鉴定针对 AcrAB-TolC 组件 AcrA 的外排泵抑制剂的结合位点。
Identification of Binding Sites for Efflux Pump Inhibitors of the AcrAB-TolC Component AcrA.
机构信息
Department of Chemistry and Biochemistry, University of Oklahoma, Norman, Oklahoma.
UT/ORNL Center for Molecular Biophysics, Biosciences Division, Oak Ridge National Laboratory, Oak Ridge, Tennessee; Graduate School of Genome Science and Technology, University of Tennessee, Knoxville, Tennessee.
出版信息
Biophys J. 2019 Feb 19;116(4):648-658. doi: 10.1016/j.bpj.2019.01.010. Epub 2019 Jan 12.
Abstract
The overexpression of multidrug efflux pumps is an important mechanism of clinical resistance in Gram-negative bacteria. Recently, four small molecules were discovered that inhibit efflux in Escherichia coli and interact with the AcrAB-TolC efflux pump component AcrA. However, the binding site(s) for these molecules was not determined. Here, we combine ensemble docking and molecular dynamics simulations with tryptophan fluorescence spectroscopy, site-directed mutagenesis, and antibiotic susceptibility assays to probe binding sites and effects of binding of these molecules. We conclude that clorobiocin and SLU-258 likely bind at a site located between the lipoyl and β-barrel domains of AcrA.
摘要
多药外排泵的过度表达是革兰氏阴性菌临床耐药的一个重要机制。最近发现了四种小分子,它们可以抑制大肠杆菌中的外排作用,并与 AcrAB-TolC 外排泵成分 AcrA 相互作用。然而,这些分子的结合位点尚未确定。在这里,我们将组合使用整体对接和分子动力学模拟与色氨酸荧光光谱法、定点突变和抗生素敏感性测定来探测这些分子的结合位点和结合效果。我们的结论是,氯羟吡啶和 SLU-258 可能结合在 AcrA 的脂酰基和β桶结构域之间的一个位点上。
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