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首页> 外文期刊>BMC Genomics >Reconstruction and analysis of the genome-scale metabolic model of schizochytrium limacinum SR21 for docosahexaenoic acid production
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Reconstruction and analysis of the genome-scale metabolic model of schizochytrium limacinum SR21 for docosahexaenoic acid production

机译:二十二碳六烯酸生产的裂殖壶菌SR21基因组规模代谢模型的重建和分析

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Schizochytrium limacinum SR21 is a potential industrial strain for docosahexaenoic acid (DHA) production that contains more than 30–40 % DHA among its total fatty acids. To resolve the DHA biosynthesis mechanism and improve DHA production at a systematic level, a genomescale metabolic model (GSMM), named iCY1170_DHA, which contains 1769 reactions, 1659 metabolites, and 1170 genes, was reconstructed. Based on genome annotation results and literature reports, a new DHA synthesis pathway based on a polyketide synthase (PKS) system was detected in S. limacinum. Similarly to conventional fatty acid synthesis, the biosynthesis of DHA via PKS requires abundant acetyl-CoA and NADPH. The in silico addition of malate and citrate led to increases of 24.5 % and 37.1?% in DHA production, respectively. Moreover, based on the results predicted by the model, six amino acids were shown to improve DHA production by experiment. Finally, 30 genes were identified as potential targets for DHA over-production using a Minimization of Metabolic Adjustment algorithm. The reconstructed GSMM, iCY1170_DHA, could be used to elucidate the mechanism by which DHA is synthesized in S. limacinum and predict the requirements of abundant acetyl-CoA and NADPH for DHA production as well as the enhanced yields achieved via supplementation with six amino acids, malate, and citrate.
机译:粟酒裂殖酵母SR21是二十二碳六烯酸(DHA)生产的潜在工业菌株,其总脂肪酸中DHA含量超过30–40%。为了解决DHA的生物合成机制并在系统水平上提高DHA的产生,重建了一个名为iCY1170_DHA的基因组规模代谢模型(GSMM),该模型包含1769个反应,1659个代谢物和1170个基因。根据基因组注释结果和文献报道,在S. limacinum中发现了一种基于聚酮合酶(PKS)系统的新DHA合成途径。与常规脂肪酸合成相似,通过PKS进行DHA的生物合成需要大量的乙酰辅酶A和NADPH。在计算机上添加苹果酸和柠檬酸可导致DHA产量分别增加24.5%和37.1%。此外,基于模型预测的结果,通过实验显示了六个氨基酸可改善DHA的产生。最后,使用最小化代谢调节算法将30个基因鉴定为DHA超量生产的潜在靶标。重建的GSMM iCY1170_DHA可用于阐明在链霉菌中合成DHA的机理,并预测丰富的乙酰辅酶A和NADPH对DHA产生的需求,以及通过补充六种氨基酸实现的增产,苹果酸和柠檬酸盐。

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