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Targeting tumor-intrinsic STK40 induces immune vulnerability and drives T cell reinvigoration.

Lili Zhu ,
Sisi Zhang ,
Botai Li ,
Xueliang Liu ,
Chen Yang ,
Xiangyu Tang ,
Jiayi Chai ,
Xupeng Yang ,
Chune Yu ,
Huiping Liao ,
Zhirui Cao ,
Long Liao ,
Wei Wang ,
Shengxian Yuan ,
Qiang Gao ,
Chong Sun ,
René Bernards ,
Yu Yang ,
Wenxin Qin ,
Cun Wang

Abstract

Immunotherapy has revolutionized cancer treatment, yet its efficacy in hepatocellular carcinoma (HCC) remains limited and the mechanisms of resistance are poorly defined. Using in vivo CRISPR-Cas9 screens, we identify serine/threonine kinase 40 (STK40) as a previously unrecognized regulator of immune evasion. Stk40 ablation synergizes with PD-1 blockade to induce tumor regression. Hepatocyte-specific Stk40 deletion abolishes tumorigenesis in hydrodynamic plasmid-driven HCC models. Mechanistically, STK40 scaffolds the COP1 ubiquitin ligase to promote interferon gamma receptor 1 (IFNGR1) degradation. Genetic depletion of Stk40 stabilizes IFNGR1, restoring tumor cell sensitivity to T cell cytotoxicity. Concurrently, Stk40 loss triggers autonomous GM-CSF secretion, enhancing the infiltration and activation of conventional type 1 dendritic cells, which promotes antigen cross-presentation and CD8+ T cell activation. Pharmacological inhibition of STK40 using LNP-siRNA, combined with PD-1 blockade, elicits potent anti-tumor responses across multiple cancer types. These findings establish STK40 as a dual-action therapeutic target to overcome resistance to anti-tumor immunity.

More about this publication

Cancer cell

Volume 44
Issue nr. 7
Pages 1496-1508.e10
Publication date 13-07-2026

Full text links

Publisher website (DOI) 10.1016/j.ccell.2026.05.001
Europe PubMed Central 42208540
Pubmed 42208540

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