Novel antimicrobial 3-phenyl-4-phenoxypyrazole derivatives target cell wall lipid intermediates with low mammalian cytotoxicity.

IF 3.9 2区 综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES
Blanca Fernandez-Ciruelos, Marco Albanese, Femke Taverne, Paul W Finn, Jerry M Wells
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Abstract

The growing crisis of antimicrobial resistance (AMR) underscores the critical need for innovative antimicrobial discoveries. Novel antibiotics targeting the bacterial cell wall remain an attractive area of research, due to their conservation and essentiality in bacteria and their absence in eukaryotic cells. Antibiotics targeting lipid II are of special interest due to the reduced potential for target modification of lipid components and their surface accessibility to inhibitors. In this study, we identified 3-phenyl-4-phenoxypyrazole analogues named PYO12 and PYO12a with bactericidal activity against gram-positive bacteria and low cytotoxicity for different types of mammalian cells. Gram-negative bacteria were resistant to PYO12 activity through extrusion of this compound via efflux pumps. Exposure to PYO12 induces expression of genes involved in resistance to antimicrobials targeting the cell wall, suggesting that PYO12 acts via binding to lipid II or other lipid intermediates involved in peptidoglycan or teichoic acid biosynthesis. Antagonism of PYO12 antibacterial activity by undecaprenyl-pyrophosphate supports the idea that PYO12 may bind to the lipid moiety of lipid II blocking the shuttling of peptidoglycan precursors across the cytoplasmic membrane. These findings open opportunities to further develop these compounds as antibiotics targeting bacterial cell wall synthesis.

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新型抗菌3-苯基-4-苯氧吡唑衍生物靶向具有低哺乳动物细胞毒性的细胞壁脂质中间体。
日益严重的抗菌素耐药性危机强调了对创新抗菌素发现的迫切需要。新型抗生素靶向细菌细胞壁仍然是一个有吸引力的研究领域,由于它们在细菌中的保护和必要性,以及它们在真核细胞中的缺失。由于脂质成分靶向修饰的潜力降低以及它们对抑制剂的表面可及性,靶向脂质II的抗生素受到特别关注。在这项研究中,我们鉴定了3-苯基-4-苯氧吡唑类似物PYO12和PYO12a,它们对革兰氏阳性细菌具有杀菌活性,对不同类型的哺乳动物细胞具有较低的细胞毒性。革兰氏阴性菌通过外排泵挤出这种化合物来抵抗PYO12活性。暴露于PYO12诱导了与针对细胞壁的抗菌剂抗性相关的基因的表达,表明PYO12通过与脂质II或其他参与肽聚糖或磷壁酸生物合成的脂质中间体结合而起作用。十一戊烯基焦磷酸对PYO12抗菌活性的拮抗作用支持了PYO12可能与脂质II的脂质部分结合,阻断肽聚糖前体在细胞质膜上的穿梭。这些发现为进一步开发这些化合物作为靶向细菌细胞壁合成的抗生素提供了机会。
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来源期刊
Scientific Reports
Scientific Reports Natural Science Disciplines-
CiteScore
7.50
自引率
4.30%
发文量
19567
审稿时长
3.9 months
期刊介绍: We publish original research from all areas of the natural sciences, psychology, medicine and engineering. You can learn more about what we publish by browsing our specific scientific subject areas below or explore Scientific Reports by browsing all articles and collections. Scientific Reports has a 2-year impact factor: 4.380 (2021), and is the 6th most-cited journal in the world, with more than 540,000 citations in 2020 (Clarivate Analytics, 2021). •Engineering Engineering covers all aspects of engineering, technology, and applied science. It plays a crucial role in the development of technologies to address some of the world''s biggest challenges, helping to save lives and improve the way we live. •Physical sciences Physical sciences are those academic disciplines that aim to uncover the underlying laws of nature — often written in the language of mathematics. It is a collective term for areas of study including astronomy, chemistry, materials science and physics. •Earth and environmental sciences Earth and environmental sciences cover all aspects of Earth and planetary science and broadly encompass solid Earth processes, surface and atmospheric dynamics, Earth system history, climate and climate change, marine and freshwater systems, and ecology. It also considers the interactions between humans and these systems. •Biological sciences Biological sciences encompass all the divisions of natural sciences examining various aspects of vital processes. The concept includes anatomy, physiology, cell biology, biochemistry and biophysics, and covers all organisms from microorganisms, animals to plants. •Health sciences The health sciences study health, disease and healthcare. This field of study aims to develop knowledge, interventions and technology for use in healthcare to improve the treatment of patients.
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