The β1,2-glucans produced by bacteria are important in invasion, survival and immunomodulation in infected hosts be they mammals or plants. However, there has been a lack of information on proteins which recognize these molecules. This is partly due to the extremely limited availability of the sequence-defined oligosaccharides and derived probes for use in the study of their interactions. Here we have used the cyclic β1,2-glucan (CβG) of the bacterial pathogen Brucella abortus, after removal of succinyl side chains, to prepare linearized oligosaccharides which were used to generate microarrays. We describe optimized conditions for partial depolymerization of the cyclic glucan by acid hydrolysis and conversion of the β1,2-gluco-oligosaccharides, with degrees of polymerization 2-13, to neoglycolipids for the purpose of generating microarrays. By microarray analyses, we show that the C-type lectin receptor DC-SIGNR, like the closely related DC-SIGN we investigated earlier, binds to the β1,2-gluco-oligosaccharides, as does the soluble immune effector serum mannose-binding protein. Exploratory studies with DC-SIGN are suggestive of the recognition also of the intact CβG by this receptor. These findings open the way to unravelling mechanisms of immunomodulation mediated by β1,2-glucans in mammalian systems.
Generation and characterization of β1,2-gluco-oligosaccharide probes from Brucella abortus cyclic β-glucan and their recognition by C-type lectins of the immune system.
从布鲁氏菌环状β-葡聚糖中生成和表征β1,2-葡糖寡糖探针及其被免疫系统C型凝集素识别
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作者:Zhang Hongtao, Palma Angelina S, Zhang Yibing, Childs Robert A, Liu Yan, Mitchell Daniel A, Guidolin Leticia S, Weigel Wilfried, Mulloy Barbara, Ciocchini Andrés E, Feizi Ten, Chai Wengang
| 期刊: | Glycobiology | 影响因子: | 3.300 |
| 时间: | 2016 | 起止号: | 2016 Oct;26(10):1086-1096 |
| doi: | 10.1093/glycob/cww041 | 研究方向: | 其它 |
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