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Structural insights into what glycan arrays tell us about how glycan-binding proteins interact with their ligands

机译:关于聚糖阵列的结构洞察力告诉我们聚糖结合蛋白如何与其配体相互作用

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摘要

Screening of glycan arrays represents a powerful, high-throughput approach to defining oligosaccharide ligands for glycan-binding receptors, commonly referred to as lectins. Correlating results from such arrays with structural analysis of receptor–ligand complexes provide one way to validate the arrays. Using examples drawn from the family of proteins that contain C-type carbohydrate-recognition domains, this review illustrates how information from the arrays reflects the way that selectivity and affinity for glycan ligands is achieved. A range of binding profiles is observed, from very restricted binding to a small set of structurally similar ligands to binding of broad classes of ligands with related terminal sugars and even to failure to bind any of the glycans on an array. These outcomes provide insights into the importance of multiple factors in defining the selectivity of these receptors, including the presence of conformationally defined units in some oligosaccharide ligands, local and extended interactions between glycans and the surfaces of receptors, and steric factors that exclude binding of some ligands.
机译:聚糖阵列的筛选代表了一种强大的,高通量的方法,可为聚糖结合受体(通常称为凝集素)定义寡糖配体。将此类阵列的结果与受体-配体复合物的结构分析进行关联提供了一种验证阵列的方法。使用从包含C型碳水化合物识别结构域的蛋白质家族中提取的实例,该综述说明了来自阵列的信息如何反映出实现对聚糖配体的选择性和亲和力的方式。观察到一系列的结合概况,从非常有限的结合到一小组结构相似的配体到广泛种类的配体与相关末端糖的结合,甚至是无法结合阵列上的任何聚糖。这些结果为了解多种因素在定义这些受体的选择性中的重要性提供了见解,包括某些寡糖配体中构象定义的单元的存在,聚糖与受体表面之间的局部和扩展相互作用以及排除某些物质结合的空间因素配体。

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