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Constraint-based metabolic targets for the improved production of heterologous compounds across molecular classification

机译:基于约束的代谢靶来改进分子分类的异源化合物的产量

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The natural products 6-deoxyerythronolide B (6dEB), erythromycin D, yersiniabactin (Ybt), and salicylate 2-O-beta-d-glucoside (SAG), representing a range of primary and secondary metabolites generated through heterologous microbial biosynthesis, were analyzed using computational metabolic engineering for the purpose of predicting improved production. Specifically, flux balance analysis allowed for the comprehensive screening of medium components and the determination of single gene deletions that resulted in improved product titers for the target compounds. Outcomes included the identification of amino acids and alternative carbon sources capable of culture medium supplementation for increased cellular production. Separately, Minimization of Metabolic Adjustment and OptForce were used to identify single gene deletion and overexpression targets, respectively, for improvements to the aforementioned biosynthetic schemes. The computational engineering predictions thus provide a starting point for experimental implementation with the goal of improving metabolic carbon flow to the compounds presented in this study, each of which possesses valuable bioactivity. (c) 2018 American Institute of Chemical Engineers
机译:自然产物6-脱氧性嗜酚醇B(6DEB),红霉素D,yersinabactin(YBT)和水杨酸盐2-β-D-葡糖苷(SAG),代表通过异源微生物生物合成产生的一系列初级和次生代谢物,利用计算代谢工程,以预测改进的生产。具体地,允许助核筛选培养基组分的助焊剂平衡分析以及导致靶化合物改善产物滴定的单一基因缺陷的测定。结果包括鉴定氨基酸和替代碳源,能够培养介质补充,用于增加细胞生产。单独地,最小化代谢调整和oldForce分别用于识别单一基因缺失和过表达靶,以改善上述生物合成方案。因此,计算工程预测提供了实验实施的起点,其目的是提高到本研究中呈现的化合物的代谢碳流动,每个目标具有有价值的生物活性。 (c)2018美国化学工程研究所

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