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Oncotarget

Anti-PD-1 Immune Checkpoint Therapy Resistance, Macrophages and the Wnt Pathway

Jan 5, 2023
Researchers discuss the resistance of MMTV New TATTAC mice to anti-PD-1 therapy, linked to macrophage infiltration, fibrosis, and the Wnt pathway in breast cancer. They monitored drug response and identified processes associated with lack of responsiveness to the treatment.
03:34

Podcast summary created with Snipd AI

Quick takeaways

  • Fibrosis in breast cancer creates an immune-tolerant microenvironment affecting patient survival.
  • Enhancing PD1 immune checkpoint therapy sensitivity involves targeting tumor microenvironment and WNT signaling pathway.

Deep dives

Challenges in Cancer Therapy: Tumor Microenvironment Factors

Identifying factors in the tumor microenvironment that contribute to tumor progression and immune tolerance is crucial in cancer therapy. In breast cancer, fibrosis plays a significant role in creating an immune tolerant microenvironment, ultimately affecting patient survival. Researchers from various institutions collaborated to investigate the association between immune tolerance and the immune checkpoint PD1. Through a study involving new TATTAC mice models and anti-PD1 therapy, they found that tumor progression was unaffected by anti-PD1 treatment, indicating resistance. Processes linked to this resistance included increased tumor-associated macrophages, epithelial to mesenchymal transition, fibroblast proliferation, and activation of the WNT signaling pathway.

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