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A novel targeted/untargeted GC-Orbitrap metabolomics methodology applied to Candida albicans and Staphylococcus aureus biofilms

机译:一种新型靶向/非靶向GC-Orbitrap代谢组学方法应用于白色念珠菌和金黄色葡萄球菌生物膜

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Introduction:ududCombined infections from Candida albicans and Staphylococcus aureus are a leading cause of death in the developed world. Evidence suggests that Candida enhances the virulence of Staphylococcus—hyphae penetrate through tissue barriers, while S. aureus tightly associates with the hyphae to obtain entry to the host organism. Indeed, in a biofilm state, C. albicans enhances the antimicrobial resistance characteristics of S. aureus. The association of these microorganisms is also associated with significantly increased morbidity and mortality. Due to this tight association we hypothesised that metabolic effects were also in evidence.ududObjectives:ududTo explore the interaction, we used a novel GC-Orbitrap-based mass spectrometer, the Q Exactive GC, which combines the high peak capacity and chromatographic resolution of gas chromatography with the sub-ppm mass accuracy of an Orbitrap system. This allows the capability to leverage the widely available electron ionisation libraries for untargeted applications, along with expanding accurate mass libraries and targeted matches based around authentic standards.ududMethods:ududOptimised C. albicans and S. aureus mono- and co-cultured biofilms were analysed using the new instrument in addition to the fresh and spent bacterial growth media.ududResults:ududThe targeted analysis experiment was based around 36 sugars and sugar phosphates, 22 amino acids and five organic acids. Untargeted analysis resulted in the detection of 465 features from fresh and spent medium and 405 from biofilm samples. Three significantly changing compounds that matched to high scoring library fragment patterns were chosen for validation.ududConclusion:ududEvaluation of the results demonstrates that the Q Exactive GC is suitable for metabolomics analysis using a targeted/untargeted methodology. Many of the results were as expected: e.g. rapid consumption of glucose and fructose from the medium regardless of the cell type. Modulation of sugar-phosphate levels also suggest that the pentose phosphate pathway could be enhanced in the cells from co-cultured biofilms. Untargeted metabolomics results suggested significant production of cell-wall biosynthesis components and the consumption of non-proteinaceous amino-acids.
机译:简介:白色念珠菌和金黄色葡萄球菌的合并感染是发达国家的主要死亡原因。有证据表明,念珠菌可增强葡萄球菌的毒性-菌丝穿透组织屏障,而金黄色葡萄球菌则与菌丝紧密结合,从而进入宿主生物体。确实,在生物膜状态下,白色念珠菌增强了金黄色葡萄球菌的抗药性。这些微生物的结合还与发病率和死亡率显着增加有关。由于这种紧密的联系,我们假设代谢作用也很明显。 ud ud目标: ud ud为探讨这种相互作用,我们使用了基于GC-Orbitrap的新型质谱仪Q Exactive GC,该质谱仪结合了高峰气相色谱的容量和色谱分辨率,以及Orbitrap系统的亚ppm质量精度。这使得能够利用广泛可用的电子电离库进行非目标应用,并基于真实标准扩展精确的质量库和目标匹配。 ud udMethods: ud ud优化的白色念珠菌和金黄色葡萄球菌单和双链除了新鲜细菌培养基和用过的细菌生长培养基以外,还使用新仪器分析了培养的生物膜。 ud ud结果: ud ud目标分析实验基于36种糖和磷酸糖,22种氨基酸和5种有机酸。无目标分析导致从新鲜和用过的培养基中检测到465个特征,从生物膜样品中检测到405个特征。选择了与高得分文库片段模式匹配的三种发生显着变化的化合物进行验证。 ud ud结论: ud ud对结果的评估表明,Q Exactive GC适用于使用靶向/非靶向方法进行代谢组学分析。许多结果均符合预期:例如无论细胞类型如何,均可从培养基中快速消耗葡萄糖和果糖。糖磷酸水平的调节还表明,共培养生物膜的细胞中磷酸戊糖途径可能得到增强。非靶向代谢组学结果表明,细胞壁生物合成成分的大量产生和非蛋白质氨基酸的消耗。

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