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基于 ZnCdSe 量子点的 (N-甲基-4-吡啶基) 卟啉-DNA 和 G-四链体相互作用的“关-开”荧光传感器。

"Turn-off-on" fluorescent sensor for (N-methyl-4-pyridyl) porphyrin -DNA and G-quadruplex interactions based on ZnCdSe quantum dots.

机构信息

College of Pharmacy, South-Central University for Nationalities, Wuhan 430074, PR China.

College of Pharmacy, South-Central University for Nationalities, Wuhan 430074, PR China.

出版信息

Anal Chim Acta. 2015 Aug 12;888:131-7. doi: 10.1016/j.aca.2015.06.053. Epub 2015 Aug 8.

DOI:10.1016/j.aca.2015.06.053
PMID:26320968
Abstract

As a new detection model, the reversible fluorescence "turn-off-on" sensor based on quantum dots (QDs) has already been successfully employed in the detections of many biochemical materials, especially in the researches on the interactions between anticancer drugs. The previous studies, however, mainly focused on simple-structured oligonucleotides and Calf thymus DNA. G-quadruplex, an important target for anti-cancer drug with special secondary structure, has been stimulating increasing research interests. In this paper, we report a new detection method based on the fluorescence "turn-off-on" model with water-soluble ZnCdSe QDs as the fluorescent probe, to analyze the interactions between anticancer drug (N-methyl-4-pyridyl) porphyrin (TMPyP) and nucleic acid, especially the G-quadruplex. The fluorescence of QDs can be quenched by TMPyP via photo-induced electron transfer and fluorescence resonance energy transfer, while on the other hand, the combination between TMPyP and G-quadruplex releases QDs from their quenchers and thus recovers the fluorescence. Most importantly, the fluorescence "turn-off-on" model has been employed, for the first time, to analyze the impacts of special factors on the interaction between TMPyP and G-quadruplex. The excellent selectivity of the system has been verified in the studies of the interactions between TMPyP and different DNAs (double-stranded DNA, single-stranded G-quadruplex, and different types of G-quadruplexes) in Na(+) or K(+)-containing buffer.

摘要

作为一种新的检测模型,基于量子点的可逆荧光“关闭-开启”传感器已经成功应用于许多生化物质的检测,特别是在抗癌药物相互作用的研究中。然而,以前的研究主要集中在简单结构的寡核苷酸和小牛胸腺 DNA 上。G-四链体是一种具有特殊二级结构的抗癌药物的重要靶标,已经引起了越来越多的研究兴趣。在本文中,我们报告了一种基于水溶性 ZnCdSe QDs 作为荧光探针的荧光“关闭-开启”模型的新检测方法,用于分析抗癌药物(N-甲基-4-吡啶基)卟啉(TMPyP)与核酸,特别是 G-四链体的相互作用。TMPyP 可以通过光诱导电子转移和荧光共振能量转移猝灭 QDs 的荧光,另一方面,TMPyP 与 G-四链体的结合将 QDs 从猝灭剂中释放出来,从而恢复荧光。最重要的是,该荧光“关闭-开启”模型首次被用于分析特殊因素对 TMPyP 与 G-四链体相互作用的影响。该系统的优异选择性已经在 TMPyP 与不同 DNA(双链 DNA、单链 G-四链体和不同类型的 G-四链体)在含 Na(+)或 K(+)的缓冲液中的相互作用研究中得到了验证。

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