression of SET-18 increased in aged worms (day 7 and day 11), attributable to elevation of global H3K36me2 and inhibition of daf-16a expression. Consequently, longevity was shortened. These findings suggested that chromatic repression mediated by tissue-specific H3K36 dimethyltransferase might be detrimental to lifespan and may have implications in human age-related diseases. : Su et al. report that a muscle-specific H3K36 dimethyltransferase SET-18 is activated in aged worm. SET-18 shortens lifespan by repressing daf-16a promoter via H3K36me2 modification. Activation of SET-18 in old age (days 7 and 11) is responsible for increased global H3K36me2 in chromatin and then represses daf-16a transcription and promotes aging of worms. Keywords: SET-18, H3K36me2 modification, lifespan, daf-16a, insulin/IGF-1-like pathway