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细胞器样隔室的细胞内构建促进. 的代谢通量

Intracellular Construction of Organelle-like Compartments Facilitates Metabolic Flux in .

机构信息

State Key Laboratory of Food Science and Resources, Jiangnan University, Wuxi, Jiangsu 214122, China.

出版信息

J Agric Food Chem. 2024 Sep 18;72(37):20582-20591. doi: 10.1021/acs.jafc.4c06895. Epub 2024 Sep 4.

DOI:10.1021/acs.jafc.4c06895
PMID:39230507
Abstract

The formation of well-designed synthetic compartments or membraneless organelles for applications in synthetic biology and cellular engineering has aroused enormous interest. However, establishing stable and robust intracellular compartments in bacteria remains a challenge. Here, we use the structured DIX domains derived from Wnt signaling pathway components, more specifically, Dvl2 and Axin1, as building blocks to generate intracellular synthetic compartments in . Moreover, the aggregation behaviors and physical properties of the DIX-based compartments can be tailored by genetically embedding a specific dimeric domain into the DIX domains. Then, a pair of interacting motifs, consisting of the aforementioned dimeric domain and its corresponding binding ligand, was incorporated to modify the client recruitment pattern of the synthetic compartments. As a proof of concept, the human milk oligosaccharide lacto--tetraose (LNT) biosynthesis pathway was selected as a model metabolic pathway. The fermentation results demonstrated that the co-compartmentalization of sequential pathway enzymes into intracellular compartments created by DIX domain, or by the DIX domain in conjunction with interacting motifs, prominently enhanced the metabolic flux and increased LNT production. These synthetic protein compartments may provide a feasible and effective tool to develop versatile organelle-like compartments in bacteria for applications in cellular engineering and synthetic biology.

摘要

用于合成生物学和细胞工程应用的精心设计的合成隔室或无膜细胞器的形成引起了极大的兴趣。然而,在细菌中建立稳定和强大的细胞内隔室仍然是一个挑战。在这里,我们使用源自 Wnt 信号通路成分的结构 DIX 结构域,更具体地说是 Dvl2 和 Axin1,作为构建块在 中生成细胞内合成隔室。此外,通过遗传嵌入特定的二聚结构域到 DIX 结构域中,可以调整基于 DIX 的隔室的聚集行为和物理性质。然后,将一对相互作用的基序(由上述二聚结构域及其相应的结合配体组成)掺入到合成隔室中来修饰客户招募模式。作为概念验证,选择人乳寡糖乳糖 - 四糖 (LNT) 生物合成途径作为模型代谢途径。发酵结果表明,将连续途径酶共隔室化到 DIX 结构域形成的细胞内隔室中,或者到 DIX 结构域与相互作用基序结合形成的隔室中,显著提高了代谢通量并增加了 LNT 的产量。这些合成蛋白隔室可能为在细菌中开发用于细胞工程和合成生物学的多功能类细胞器隔室提供一种可行且有效的工具。

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