Molecular Oncology (Oct 2021)

Lipocalin 2 promotes inflammatory breast cancer tumorigenesis and skin invasion

  • Emilly S. Villodre,
  • Xiaoding Hu,
  • Richard Larson,
  • Pascal Finetti,
  • Kristen Gomez,
  • Wintana Balema,
  • Shane R. Stecklein,
  • Ginette Santiago‐Sanchez,
  • Savitri Krishnamurthy,
  • Juhee Song,
  • Xiaoping Su,
  • Naoto T. Ueno,
  • Debu Tripathy,
  • Steven Van Laere,
  • François Bertucci,
  • Pablo Vivas‐Mejía,
  • Wendy A. Woodward,
  • Bisrat G. Debeb

DOI
https://doi.org/10.1002/1878-0261.13074
Journal volume & issue
Vol. 15, no. 10
pp. 2752 – 2765

Abstract

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Inflammatory breast cancer (IBC) is an aggressive form of primary breast cancer characterized by rapid onset and high risk of metastasis and poor clinical outcomes. The biological basis for the aggressiveness of IBC is still not well understood and no IBC‐specific targeted therapies exist. In this study, we report that lipocalin 2 (LCN2), a small secreted glycoprotein belonging to the lipocalin superfamily, is expressed at significantly higher levels in IBC vs non‐IBC tumors, independently of molecular subtype. LCN2 levels were also significantly higher in IBC cell lines and in their culture media than in non‐IBC cell lines. High expression was associated with poor‐prognosis features and shorter overall survival in IBC patients. Depletion of LCN2 in IBC cell lines reduced colony formation, migration, and cancer stem cell populations in vitro and inhibited tumor growth, skin invasion, and brain metastasis in mouse models of IBC. Analysis of our proteomics data showed reduced expression of proteins involved in cell cycle and DNA repair in LCN2‐silenced IBC cells. Our findings support that LCN2 promotes IBC tumor aggressiveness and offer a new potential therapeutic target for IBC.

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