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SIGLEC10 Macrophages Drive Gastric Cancer Progression by Suppressing CD8 T Cell Function

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Abstract

Existing immune checkpoint inhibitors focus on activating T cells and show limited effectiveness in gastric cancer (GC). SIGLEC10 is identified as a novel tumor-associated macrophage-related immune checkpoint in other cancer types. However, its immunosuppressive role and clinical significance in GC remain unclear. In this study, we find a dominant expression of SIGLEC10 on CD68 macrophages in GC. SIGLEC10 can suppress the proliferation and function of tumor-infiltrating CD8 T cells in vitro via the Akt/P38/Erk signaling pathway. Furthermore, in ex vivo and in vivo models, SIGLEC10 blockade promotes CD8 T cell effector function. Finally, SIGLEC10 macrophages are positively correlated with the adverse prognosis of GC. Our study highlights that SIGLEC10 directly suppresses T cell function and serves as a promising target for immunotherapy and suggests SIGLEC10 macrophages as a novel potential predictor of the clinical prognosis of GC.

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