March 3, 2026Open Access

DUSP22 dephosphorylates LGALS1 to enhance T cell-driven antitumor immunity

Key Points

DUSP22 dephosphorylates LGALS1, enhancing T cell-driven antitumor immunity in breast cancer.
The DUSP22-LGALS1 axis reveals a critical mechanism that shifts the tumor microenvironment from immunosuppressive.
Assessment of the phosphorylation-dependent interaction indicates potential therapeutic avenues for immune checkpoint blockade resistance.
Targeting DUSP22 may enable effective strategies against resistant breast cancer, but clinical translation needs further exploration.

Abstract

Our findings unveil a novel phosphorylation-dependent DUSP22-LGALS1 axis that reprograms the immunosuppressive TME. This work thus proposes a promising therapeutic strategy to overcome immune checkpoint blockade resistance in breast cancer.

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DUSP22 dephosphorylates LGALS1 to enhance T cell-driven antitumor immunity

Key Points

Abstract

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