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Pictet-Spengler ligation for protein chemical modification

机译:Pictet-Spengler连接用于蛋白质化学修饰

摘要

Aldehyde- and ketone-functionalized proteins are promising new substrates for the development of chemically modified biotherapeutics and protein-based materials. Their reactive carbonyl groups are typically conjugated with a-effect nucleophiles, such as substituted hydrazines and alkoxyamines, to generate hydrazones and oximes, respectively. However, the resulting C═N linkages are susceptible to hydrolysis under physiologically relevant conditions, which limits their utility in biological systems. Here we introduce a Pictet-Spengler ligation that is based on the classic Pictet-Spengler reaction of aldehydes and tryptamine nucleophiles. The ligation exploits the bioorthogonal reaction of aldehydes and alkoxyamines to form an intermediate oxyiminium ion; this intermediate undergoes intramolecular C—C bond formation with an indole nucleophile to form an oxacarboline product that is hydrolytically stable. The reaction was utilized for site-specific chemical modification of glyoxal- and formylglycine-functionalized proteins, including an aldehyde-tagged variant of the therapeutic monoclonal antibody Herceptin. In conjunction with techniques for site-specific introduction of aldehydes into proteins, the Pictet-Spengler ligation offers a new means to generate stable bioconjugates for medical and materials applications.
机译:醛和酮官能化的蛋白质是用于化学修饰的生物疗法和蛋白质基材料开发的有希望的新底物。它们的反应性羰基通常与α-效果亲核试剂(例如取代的肼和烷氧基胺)缀合,分别产生和肟。然而,所得的C═N键在生理相关条件下易水解,这限制了它们在生物系统中的应用。在这里,我们介绍一种基于经典Pictet-Spengler反应的醛和色胺类亲核试剂的Pictet-Spengler连接。连接利用醛和烷氧基胺的生物正交反应形成中间体氧亚胺离子。该中间体与吲哚亲核体发生分子内C-C键形成,形成水解稳定的氧杂咔啉产物。该反应用于乙二醛和甲酰甘氨酸功能化蛋白的位点特异性化学修饰,包括治疗性单克隆抗体赫赛汀的醛标记变体。 Pictet-Spengler连接技术结合了将醛类特异性引入蛋白质的技术,提供了一种生成稳定的生物共轭物的新方法,可用于医疗和材料应用。

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