Activity of the streptogramin antibiotic etamycin against methicillin-resistant Staphylococcus aureus

被引:0
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作者
Nina M Haste
Varahenage R Perera
Katherine N Maloney
Dan N Tran
Paul Jensen
William Fenical
Victor Nizet
Mary E Hensler
机构
[1] Skaggs School of Pharmacy and Pharmaceutical Sciences,Department of Pediatrics
[2] University of California-San Diego,undefined
[3] Center for Marine Biotechnology and Biomedicine,undefined
[4] Scripps Institution of Oceanography,undefined
[5] University of California-San Diego,undefined
[6] University of California-San Diego,undefined
[7] 4Current address: Department of Chemistry,undefined
[8] Harvey Mudd College,undefined
[9] Claremont,undefined
[10] CA 91711,undefined
[11] USA.,undefined
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关键词
etamycin; marine-derived actinomycete; MRSA; streptogramin;
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摘要
The alarming rise of hospital- and community-associated methicillin-resistant Staphylococcus aureus (HA- and CA-MRSA) infections has prompted a desperate search for novel antibiotics. We discovered the streptogramin etamycin produced by an actinomycete species isolated from the coast of Fiji, the first time this antibiotic has been identified from a marine microbe. Etamycin was extracted and purified from this strain (CNS-575) and identified as a three-rotamer species by 2D NMR spectroscopy. Etamycin demonstrated potent activity against HA- and CA-MRSA in microbroth dilution assays, with minimum inhibitory concentrations (MIC) as low as 1–2 mg l−1 against HA- and CA-MRSA strains. Furthermore, etamycin was also active against other Gram-positive and several Gram-negative pathogens and was found to be non-cytotoxic at concentrations more than 20-fold above MIC. Etamycin displayed favorable time-kill kinetics compared with the first-line MRSA antibiotic, vancomycin, and also conferred significant protection from mortality in a murine model of systemic lethal MRSA infection. These data emphasize the utility of the marine environment as a relatively untapped source of antibiotics against major drug-resistant human pathogens. These studies will also guide future isolation and preclinical development of depsipeptide anti-MRSA compounds from marine-derived actinomycetes.
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页码:219 / 224
页数:5
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