Breast Cancer Research (Aug 2024)

The SEMA3F-NRP1/NRP2 axis is a key factor in the acquisition of invasive traits in in situ breast ductal carcinoma

  • Núria Moragas,
  • Patricia Fernandez-Nogueira,
  • Leire Recalde-Percaz,
  • Jamie L. Inman,
  • Anna López-Plana,
  • Helga Bergholtz,
  • Aleix Noguera-Castells,
  • Pedro J. del Burgo,
  • Xieng Chen,
  • Therese Sorlie,
  • Pere Gascón,
  • Paloma Bragado,
  • Mina Bissell,
  • Neus Carbó,
  • Gemma Fuster

DOI
https://doi.org/10.1186/s13058-024-01871-0
Journal volume & issue
Vol. 26, no. 1
pp. 1 – 23

Abstract

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Abstract Background A better understanding of ductal carcinoma in situ (DCIS) is urgently needed to identify these preinvasive lesions as distinct clinical entities. Semaphorin 3F (SEMA3F) is a soluble axonal guidance molecule, and its coreceptors Neuropilin 1 (NRP1) and NRP2 are strongly expressed in invasive epithelial BC cells. Methods We utilized two cell line models to represent the progression from a healthy state to the mild-aggressive or ductal carcinoma in situ (DCIS) stage and, ultimately, to invasive cell lines. Additionally, we employed in vivo models and conducted analyses on patient databases to ensure the translational relevance of our results. Results We revealed SEMA3F as a promoter of invasion during the DCIS-to-invasive ductal carcinoma transition in breast cancer (BC) through the action of NRP1 and NRP2. In epithelial cells, SEMA3F activates epithelialmesenchymal transition, whereas it promotes extracellular matrix degradation and basal membrane and myoepithelial cell layer breakdown. Conclusions Together with our patient database data, these proof-of-concept results reveal new SEMA3F-mediated mechanisms occurring in the most common preinvasive BC lesion, DCIS, and represent potent and direct activation of its transition to invasion. Moreover, and of clinical and therapeutic relevance, the effects of SEMA3F can be blocked directly through its coreceptors, thus preventing invasion and keeping DCIS lesions in the preinvasive state.

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