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Broad-spectrum antibiotic activity of the arylomycin natural products is masked by natural target mutations

机译:天然目标突变掩盖了arylomycin天然产物的广谱抗生素活性

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摘要

Novel classes of broad-spectrum antibiotics are needed to treat multidrug-resistant pathogens. The arylomycin class of natural products inhibits a promising antimicrobial target, type I signal peptidase (SPase), but upon initial characterization appeared to lack whole-cell activity against most pathogens. Here, we show that Staphylococcus epidermidis, which is sensitive to the arylomycins, evolves resistance via mutations in SPase and that analogous mutations are responsible for the natural resistance of Staphylococcus aureus, Escherichia coli, and Pseudomonas aeruginosa. We identify diverse bacteria lacking these mutations and demonstrate that most are sensitive to the arylomycins. The results illustrate that the arylomycins have a broad-spectrum of activity and are viable candidates for development into therapeutics. The results also raise the possibility that naturally occurring resistance may have masked other natural product scaffolds that might be developed into therapeutics.
机译:需要新型的广谱抗生素来治疗具有多重耐药性的病原体。天然产品的arylomycin类可抑制有希望的抗微生物靶标I型信号肽酶(SPase),但在最初表征后似乎缺乏针对大多数病原体的全细胞活性。在这里,我们显示出对表霉素敏感的表皮葡萄球菌通过SPase中的突变产生耐药性,并且类似的突变是金黄色葡萄球菌,大肠杆菌和铜绿假单胞菌的天然耐药性的原因。我们发现缺乏这些突变的各种细菌,并表明大多数细菌对arylomycins敏感。结果表明,arylomycins具有广谱的活性,是发展成为治疗药物的可行候选药物。结果还增加了天然产生的抗性可能掩盖了可能发展为治疗剂的其他天然产物支架的可能性。

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