Scientific Reports (Apr 2017)

Sensitization of glioblastoma tumor micro-environment to chemo- and immunotherapy by Galectin-1 intranasal knock-down strategy

  • Matthias Van Woensel,
  • Thomas Mathivet,
  • Nathalie Wauthoz,
  • Rémi Rosière,
  • Abhishek D. Garg,
  • Patrizia Agostinis,
  • Véronique Mathieu,
  • Robert Kiss,
  • Florence Lefranc,
  • Louis Boon,
  • Jochen Belmans,
  • Stefaan W. Van Gool,
  • Holger Gerhardt,
  • Karim Amighi,
  • Steven De Vleeschouwer

DOI
https://doi.org/10.1038/s41598-017-01279-1
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 14

Abstract

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Abstract In this study, we evaluated the consequences of reducing Galectin-1 (Gal-1) in the tumor micro-environment (TME) of glioblastoma multiforme (GBM), via nose-to-brain transport. Gal-1 is overexpressed in GBM and drives chemo- and immunotherapy resistance. To promote nose-to-brain transport, we designed siRNA targeting Gal-1 (siGal-1) loaded chitosan nanoparticles that silence Gal-1 in the TME. Intranasal siGal-1 delivery induces a remarkable switch in the TME composition, with reduced myeloid suppressor cells and regulatory T cells, and increased CD4+ and CD8+ T cells. Gal-1 knock-down reduces macrophages’ polarization switch from M1 (pro-inflammatory) to M2 (anti-inflammatory) during GBM progression. These changes are accompanied by normalization of the tumor vasculature and increased survival for tumor bearing mice. The combination of siGal-1 treatment with temozolomide or immunotherapy (dendritic cell vaccination and PD-1 blocking) displays synergistic effects, increasing the survival of tumor bearing mice. Moreover, we could confirm the role of Gal-1 on lymphocytes in GBM patients by matching the Gal-1 expression and their T cell signatures. These findings indicate that intranasal siGal-1 nanoparticle delivery could be a valuable adjuvant treatment to increase the efficiency of immune-checkpoint blockade and chemotherapy.