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双鏻两亲物揭示了革兰氏阴性菌的消毒剂抗性及细胞膜相互作用。

Bisphosphonium Amphiphiles Yield Insights into Gram-Negative Bacterial Disinfectant Resistance and Cell Membrane Interactions.

作者信息

Bezold Elise L, Young Abigail L E, Jaworski Carson J, Minbiole Kevin P C, Sanchez Christian A, Wuest William M

机构信息

Department of Chemistry, Emory University, Atlanta, Georgia 30322, United States.

Department of Chemistry and Biochemistry, Samford University, Birmingham, Alabama 35229, United States.

出版信息

ACS Omega. 2025 Jun 5;10(23):25076-25083. doi: 10.1021/acsomega.5c03308. eCollection 2025 Jun 17.

Abstract

As microbial resistance to commercially available disinfectants has increased over recent decades, the development of new biocides with distinct mechanisms of action has become a priority. Accordingly, our groups have developed and investigated quaternary phosphonium compounds (QPCs) that have displayed novel mechanisms of bactericidal activity against Gram-negative bacterial species. We aimed to characterize the structure-activity relationship of the cation-separating linker length of diphenylphosphonium scaffolds on membrane interactions and resistance mechanisms using Gram-negative model bacterium Pseudomonas aeruginosa (PAO1 and PA14). Antibacterial activity against lab strain PAO1 and a panel of P. aeruginosa clinical isolates from facilities in Ukraine exhibited potent activity with minimum inhibitory concentrations of 2-4 μM. Surprisingly, the linker length minimally affected the inner-membrane specificity of the QPCs. In comparing the known resistance mechanism for these QPCs, we found that the shorter linker lengths were much more susceptible to efflux by the SmvRA system than the longer linker chain bolaamphiphilic compounds. Additionally, we determined the critical micelle concentration of the QPCs and found that supramolecular aggregation properties do not correlate with the distinct inner-membrane-targeting mechanism of the QPCs. These results represent important advances in the structure-guided investigation of inner-membrane-selective disinfectants.

摘要

近几十年来,随着微生物对市售消毒剂的耐药性增加,开发具有独特作用机制的新型杀菌剂已成为当务之急。因此,我们的团队开发并研究了季鏻化合物(QPCs),它们对革兰氏阴性菌表现出新颖的杀菌活性机制。我们旨在利用革兰氏阴性模式菌铜绿假单胞菌(PAO1和PA14),表征二苯基鏻支架的阳离子分离连接子长度对膜相互作用和耐药机制的构效关系。对实验室菌株PAO1和一组来自乌克兰医疗机构的铜绿假单胞菌临床分离株的抗菌活性显示出强效活性,最低抑菌浓度为2-4μM。令人惊讶的是,连接子长度对QPCs的内膜特异性影响最小。在比较这些QPCs已知的耐药机制时,我们发现较短的连接子长度比较长的连接子链双亲性化合物更容易受到SmvRA系统外排的影响。此外,我们测定了QPCs的临界胶束浓度,发现超分子聚集性质与QPCs独特的内膜靶向机制无关。这些结果代表了在内膜选择性消毒剂的结构导向研究方面的重要进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3180/12177629/5d3279e4f416/ao5c03308_0001.jpg

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