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首页> 外文期刊>Applied Biochemistry and Biotechnology >The pH Shift and Precursor Feeding Strategy in a Low-Toxicity FR-008/Candicidin Derivative CS103 Fermentation Bioprocess by a Mutant of Streptomyces sp. FR-008
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The pH Shift and Precursor Feeding Strategy in a Low-Toxicity FR-008/Candicidin Derivative CS103 Fermentation Bioprocess by a Mutant of Streptomyces sp. FR-008

机译:链霉菌突变体在低毒性FR-008 /大刀豆素衍生物CS103发酵生物过程中的pH改变和前体进料策略。 FR-008

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摘要

CS103, the novel derivative of polyene macrolides antibiotic FR-008/candicidin with lower toxicity has been isolated from the culture mycelia of the mutant of Streptomyces sp. FR-008, with targeted deletions of the fscP cytochrome P450 gene from its chromosome. To enhance biosynthesis of CS103, pH shift and precursor feeding strategy for fermentation process by the mutant of Streptomyces sp. FR-008 in a stirred tank bioreactor was developed. According to the process parameters analysis, the effectiveness of the strategy was examined and confirmed by experiments. A maximal CS103 concentration of 139.98 μg/mL was obtained, 2.05-fold higher than that in the pH-uncontrolled fermentation. Compared to other three cases as pH-uncontrolled, pH-controlled, and two-stage pH-controlled batch cultures, the proposed “pH shift and precursor feeding strategy” effectively avoided the scarcity of the antibiotic precursor, increased the CS103 yield from biomass (Y P/X) and substrate (Y P/S) by 110.61% and 48.52%, respectively, and at the time the fermentation time was shortened from 120 to 96 h. The highest CS103 production rate (1.46 μg mL?1 h?1) of the pH shift and precursor feeding strategy was 284.21%, 97.30%, and 58.70% higher than that of pH-uncontrolled, pH-controlled, and two-stage pH-controlled batch culture cases, respectively.
机译:CS103,一种具有较低毒性的多烯大环内酯类抗生素FR-008 / candicidin的新型衍生物,已从链霉菌(Streptomyces sp。)突变体的培养菌丝体中分离得到。 FR-008,其染色体上的fscP细胞色素P450基因有针对性地缺失。为了增强CS103的生物合成,利用链霉菌sp。的突变体进行发酵过程中的pH改变和前体补料策略。开发了搅拌釜生物反应器中的FR-008。通过对工艺参数的分析,验证了该策略的有效性,并通过实验进行了验证。获得的最大CS103浓度为139.98μg/ mL,比pH不受控制的发酵高2.05倍。相较于其他三种情况,如pH不受控制,pH控制和两阶段pH控制的分批培养,建议的“ pH转换和前体进料策略”有效地避免了抗生素前体的稀缺性,增加了生物质的CS103产量( YP / X 和底物(YP / S )分别降低了110.61%和48.52%,并且发酵时间从120 h缩短至96 h。 pH改变和前体进料策略的最高CS103生产率(1.46μgmL?1 h?1 )比不受控制的pH值分别高284.21%,97.30%和58.70%。控制和两阶段pH控制的分批培养箱。

著录项

  • 来源
    《Applied Biochemistry and Biotechnology》 |2009年第3期|673-686|共14页
  • 作者单位

    State Key Laboratory of Bioreactor Engineering East China University of Science and Technology Shanghai 200237 People’s Republic of China;

    State Key Laboratory of Bioreactor Engineering East China University of Science and Technology Shanghai 200237 People’s Republic of China;

    State Key Laboratory of Bioreactor Engineering East China University of Science and Technology Shanghai 200237 People’s Republic of China;

    Laboratory of Microbial Metabolism and School of Life Science ampamp Biotechnology Shanghai Jiaotong University Shanghai 200030 People’s Republic of China;

    Laboratory of Microbial Metabolism and School of Life Science ampamp Biotechnology Shanghai Jiaotong University Shanghai 200030 People’s Republic of China;

    State Key Laboratory of Bioreactor Engineering East China University of Science and Technology Shanghai 200237 People’s Republic of China;

    State Key Laboratory of Bioreactor Engineering East China University of Science and Technology Shanghai 200237 People’s Republic of China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Two-stage pH control strategy; Precursor feeding; Polyene macrolides antibiotic; Low-toxicity FR-008/candicidin; Fermentation;

    机译:两阶段pH控制策略;前体进料;大环内酯类抗生素;低毒FR-008 / candicidin;发酵;

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