Ka. Ohemeng et al., DNA GYRASE INHIBITORY AND ANTIMICROBIAL ACTIVITIES OF SOME DIPHENIC ACID MONOHYDROXAMIDES, Journal of medicinal chemistry, 40(20), 1997, pp. 3292-3296
The synthesis and inhibitory activity against DNA gyrase of a series o
f diphenic acid monohydroxamides 4a-f are described. A protocol of two
biological assays showed conclusively that inhibition occurs specific
ally at the DNA-DNA gyrase complex and is not, attributable to nonspec
ific inhibition. In the enzyme assays, 4c was as potent as the prototy
pical quinolone, nalidixic acid (1), with an IC50 value of 58.3 mu g/m
L compared to 52 mu g/mL for 1. MIC activity against bacterial strains
showed a systematic drop for all compounds relative to 1. compounds 4
e-e, the addition of PMBN produced dramatic increases in MIC activity
indicating that activity is likely to be related to membrane transport
. Molecular modeling of 4a indicates that the diphenic acid monohydrox
amides can bind to the DNA-DNA gyrase complex in a similar fashion as
that hypothesized for the quinolone series according to the hypothesis
suggested by Shen et al. but may not self-associate by pi-pi stacking
. In contrast to the quinolone series, as the diphenic acid monohydrox
amides are shown by molecular mechanics minimizations to be nonplanar,
they may present novel approaches far chemotherapeutic intervention w
ith a potential for decreased side effects.