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含有反式-5,6-或5,7-稠环骨架的2',3'-反式桥连核酸的二核苷酸的合成与结构分析。

Synthesis and structural analysis of dinucleotides containing 2',3'-trans-bridged nucleic acids with trans-5,6- or 5,7-fused ring skeleton.

作者信息

Osawa Takashi, Nakanishi Ryota, Uda Keito, Muramoto So, Obika Satoshi

机构信息

Graduate School of Pharmaceutical Science, Osaka University, 1-6 Yamadaoka, Suita, Osaka, 565-0871, Japan.

Institute for Open and Transdisciplinary Research Initiatives, Osaka University, 1-3 Yamadaoka, Suita, Osaka, 565-0871, Japan.

出版信息

Commun Chem. 2025 Mar 22;8(1):87. doi: 10.1038/s42004-025-01486-2.

Abstract

Artificial nucleic acids in which the conformation of the sugar or phosphate backbone of the oligonucleotide is appropriately fixed can form stable duplexes. In this study, we designed dinucleotides containing 2',3'-trans-bridged nucleic acids (2',3'-trans-BNAs) based on the idea that the sugar conformation and torsions angles δ, ε, ζ, α, and β of the backbone can be controlled by a 5,6- or 5,7-membered trans-fused ring skeleton cyclized between the 2'- and 3'-positions of the sugar moiety. Given that the construction of trans-5,6-fused ring skeletons is synthetically challenging, the synthesis was optimized and a detailed structural analysis of these new bridged 2',3'-trans-BNA systems was conducted. The 2',3'-trans-BNAs could be synthesized from a commercially available D-glucose derivative with the key intramolecular gold-catalyzed cyclization reaction achieved using a cyclization precursor bearing an intramolecular hydroxy group and an internal alkyne. Structural analysis of the 2',3'-trans-BNAs showed an N-type sugar conformation for all the derivatives, which is similar to that in RNA-duplex, and the ζ and α torsion angles for the 2',3'-trans-BNAs were a characteristic feature of the compounds that differ from the corresponding angles of the natural duplexes.

摘要

寡核苷酸糖或磷酸骨架构象得到适当固定的人工核酸能够形成稳定的双链体。在本研究中,我们基于糖构象以及骨架的扭转角δ、ε、ζ、α和β可通过在糖部分的2'-和3'-位之间环化的5,6-或5,7-元反式稠合环骨架来控制这一理念,设计了含有2',3'-反式桥连核酸(2',3'-trans-BNAs)的二核苷酸。鉴于反式5,6-稠合环骨架的构建在合成上具有挑战性,我们对合成进行了优化,并对这些新型桥连2',3'-trans-BNA体系进行了详细的结构分析。2',3'-trans-BNAs可由市售的D-葡萄糖衍生物合成,关键的分子内金催化环化反应通过使用带有分子内羟基和内部炔烃的环化前体来实现。2',3'-trans-BNAs的结构分析表明,所有衍生物均具有N型糖构象,这与RNA双链体中的构象相似,并且2',3'-trans-BNAs的ζ和α扭转角是这些化合物的特征,与天然双链体的相应角度不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dfe8/11929919/c69b0885e84c/42004_2025_1486_Fig1_HTML.jpg

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