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首页> 外文期刊>BMC Systems Biology >Systems approach to investigating host-pathogen interactions in infections with the biothreat agent Francisella. Constraints-based model of Francisella tularensis
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Systems approach to investigating host-pathogen interactions in infections with the biothreat agent Francisella. Constraints-based model of Francisella tularensis

机译:研究生物威胁剂弗朗西斯菌感染中宿主-病原体相互作用的系统方法。图拉弗朗西斯菌的基于约束的模型

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Background Francisella tularensis is a prototypic example of a pathogen for which few experimental datasets exist, but for which copious high-throughout data are becoming available because of its re-emerging significance as biothreat agent. The virulence of Francisella tularensis depends on its growth capabilities within a defined environmental niche of the host cell. Results We reconstructed the metabolism of Francisella as a stoichiometric matrix. This systems biology approach demonstrated that changes in carbohydrate utilization and amino acid metabolism play a pivotal role in growth, acid resistance, and energy homeostasis during infection with Francisella. We also show how varying the expression of certain metabolic genes in different environments efficiently controls the metabolic capacity of F. tularensis. Selective gene-expression analysis showed modulation of sugar catabolism by switching from oxidative metabolism (TCA cycle) in the initial stages of infection to fatty acid oxidation and gluconeogenesis later on. Computational analysis with constraints derived from experimental data revealed a limited set of metabolic genes that are operational during infection. Conclusions This integrated systems approach provides an important tool to understand the pathogenesis of an ill-characterized biothreat agent and to identify potential novel drug targets when rapid target identification is required should such microbes be intentionally released or become epidemic.
机译:背景图拉弗朗西斯菌是一种病原体的典型例子,该病原体的实验数据集很少,但由于其作为生物威胁剂的重新出现的意义,因此可获得大量高通量数据。图拉弗朗西斯菌的毒性取决于其在宿主细胞确定的环境环境中的生长能力。结果我们重建了弗朗西斯菌的代谢为化学计量矩阵。该系统生物学方法证明,在弗朗西斯菌感染期间,碳水化合物利用和氨基酸代谢的变化在生长,耐酸和能量稳态方面起着关键作用。我们还显示了如何在不同的环境中改变某些代谢基因的表达有效地控制图拉山毛榉的代谢能力。选择性基因表达分析显示,糖的分解代谢通过从感染初期的氧化代谢(TCA循环)切换到后来的脂肪酸氧化和糖异生而得到调节。从实验数据得出的限制条件下的计算分析表明,在感染期间可操作的代谢基因有限。结论该综合系统方法为了解病原性生物威胁剂的发病机理和在需要快速鉴定目标微生物(如果有意释放或成为流行病)时鉴定潜在的新型药物目标提供了重要的工具。

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