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综合化学酶法合成全面硫酸化神经节苷脂聚糖文库,以揭示功能糖基组学和唾液酸糖基组学。

Integrated chemoenzymatic synthesis of a comprehensive sulfated ganglioside glycan library to decipher functional sulfoglycomics and sialoglycomics.

机构信息

State Key Laboratory of Chemical Biology, Carbohydrate-Based Drug Research Center, Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai, China.

University of Chinese Academy of Sciences, Beijing, China.

出版信息

Nat Chem. 2024 Jun;16(6):881-892. doi: 10.1038/s41557-024-01540-x. Epub 2024 Jun 6.

Abstract

Ganglioside glycans are ubiquitous and complex biomolecules that are involved in a wide range of biological functions and disease processes. Variations in sialylation and sulfation render the structural complexity and diversity of ganglioside glycans, and influence protein-carbohydrate interactions. Structural and functional insights into the biological roles of these glycans are impeded due to the limited accessibility of well-defined structures. Here we report an integrated chemoenzymatic strategy for expeditious and systematic synthesis of a comprehensive 65-membered ganglioside glycan library covering all possible patterns of sulfation and sialylation. This strategy relies on the streamlined modular assembly of three common sialylated precursors by highly stereoselective iterative sialylation, modular site-specific sulfation through flexible orthogonal protecting-group manipulations and enzymatic-catalysed diversification using three sialyltransferase modules and a galactosidase module. These diverse ganglioside glycans enable exploration into their structure-function relationships using high-throughput glycan microarray technology, which reveals that different patterns of sulfation and sialylation on these glycans mediate their unique binding specificities.

摘要

神经节苷脂糖是广泛存在且复杂的生物分子,参与多种生物学功能和疾病过程。唾液酸化和硫酸化的差异赋予了神经节苷脂糖的结构复杂性和多样性,并影响了蛋白质-碳水化合物的相互作用。由于缺乏明确结构的可及性,这些糖的生物学功能的结构和功能见解受到阻碍。在这里,我们报告了一种综合的化学酶策略,用于快速系统地合成涵盖所有可能的硫酸化和唾液酸化模式的全面的 65 成员神经节苷脂糖库。该策略依赖于通过高度立体选择性的迭代唾液酸化,通过灵活的正交保护基操作进行模块化的特异性硫酸化,以及使用三个唾液酸转移酶模块和一个半乳糖苷酶模块进行酶促多样化,对三种常见的唾液酸化前体进行流线型模块化组装。这些不同的神经节苷脂糖可以使用高通量糖微阵列技术探索它们的结构-功能关系,这表明这些糖上不同的硫酸化和唾液酸化模式介导了它们独特的结合特异性。

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