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首页> 外文期刊>ACS Omega >Carvacrol Targets SarA and CrtM of Methicillin-Resistant Staphylococcus aureus to Mitigate Biofilm Formation and Staphyloxanthin Synthesis: An In Vitro and In Vivo Approach
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Carvacrol Targets SarA and CrtM of Methicillin-Resistant Staphylococcus aureus to Mitigate Biofilm Formation and Staphyloxanthin Synthesis: An In Vitro and In Vivo Approach

机译:Carvacrol靶向甲氧西林耐金黄色葡萄球菌的SARA和CRTM,以减轻生物膜形成和葡萄球子蒽合成:体外和体内方法

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Carvacrol is an essential oil traditionally used in culinary processes as spice due to its aromatic nature and also known for various biological activities. In the present study, the antivirulence efficacy of carvacrol against methicillin-resistant Staphylococcus aureus (MRSA) is explored. MRSA is an opportunistic pathogen capable of causing various superficial and systemic infections in humans. Biofilm formation and virulence factors of MRSA are responsible for its pathogenesis and resistance. Hence, the aim of this study was to explore the antibiofilm and antivirulence efficacy of carvacrol against MRSA. Carvacrol at 75 μg/mL inhibited MRSA biofilm by 93%, and it also decreased the biofilm formation on polystyrene and glass surfaces. Further, microscopic analyses revealed the reduction in microcolony formation and collapsed structure of biofilm upon carvacrol treatment. The growth curve analysis and the Alamar blue assay showed the nonfatal effect of carvacrol on MRSA. Further, carvacrol significantly reduced the production of MRSA biofilm-associated slime and extracellular polysaccharide. In addition, carvacrol strongly inhibited the antioxidant pigment staphyloxanthin and its intermediates’ synthesis in MRSA. Inhibition of biofilm and staphyloxanthin by carvacrol enhanced the susceptibility of MRSA to oxidants and healthy human blood. Quantitative polymerase chain reaction (qPCR) analysis unveiled the downregulation of sarA -mediated biofilm gene expression and staphyloxanthin-associated crtM gene expression. The sarA -dependent antibiofilm potential of carvacrol was validated using S. aureus Newman wild-type and isogenic ΔsarA strains. In silico molecular docking analysis showed the high binding efficacy of carvacrol with staphylococcal accessory regulator A (SarA) and 4,4′-diapophytoene synthase (CrtM) when compared to positive controls. Furthermore, the in vivo efficacy of carvacrol against MRSA infection was demonstrated using the model organism Galleria mellonella . The results revealed the nontoxic nature of carvacrol to the larvae and the rescuing potential of carvacrol against MRSA infection. Finally, the current study reveals the potential of carvacrol in inhibiting the biofilm formation and staphyloxanthin synthesis of MRSA by targeting the global regulator SarA and a novel antivirulence target CrtM.
机译:Carvacrol是一种传统上用于烹饪过程中的精油,因为它是由于其芳香性质,也以各种生物活性所知为香料。在本研究中,探讨了钙氨基抗甲氧西林抗甲氧基硫脲的抗血管效应金黄色葡萄球菌(MRSA)。 MRSA是一种能够在人类中引起各种肤浅和全身感染的机会主义病原体。 MRSA的生物膜形成和毒力因子是其发病机制和抗性的原因。因此,本研究的目的是探讨碳酸抗MRSA的抗血栓管和抗血管效果。 75μg/ ml的碳酸抑制MRSA生物膜达93%,也降低了聚苯乙烯和玻璃表面上的生物膜形成。此外,微观分析显示,在碳酸处理时生物膜的微胶体形成和塌陷结构的降低。生长曲线分析和Alamar蓝色测定表明爬行动物对MRSA的非分发作用。此外,Carvacrol显着降低了MRSA生物膜相关粘液和细胞外多糖的产生。此外,Carvacrol强烈抑制抗氧化颜料葡萄糖氧化蛋白和其中间体在MRSA的合成。通过爬行动物的抑制生物膜和葡萄糖蒽蛋白增强了MRSA对氧化剂和健康人血的易感性。定量聚合酶链式反应(QPCR)分析推出了 SARA介质的生物膜基因表达和葡萄糖蒽蛋白相关的 CRTM基因表达的下调。使用 S验证了胰岛素的 Sara依赖性抗生素潜力。金黄色葡萄球菌Newman野生型和中源性δ Sara菌株。在硅分子对接分析中,碳酸葡萄球菌与阳性对照相比,碳酸与葡萄球菌辅助调节剂A(SARA)和4,4'-二苯二酚合酶(CRTM)的高结合疗效。此外,使用模型生物甲烯乳粥,证明了克拉吡咯对MRSA感染的体内疗效的。结果表明,蟑螂对幼虫的无毒性质以及爬血液对MRSA感染的救援潜力。最后,目前的研究揭示了Carvacrol在抑制生物膜形成和葡萄球子体的潜力,通过靶向全球调节赛和新的抗血量靶标CRTm。

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