Cell Death and Disease (Mar 2024)

Antibiotics treatment promotes vasculogenesis in the brain of glioma-bearing mice

  • Maria Rosito,
  • Javeria Maqbool,
  • Alice Reccagni,
  • Ottavia Giampaoli,
  • Fabio Sciubba,
  • Fabrizio Antonangeli,
  • Ferdinando Scavizzi,
  • Marcello Raspa,
  • Federica Cordella,
  • Lucrezia Tondo,
  • Silvia Di Angelantonio,
  • Flavia Trettel,
  • Alfredo Miccheli,
  • Giuseppina D’Alessandro,
  • Cristina Limatola

DOI
https://doi.org/10.1038/s41419-024-06578-w
Journal volume & issue
Vol. 15, no. 3
pp. 1 – 18

Abstract

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Abstract In recent years, several studies described the close relationship between the composition of gut microbiota and brain functions, highlighting the importance of gut-derived metabolites in mediating neuronal and glial cells cross-talk in physiological and pathological condition. Gut dysbiosis may affects cerebral tumors growth and progression, but the specific metabolites involved in this modulation have not been identified yet. Using a syngeneic mouse model of glioma, we have investigated the role of dysbiosis induced by the administration of non-absorbable antibiotics on mouse metabolome and on tumor microenvironment. We report that antibiotics treatment induced: (1) alteration of the gut and brain metabolome profiles; (2) modeling of tumor microenvironment toward a pro-angiogenic phenotype in which microglia and glioma cells are actively involved; (3) increased glioma stemness; (4) trans-differentiation of glioma cells into endothelial precursor cells, thus increasing vasculogenesis. We propose glycine as a metabolite that, in ABX-induced dysbiosis, shapes brain microenvironment and contributes to glioma growth and progression.