Published January 12, 2020 | Version v1
Journal article Open

TGF-β inhibition combined with cytotoxic nanomedicine normalizes triple negative breast cancer microenvironment towards anti-tumor immunity

Creators

  • 1. University of Cyprus
  • 2. University of Cyrpus
  • 3. European University Cyprus
  • 4. The University of Tokyo
  • 5. Center for the Study of Haematological Malignancies
  • 6. Center for the Study of Haematological Diseases
  • 7. Karaiskakio Foundation
  • 8. Center for Study of Haematological Diseases
  • 9. Innovation Center of NanoMedicine, Kawasaki Institute of Industrial Promotion

Description

Tumor normalization strategies aim to improve tumor blood vessel functionality (i.e., perfusion) by reducing the hyper-permeability of tumor vessels or restoring compressed vessels. Despite progress in strategies to normalize the tumor microenvironment (TME), their combinatorial antitumor effects with nanomedicine and immunotherapy remain unexplored. Methods: Here, we re-purposed the TGF-β inhibitor tranilast, an approved anti-fibrotic and antihistamine drug, and combined it with Doxil nanomedicine to normalize the TME, increase perfusion and oxygenation, and enhance anti-tumor immunity. Specifically, we employed two triple-negative breast cancer (TNBC) mouse models to primarily evaluate the therapeutic and normalization effects of tranilast combined with doxorubicin and Doxil. We demonstrated the optimized normalization effects of tranilast combined with Doxil and extended our analysis to
investigate the effect of TME normalization to the efficacy of immune checkpoint inhibitors. Results: Combination of tranilast with Doxil caused a pronounced reduction in extracellular matrix components and an increase in the intratumoral vessel diameter and pericyte coverage, indicators of TME normalization. These modifications resulted in a significant increase in tumor perfusion and
oxygenation and enhanced treatment efficacy as indicated by the notable reduction in tumor size. Tranilast further normalized the immune TME by restoring the infiltration of T cells and increasing the fraction of T cells that migrate away from immunosuppressive cancer-associated fibroblasts. Furthermore, we found that combining tranilast with Doxil nanomedicine, significantly improved
immunostimulatory M1 macrophage content in the tumorigenic tissue and improved the efficacy of the immune checkpoint blocking antibodies anti-PD-1/anti-CTLA-4. Conclusion: Combinatorial treatment of tranilast with Doxil optimizes TME normalization,
improves immunostimulation and enhances the efficacy of immunotherapy. 

Files

Panagi_etal_Theranostics_2020.pdf

Files (3.0 MB)

Name Size Download all
md5:2bec7ca35bb29037d76fc25e878a165c
3.0 MB Preview Download

Additional details

Funding

REENGINEERINGCANCER – Re-engineering the tumor microenvironment to alleviate mechanical stresses and improve chemotherapy 336839
European Commission