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. 2025 Jan 16.
doi: 10.1038/s41587-024-02535-2. Online ahead of print.

Multiplexed inhibition of immunosuppressive genes with Cas13d for combinatorial cancer immunotherapy

Feifei Zhang #  1   2   3 Ryan D Chow #  1   2   3   4   5 Emily He  1   2   3   6 Chuanpeng Dong  1   2   3 Shan Xin  1   2   3 Daniyal Mirza  1   2   3   6 Yanzhi Feng  1   2   3   7 Xiaolong Tian  1   2   3 Nipun Verma  1   2   3   8 Medha Majety  1   2   3   6 Yueqi Zhang  1   2   3 Guangchuan Wang  9   10   11   12 Sidi Chen  13   14   15   16   17   18   19   20   21   22   23
Affiliations

Multiplexed inhibition of immunosuppressive genes with Cas13d for combinatorial cancer immunotherapy

Feifei Zhang et al. Nat Biotechnol. .

Erratum in

Abstract

The complex nature of the immunosuppressive tumor microenvironment (TME) requires multi-agent combinations for optimal immunotherapy. Here we describe multiplex universal combinatorial immunotherapy via gene silencing (MUCIG), which uses CRISPR-Cas13d to silence multiple endogenous immunosuppressive genes in the TME, promoting TME remodeling and enhancing antitumor immunity. MUCIG vectors targeting four genes delivered by adeno-associated virus (AAV) (Cd274/Pdl1, Lgals9/Galectin9, Lgals3/Galectin3 and Cd47; AAV-Cas13d-PGGC) demonstrate significant antitumor efficacy across multiple syngeneic tumor models, remodeling the TME by increasing CD8+ T-cell infiltration while reducing neutrophils. Whole transcriptome profiling validates the on-target knockdown of the four target genes and shows limited potential off-target or downstream gene alterations. AAV-Cas13d-PGGC outperforms corresponding shRNA treatments and individual gene knockdown. We further optimize MUCIG by employing high-fidelity Cas13d (hfCas13d), which similarly showed potent gene silencing and in vivo antitumor efficacy, without weight loss or liver toxicity. MUCIG represents a universal method to silence multiple immune genes in vivo in a programmable manner, offering broad efficacy across multiple tumor types.

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Conflict of interest statement

Competing interests: S.C. is a (co)founder of EvolveImmune Tx, Cellinfinity Bio, MagicTime Med and Chen Consulting. A patent application (WO2023196711A3, worldwide) has been filed by Yale University related to this study. The other authors declare no competing interests.

Update of

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