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用于生物传感的GM3、GM2和GM1模拟物:化学酶合成、目标亲和力及900兆赫核磁共振分析

GM3, GM2 and GM1 mimics designed for biosensing: chemoenzymatic synthesis, target affinities and 900 MHz NMR analysis.

作者信息

Pukin Aliaksei V, Weijers Carel A G M, van Lagen Barend, Wechselberger Rainer, Sun Bin, Gilbert Michel, Karwaski Marie-France, Florack Dion E A, Jacobs Bart C, Tio-Gillen Anne P, van Belkum Alex, Endtz Hubert P, Visser Gerben M, Zuilhof Han

机构信息

Laboratory of Organic Chemistry, Wageningen University, Dreijenplein 8, 6703 HB, Wageningen, The Netherlands.

出版信息

Carbohydr Res. 2008 Mar 17;343(4):636-50. doi: 10.1016/j.carres.2008.01.007. Epub 2008 Jan 16.

Abstract

Undec-10-enyl, undec-10-ynyl and 11-azidoundecyl glycoside analogues corresponding to the oligosaccharides of human gangliosides GM3, GM2 and GM1 were synthesized in high yields using glycosyltransferases from Campylobacter jejuni. Due to poor water solubility of the substrates, the reactions were carried out in methanol-water media, which for the first time were shown to be compatible with the C. jejuni alpha-(2-->3)-sialyltransferase (CST-06) and beta-(1-->4)-N-acetylgalactosaminyltransferase (CJL-30). Bioequivalence of our synthetic analogues and natural gangliosides was examined by binding to Vibrio cholerae toxin and to the B subunit of Escherichia coli heat-labile enterotoxin. This bioequivalence was confirmed by binding mouse and human monoclonal antibodies to GM1 and acute phase sera containing IgM and IgG antibodies to GM1 from patients with the immune-mediated polyneuropathy Guillain-Barré syndrome. The synthesized compounds were analyzed by 1D and 2D 900 MHz NMR spectroscopy. TOCSY and DQF-COSY experiments in combination with 13C-1H correlation measurements (HSQC, HMBC) were carried out for primary structural characterization, and a complete assignment of all 1H and 13C chemical shifts is presented.

摘要

使用空肠弯曲菌的糖基转移酶,以高产率合成了与人类神经节苷脂GM3、GM2和GM1的寡糖相对应的十一碳-10-烯基、十一碳-10-炔基和11-叠氮基十一烷基糖苷类似物。由于底物的水溶性较差,反应在甲醇-水介质中进行,首次证明该介质与空肠弯曲菌α-(2→3)-唾液酸转移酶(CST-06)和β-(1→4)-N-乙酰半乳糖胺转移酶(CJL-30)兼容。通过与霍乱弧菌毒素和大肠杆菌不耐热肠毒素的B亚基结合,检测了我们合成的类似物与天然神经节苷脂的生物等效性。通过将小鼠和人类单克隆抗体与GM1结合以及将含有免疫介导性多发性神经病吉兰-巴雷综合征患者针对GM1的IgM和IgG抗体的急性期血清结合,证实了这种生物等效性。通过一维和二维900 MHz核磁共振光谱对合成的化合物进行了分析。进行了全相关谱(TOCSY)和双量子滤波相关谱(DQF-COSY)实验,并结合13C-1H相关测量(HSQC、HMBC)进行一级结构表征,给出了所有1H和13C化学位移的完整归属。

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