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Base editing of the mutated TERT promoter inhibits liver tumor growth

Gaoxiang Zhao, Qingxia Ma, Yang Huang, Hongfei Jiang, Qianqian Xu, Shudi Luo, Zhaoyuan Meng, Juanjuan Liu, Lei Zhu, Qian Lin, Min Li, Jing Fang, Leina Ma, Wensheng Qiu, Zhengwei Mao, Zhimin Lu

2023Hepatology18 citationsDOIOpen Access PDF

Abstract

BACKGROUND AND AIMS: Base editing has shown great potential for treating human diseases with mutated genes. However, its potential for treating HCC has not yet been explored. APPROACH AND RESULTS: We employed adenine base editors (ABEs) to correct a telomerase reverse transcriptase ( TERT ) promoter mutation, which frequently occurs in various human cancers, including HCC. The mutated TERT promoter -124 C>T is corrected to -124 C by a single guide (sg) RNA-guided and deactivated Campylobacter jejuni Cas9 (CjCas9)-fused adenine base editor (CjABE). This edit impairs the binding of the E-twenty six/ternary complex factor transcription factor family, including E-twenty six-1 and GABPA, to the TERT promoter, leading to suppressed TERT promoter and telomerase activity, decreased TERT expression and cell proliferation, and increased cell senescence. Importantly, injection of adeno-associated viruses expressing sgRNA-guided CjABE or employment of lipid nanoparticle-mediated delivery of CjABE mRNA and sgRNA inhibits the growth of liver tumors harboring TERT promoter mutations. CONCLUSIONS: These findings demonstrate that a sgRNA-guided CjABE efficiently converts the mutated TERT promoter -124 C>T to -124 C in HCC cells and underscore the potential to treat HCC by the base editing-mediated correction of TERT promoter mutations.

Topics & Concepts

TelomeraseTelomerase reverse transcriptaseBiologySubgenomic mRNAMolecular biologyPromoterGeneTranscription (linguistics)Cancer researchRNAGene expressionGeneticsPhilosophyLinguisticsRNA regulation and diseaseCRISPR and Genetic EngineeringVirus-based gene therapy research
Base editing of the mutated TERT promoter inhibits liver tumor growth | Litcius