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Macrocyclic DNA-Mismatch-Binding Ligands: Structural Determinants of Selectivity

✍ Scribed by Anton Granzhan; Eric Largy; Nicolas Saettel; Marie-Paule Teulade-Fichou


Publisher
John Wiley and Sons
Year
2009
Tongue
English
Weight
869 KB
Volume
16
Category
Article
ISSN
0947-6539

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✦ Synopsis


Abstract

A collection of 15 homodimeric and 5 heterodimeric macrocyclic bisintercalators was prepared by one‐ or two‐step condensation of aromatic dialdehydes with aliphatic diamines; notably, the heterodimeric scaffolds were synthesized for the first time. The binding of these macrocycles to DNA duplexes containing a mispaired thymine residue (TX), as well as to the fully paired control (TA), was investigated by thermal denaturation and fluorescent‐intercalator‐displacement experiments. The bisnaphthalene derivatives, in particular, the 2,7‐disubstituted ones, have the highest selectivity for the TX mismatches, as these macrocycles show no apparent binding to the fully paired DNA. By contrast, other macrocyclic ligands, as well as seven conventional DNA binders, show lesser or no selectivity for the mismatch sites. The study demonstrates that the topology of the ligands plays a crucial role in determining the mismatch‐binding affinity and selectivity of the macrocyclic bisintercalators.


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