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CEBPB-high dormant tumor cells drive immune evasion via S100A8 orchestrated tumor-associated macrophages reprogramming - PubMed

4 days ago
  • #CEBPB
  • #Immune Evasion
  • #Tumor Dormancy
  • CEBPB-high dormant tumor cells drive immune evasion in Triple Negative Breast Cancer (TNBC).
  • Dormant tumor cells resist immune checkpoint blockade (ICB) therapy and reside in an immunosuppressive niche.
  • CEBPB maintains tumor dormancy by activating cell cycle negative regulators like CCNG2.
  • CEBPB orchestrates a tumor-supportive microenvironment by recruiting and polarizing M2 macrophages and suppressing T cells.
  • S100A8 is a key transcriptional target of CEBPB that promotes M2 macrophage polarization.
  • Targeting CEBPB or S100A8 can overcome ICB resistance and remodel the tumor microenvironment.
  • The CEBPB-S100A8 axis is a promising therapeutic target to enhance ICB efficacy in TNBC.