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. 2000 Aug;19(8):1327-36.
doi: 10.1080/15257770008033055.

6-hydroxy derivative as new desfluoroquinolone (DFQ): synthesis and DNA-binding study

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6-hydroxy derivative as new desfluoroquinolone (DFQ): synthesis and DNA-binding study

O Tabarrini et al. Nucleosides Nucleotides Nucleic Acids. 2000 Aug.

Abstract

A new 6-desfluoroquinolone derivative, characterized by the presence of a 6-hydroxyl group instead of the usual fluorine atom at the C-6 position, was synthesized with the aim to better understand the mechanistic role of the C-6 substituent in the quinolone/DNA/DNA-gyrase interaction. The antibacterial activity unambiguously shows that the hydroxyl group is a good substitute for the C-6 fluorine atom, especially against Gram-positive bacteria. On the contrary, it is a very weak inhibitor of the target DNA gyrase, displaying the highest IC50 value observed for all the C-6 substituted analogues. This behaviour could be explained on the basis of its DNA binding properties.

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