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Oxidation of 5-methylaminomethyl uridine (mnm⁵U) by Oxone Leads to Aldonitrone Derivatives.

Qishun ZhouBao Tram Vu NgocGrazyna LeszczynskaJean-Luc StiglianiGeneviève Pratviel
Published in: Biomolecules (2018)
Oxidative RNA damage is linked to cell dysfunction and diseases. The present work focuses on the in vitro oxidation of 5-methylaminomethyl uridine (mnm⁵U), which belongs to the numerous post-transcriptional modifications that are found in tRNA. The reaction of oxone with mnm⁵U in water at pH 7.5 leads to two aldonitrone derivatives. They form by two oxidation steps and one dehydration step. Therefore, the potential oxidation products of mnm⁵U in vivo may not be only aldonitrones, but also hydroxylamine and imine derivatives (which may be chemically more reactive). Irradiation of aldonitrone leads to unstable oxaziridine derivatives that are susceptible to isomerization to amide or to hydrolysis to aldehyde derivative.
Keyphrases
  • hydrogen peroxide
  • structure activity relationship
  • electron transfer
  • oxidative stress
  • gene expression
  • visible light
  • single cell
  • stem cells
  • cell therapy
  • risk assessment
  • radiation therapy
  • human health
  • climate change