Cancers (Feb 2021)

miR-21 Plays a Dual Role in Tumor Formation and Cytotoxic Response in Breast Tumors

  • Tu Dan,
  • Anuradha A. Shastri,
  • Ajay Palagani,
  • Simone Buraschi,
  • Thomas Neill,
  • Jason E. Savage,
  • Aastha Kapoor,
  • Tiziana DeAngelis,
  • Sankar Addya,
  • Kevin Camphausen,
  • Renato V. Iozzo,
  • Nicole L. Simone

DOI
https://doi.org/10.3390/cancers13040888
Journal volume & issue
Vol. 13, no. 4
p. 888

Abstract

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Breast cancer (BrCa) relies on specific microRNAs to drive disease progression. Oncogenic miR-21 is upregulated in many cancers, including BrCa, and is associated with poor survival and treatment resistance. We sought to determine the role of miR-21 in BrCa tumor initiation, progression and treatment response. In a triple-negative BrCa model, radiation exposure increased miR-21 in both primary tumor and metastases. In vitro, miR-21 knockdown decreased survival in all BrCa subtypes in the presence of radiation. The role of miR-21 in BrCa initiation was evaluated by implanting wild-type miR-21 BrCa cells into genetically engineered mouse models where miR-21 was intact, heterozygous or globally ablated. Tumors were unable to grow in the mammary fat pads of miR-21−/− mice, and grew in ~50% of miR-21+/− and 100% in miR-21+/+ mice. The contribution of miR-21 to progression and metastases was tested by crossing miR-21−/− mice with mice that spontaneously develop BrCa. The global ablation of miR-21 significantly decreased the tumorigenesis and metastases of BrCa, while sensitizing tumors to radio- and chemotherapeutic agents via Fas/FasL-dependent apoptosis. Therefore, targeting miR-21 alone or in combination with various radio or cytotoxic therapies may represent novel and efficacious therapeutic modalities for the future treatment of BrCa patients.

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