Highlights
• M2-polarized TAMs driver immunosuppression and progression in PC, strongly correlating with poor patient prognosis.
• Targeting TAMs via CSF-1R, STAT3, or CD40 reprogram the TME, reducing M2-like TAMs and promoting anti-tumor immunity.
• TAM interventions combined with (PD-1/PD-L1 blockade or chemotherapy shown synergistic effects in preclinical and clinical studies.
• Targeting galectin-9/TIM-3, SYK, or exosomal microRNA signaling disrupts pro-tumorigenic TAM-cancer cell crosstalk.
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