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血吸虫衍生寡-α-(1-2)-岩藻糖基的合成及抗体结合研究。

Synthesis and Antibody Binding Studies of Schistosome-Derived Oligo-α-(1-2)-l-Fucosides.

机构信息

Leiden Institute of Chemistry, Leiden University, Einsteinweg 55, 2333CC Leiden, The Netherlands.

Department of Parasitology, Leiden University Medical Center, 2333ZA Leiden, The Netherlands.

出版信息

Molecules. 2021 Apr 13;26(8):2246. doi: 10.3390/molecules26082246.

Abstract

Schistosomiasis is caused by blood-dwelling parasitic trematodes of the genus and is classified by the WHO as the second most socioeconomically devastating parasitic disease, second only to malaria. expresses a complex array of glycans as part of glycoproteins and glycolipids that can be targeted by both the adaptive and the innate part of the immune system. Some of these glycans can be used for diagnostic purposes. A subgroup of schistosome glycans is decorated with unique α-(1-2)-fucosides and it has been shown that these often multi-fucosylated fragments are prime targets for antibodies generated during infection. Since these α-(1-2)-fucosides cannot be obtained in sufficient purity from biological sources, we set out to develop an effective route of synthesis towards α-(1-2)-oligofucosides of varying length. Here we describe the exploration of two different approaches, starting from either end of the fucose chains. The oligosaccharides have been attached to gold nanoparticles and used in an enzyme-linked immunosorbent assay ELISA and a microarray format to probe antibody binding. We show that binding to the oligofucosides of antibodies in sera of infected people depends on the length of the oligofucose chains, with the largest glycans showing most binding.

摘要

血吸虫病是由血生寄生吸虫属的寄生虫引起的,世界卫生组织将其列为第二大致残疾病,仅次于疟疾。血吸虫表达一系列复杂的糖基作为糖蛋白和糖脂的一部分,可被免疫系统的适应性和固有部分靶向。其中一些糖基可用于诊断目的。血吸虫糖的一个亚组用独特的α-(1-2)-岩藻糖基修饰,已经表明这些通常多岩藻糖基化的片段是感染期间产生的抗体的主要靶标。由于这些α-(1-2)-岩藻糖基不能从生物来源中以足够的纯度获得,我们着手开发一种有效的合成方法来制备不同长度的α-(1-2)-低聚岩藻糖。在这里,我们描述了从糖链的两端开始的两种不同方法的探索。将寡糖连接到金纳米粒子上,并用于酶联免疫吸附测定 (ELISA) 和微阵列格式来探测抗体结合。我们表明,与感染患者血清中抗体的低聚岩藻糖的结合取决于低聚岩藻糖链的长度,最长的糖显示出最大的结合。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db80/8068878/e3d4a1fe1d32/molecules-26-02246-g001.jpg

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