Engineering silica nanocoated whole-cell asymmetric biocatalyst for efficient preparation of a key chiral intermediate of (S)-Rivastigmine.

IF 4.1 2区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Journal of biotechnology Pub Date : 2025-01-13 DOI:10.1016/j.jbiotec.2025.01.005
Baoling Chen, Hang Yang, Ruixuan Bai, Xiaotong Du, Yue Gao, Liangyu Zheng
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Abstract

In our previous study, the whole cells containing an aldo-keto reductase (yhdN) and glucose dehydrogenase (GDH) were constructed and applied in a stereoselective carbonyl reduction reaction to prepare (S)-NEMCA-HEPE, being a key chiral intermediate of (S)-Rivastigmine which is widely prescribed for the treatment of Alzheimer's disease. Although the conversion and enantiomeric excess (e.e.) could reach to 78.2 % and 99 %, respectively, ionic liquid as an additive was required to improve the permeability of cell membrane. To further simplify the reaction, the molecular docking and saturation mutagenesis technology were used here to obtain an activity-improved yhdN variant such as G19A. And then, both excellent conversion and e.e. of 99 % for (S)-NEMCA-HEPE could be achieved within 40 min by using only G19A-GDH whole cell as a catalyst without any additive. However, the use of the whole cells still faces the issues of poor operation stability and adverse application prospect. Subsequently, a hydrophobic "cell-in-shell" complex of G19A-GDH@O-Silica was constructed by using a silica nanocoated technology. The obtained G19A-GDH@O-Silica exhibited an excellent conversion towards the asymmetric carbonyl reduction, and a good tolerance in changing thermal, pH, and storage environmental. Giving 76.3 % of reaction conversion even after the 11th cycle of reuse, indicated that G19A-GDH@O-Silica also possessed ideal recyclability. The aim of this study is to provide a rapid, and cost-effective nanocoated whole-cell biocatalyst for efficient preparation of (S)-NEMCA-HEPE. The simplicity and robustness of the immobilization approach may become a powerful tool to utilize whole-cell catalysts towards organic catalysis.

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工程二氧化硅纳米包被全细胞不对称生物催化剂高效制备(S)-利瓦斯汀关键手性中间体。
在我们之前的研究中,我们构建了含有醛酮还原酶(yhdN)和葡萄糖脱氢酶(GDH)的全细胞,并将其应用于立体选择性羰基还原反应,制备了(S)-利瓦斯蒂明的关键手性中间体(S)- nema - hepe,后者被广泛用于治疗阿尔茨海默病。虽然转化率和对映体过剩量(e.e)可分别达到78.2% %和99 %,但要提高细胞膜的通透性,需要离子液体作为添加剂。为了进一步简化反应,本文采用分子对接和饱和诱变技术获得了活性改进的yhdN变体,如G19A。在不添加任何添加剂的情况下,仅使用G19A-GDH全细胞作为催化剂,在40 min内即可实现(S)-NEMCA-HEPE的良好转化率和99% %的e.e.。然而,整体电池的使用仍然面临着运行稳定性差和应用前景不利的问题。随后,利用二氧化硅纳米涂层技术构建了疏水的“壳中细胞”复合物G19A-GDH@O-Silica。得到的G19A-GDH@O-Silica对不对称羰基还原具有良好的转化率,并且对温度、pH和储存环境的变化具有良好的耐受性。在11次循环使用后,反应转化率仍为76.3% %,表明G19A-GDH@O-Silica也具有理想的可回收性。本研究的目的是为高效制备(S)-NEMCA-HEPE提供一种快速、经济的纳米包被全细胞生物催化剂。固定化方法的简单性和稳健性可能成为利用全细胞催化剂进行有机催化的有力工具。
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来源期刊
Journal of biotechnology
Journal of biotechnology 工程技术-生物工程与应用微生物
CiteScore
8.90
自引率
2.40%
发文量
190
审稿时长
45 days
期刊介绍: The Journal of Biotechnology has an open access mirror journal, the Journal of Biotechnology: X, sharing the same aims and scope, editorial team, submission system and rigorous peer review. The Journal provides a medium for the rapid publication of both full-length articles and short communications on novel and innovative aspects of biotechnology. The Journal will accept papers ranging from genetic or molecular biological positions to those covering biochemical, chemical or bioprocess engineering aspects as well as computer application of new software concepts, provided that in each case the material is directly relevant to biotechnological systems. Papers presenting information of a multidisciplinary nature that would not be suitable for publication in a journal devoted to a single discipline, are particularly welcome.
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