Cancers (Nov 2020)

Targeting Neuropilin-1 with Nanobodies Reduces Colorectal Carcinoma Development

  • Yannick De Vlaeminck,
  • Stefano Bonelli,
  • Robin Maximilian Awad,
  • Maarten Dewilde,
  • Sabrina Rizzolio,
  • Quentin Lecocq,
  • Evangelia Bolli,
  • Ana Rita Santos,
  • Damya Laoui,
  • Steve Schoonooghe,
  • Luca Tamagnone,
  • Cleo Goyvaerts,
  • Massimiliano Mazzone,
  • Karine Breckpot,
  • Jo A. Van Ginderachter

DOI
https://doi.org/10.3390/cancers12123582
Journal volume & issue
Vol. 12, no. 12
p. 3582

Abstract

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Neuropilin-1 (NRP-1) is a co-receptor for semaphorins and vascular endothelial growth factor (VEGF) family members that can be expressed on cancer cells and tumor-infiltrating myeloid, endothelial and lymphoid cells. It has been linked to a tumor-promoting environment upon interaction with semaphorin 3A (Sema3A). Nanobodies (Nbs) targeting NRP-1 were generated for their potential to hamper the NRP-1/Sema3A interaction and their impact on colorectal carcinoma (CRC) development was evaluated in vivo through the generation of anti-NRP-1-producing CRC cells. We observed that tumor growth was significantly delayed and survival prolonged when the anti-NRP-1 Nbs were produced in vivo. We further analyzed the tumor microenvironment and observed that the pro-inflammatory MHC-IIhigh/trophic MHC-IIlow macrophage ratio was increased in tumors that produce anti-NRP-1 Nbs. This finding was corroborated by an increase in the expression of genes associated with MHC-IIhigh macrophages and a decrease in the expression of MHC-IIlow macrophage-associated genes in the macrophage pool sorted from anti-NRP-1 Nb-producing tumors. Moreover, we observed a significantly higher percentage of tumor-associated antigen-specific CD8+ T cells in tumors producing anti-NRP-1 Nbs. These data demonstrate that an intratumoral expression of NRP-1/Sema3A blocking biologicals increases anti-tumor immunity.

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