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用于形成三链体寡核苷酸的补骨脂素共轭核苷类似物的开发与功能评估

Development and functional evaluation of a psoralen-conjugated nucleoside mimic for triplex-forming oligonucleotides.

作者信息

Mikame Yu, Toyama Haruki, Dohno Chikara, Wada Takehiko, Yamayoshi Asako

机构信息

Chemistry of Functional Molecules, Graduate School of Biomedical Sciences, Nagasaki University, Nagasaki, Japan.

SANKEN (The Institute of Scientific and Industrial Research), Osaka University, Osaka, Japan.

出版信息

Commun Chem. 2025 Jan 22;8(1):18. doi: 10.1038/s42004-025-01416-2.

Abstract

Psoralen-conjugated triplex-forming oligonucleotides (Ps-TFOs) have been employed for the photodynamic regulation of gene expression by the photo-cross-linking of psoralen with the target DNA. However, stable triplex formation requires a consecutive purine base sequence in one strand of the target DNA duplexes. The pyrimidine-base interruption in the consecutive purine base sequence drastically decreases the thermodynamic stability of the corresponding triplex, which hampers the TFO application. Here, we propose a design of the Ps-TFO for stable triplex formation with target DNA sequences containing pyrimidine-base interruptions under physiological conditions. This Ps-TFO, named 1'(one)-psoralen-conjugated triplex-forming oligonucleotide (OPTO), incorporates a synthesized nucleoside mimic 1'-psoralen-conjugated deoxyribose to increase the thermodynamic stability of the corresponding triplex by the intercalation of psoralen. The triplex-forming abilities of the OPTO were successfully demonstrated in combination with LNA and 5-methylcytosine, indicating that the use of OPTO will expand the range of the target sequences of TFO for photodynamic gene regulation.

摘要

补骨脂素缀合的三链形成寡核苷酸(Ps-TFOs)已被用于通过补骨脂素与靶DNA的光交联来进行基因表达的光动力调节。然而,稳定的三链体形成需要靶DNA双链体的一条链中具有连续的嘌呤碱基序列。连续嘌呤碱基序列中的嘧啶碱基中断会大大降低相应三链体的热力学稳定性,这阻碍了TFO的应用。在此,我们提出了一种Ps-TFO的设计,用于在生理条件下与含有嘧啶碱基中断的靶DNA序列形成稳定的三链体。这种Ps-TFO,名为1'(一)-补骨脂素缀合的三链形成寡核苷酸(OPTO),掺入了一种合成的核苷类似物1'-补骨脂素缀合的脱氧核糖,通过补骨脂素的嵌入来提高相应三链体的热力学稳定性。OPTO与锁核酸(LNA)和5-甲基胞嘧啶结合成功地证明了其三链体形成能力,表明OPTO的使用将扩大用于光动力基因调节的TFO的靶序列范围。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d3db/11754458/b56334c63a3e/42004_2025_1416_Fig1_HTML.jpg

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