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Analysis of Metabolic Evolution in Bacteria Using Whole-Genome Metabolic Models

机译:使用全基因组代谢模型分析细菌的代谢进化

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Recent advances in the automation of metabolic model reconstruction have led to the availability of draft-quality metabolic models (predicted reaction complements) for multiple bacterial species. These reaction complements can be considered as trait representations and can be used for ancestral state reconstruction, to infer the most likely metabolic complements of common ancestors of all bacteria with generated metabolic models. We present here an ancestral state reconstruction for 141 extant bacteria and analyse the reaction gains and losses for these bacteria with respect to their lifestyles and pathogenic nature. A simulated annealing approach is used to look at coordinated metabolic gains and losses in two bacteria. The main losses of Onion yellows phytoplasma OY-M, an obligate intracellular pathogen, are shown (as expected) to be in cell wall biosynthesis. The metabolic gains made by Clostridium difficile CD196 in adapting to its current habitat in the human colon is also analysed. Our analysis shows that the capability to utilize N-Acetyl-neuraminic acid as a carbon source has been gained, rather than having been present in the Clostridium ancestor, as has the capability to synthe-sise phthiocerol dimycocerosate which could potentially aid the evasion of the host immune response. We have shown that the availability of large numbers of metabolic models, along with conventional approaches, has enabled a systematic method to analyse metabolic evolution in the bacterial domain.
机译:代谢模型重建自动化的最新进展已导致可用于多种细菌的高质量草图模型(预测的反应补体)的可用性。这些反应补体可被视为特征表征,并可用于祖先状态重建,以利用生成的代谢模型推断所有细菌的共同祖先最可能的代谢补体。我们在这里介绍了141种现存细菌的祖先状态重建,并针对这些细菌的生活方式和致病性分析了这些细菌的反应得失。模拟退火方法用于查看两种细菌的​​代谢代谢协调性。如预期的那样,洋葱黄细胞质体OY-M(一种专性的细胞内病原体)的主要损失显示在细胞壁生物合成中。还分析了艰难梭菌CD196在适应其目前在人类结肠中的栖息地时所获得的代谢增益。我们的分析表明,已经获得了利用N-乙酰基神经氨酸作为碳源的能力,而不是存在于梭状芽胞杆菌中,因为它具有合成邻苯二酚二硬脂酸酯的能力,这可能有助于逃避宿主免疫反应。我们已经表明,大量代谢模型的可用性以及常规方法已经使系统的方法能够分析细菌域中的代谢过程。

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