| Literature DB >> 26456734 |
Ronald E Painter1, Gregory C Adam2, Marta Arocho3, Edward DiNunzio1, Robert G K Donald4, Karen Dorso4, Olga Genilloud5, Charles Gill4, Michael Goetz3, Nichelle N Hairston4, Nicholas Murgolo6, Bakela Nare4, David B Olsen4, Maryann Powles4, Fred Racine4, Jing Su3, Francisca Vicente5, Douglas Wisniewski4, Li Xiao3, Milton Hammond4, Katherine Young7.
Abstract
Resistance to existing classes of antibiotics drives the need for discovery of novel compounds with unique mechanisms of action. Nargenicin A1, a natural product with limited antibacterial spectrum, was rediscovered in a whole-cell antisense assay. Macromolecular labeling in both Staphylococcus aureus and an Escherichia coli tolC efflux mutant revealed selective inhibition of DNA replication not due to gyrase or topoisomerase IV inhibition. S. aureus nargenicin-resistant mutants were selected at a frequency of ∼1 × 10(-9), and whole-genome resequencing found a single base-pair change in the dnaE gene, a homolog of the E. coli holoenzyme α subunit. A DnaE single-enzyme assay was exquisitely sensitive to inhibition by nargenicin, and other in vitro characterization studies corroborated DnaE as the target. Medicinal chemistry efforts may expand the spectrum of this novel mechanism antibiotic.Entities:
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Year: 2015 PMID: 26456734 DOI: 10.1016/j.chembiol.2015.08.015
Source DB: PubMed Journal: Chem Biol ISSN: 1074-5521