Protein rational design and modification of erythrose reductase for the improvement of erythritol production in Yarrowia lipolytica.

IF 3.5 3区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Bioprocess and Biosystems Engineering Pub Date : 2024-10-01 Epub Date: 2024-07-05 DOI:10.1007/s00449-024-03057-6
Lianggang Huang, Wenjia Wang, Kai Wang, Yurong Li, Junping Zhou, Aiping Pang, Bo Zhang, Zhiqiang Liu, Yuguo Zheng
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Abstract

Erythritol is a natural non-caloric sweetener, which is produced by fermentation and extensively applied in food, medicine and chemical industries. The final step of the erythritol synthesis pathway is involved in erythritol reductase, whose activity and NADPH-dependent become the limiting node of erythritol production efficiency. Herein, we implemented a strategy combining molecular docking and thermal stability screening to construct an ER mutant library. And we successfully obtained a double mutant ERK26N/V295M (ER*) whose catalytic activity was 1.48 times that of wild-type ER. Through structural analysis and MD analysis, we found that the catalytic pocket and the enzyme stability of ER* were both improved. We overexpressed ER* in the engineered strain ΔKU70 to obtain the strain YLE-1. YLE-1 can produce 39.47 g/L of erythritol within 144 h, representing a 35% increase compared to the unmodified strain, and a 10% increase compared to the strain overexpressing wild-type ER. Considering the essentiality of NADPH supply, we further co-expressed ER* with two genes from the oxidative phase of PPP, ZWF1 and GND1. This resulted in the construction of YLE-3, which exhibited a significant increase in production, producing 47.85 g/L of erythritol within 144 h, representing a 63.90% increase compared to the original chassis strain. The productivity and the yield of the engineered strain YLE-3 were 0.33 g/L/h and 0.48 g/g glycerol, respectively. This work provided an ER mutation with excellent performance, and also proved the importance of cofactors in the process of erythritol synthesis, which will promote the industrial production of erythritol by metabolic engineering of Y. lipolytica.

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合理设计和改造赤藓酮糖还原酶,提高脂肪分解亚罗酵母的赤藓糖醇产量。
赤藓糖醇是一种天然无热量甜味剂,由发酵法生产,广泛应用于食品、医药和化工行业。赤藓糖醇合成途径的最后一步涉及赤藓糖醇还原酶,其活性和 NADPH 依赖性成为赤藓糖醇生产效率的限制性节点。在此,我们采用分子对接和热稳定性筛选相结合的策略,构建了ER突变体库。我们成功地获得了双突变体ERK26N/V295M(ER*),其催化活性是野生型ER的1.48倍。通过结构分析和 MD 分析,我们发现 ER* 的催化口袋和酶稳定性都得到了改善。我们在工程菌株ΔKU70中过表达了ER*,得到了菌株YLE-1。YLE-1 在 144 小时内可生产 39.47 克/升赤藓糖醇,与未改造菌株相比提高了 35%,与过表达野生型 ER 的菌株相比提高了 10%。考虑到 NADPH 供应的重要性,我们进一步将 ER* 与 PPP 氧化阶段的两个基因 ZWF1 和 GND1 共同表达。结果构建出了 YLE-3,它的产量有了显著提高,在 144 小时内生产了 47.85 克/升赤藓糖醇,与原始基质菌株相比提高了 63.90%。工程菌株 YLE-3 的生产率和产量分别为 0.33 克/升/小时和 0.48 克/克甘油。这项工作提供了一种性能优异的ER突变,同时也证明了辅助因子在赤藓糖醇合成过程中的重要性,这将促进脂溶性酵母菌代谢工程赤藓糖醇的工业化生产。
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来源期刊
Bioprocess and Biosystems Engineering
Bioprocess and Biosystems Engineering 工程技术-工程:化工
CiteScore
7.90
自引率
2.60%
发文量
147
审稿时长
2.6 months
期刊介绍: Bioprocess and Biosystems Engineering provides an international peer-reviewed forum to facilitate the discussion between engineering and biological science to find efficient solutions in the development and improvement of bioprocesses. The aim of the journal is to focus more attention on the multidisciplinary approaches for integrative bioprocess design. Of special interest are the rational manipulation of biosystems through metabolic engineering techniques to provide new biocatalysts as well as the model based design of bioprocesses (up-stream processing, bioreactor operation and downstream processing) that will lead to new and sustainable production processes. Contributions are targeted at new approaches for rational and evolutive design of cellular systems by taking into account the environment and constraints of technical production processes, integration of recombinant technology and process design, as well as new hybrid intersections such as bioinformatics and process systems engineering. Manuscripts concerning the design, simulation, experimental validation, control, and economic as well as ecological evaluation of novel processes using biosystems or parts thereof (e.g., enzymes, microorganisms, mammalian cells, plant cells, or tissue), their related products, or technical devices are also encouraged. The Editors will consider papers for publication based on novelty, their impact on biotechnological production and their contribution to the advancement of bioprocess and biosystems engineering science. Submission of papers dealing with routine aspects of bioprocess engineering (e.g., routine application of established methodologies, and description of established equipment) are discouraged.
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