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金黄色葡萄球菌、铜绿假单胞菌和土拉弗朗西斯菌中小多重耐药转运蛋白的功能混杂性。

Functional promiscuity of small multidrug resistance transporters from Staphylococcus aureus, Pseudomonas aeruginosa, and Francisella tularensis.

机构信息

Department of Biochemistry, University of Wisconsin-Madison, Madison, Wisconsin, USA.

出版信息

Mol Microbiol. 2024 Apr;121(4):798-813. doi: 10.1111/mmi.15231. Epub 2024 Jan 29.

Abstract

Small multidrug resistance transporters efflux toxic compounds from bacteria and are a minimal system to understand multidrug transport. Most previous studies have focused on EmrE, the model SMR from Escherichia coli, finding that EmrE has a broader substrate profile than previously thought and that EmrE may perform multiple types of transport, resulting in substrate-dependent resistance or susceptibility. Here, we performed a broad screen to identify potential substrates of three other SMRs: PAsmr from Pseudomonas aeruginosa; FTsmr from Francisella tularensis; and SAsmr from Staphylococcus aureus. This screen tested metabolic differences in E. coli expressing each transporter versus an inactive mutant, for a clean comparison of sequence and substrate-specific differences in transporter function, and identified many substrates for each transporter. In general, resistance compounds were charged, and susceptibility substrates were uncharged, but hydrophobicity was not correlated with phenotype. Two resistance hits and two susceptibility hits were validated via growth assays and IC50 calculations. Susceptibility is proposed to occur via substrate-gated proton leak, and the addition of bicarbonate antagonizes the susceptibility phenotype, consistent with this hypothesis.

摘要

小多重耐药转运蛋白将有毒化合物从细菌中排出,是理解多药转运的最小系统。大多数先前的研究都集中在 EmrE 上,即大肠杆菌的模型 SMR,发现 EmrE 的底物谱比以前认为的要广,并且 EmrE 可能执行多种类型的转运,导致底物依赖性耐药或敏感。在这里,我们进行了广泛的筛选,以确定其他三种 SMR 的潜在底物:铜绿假单胞菌中的 PAsmr;土拉弗朗西斯菌中的 FTsmr;和金黄色葡萄球菌中的 SAsmr。该筛选针对表达每种转运蛋白的大肠杆菌与无活性突变体之间的代谢差异进行了测试,以便对转运蛋白功能的序列和底物特异性差异进行干净的比较,并为每种转运蛋白鉴定了许多底物。一般来说,耐药化合物带电荷,而敏感底物不带电荷,但疏水性与表型无关。通过生长测定和 IC50 计算验证了两个耐药性命中和两个敏感性命中。通过底物门控质子泄漏来提出敏感性,并且添加重碳酸盐拮抗敏感性表型,这与该假设一致。

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