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首页> 外文期刊>Angewandte Chemie >Glycopeptide Mimetics Recapitulate High-Mannose-Type Oligosaccharide Binding and Function
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Glycopeptide Mimetics Recapitulate High-Mannose-Type Oligosaccharide Binding and Function

机译:糖肽模拟物概括了高甘露糖型寡糖的结合和功能

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摘要

High-mannose-type glycans (HMTGs) decorating viral spike proteins are targets for virus neutralization. For carbohydrate-binding proteins, multivalency is important for high avidity binding and potent inhibition. To define the chemical determinants controlling multivalent interactions we designed glycopeptide HMTG mimetics with systematically varied mannose valency and spacing. Using the potent antiviral lectin griffithsin (GRFT) as a model, we identified by NMR spectroscopy, SPR, analytical ultracentrifugation, and microcalorimetry glycopeptides that fully recapitulate the specificity and kinetics of binding to Man(9)GlcNAc(2)Asn and a synthetic nonamannoside. We find that mannose spacing and valency dictate whether glycopeptides engage GRFT in a face-to-face or an intermolecular binding mode. Surprisingly, although face-to-face interactions are of higher affinity, intermolecular interactions are longer lived. These findings yield key insights into mechanisms involved in glycan-mediated viral inhibition.
机译:装饰病毒刺突蛋白的高甘露糖型聚糖(HMTG)是病毒中和的目标。对于碳水化合物结合蛋白,多价对于高亲和力结合和有效抑制很重要。为了定义控制多价相互作用的化学决定因素,我们设计了糖肽HMTG模拟物,其系统地改变了甘露糖的化合价和间隔。使用有效的抗病毒凝集素格里菲辛(GRFT)作为模型,我们通过NMR光谱,SPR,分析超速离心和微量量热法糖肽鉴定出了糖肽,这些糖肽充分概括了与Man(9)GlcNAc(2)Asn和合成的壬菜子糖苷结合的特异性和动力学。 。我们发现,甘露糖的间距和化合价决定了糖肽是面对面还是分子间结合模式参与GRFT。出人意料的是,尽管面对面的相互作用具有更高的亲和力,但分子间的相互作用寿命更长。这些发现对涉及聚糖介导的病毒抑制的机制产生了重要的见解。

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