Nucleic Acid-to-Small Molecule Converter through Amplified Hairpin DNA Circuits

被引:14
|
作者
Morihiro, Kunihiko [1 ]
Tomida, Yasuhiro [1 ]
Fukui, Daisuke [1 ]
Hasegawa, Manami [1 ]
Okamoto, Akimitsu [1 ]
机构
[1] Univ Tokyo, Dept Chem & Biotechnol, 7-3-1 Hongo,Bunkyo Ku, Tokyo 1138656, Japan
关键词
Antitumor Agents; Dyes; Nucleic Acids; Prodrugs; Self-Assembly; HYBRIDIZATION CHAIN-REACTION; TEMPLATED CHEMISTRY; PRODRUG; REDUCTION; MICRORNA; RNA; GLUCURONIDE; ACTIVATION; VERSATILE; PROFILE;
D O I
10.1002/anie.202306587
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Many microRNAs (miRNAs) are characteristically found in cancer cells, making miRNAs promising marker biomolecules for cancer diagnosis and therapeutics. However, it is challenging to use miRNA as a cancer signature because it is difficult to convert the nucleic acid sequence information into molecular functionality. To address this challenge, we realize nucleic acid-to-small molecule converters using hairpin DNA circuits. Harnessing a Staudinger reduction as a trigger for the conversion, we constructed hybridization chain reaction (HCR) and catalytic hairpin assembly (CHA) circuits that respond to oncogenic miR-21. Fluorophore and dye molecules were released in response to miR-21 through the HCR, providing fluorogenic and chromogenic readouts. Selective cytotoxicity in miR-21-abundant cells was realized by the CHA to release the anticancer drug SN-38. This would be the first example of selective activation of a small-molecule prodrug triggered by oncogenic miRNA in human living cells. We realize the conversion of nucleic acid input into small molecule output using hairpin DNA circuits. The systems are combined with the biorthogonal Staudinger reduction to release fluorophore, dye, and anticancer agent triggered by oncogenic miR-21. Our approach would have great potential for efficient detection and chemotherapy of cancers based on nucleic acid expression profiles.image
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页数:7
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