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首页> 外文期刊>BMC Systems Biology >Use of genome-scale models to get new insights into the marine actinomycete genus Salinispora
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Use of genome-scale models to get new insights into the marine actinomycete genus Salinispora

机译:利用基因组规模的模型来获得对海洋放线菌属Salinispora的新见解

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There is little published regarding metabolism of Salinispora species. In continuation with efforts performed towards this goal, this study is focused on new insights into the metabolism of the three-identified species of Salinispora using constraints-based modeling. At present, only one manually curated genome-scale metabolic model (GSM) for Salinispora tropica strain CNB-440T has been built despite the role of Salinispora strains in drug discovery. Here, we updated, and expanded the scope of the model of Salinispora tropica CNB-440T, and GSMs were constructed for two sequenced type strains covering the three-identified species. We also constructed a Salinispora core model that contains the genes shared by 93 sequenced strains and a few non-conserved genes associated with essential reactions. The models predicted no auxotrophies for essential amino acids, which was corroborated experimentally using a defined minimal medium (DMM). Experimental observations suggest possible sulfur accumulation. The Core metabolic content shows that the biosynthesis of specialised metabolites is the less conserved subsystem. Sets of reactions were analyzed to explore the differences between the reconstructions. Unique reactions associated to each GSM were mainly due to genome sequence data except for the ST-CNB440 reconstruction. In this case, additional reactions were added from experimental evidence. This reveals that by reaction content the ST-CNB440 model is different from the other species models. The differences identified in reaction content between models gave rise to different functional predictions of essential nutrient usage by each species in DMM. Furthermore, models were used to evaluate in silico single gene knockouts under DMM and complex medium. Cluster analysis of these results shows that ST-CNB440, and SP-CNR114 models are more similar when considering predicted essential genes. Models were built for each of the three currently identified Salinispora species, and a core model representing the conserved metabolic capabilities of Salinispora was constructed. Models will allow in silico metabolism studies of Salinispora strains, and help researchers to guide and increase the production of specialised metabolites. Also, models can be used as templates to build GSMs models of closely related organisms with high biotechnology potential.
机译:关于盐藻属物种代谢的报道很少。在朝着这一目标进行的努力的基础上,本研究集中在使用基于约束的建模方法对盐沼菌的三个鉴定物种的新认识上。目前,尽管Salinispora菌株在药物发现中发挥了作用,但仅建立了一个热带沙门氏菌CNB-440T人工策划的基因组规模代谢模型(GSM)。在这里,我们更新并扩展了热带盐藻CNB-440T模型的范围,并针对覆盖三个鉴定物种的两个测序菌株构建了GSM。我们还构建了Salinispora核心模型,该模型包含93个测序菌株共有的基因以及一些与基本反应相关的非保守基因。该模型预测必需氨基酸没有营养缺陷型,使用限定的基本培养基(DMM)实验证实了这一点。实验观察表明可能存在硫积累。核心代谢含量表明,专门代谢物的生物合成是较不保守的子系统。分析了几组反应以探索重建之间的差异。除ST-CNB440重建外,与每个GSM相关的独特反应主要归因于基因组序列数据。在这种情况下,实验证据会增加其他反应。这表明ST-CNB440模型的反应含量与其他物种模型不同。在模型之间确定的反应含量上的差异引起了DMM中每种物种必需营养素使用的不同功能预测。此外,使用模型评估DMM和复杂培养基下的计算机单基因敲除。这些结果的聚类分析表明,当考虑预测的必需基因时,ST-CNB440和SP-CNR114模型更相似。为当前鉴定的三种沙利氏菌物种建立了模型,并构建了代表沙氏菌保守代谢能力的核心模型。该模型将允许对Salinispora菌株进行计算机代谢研究,并帮助研究人员指导和增加专门代谢产物的产生。此外,可以将模型用作构建具有高度生物技术潜力的紧密相关生物的GSM模型的模板。

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