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Genetically-encoded fragment-based discovery of glycopeptide ligands for DC-SIGN

机译:基于血管肽配体的基于遗传编码的片段的DC标志的发现

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We have employed genetically-encoded fragment-based discovery to identify novel glycopeptides with affinity for the dendritic cell receptor DC-SIGN. Starting from libraries of 108mannose-conjugated peptides, we identified glycopeptides that exhibited up to a 650-fold increase in multivalent binding affinity for DC-SIGN, which is also preserved in cells. Monovalently, our most potent glycopeptides have a similar potency to a Man3oligosaccharide, representing a 15-fold increase in activity compared to mannose. These compounds represent the first examples of glycopeptide ligands that target the CRD of DC-SIGN. The natural framework of glycopeptide conjugates and the simplicity of orthogonal conjugation to make these glycopeptides anticipates a promising future for development of DC-SIGN-targeting moieties.
机译:我们使用基因编码的基于片段的发现,以鉴定具有对树突细胞受体DC-符号的亲和力的新型糖肽。 从108mannose缀合的肽的文库开始,我们鉴定了糖肽,其表现出高达650倍的多价结合亲和力的增加,该DC标志也被保存在细胞中。 在一起,我们最有效的糖肽具有与Man3醇糖具有相似的效力,与甘露糖相比,该活性增加了15倍。 这些化合物代表靶向DC标志的CRD的糖肽配体的第一实例。 糖肽缀合物的天然骨架和正交缀合的简单性,使这些糖肽的术预期为DC标志靶向部分的发展有望的未来。

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