首页> 外文期刊>Tetrahedron, Asymmetry: The International Journal for Repid Publication on all Aspects of Asymmetry in Orgainc, Inorganic, Organometallic, Physical and Bio-Organic Chemistry >Synthesis of 2-C-branched derivatives of D-mannose: 2-C-aminomethyl-D-mannose binds to the human C-type lectin DC-SIGN with affinity greater than an order of magnitude compared to that of D-mannose
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Synthesis of 2-C-branched derivatives of D-mannose: 2-C-aminomethyl-D-mannose binds to the human C-type lectin DC-SIGN with affinity greater than an order of magnitude compared to that of D-mannose

机译:D-甘露糖的2-C支链衍生物的合成:2-C-氨基甲基-D-甘露糖以比D-甘露糖亲和力大一个数量级的方式与人C型凝集素DC-SIGN结合。

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摘要

2-C-Substituted branched D-mannose analogues are novel monosaccharides, readily obtained from a Kiliani-acetonation sequence on D-fructose, followed by subsequent functional group manipulation. 2-C-Azidomethyl-D-mannose and 2-C-aminomethylD-marmose bind to the C-type lectin DC-SIGN (CD209) with significantly greater affinity than mannose. In particular, 2-C-aminomethyl-D-mannose exhibits a comparative 48-fold increase in binding as determined using a surface plasmon resonance-based competition assay. DC-SIGN is an important cell-surface type II transmembrane protein that interacts with blood group antigens, endogenous glycoproteins such as ICAM-3, and also deadly pathogens such as the human immunodeficiency and hepatitis C viruses. The effective use of small compounds to block target binding by mannose-selective C-type lectins at sub-millimolar concentrations has not been shown previously; thus, these data represent a very attractive thoroughfare to novel antiviral and immunomodulatory drug development. @ 2007 Elsevier Ltd. All rights reserved.
机译:2-C取代的支链D-甘露糖类似物是新型单糖,可从D-果糖上的Kiliani-丙酮化序列中轻松获得,然后进行后续官能团操作。 2-C-叠氮基甲基-D-甘露糖和2-C-氨基甲基D-marmose以比甘露糖大得多的亲和力与C型凝集素DC-SIGN(CD209)结合。特别地,如使用基于表面等离振子共振的竞争测定法所确定的,2-C-氨基甲基-D-甘露糖显示出相对48倍的结合增加。 DC-SIGN是一种重要的细胞表面II型跨膜蛋白,可与血型抗原,内源糖蛋白(如ICAM-3)以及致命病原体(如人类免疫缺陷和丙型肝炎病毒)相互作用。以前尚未显示过使用小化合物有效阻止亚毫摩尔浓度的甘露糖选择性C型凝集素与靶标结合的现象。因此,这些数据代表了对新型抗病毒和免疫调节药物开发非常有吸引力的通途。 @ 2007 Elsevier Ltd.保留所有权利。

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