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首页> 外文期刊>Analytical Biochemistry: An International Journal of Analytical and Preparative Methods >Assessing the inhibitory potency of galectin ligands identified from combinatorial (glyco)peptide libraries using surface plasmon resonance spectroscopy
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Assessing the inhibitory potency of galectin ligands identified from combinatorial (glyco)peptide libraries using surface plasmon resonance spectroscopy

机译:使用表面等离振子共振光谱法评估从组合(糖)肽库中鉴定的半乳糖凝集素配体的抑制能力

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Combinatorial (glyco)peptide libraries offer the possibility to define effective inhibitors of protein (lectin)-glycan interactions. If a (glyco)peptide surpasses the inhibitory potency of the free sugar, then the new peptide-lectin contacts underlying the affinity enhancement may guide further rational drug design. Focusing on the adhesion/growth regulatory human galectins 1 and 3, a screening of three combinatorial solid-phase (glyco)peptide libraries, containing Gal(beta 1-O)Thr, Gal(P1-S)Cys/Gal(beta 1-N)Asn, and Lac(beta 1-O)Thr, with the fluorescently labeled lectins had led to a series of lead compounds. To define the inhibitory potency of a selection of resynthesized (glyco)peptides systematically, a surface plasmon resonance-based inhibition assay with immobilized asialofetuin was set up. (Glyco)Peptides with up to 66-fold potency relative to free lactose as inhibitor were characterized. The presence of lactose in the most effective glycopeptides indicated the presence of affinity-enhancing peptide-lectin contacts. In addition to drug design, they may be helpful for fine-structural analysis of the binding sites. (C) 2008 Elsevier Inc. All rights reserved.
机译:组合(糖)肽库提供了定义蛋白质(凝集素)-聚糖相互作用的有效抑制剂的可能性。如果(糖)肽超过了游离糖的抑制能力,则亲和力增强基础上的新的肽-凝集素接触可指导进一步合理的药物设计。着重于粘附/生长调节人半乳糖凝集素1和3,筛选了三个包含Gal(β1-O)Thr,Gal(P1-S)Cys / Gal(β1- N)Asn和带有荧光标记的凝集素的Lac(β1-O)Thr导致了一系列先导化合物。为了系统地定义重新合成的(糖)肽选择的抑制能力,建立了基于表面等离振子共振的固定化去唾液酸铁蛋白的抑制试验。相对于作为抑制剂的游离乳糖,具有高达66倍效能的(糖)肽被表征。最有效的糖肽中乳糖的存在表明存在亲和力增强的肽-凝集素接触。除药物设计外,它们还可用于结合位点的精细结构分析。 (C)2008 Elsevier Inc.保留所有权利。

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