| Literature DB >> 19965760 |
Marcus J Edwards1, Ruth H Flatman, Lesley A Mitchenall, Clare E M Stevenson, Tung B K Le, Thomas A Clarke, Adam R McKay, Hans-Peter Fiedler, Mark J Buttner, David M Lawson, Anthony Maxwell.
Abstract
Simocyclinones are bifunctional antibiotics that inhibit bacterial DNA gyrase by preventing DNA binding to the enzyme. We report the crystal structure of the complex formed between the N-terminal domain of the Escherichia coli gyrase A subunit and simocyclinone D8, revealing two binding pockets that separately accommodate the aminocoumarin and polyketide moieties of the antibiotic. These are close to, but distinct from, the quinolone-binding site, consistent with our observations that several mutations in this region confer resistance to both agents. Biochemical studies show that the individual moieties of simocyclinone D8 are comparatively weak inhibitors of gyrase relative to the parent compound, but their combination generates a more potent inhibitor. Our results should facilitate the design of drug molecules that target these unexploited binding pockets.Entities:
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Year: 2009 PMID: 19965760 DOI: 10.1126/science.1179123
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728