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Developing an endogenous quorum-sensing based CRISPRi circuit for autonomous and tunable dynamic regulation of multiple targets in Streptomyces

机译:开发基于内源性频率感应的CRIPRI电路,用于链霉菌中多个靶标的自主和可调动态调节

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摘要

Quorum-sensing (QS) mediated dynamic regulation has emerged as an effective strategy for optimizing product titers in microbes. However, these QS-based circuits are often created on heterologous systems and require careful tuning via a tedious testing/optimization process. This hampers their application in industrial microbes. Here, we design a novel QS circuit by directly integrating an endogenous QS system with CRISPRi (named EQCi) in the industrial rapamycin-producing strain Streptomyces rapamycinicus. EQCi combines the advantages of both the QS system and CRISPRi to enable tunable, autonomous, and dynamic regulation of multiple targets simultaneously. Using EQCi, we separately downregulate three key nodes in essential pathways to divert metabolic flux towards rapamycin biosynthesis and significantly increase its titers. Further application of EQCi to simultaneously regulate these three key nodes with fine-tuned repression strength boosts the rapamycin titer by similar to 660%, achieving the highest reported titer (1836 +/- 191 mg/l). Notably, compared to static engineering strategies, which result in growth arrest and suboptimal rapamycin titers, EQCi-based regulation substantially promotes rapamycin titers without affecting cell growth, indicating that it can achieve a trade-off between essential pathways and product synthesis. Collectively, this study provides a convenient and effective strategy for strain improvement and shows potential for application in other industrial microorganisms.
机译:仲裁传感(QS)介导的动态调节已成为优化微生物中产品滴度的有效策略。然而,这些基于QS的电路通常在异源系统上创建,并且需要通过繁琐的测试/优化过程进行仔细调整。这堵塞了​​他们在工业微生物中的应用。在这里,我们通过直接将内源性QS系统直接整合在工业雷帕霉素的菌株Streptomyces雷帕霉素中的内源性QS系统与CRISPRI(名为EQCI)的内源性QS系统直接集成。 EQCI结合了QS系统和CRISPRI的优点,以便同时调谐,自主和动态和动态调节多个目标。使用EQCI,我们单独下调三个关键节点在必要的途径中,以将代谢助焊剂转移到雷帕霉素生物合成,并显着增加其滴度。 EQCI的进一步应用同时调节具有微调抑制强度的三个关键节点,使雷帕霉素滴度促进相似的660%,实现最高报告的滴度(1836 +/- 191 mg / L)。值得注意的是,与静态工程策略相比,导致生长停滞和次优雷帕霉素滴度,基于EQCI的调节基本上促进了雷帕霉素滴度而不影响细胞生长,表明它可以在必要的途径和产品合成之间实现权衡。本研究统称,提供了一种方便且有效的应变改善策略,并显示出在其他工业微生物中的应用潜力。

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  • 来源
    《Nucleic Acids Research》 |2020年第14期|共15页
  • 作者单位

    Chinese Acad Sci CAS Ctr Excellence Mol Plant Sci Shanghai Inst Plant Physiol &

    Ecol Key Lab Synthet Biol Shanghai 200032 Peoples R China;

    Chinese Acad Sci CAS Ctr Excellence Mol Plant Sci Shanghai Inst Plant Physiol &

    Ecol Key Lab Synthet Biol Shanghai 200032 Peoples R China;

    Chinese Acad Sci CAS Ctr Excellence Mol Plant Sci Shanghai Inst Plant Physiol &

    Ecol Key Lab Synthet Biol Shanghai 200032 Peoples R China;

    Zhejiang Med LTD XinChang Pharmaceut Factory Xinchang 312500 Zhejiang Peoples R China;

    Shanghai Normal Univ Coll Life Sci Shanghai 200234 Peoples R China;

    Chinese Acad Sci CAS Ctr Excellence Mol Plant Sci Shanghai Inst Plant Physiol &

    Ecol Key Lab Synthet Biol Shanghai 200032 Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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