Expanding the chitin oligosaccharide portfolio by engineering NodC chitin synthases in Escherichia coli

IF 3.6 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Current Research in Biotechnology Pub Date : 2024-01-01 DOI:10.1016/j.crbiot.2024.100255
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Abstract

Synthetic biology greatly accelerated the building process of potential microbial cell factories for the production of industrially relevant compounds, e.g., chitooligosaccharides (COS) which have an enormous application potential in multiple industries, i.e., pharma, cosmetics and agrifood. COS are produced by the heterologous expression of the chitin oligosaccharide synthase, NodC, in Escherichia coli, mainly yielding mixtures of chitintetraose (A4) and/or chitinpentaose (A5). We rationalised here product formation limitations based on molecular modelling of the structures of several NodC enzymes. We used this information to protein engineer NodC, rendering longer COS. Hence, an in vivo platform of defined COS-producing strains with different degrees of polymerisation was developed and experimentally characterised. Significantly, several strains were producing long COS, such as chitinhexaose (A6) and −heptaose (A7), not identified in any other natural producer. Additionally, other engineered strains efficiently produce almost 100% specific A4 or A5 product. Altogether, our results indicate that electrostatics-driven dynamics effects are to be considered in the molecular ruler hypothesis. Charge density at the transmembrane helices of NodC affects the opening of the integral binding pocket and in this way the length of the produced chitin oligomers can be modulated. As a result, the internal ruler mechanism elaborated and validated in this manuscript can serve as a guideline to perform site-directed mutagenesis at positions in related NodC and chitin synthase enzymes for both industrial applications as for identification of therapeutic targets.

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通过在大肠杆菌中改造 NodC 几丁质合成酶来扩展几丁质寡糖组合
合成生物学大大加快了生产工业相关化合物的潜在微生物细胞工厂的建设进程,例如壳寡糖(COS),它在制药、化妆品和农业食品等多个行业具有巨大的应用潜力。COS 是通过在大肠杆菌中异源表达几丁质寡糖合成酶 NodC 而产生的,主要生成几丁质四糖(A4)和/或几丁质五糖(A5)的混合物。我们根据几种 NodC 酶的分子结构建模,合理解释了产品形成的局限性。我们利用这些信息对 NodC 进行了蛋白质工程改造,使其具有更长的 COS。因此,我们开发了一个具有不同聚合度的 COS 生产菌株的体内平台,并对其进行了实验鉴定。值得注意的是,有几株菌株正在生产长COS,如甲壳素六糖(A6)和七糖(A7),这在任何其他天然生产者中都没有发现。此外,其他工程菌株也能高效生产几乎 100% 的特异性 A4 或 A5 产品。总之,我们的研究结果表明,分子尺假说应考虑静电驱动的动力学效应。NodC 跨膜螺旋上的电荷密度会影响整体结合口袋的打开,从而调节所产生的几丁质低聚物的长度。因此,本手稿中阐述和验证的内部标尺机制可作为对相关 NodC 和几丁质合成酶的位置进行定点诱变的指南,既可用于工业应用,也可用于确定治疗靶点。
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来源期刊
Current Research in Biotechnology
Current Research in Biotechnology Biochemistry, Genetics and Molecular Biology-Biotechnology
CiteScore
6.70
自引率
3.60%
发文量
50
审稿时长
38 days
期刊介绍: Current Research in Biotechnology (CRBIOT) is a new primary research, gold open access journal from Elsevier. CRBIOT publishes original papers, reviews, and short communications (including viewpoints and perspectives) resulting from research in biotechnology and biotech-associated disciplines. Current Research in Biotechnology is a peer-reviewed gold open access (OA) journal and upon acceptance all articles are permanently and freely available. It is a companion to the highly regarded review journal Current Opinion in Biotechnology (2018 CiteScore 8.450) and is part of the Current Opinion and Research (CO+RE) suite of journals. All CO+RE journals leverage the Current Opinion legacy-of editorial excellence, high-impact, and global reach-to ensure they are a widely read resource that is integral to scientists' workflow.
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