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Bacterial cytological profiling rapidly identifies the cellular pathways targeted by antibacterial molecules

机译:细菌细胞学分析可快速识别抗菌分子靶向的细胞途径

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摘要

Identifying the mechanism of action for antibacterial compounds is essential for understanding how bacteria interact with one another and with other cell types and for antibiotic discovery efforts, but determining a compound's mechanism of action remains a serious challenge that limits both basic research and antibacterial discovery programs. Here, we show that bacterial cytological profiling (BCP) is a rapid and powerful approach for identifying the cellular pathway affected by antibacterial molecules. BCP can distinguish between inhibitors that affect different cellular pathways as well as different targets within the same pathway. We use BCP to demonstrate that spirohexenolide A, a spirotetronate that is active against methicillin-resistant Staphylococcus aureus, rapidly collapses the proton motive force. BCP offers a simple, one-step assay that can be broadly applied, solving the longstanding problem of how to rapidly determine the cellular target of thousands of compounds.
机译:鉴定抗菌化合物的作用机理对于理解细菌如何与其他细胞类型相互作用以及对于抗生素发现工作至关重要,但是确定一种化合物的作用机理仍然是一个严峻的挑战,限制了基础研究和抗菌发现计划。在这里,我们表明细菌细胞学分析(BCP)是一种快速有效的方法,可用于鉴定受抗菌分子影响的细​​胞途径。 BCP可以区分影响不同细胞途径以及同一途径内不同靶标的抑制剂。我们使用BCP来证明spirohexenolide A,一种对抗耐甲氧西林的金黄色葡萄球菌有活性的spirotetronate,会迅速破坏质子原动力。 BCP提供了一种简单的一步测定法,可广泛应用,解决了长期存在的问题,即如何快速确定数千种化合物的细胞靶标。

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