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A Chemically Induced CRISPR/dCas13 FCPF Platform for Precise and Programmable RNA Regulation

Journal of Medicinal Chemistry. 2025-06;

Sebastian Hasselbeck; Jianhui Wang; Zhaodai Bai; Tobias H fner; Gerhard Hummer; Phillip Grote; Xinlai Cheng

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摘要

Alternative splicing enhances proteomic diversity, yet its dysregulation drives cancer, neurodegeneration, and inherited disease. Small-molecule splicing modulators, while clinically validated, like risdiplam, often lack locus specificity, producing off-target effects. CRISPR/Cas13 enables programmable transcript-level targeting, but dCas13 fusion effectors are bulky and can hamper delivery and RNA homeostasis. Building on our previous Chem-CRISPR/dCas9 FCPF system for epigenome editing, we now introduce Chem-CRISPR/dCas13 FCPF , a modular platform that covalently tethers a perfluorobiphenyl-tagged small molecule to dCas13 via a four-residue FCPF -clamp tag. Guided by crRNAs, dRfxCas13d FCPF recruits a risdipla... More

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