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Alkaline Phosphatase-Controllable and Red Light-Activated RNA Modification Approach for Precise Tumor Suppression

化学 核糖核酸 RNA干扰 单线态氧 碱性磷酸酶 磷酸酶 生物化学 癌症研究 生物物理学 基因 生物 氧气 有机化学
作者
Jing Fang,Yali Feng,Yuqi Zhang,Anna Wang,Jiachen Li,Chaoxiang Cui,Yirui Guo,Jinfeng Zhu,Zhengzhong Lv,Zhong-Sheng Zhao,Chenjie Xu,Haibin Shi,Jing Fang,Yali Feng,Yuqi Zhang,Anna Wang,Jiachen Li,Chaoxiang Cui,Yirui Guo,Jinfeng Zhu
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:144 (50): 23061-23072 被引量:51
标识
DOI:10.1021/jacs.2c10409
摘要

RNA interference (RNAi) has proved to be a promising modality for disease treatment. However, the promise of conventional RNA therapeutics for clinical application is severely impeded by low delivery efficiency and susceptibility of RNAs to serum RNases. Therefore, developing advanced RNAi technology is an increasing demand for achieving precise medicine. Herein, for the first time, we propose an alkaline phosphatase (ALP)-controllable and red light-activated RNA modification (ALARM) approach for anti-tumor therapeutic application. An ALP-responsive NIR fluorogenic probe f-RCP consisting of a tumor-targeting cyclic RGD peptide, an ALP-activated photosensitizer CyOP, and an 1O2-susceptible furan module for RNA modification was rationally designed and synthesized. Studies have demonstrated that f-RCP can specifically target to liver carcinoma HepG2 cells and spontaneously emit activated NIR/photoacoustic signals upon cleavage by the ALP enzyme, allowing for sensitive detection of ALP-positive tumors. More notably, we surprisingly found that the capability of f-RCP producing singlet oxygen (1O2) under red light irradiation could be simultaneously unlocked, which can ignite the covalent cyclization reaction between furan and nucleobases of intracellular RNA molecules, leading to significant mitochondrial damage and severe apoptosis of tumor cells, in consequence realizing efficient tumor suppression. Most importantly, the potential therapeutic mechanism was first explored on the transcriptomic level. This delicate ALARM strategy may open up new insights into cancer gene therapy.
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