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Deciphering Structural Elements of Mucin Glycoprotein Recognition

机译:黏蛋白糖蛋白识别的解读结构要素

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摘要

Mucin glycoproteins present a complex structural landscape arising from the multiplicity of glycosylation patterns afforded by their numerous serine and threonine glycosylation sites, often in clusters, and with variations in respective glycans. To explore the structural complexities in such glycoconjugates we used NMR to systematically analyze the conformational effects of glycosylation density within a cluster of sites. This allows correlation with molecular recognition through analysis of interactions between these and other glycopeptides, with antibodies, lectins, and sera, using a glycopeptide microarray. Selective antibody interactions with discrete conformational elements, reflecting aspects of the peptide and disposition of GalNAc residues are observed. Our results help bridge the gap between conformational properties and molecular recognition of these molecules, with implications for their physiological roles. Features of the native mucin motifs impact their relative immunogenicity and are accurately encoded in the antibody binding site, with the conformational integrity being preserved in isolated glycopeptides, as reflected in the antibody binding profile to array components.
机译:粘蛋白糖蛋白提出了由其许多丝氨酸和苏氨酸糖基化位点提供的糖基化图案的多种糖基化图案产生的复杂结构景观,通常在簇中,以及各种聚糖的变化。为了探讨这些糖核缀合物中的结构复杂性,我们使用NMR来系统地分析糖基化密度在位点簇内的构象效应。这允许通过分析这些和其他糖肽之间的相互作用,使用糖肽微阵列的抗体,凝集素和血清分析与分子识别的相关性。观察到与离散构象元素的选择性抗体相互作用,反射肽的方面和Galnac残基的布置的方面。我们的结果有助于弥合构象性质与这些分子的分子识别之间的差距,具有对其生理作用的影响。天然粘蛋白基序的特征会影响其相对免疫原性并且在抗体结合位点中精确地编码,具有在分离的糖肽中保存的构象完整性,如在阵列组分的抗体结合曲线中反映。

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