简易地图引导逐步一锅多酶(StOPMe)合成和多重测定鉴定功能性四糖核心-人乳低聚糖。

IF 8.7 Q1 CHEMISTRY, MULTIDISCIPLINARY JACS Au Pub Date : 2025-01-27 eCollection Date: 2025-02-24 DOI:10.1021/jacsau.4c01094
Yuanyuan Bai, Anand Kumar Agrahari, Libo Zhang, Hai Yu, Xiaoxiao Yang, Zimin Zheng, William Su, Jingxin Fu, Xi Chen
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引用次数: 0

摘要

碳水化合物是生物学和医学上重要的分子,其合成和应用越来越受到人们的关注。与核酸和蛋白质的生物合成过程不同,碳水化合物的生物合成不是模板驱动的,更具挑战性,并且经常导致产品变化。代替碳水化合物生物合成的模板,我们在此描述了设计酶组装合成图(EASyMaps)作为蓝图的新概念,以指导糖基转移酶依赖的逐步一锅多酶(StOPMe)合成,以目标导向的方式系统地获取结构多样的碳水化合物。该策略用于构建包含四糖核的人乳寡糖(HMOs)的综合文库,该文库具有更复杂的HMOs共享的多种功能重要聚糖表位。四糖核hmo是大规模生产和开发基于hmo的营养保健品的有吸引力的候选者。为了实现含有Neu5Acα2-6GlcNAc成分的靶标的制备规模合成,我们在大肠杆菌中成功表达了人α2-6-唾液基转移酶hST6GALNAC5。制备了具有控制糖价的新糖蛋白,并将其固定在荧光磁珠上。多重头分析揭示了来自植物、流感病毒、人类和细菌的聚糖结合蛋白的配体,确定了有希望的功能应用的HMO靶标。设计EASyMaps作为蓝图的概念,以系统的目标导向的方式指导StOPMe合成,广泛适用于hmo合成之外的领域。高效的StOPMe工艺适用于复杂碳水化合物的大规模生产,并有可能实现自动化。
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EASyMap-Guided Stepwise One-Pot Multienzyme (StOPMe) Synthesis and Multiplex Assays Identify Functional Tetraose-Core-Human Milk Oligosaccharides.

Carbohydrates are biologically and medicinally important molecules that are attracting growing attention to their synthesis and applications. Unlike the biosynthetic processes for nucleic acids and proteins, carbohydrate biosynthesis is not template-driven, more challenging, and often leads to product variations. In lieu of templates for carbohydrate biosynthesis, we describe herein a new concept of designing enzyme assembly synthetic maps (EASyMaps) as blueprints to guide glycosyltransferase-dependent stepwise one-pot multienzyme (StOPMe) synthesis to systematically access structurally diverse carbohydrates in a target-oriented manner. The strategy is demonstrated for the construction of a comprehensive library of tetraose-core-containing human milk oligosaccharides (HMOs) presenting diverse functional important glycan epitopes shared by more complex HMOs. The tetraose-core-HMOs are attractive candidates for large-scale production and for the development of HMO-based nutraceuticals. To achieve the preparative-scale synthesis of targets containing a Neu5Acα2-6GlcNAc component, a human α2-6-sialyltransferase hST6GALNAC5 is successfully expressed in E. coli. Neoglycoproteins with controlled glycan valencies are prepared and immobilized on fluorescent magnetic beads. Multiplex bead assays reveal ligands of glycan-binding proteins from plants, influenza viruses, human, and bacteria, identifying promising HMO targets for functional applications. The concept of designing EASyMaps as blueprints to guide StOPMe synthesis in a systematic target-oriented manner is broadly applicable beyond the synthesis of HMOs. The efficient StOPMe process is suitable for the large-scale production of complex carbohydrates and can be potentially adapted for automation.

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