International Journal of Molecular Sciences (Dec 2021)

Human TRMT112-Methyltransferase Network Consists of Seven Partners Interacting with a Common Co-Factor

  • Baiba Brūmele,
  • Margit Mutso,
  • Lilian Telanne,
  • Kadri Õunap,
  • Karīna Spunde,
  • Aare Abroi,
  • Reet Kurg

DOI
https://doi.org/10.3390/ijms222413593
Journal volume & issue
Vol. 22, no. 24
p. 13593

Abstract

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Methylation is an essential epigenetic modification mainly catalysed by S-Adenosyl methionine-dependent methyltransferases (MTases). Several MTases require a cofactor for their metabolic stability and enzymatic activity. TRMT112 is a small evolutionary conserved protein that acts as a co-factor and activator for different MTases involved in rRNA, tRNA and protein methylation. Using a SILAC screen, we pulled down seven methyltransferases—N6AMT1, WBSCR22, METTL5, ALKBH8, THUMPD2, THUMPD3 and TRMT11—as interaction partners of TRMT112. We showed that TRMT112 stabilises all seven MTases in cells. TRMT112 and MTases exhibit a strong mutual feedback loop when expressed together in cells. TRMT112 interacts with its partners in a similar way; however, single amino acid mutations on the surface of TRMT112 reveal several differences as well. In summary, mammalian TRMT112 can be considered as a central “hub” protein that regulates the activity of at least seven methyltransferases.

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