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. 2025 May;43(5):752-761.
doi: 10.1038/s41587-024-02282-4. Epub 2024 Jun 25.

In vivo AAV-SB-CRISPR screens of tumor-infiltrating primary NK cells identify genetic checkpoints of CAR-NK therapy

Lei Peng #  1   2   3 Paul A Renauer #  1   2   3   4   5 Giacomo Sferruzza  1   2   3 Luojia Yang  1   2   3   4   5 Yongji Zou  1   2   3 Zhenghao Fang  1   2   3 Jonathan J Park  1   2   3   4   5   6 Ryan D Chow  1   2   3   4   5   6 Yueqi Zhang  1   2   3 Qianqian Lin  1   2   3 Meizhu Bai  1   2   3 Angelica Sanchez  1   2   3   7 Yongzhan Zhang  1   2   3 Stanley Z Lam  1   2   3 Lupeng Ye  8   9   10   11 Sidi Chen  12   13   14   15   16   17   18   19   20   21   22   23   24
Affiliations

In vivo AAV-SB-CRISPR screens of tumor-infiltrating primary NK cells identify genetic checkpoints of CAR-NK therapy

Lei Peng et al. Nat Biotechnol. 2025 May.

Abstract

Natural killer (NK) cells have clinical potential against cancer; however, multiple limitations hinder the success of NK cell therapy. Here, we performed unbiased functional mapping of tumor-infiltrating NK (TINK) cells using in vivo adeno-associated virus (AAV)-SB (Sleeping Beauty)-CRISPR (clustered regularly interspaced short palindromic repeats) screens in four solid tumor mouse models. In parallel, we characterized single-cell transcriptomic landscapes of TINK cells, which identified previously unexplored subpopulations of NK cells and differentially expressed TINK genes. As a convergent hit, CALHM2-knockout (KO) NK cells showed enhanced cytotoxicity and tumor infiltration in mouse primary NK cells and human chimeric antigen receptor (CAR)-NK cells. CALHM2 mRNA reversed the CALHM2-KO phenotype. CALHM2 KO in human primary NK cells enhanced their cytotoxicity, degranulation and cytokine production. Transcriptomics profiling revealed CALHM2-KO-altered genes and pathways in both baseline and stimulated conditions. In a solid tumor model resistant to unmodified CAR-NK cells, CALHM2-KO CAR-NK cells showed potent in vivo antitumor efficacy. These data identify endogenous genetic checkpoints that naturally limit NK cell function and demonstrate the use of CALHM2 KO for engineering enhanced NK cell-based immunotherapies.

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Conflict of interest statement

Competing interests: A patent was filed by Yale University regarding the data in this study, which was licensed to Cellinfinity Bio, a Yale biotech startup founded by S.C. S.C. is also a founder or cofounder of EvolveImmune, NumericGlobal, MagicTime Med and Chen Consulting, all unrelated to this study. The other authors declare no competing interests.

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