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同源和异源多价岩藻糖基化和唾液酸化寡糖缀合物的合成:预活化的α-甲氧基胺精密大分子及其与多瘤病毒衣壳蛋白的结合

Synthesis of Homo- and Heteromultivalent Fucosylated and Sialylated Oligosaccharide Conjugates Preactivated -Methyloxyamine Precision Macromolecules and Their Binding to Polyomavirus Capsid Proteins.

作者信息

Konietzny Patrick B, Freytag Jasmin, Feldhof Melina I, Müller Joshua C, Ohl Daniel, Stehle Thilo, Hartmann Laura

机构信息

Department of Organic and Macromolecular Chemistry, Heinrich-Heine-University Düsseldorf, Universitätsstraße 1, Düsseldorf 40225, Germany.

Interfaculty Institute of Biochemistry, University of Tübingen, Auf der Morgenstelle 34, Tübingen 72076, Germany.

出版信息

Biomacromolecules. 2022 Dec 12;23(12):5273-5284. doi: 10.1021/acs.biomac.2c01092. Epub 2022 Nov 18.

DOI:10.1021/acs.biomac.2c01092
PMID:36398945
Abstract

Glycoconjugates are a versatile class of bioactive molecules that have found application as vaccines and antivirals and in cancer therapy. Their synthesis typically involves elaborate functionalization and use of protecting groups on the carbohydrate component in order to ensure efficient and selective conjugation. Alternatively, non-functionalized, non-protected carbohydrates isolated from biological sources or derived through biotechnological methods can be directly conjugated -methyloxyamine groups. In this study, we introduce such -methyloxyamine groups into a variety of multivalent scaffolds─from small to oligomeric to polymeric scaffolds─making use of solid-phase polymer synthesis to assemble monodisperse sequence-defined macromolecules. These scaffolds are then successfully functionalized with different types of human milk oligosaccharides deriving a library of homo- and heteromultivalent glycoconjugates. Glycomacromolecules presenting oligosaccharide side chains with either α2,3- or α2,6-linked terminal sialic acid are used in a binding study with two types of polyomavirus capsid proteins showing that the multivalent presentation through the -methyloxyamine-derived scaffolds increases the number of contacts with the protein. Overall, a straightforward route to derive glycoconjugates from complex oligosaccharides with high variability yet control in the multivalent scaffold is presented, and applicability of the derived structures is demonstrated.

摘要

糖缀合物是一类多功能的生物活性分子,已被用作疫苗、抗病毒药物以及用于癌症治疗。它们的合成通常涉及对碳水化合物组分进行精细的官能化和使用保护基,以确保高效且选择性的共轭。另外,从生物来源分离或通过生物技术方法衍生的未官能化、未保护的碳水化合物可以直接与甲氧基胺基团共轭。在本研究中,我们利用固相聚合物合成来组装单分散的序列定义大分子,将此类甲氧基胺基团引入多种多价支架中,从小分子到寡聚物再到聚合物支架。然后,这些支架成功地用不同类型的人乳寡糖进行官能化,得到了同价和异价糖缀合物文库。带有α2,3-或α2,6-连接的末端唾液酸的寡糖侧链的糖大分子用于与两种多瘤病毒衣壳蛋白的结合研究,结果表明通过甲氧基胺衍生的支架进行多价呈现增加了与蛋白质的接触数量。总体而言,本文提出了一种从复杂寡糖衍生糖缀合物的直接途径,该途径在多价支架中具有高变异性但可控性,并证明了所衍生结构的适用性。

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Step-Growth Glycopolymers with a Defined Tacticity for Selective Carbohydrate-Lectin Recognition.具有确定立构规整性的逐步增长糖聚物用于选择性碳水化合物-凝集素识别。
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