PLoS ONE (Jan 2024)

3-nitropyridine analogues as novel microtubule-targeting agents.

  • Jean Herman,
  • Els Vanstreels,
  • Dorothée Bardiot,
  • Andrea E Prota,
  • Natacha Gaillard,
  • Ling-Jie Gao,
  • Thomas Vercruysse,
  • Leentje Persoons,
  • Tinne Daems,
  • Mark Waer,
  • Piet Herdewijn,
  • Thierry Louat,
  • Michel O Steinmetz,
  • Steven De Jonghe,
  • Ben Sprangers,
  • Dirk Daelemans

DOI
https://doi.org/10.1371/journal.pone.0307153
Journal volume & issue
Vol. 19, no. 11
p. e0307153

Abstract

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Microtubule-targeting agents are an important class of anti-cancer drugs; their full potential is however not realized because of significant myelotoxicity and neurotoxicity. We here report 3-nitropyridine analogues as a novel group of microtubule-targeting agents with potent anti-cancer effects against a broad range of cancer types. We show that these 3-nitropyridines induce cell cycle arrest in the G2-M phase and inhibit tubulin polymerization by interacting with tubulin. Determination of the tubulin-4AZA2996 structure by X-ray crystallography demonstrated that this class of compounds binds to the colchicine-site of tubulin. Furthermore, the anti-cancer effect was demonstrated both in vitro and in vivo in a murine heterotopic xenograft model of colon cancer. When administered intravenously, 4AZA2891 effectively inhibited cancer growth. Whereas 3-nitropyridine compounds do not induce myelotoxicity at pharmacological doses, the neurotoxicity associated with microtubule-targeting agents is still present.