Bridging Ligand Length Controls AT Selectivity and Enantioselectivity of Binuclear Ruthenium Threading Intercalators |
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| Authors: | Johan R Johansson Yubo Wang Dr Mattias P Eng Prof Nina Kann Prof Per Lincoln Dr Johanna Andersson |
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| Institution: | 1. Department of Chemical and Biological Engineering, Chalmers University of Technology, 412 96 Gothenburg (Sweden), Fax: (+46)?31‐772‐38‐58;2. Pharmacy Department, Clinical Pharmacist Group, First Affiliated Hospital of Xinjiang Medical University, No.137 LiYuShan Mountain Road, Urumqi, Xinjiang, 830054 (P.R. China);3. Department of Physics, University of Gothenburg, 412 96 Gothenburg (Sweden) |
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| Abstract: | The slow dissociation of DNA threading intercalators makes them interesting as model compounds in the search for new DNA targeting drugs, as there appears to be a correlation between slow dissociation and biological activity. Thus, it would be of great value to understand the mechanisms controlling threading intercalation, and for this purpose we have investigated how the length of the bridging ligand of binuclear ruthenium threading intercalators affects their DNA binding properties. We have synthesised a new binuclear ruthenium threading intercalator with slower dissociation kinetics from ct‐DNA than has ever been observed for any ruthenium complex with any type of DNA, a property that we attribute to the increased distance between the ruthenium centres of the new complex. By comparison with previously studied ruthenium complexes, we further conclude that elongation of the bridging ligand reduces the sensitivity of the threading interaction to DNA flexibility, resulting in a decreased AT selectivity for the new complex. We also find that the length of the bridging ligand affects the enantioselectivity with increasing preference for the ΔΔ enantiomer as the bridging ligand becomes longer. |
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| Keywords: | DNA intercalation kinetics ruthenium sequence selectivity |
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