Lewis X (Lex)-containing glycans play important roles in numerous cellular processes. However, the absence of robust, facile, and cost-effective methods for the synthesis of Lex and its structurally related analogs has severely hampered the elucidation of the specific functions of these glycan epitopes. Here we demonstrate that chemically defined guanidine 5′-diphosphate-β-l-fucose (GDP-fucose), the universal fucosyl donor, the Lex trisaccharide, and their C-5 substituted derivatives can be synthesized on preparative scales, using a chemoenzymatic approach. This method exploits l-fucokinase/GDP-fucose pyrophosphorylase (FKP), a bifunctional enzyme isolated from Bacteroides fragilis 9343, which converts l-fucose into GDP-fucose via a fucose-1-phosphate (Fuc-1-P) intermediate. Combining the activities of FKP and a Helicobacter pylori α1,3 fucosyltransferase, we prepared a library of Lex trisaccharide glycans bearing a wide variety of functional groups at the fucose C-5 position. These neoglycoconjugates will be invaluable tools for studying Lex-mediated biological processes.
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机译:含有Lewis X(Le x )的聚糖在许多细胞过程中起着重要作用。然而,由于缺乏可靠,简便且具有成本效益的Le x 及其结构类似物的合成方法,严重阻碍了对这些聚糖表位的特定功能的阐明。在这里,我们证明了可以合成化学定义的胍5'-二磷酸-β-1-岩藻糖(GDP-岩藻糖),通用岩藻糖基供体,Le x 三糖及其C-5取代衍生物使用化学酶法在制备规模上进行。这种方法利用了l-岩藻糖激酶/ GDP-岩藻糖焦磷酸化酶(FKP),这是一种从脆弱拟杆菌9343分离的双功能酶,该酶通过1-岩藻糖(Fuc-1-P)中间体将L-岩藻糖转化为GDP-岩藻糖。结合FKP和幽门螺杆菌α1,3岩藻糖基转移酶的活性,我们制备了一个在岩藻糖C-5位置带有多种官能团的Le x 三糖聚糖文库。这些新糖缀合物将是研究Le x 介导的生物学过程的宝贵工具。
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