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通过纳入硫胺素的动态调控增强1,4-丁二醇的从头合成。

Enhanced 1,4-Butanediol de Novo Synthesis in by Incorporating Dynamic Regulation of Thiamine.

作者信息

Guo Hongwei, Zeng Yaqing, Zhu Mengqi, Huang Tianqiu, Wang Weigao, Madzak Catherine, Zhao Jun, Sun Xiaohui, Chen Hongwen, Chen Guo

机构信息

Department of Biotechnology and Bioengineering, School of Chemical Engineering, Huaqiao University, 668 Jimei Road, Amoy 361021, Fujian, China.

Department of Chemical Engineering, Stanford University, Stanford 94305, California, United States.

出版信息

ACS Synth Biol. 2025 Jul 18;14(7):2572-2583. doi: 10.1021/acssynbio.5c00015. Epub 2025 Jul 3.

Abstract

1,4-Butanediol (1,4-BDO), one of the most important platform diols, has been widely utilized as a comonomer to manufacture several million tons of polymers every year. Microbial synthesis of the non-natural 1,4-BDO is extremely challenging. Although several artificial routes have been proposed and applied in , among them, the branching metabolic flux from α-ketoglutarate (α-KG) to the artificial route was considered the most thermodynamically efficient solution. Establishing a 1,4-BDO synthesis route in , a native α-KG and succinate hyperproducer, should have high potential. A CoA-dependent 1,4-BDO synthesis route was introduced into , followed by the investigation of rate-limiting steps, optimization of the thiamine dosage, improvement of the precursor and cofactor availability, and deletion of the competition step. It was illustrated that 1,4-BDO synthesis was susceptible to metabolic throughput of the GABA-succinate shunt and NADPH availability. Also, there was a trade-off between cellular growth and 1,4-BDO synthesis. A combinational strategy, in which hereditary dynamic regulation of thiamine was incorporated into those positive metabolic modifications, was implemented, and 6217.1 mg·L 1,4-BDO was achieved under the batch fermentation model. This work also demonstrated the high potential and capacity for biosynthesis of non-nature chemicals from TCA intermediates in the yeast cells, and provided a novel clue to rebalance the metabolic flux between the heterologous pathway and central metabolism.

摘要

1,4-丁二醇(1,4-BDO)是最重要的平台二醇之一,每年被广泛用作共聚单体来生产数百万吨聚合物。非天然1,4-丁二醇的微生物合成极具挑战性。尽管已经提出并应用了几种人工途径,其中,从α-酮戊二酸(α-KG)到人工途径的分支代谢通量被认为是最具热力学效率的解决方案。在天然的α-KG和琥珀酸高产菌株中建立1,4-丁二醇合成途径应该具有很高的潜力。将一条依赖辅酶A的1,4-丁二醇合成途径引入该菌株,随后研究限速步骤、优化硫胺素剂量、提高前体和辅因子的可用性,并删除竞争步骤。结果表明,1,4-丁二醇的合成易受GABA-琥珀酸分流的代谢通量和NADPH可用性的影响。此外,细胞生长和1,4-丁二醇合成之间存在权衡。实施了一种组合策略,即将硫胺素的遗传动态调控纳入这些积极的代谢修饰中,在分批发酵模型下实现了6217.1 mg·L的1,4-丁二醇产量。这项工作还证明了酵母细胞中利用三羧酸循环中间体生物合成非天然化学品的巨大潜力和能力,并为重新平衡异源途径和中心代谢之间的代谢通量提供了新线索。

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