G4-Ligand Conjugated Oligonucleotides Mediate Selective Binding and Stabilization of Individual G4 DNA Structures

寡核苷酸 DNA 计算生物学 共轭体系 人类基因组 基因组 基因 配体(生物化学) 生物 转录因子 化学 细胞生物学 遗传学 受体 有机化学 聚合物
作者
Andreas Berner,Rabindra Nath Das,Naresh Bhuma,Justyna Gołębiewska,Alva Abrahamsson,Måns Andréasson,Namrata Chaudhari,Mara Doimo,Partha Pratim Bose,Karam Chand,Roger Strömberg,Sjoerd Wanrooij,Erik Chorell
标识
DOI:10.1101/2023.09.20.558437
摘要

ABSTRACT G-quadruplex (G4) DNA structures are prevalent secondary DNA structures implicated in fundamental cellular functions such as replication and transcription. Furthermore, G4 structures are directly correlated to human diseases such as cancer and have been highlighted as promising therapeutic targets for their ability to regulate disease-causing genes, e.g., oncogenes. Small molecules that bind and stabilize these structures are thus valuable from a therapeutic perspective and helpful in studying the biological functions of G4 structures. However, there are hundreds of thousands of G4 DNA motifs in the human genome, and a longstanding problem in the field is how to achieve specificity amongst these different G4 structures. Here, we have developed a strategy to selectively target an individual G4 DNA structure. The strategy is based on a ligand that binds and stabilizes G4s without selectivity, conjugated to a guide oligonucleotide, that specifically directs the G4 Ligand conjugated Oligo (GL-O) to the single target G4 structure. By employing various biophysical and biochemical techniques, we show that the developed method enables the targeting of a unique, specific G4 structure without impacting other off-target G4 formations. Considering the vast amounts of G4s in the human genome, this represents a promising strategy to study the presence and functions of individual G4s but may also hold potential as a future therapeutic modality.
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