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通过“停走”策略简化复杂 N-聚糖的化学酶合成。

Streamlining the chemoenzymatic synthesis of complex N-glycans by a stop and go strategy.

机构信息

Complex Carbohydrate Research Center, University of Georgia, Athens, GA, USA.

Department of Chemical Biology and Drug Discovery, Utrecht Institute for Pharmaceutical Sciences, and Bijvoet Center for Biomolecular Research, Utrecht University, Utrecht, The Netherlands.

出版信息

Nat Chem. 2019 Feb;11(2):161-169. doi: 10.1038/s41557-018-0188-3. Epub 2018 Dec 10.

Abstract

Contemporary chemoenzymatic approaches can provide highly complex multi-antennary N-linked glycans. These procedures are, however, very demanding and typically involve as many as 100 chemical steps to prepare advanced intermediates that can be diversified by glycosyltransferases in a branch-selective manner to give asymmetrical structures commonly found in nature. Only highly specialized laboratories can perform such syntheses, which greatly hampers progress in glycoscience. Here we describe a biomimetic approach in which a readily available bi-antennary glycopeptide can be converted in ten or fewer chemical and enzymatic steps into multi-antennary N-glycans that at each arm can be uniquely extended by glycosyltransferases to give access to highly complex asymmetrically branched N-glycans. A key feature of our approach is the installation of additional branching points using recombinant MGAT4 and MGAT5 in combination with unnatural sugar donors. At an appropriate point in the enzymatic synthesis, the unnatural monosaccharides can be converted into their natural counterpart, allowing each arm to be elaborated into a unique appendage.

摘要

当代的化学酶法方法可以提供高度复杂的多天线 N 连接聚糖。然而,这些程序要求非常高,通常需要多达 100 个化学步骤来制备可通过糖基转移酶以支链选择性方式多样化的高级中间体,以产生自然界中常见的不对称结构。只有高度专业化的实验室才能进行这样的合成,这极大地阻碍了糖科学的发展。在这里,我们描述了一种仿生方法,其中一种现成的双天线糖肽可以在 10 个或更少的化学和酶步骤中转化为多天线 N-聚糖,在每个臂上都可以通过糖基转移酶独特地延伸,从而获得高度复杂的不对称支化 N-聚糖。我们方法的一个关键特征是使用重组 MGAT4 和 MGAT5 以及非天然糖供体来安装额外的分支点。在酶合成的适当阶段,可以将非天然单糖转化为其天然对应物,从而使每个臂都可以精心设计成独特的附属物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3b13/6347513/e63544fd5fca/nihms-1511924-f0002.jpg

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