Issue 18, 2013

A label-free and sensitive fluorescence strategy for screening ligands binding to poly(dA) based on exonuclease I-assisted background noise reduction

Abstract

A simple, rapid, label-free, and sensitive fluorescence strategy has been developed for screening the ligands binding to poly(dA) based on exonuclease I-assisted background noise reduction. In this strategy, we have designed 16-repeat deoxyribonucleic acids (A16) as a DNA probe and a double-stranded-chelating dye SYBR Green I (SG I) as a fluorescence dye. Exonuclease I (Exo I), a sequence-independent nuclease, was selected to digest the single-stranded DNA probe to minimize the background fluorescence signal. As a result, in the absence of the target molecular coralyne, A16 is digested by Exo I from its 3′ end. This leads to low background fluorescence due to the weak electrostatic interaction between SG I and mononucleotides (dA). On the other hand, the presence of coralyne can induce the single-stranded A16 to form the homo-adenine DNA duplex, and Exo I is inactive to this duplex structure, resulting in a remarkable fluorescence response. Upon background noise reduction, the sensitivity is improved significantly, with a detection limit of 3.5 nM, which is much lower than almost all the previously reported methods. Moreover, this method could extend the application to recognition interaction between ligands and functional nucleic acids and it could find wide applications in the screening of potential therapeutic molecules.

Graphical abstract: A label-free and sensitive fluorescence strategy for screening ligands binding to poly(dA) based on exonuclease I-assisted background noise reduction

Supplementary files

Article information

Article type
Paper
Submitted
14 Jun 2013
Accepted
11 Jul 2013
First published
11 Jul 2013

Anal. Methods, 2013,5, 4852-4858

A label-free and sensitive fluorescence strategy for screening ligands binding to poly(dA) based on exonuclease I-assisted background noise reduction

H. Wang, Y. Li, K. Huang, X. Liu, Yan-E. Yang and Y. Liu, Anal. Methods, 2013, 5, 4852 DOI: 10.1039/C3AY40974K

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