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High-frequency transposition for determining antibacterial mode of action

机译:高频换位确定抗菌作用方式

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摘要

Connecting bacterial growth inhibitors to molecular targets at the whole-cell level is a major impediment to antibacterial development. Herein we report the design of a highly efficient and versatile bacteriophage-based mariner transposon delivery system in Staphylococcus aureus for determining inhibitor mode of action. Using bacteriophage-mediated delivery of concatameric minitransposon cassettes, we generated nonclonal transposant libraries with genome-wide insertion-site coverage in either laboratory or methicillin- resistant strain backgrounds and screened for drug resistance in situ on a single agar plate in one step. A gradient of gene-target expression levels, along with a correspondingly diverse assortment of drug-resistant phenotypes, was achieved by fitting the transposon cassette with a suite of outward-facing promoters. Using a panel of antibiotics, we demonstrate the ability to unveil not only an inhibitor's molecular target but also its route of cellular entry, efflux susceptibility and other off-target resistance mechanisms.
机译:将细菌生长抑制剂与全细胞水平的分子靶标连接是抗菌发展的主要障碍。本文中,我们报告了金黄色葡萄球菌中高效,多功能的基于噬菌体的水手转座子递送系统的设计,以确定抑制剂的作用方式。使用噬菌体介导的顺应性小转座子盒的传递,我们在实验室或耐甲氧西林的菌株背景中生成了具有全基因组插入位点覆盖范围的非克隆转座子文库,并一步一步在单个琼脂平板上筛选了耐药性。通过将转座子盒与一系列面向外的启动子装配在一起,可以实现基因靶标表达水平的梯度以及相应的多种耐药表型分类。通过使用一组抗生素,我们证明了不仅能够揭示抑制剂的分子靶标,还可以揭示其细胞进入途径,外排敏感性和其他脱靶耐药机制。

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