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首页> 外文期刊>Antonie van Leeuwenhoek: Journal of Microbiology and serology >Reconstruction of the Saccharopolyspora erythraea genome-scale model and its use for enhancing erythromycin production
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Reconstruction of the Saccharopolyspora erythraea genome-scale model and its use for enhancing erythromycin production

机译:糖多孢菌红斑病基因组规模模型的重建及其在提高红霉素生产中的应用

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摘要

Genome-scale metabolic reconstructions are routinely used for the analysis and design of metabolic engineering strategies for production of primary metabolites. The use of such reconstructions for metabolic engineering of antibiotic production is not common due to the lack of simple design algorithms in the absence of a cellular growth objective function. Here, we present the metabolic network reconstruction for the erythromycin producer Saccharopolyspora ery-thraea NRRL23338. The model was manually curated for primary and secondary metabolism pathways and consists of 1,482 reactions (2,075 genes) and 1,646 metabolites. As part of the model validation, we explored the potential benefits of supplying amino acids and identified five amino acids compatible" with erythromycin production, whereby if glucose is supplemented with this amino acid on a carbon mole basis, the in silico model predicts that high erythromycin yield is possible without lowering biomass yield. Increased erythromycin titre was confirmed for four of the five amino acids, namely valine, isoleucine, threonine and proline. In bioreactor experiments, supplementation with 2.5 % carbon mole of valine increased the growth rate by 20 % and simultaneously the erythromycin yield on biomass by 50 %. The model presented here can be used as a framework for the future integration of high-throughput biological data sets in S. erythraea and ultimately to realise strain designs capable of increasing erythromycin production closer to the theoretical yield.
机译:基因组规模的代谢重建通常用于分析和设计代谢工程策略以生产初级代谢产物。由于在缺乏细胞生长目标功能的情况下缺乏简单的设计算法,因此这种重建在抗生素生产的代谢工程中的使用并不常见。在这里,我们介绍了红霉素生产商红多孢菌NRRL23338的代谢网络重建。该模型是针对主要和次要代谢途径进行手动管理的,由1,482个反应(2,075个基因)和1,646个代谢物组成。作为模型验证的一部分,我们探索了提供氨基酸的潜在好处,并确定了与“红霉素生产”兼容的五个氨基酸,从而,如果葡萄糖在碳摩尔基础上补充了该氨基酸,则硅酸模型预测高红霉素在不降低生物质产量的情况下也可以提高产量,确认缬氨酸,异亮氨酸,苏氨酸和脯氨酸这五个氨基酸中的四个氨基酸的红霉素滴定度增加;在生物反应器实验中,补充2.5%碳摩尔数的缬氨酸可使生长速度提高20%,同时提出的红霉素在生物质上的产率提高了50%,此处介绍的模型可以用作将来整合红细菌中高通量生物学数据集的框架,并最终实现能够提高红霉素产量的菌株设计,使其更接近理论值让。

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