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高等阶 G-四链体结构与卟啉配体:走向明确的关系。

Higher-order G-quadruplex structures and porphyrin ligands: Towards a non-ambiguous relationship.

机构信息

Department of Pharmacy, University of Naples Federico II, via Domenico Montesano 49, 80131 Naples, Italy.

Department of Chemical Sciences, University of Catania, viale Andrea Doria 6, 95125 Catania, Italy.

出版信息

Int J Biol Macromol. 2024 May;268(Pt 2):131801. doi: 10.1016/j.ijbiomac.2024.131801. Epub 2024 Apr 25.

DOI:10.1016/j.ijbiomac.2024.131801
PMID:38670185
Abstract

Herein, we evaluated the interaction of the tetracationic porphyrin HTCPPSpm4 with three distinct DNA G-quadruplex (G4) models, i.e., the tetramolecular G4 d(TGGGGT) (Q), the 5'-5' stacked G4-dimer [d(CGGAGGT)] (Q), and a mixture of 5'-5' stacked G-wires [d(5'-CGGT-3'-3'-GGC-5')] (Q). The combined data obtained from UV-Vis, CD, fluorescence, PAGE, RLS, AFM, NMR, and HPLC-SEC experiments allowed us to shed light on the binding mode of HTCPPSpm4 with the three G4 models differing for the type and the number of available G4 ending faces, the length of the G4 units, and the number of stacked G4 building blocks. Specifically, we found that HTCPPSpm4 interacted with the shortest Q as an end-stacking ligand, whereas the groove binding mode was ascertained in the case of the Q and Q G4 models. In the case of the interaction with Q and Q, we found that HTCPPSpm4 induces the formation of supramolecular aggregates at porphyrin/G4 ratios higher than 2:1, whereas no significant aggregation was observed for the interaction with Q up to the 5:1 ratio. These results unambiguously demonstrated the suitability of porphyrins for the development of specific G4 ligands or G4-targeting diagnostic probes, being HTCPPSpm4 capable to distinguish between different G4s.

摘要

在此,我们评估了四正离子卟啉 HTCPPSpm4 与三种不同的 DNA G-四链体 (G4) 模型的相互作用,即四聚体 G4 d(TGGGGT) (Q)、5'-5' 堆叠 G4-二聚体 [d(CGGAGGT)] (Q) 和 5'-5' 堆叠 G-线 [d(5'-CGGT-3'-3'-GGC-5')] (Q) 的混合物。通过紫外-可见、圆二色性、荧光、PAGE、RLS、AFM、NMR 和 HPLC-SEC 实验获得的综合数据使我们能够阐明 HTCPPSpm4 与三种 G4 模型的结合模式,这些模型在可用 G4 端面对的数量和类型、G4 单元的长度和堆叠的 G4 构建块的数量方面存在差异。具体而言,我们发现 HTCPPSpm4 与最短的 Q 作为末端堆叠配体相互作用,而在 Q 和 Q G4 模型的情况下则确定了沟槽结合模式。在与 Q 和 Q 的相互作用中,我们发现 HTCPPSpm4 在卟啉/G4 比高于 2:1 时诱导超分子聚集体的形成,而与 Q 的相互作用直到 5:1 比时都没有观察到明显的聚集。这些结果明确表明卟啉适合开发特定的 G4 配体或 G4 靶向诊断探针,HTCPPSpm4 能够区分不同的 G4。

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