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A Click Chemistry Approach to Developing Molecularly Targeted DNA Scissors
Authors:Teresa Lauria  Dr. Creina Slator  Prof. Vickie McKee  Dr. Markus Müller  Samuele Stazzoni  Antony L. Crisp  Prof. Thomas Carell  Prof. Andrew Kellett
Affiliation:1. School of Chemical Sciences and National Institute for Cellular Biotechnology, Dublin City University, Glasnevin, Dublin, 9 Ireland;2. Department of Chemistry, Ludwig-Maximilians-Universität, Butenandtstrasse 5–13, 81377 Munich, Germany
Abstract:Nucleic acid click chemistry was used to prepare a family of chemically modified triplex forming oligonucleotides (TFOs) for application as a new gene-targeted technology. Azide-bearing phenanthrene ligands—designed to promote triplex stability and copper binding—were ‘clicked’ to alkyne-modified parallel TFOs. Using this approach, a library of TFO hybrids was prepared and shown to effectively target purine-rich genetic elements in vitro. Several of the hybrids provide significant stabilisation toward melting in parallel triplexes (>20 °C) and DNA damage can be triggered upon copper binding in the presence of added reductant. Therefore, the TFO and ‘clicked’ ligands work synergistically to provide sequence-selectivity to the copper cutting unit which, in turn, confers high stabilisation to the DNA triplex. To extend the boundaries of this hybrid system further, a click chemistry-based di-copper binding ligand was developed to accommodate designer ancillary ligands such as DPQ and DPPZ. When this ligand was inserted into a TFO, a dramatic improvement in targeted oxidative cleavage is afforded.
Keywords:chemical nuclease  click chemistry  copper  DNA damage  DNA triplexes
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