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C5 修饰呋喃碱基 PNAs 的合成及交联性能的改善。

Synthesis and Improved Cross-Linking Properties of C5-Modified Furan Bearing PNAs.

机构信息

Organic and Biomimetic Chemistry Research Group, Department of Organic and Macromolecular Chemistry, Ghent University, Krijgslaan 281-S4, 9000 Gent, Belgium.

Department of Chemistry, Life Sciences and Environmental Sustainability, University of Parma, Parco Area delle Scienze 17/A, 43124 Parma, Italy.

出版信息

Molecules. 2017 Nov 20;22(11):2010. doi: 10.3390/molecules22112010.

Abstract

Over the past decades, peptide nucleic acid/DNA (PNA:DNA) duplex stability has been improved via backbone modification, often achieved via introducing an amino acid side chain at the α- or γ-position in the PNA sequence. It was previously shown that interstrand cross-linking can further enhance the binding event. In this work, we combined both strategies to fine-tune PNA crosslinking towards single stranded DNA sequences using a furan oxidation-based crosslinking method; for this purpose, γ-l-lysine and γ-l-arginine furan-PNA monomers were synthesized and incorporated in PNA sequences via solid phase synthesis. It was shown that the l-lysine γ-modification had a beneficial effect on crosslink efficiency due to pre-organization of the PNA helix and a favorable electrostatic interaction between the positively-charged lysine and the negatively-charged DNA backbone. Moreover, the crosslink yield could be optimized by carefully choosing the type of furan PNA monomer. This work is the first to describe a selective and biocompatible furan crosslinking strategy for crosslinking of γ-modified PNA sequences towards single-stranded DNA.

摘要

在过去的几十年中,通过对核酸的主链进行修饰,肽核酸/DNA(PNA:DNA)双链体的稳定性得到了提高,通常是通过在 PNA 序列的α-或γ-位引入氨基酸侧链来实现的。先前的研究表明,链间交联可以进一步增强结合事件。在这项工作中,我们结合了这两种策略,使用基于呋喃氧化的交联方法来微调 PNA 与单链 DNA 序列的交联;为此,合成了γ-l-赖氨酸和γ-l-精氨酸呋喃-PNA 单体,并通过固相合成将其掺入 PNA 序列中。结果表明,由于 PNA 螺旋的预组织和带正电荷的赖氨酸与带负电荷的 DNA 骨架之间的有利静电相互作用,l-赖氨酸γ-修饰对交联效率有有益的影响。此外,可以通过仔细选择呋喃 PNA 单体的类型来优化交联产率。这项工作首次描述了一种选择性和生物相容性的呋喃交联策略,用于将γ-修饰的 PNA 序列交联到单链 DNA 上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/29c2/6150320/525ffbbc53da/molecules-22-02010-sch001.jpg

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