4.3 Review

Lysine Methyltransferases Signaling: Histones are Just the Tip of the Iceberg

Journal

CURRENT PROTEIN & PEPTIDE SCIENCE
Volume 21, Issue 7, Pages 655-674

Publisher

BENTHAM SCIENCE PUBL LTD
DOI: 10.2174/1871527319666200102101608

Keywords

Lysine methylation; protein lysine methyltransferases; KMT; cancer; histone; signalling

Funding

  1. Agence Nationale de la Recherche
  2. Fondation ARC
  3. Ligue contre le Cancer [ANR-AAP-CE11JCJC2016]
  4. Fondation pour la Recherche Medicale [ECO20170637491]

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Protein lysine methylation is a functionally diverse post-translational modification involved in various major cellular processes. Lysine methylation can modulate proteins activity, stability, localization, and/or interaction, resulting in specific downstream signaling and biological outcomes. Lysine methylation is a dynamic and fine-tuned process, deregulation of which often leads to human pathologies. In particular, the lysine methylome and its associated signaling network can be linked to carcinogenesis and cancer progression. Histone modifications and chromatin regulation is a major aspect of lysine metbylation importance, but increasing evidence suggests that a high relevance and impact of non-histone lysine methylation signaling has emerged in recent years. In this review, we draw an updated picture of the current scientific knowledge regarding non-histone lysine methylation signaling and its implication in physiological and pathological processes. We aim to demonstrate the significance of lysine methylation as a major and yet underestimated posttranslational modification, and to raise the importance of this modification in both epigenetic and cellular signaling by focusing on the observed activities of SET- and 7 beta-strand-containing human lysine methyltransferases. Recent evidence suggests that what has been observed so far regarding lysine methylation's implication in human pathologies is only the tip of the iceberg. Therefore, the exploration of the methylome network raises the possibility to use these enzymes and their substrates as promising new therapeutic targets for the development of future epigenetic and methyllysine signaling cancer treatments.

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