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Genomic, Transcriptomic and Metabolomic Studies of Two Well-Characterized, Laboratory-Derived Vancomycin-Intermediate Staphylococcus aureus Strains Derived from the Same Parent Strain

机译:同一亲本菌株衍生的两个良好表征的实验室衍生万古霉素中间金黄色葡萄球菌菌株的基因组,转录组和代谢组学研究

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Complete genome comparisons, transcriptomic and metabolomic studies were performed on two laboratory-selected, well-characterized vancomycin-intermediate Staphylococcus aureus (VISA) derived from the same parent MRSA that have changes in cell wall composition and decreased autolysis. A variety of mutations were found in the VISA, with more in strain 13136p−m+V20 (vancomycin MIC = 16 µg/mL) than strain 13136p−m+V5 (MIC = 8 µg/mL). Most of the mutations have not previously been associated with the VISA phenotype; some were associated with cell wall metabolism and many with stress responses, notably relating to DNA damage. The genomes and transcriptomes of the two VISA support the importance of gene expression regulation to the VISA phenotype. Similarities in overall transcriptomic and metabolomic data indicated that the VISA physiologic state includes elements of the stringent response, such as downregulation of protein and nucleotide synthesis, the pentose phosphate pathway and nutrient transport systems. Gene expression for secreted virulence determinants was generally downregulated, but was more variable for surface-associated virulence determinants, although capsule formation was clearly inhibited. The importance of activated stress response elements could be seen across all three analyses, as in the accumulation of osmoprotectant metabolites such as proline and glutamate. Concentrations of potential cell wall precursor amino acids and glucosamine were increased in the VISA strains. Polyamines were decreased in the VISA, which may facilitate the accrual of mutations. Overall, the studies confirm the wide variability in mutations and gene expression patterns that can lead to the VISA phenotype.
机译:完整的基因组比较,转录组学和代谢组学研究是在两个实验室选择的,特性良好的万古霉素-中间金黄色葡萄球菌(VISA)上进行的,这些金黄色葡萄球菌来源于同一对母体MRSA,细胞壁组成发生变化,自溶减少。在VISA中发现了多种突变,其中菌株13136p - m + V20(万古霉素MIC = 16 µg / mL)比菌株13136p -<更多/ sup> m + V5(MIC = 8 µg / mL)。大多数突变以前并未与VISA表型相关。一些与细胞壁代谢有关,许多与应激反应有关,特别是与DNA损伤有关。两个VISA的基因组和转录组支持基因表达调节对VISA表型的重要性。总体转录组和代谢组学数据的相似性表明,VISA的生理状态包括严格反应的要素,例如蛋白质和核苷酸合成的下调,磷酸戊糖途径和营养物转运系统。尽管明显抑制了胶囊的形成,但分泌的毒力决定簇的基因表达通常被下调,但与表面相关的毒力决定簇的基因表达却更多。在所有三个分析中都可以看到激活的应激反应元件的重要性,例如渗透保护剂代谢产物(如脯氨酸和谷氨酸)的积累。在VISA菌株中,潜在的细胞壁前体氨基酸和氨基葡萄糖的浓度增加。 VISA中的多胺含量降低,这可能有助于突变的产生。总的来说,研究证实了突变和基因表达模式的广泛变异,可能导致VISA表型的出现。

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