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首页> 外文期刊>Journal of peptide science: An official publication of the European Peptide Society >A backbone amide protecting group for overcoming difficult sequences and suppressing aspartimide formation
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A backbone amide protecting group for overcoming difficult sequences and suppressing aspartimide formation

机译:用于克服困难序列并抑制天冬酰胺形成的主链酰胺保护基

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摘要

A backbone amide bond protecting group, 2-hydroxy-4-methoxy-5-nitrobenzyl (Hmnb), improved the synthesis of aggregation and aspartimide-prone peptides. Introduction of Hmnb is automated and carried out during peptide assembly by addition of 4-methoxy-5-nitrosalicylaldehyde to the peptidyl-resin and on-resin reduction to the secondary amine. Acylation of the hindered secondary amine is aided by the formation of an internal nitrophenol ester that undergoes a favourable O, N intramolecular acyl transfer. This activated ester participates in the coupling and generally gives complete reaction with standard coupling conditions. Hmnb is easily available in a single preparative step from commercially available material. Different methods for removing the amide protecting group were explored. The protecting group is labile to acidolysis, following reduction of the nitro group to the aniline. The two main uses of backbone protection of preventing aspartimide formation and of overcoming difficult sequences are demonstrated, first with the synthesis of a challenging aspartimide-prone test sequence and then with the classic difficult sequence ACP (65-74) and a 23-mer homopolymer of polyalanine. Copyright (C) 2016 European Peptide Society and John Wiley & Sons, Ltd.
机译:骨架酰胺键保护基团2-羟基-4-甲氧基-5-硝基苄基(Hmnb)改善了聚集和天冬酰胺易肽的合成。 Hmnb的引入是自动化的,并且在肽组装过程中通过向肽基树脂中添加4-甲氧基-5-硝基水杨醛和在树脂上还原成仲胺来进行。受阻仲胺的酰化反应是通过形成内部硝基酚酯来实现的,该硝基酚酯会经历良好的O,N分子内酰基转移。该活化的酯参与偶联并且通常在标准偶联条件下完全反应。 Hmnb可以很容易地在一个制备步骤中从市售材料中获得。探索了用于除去酰胺保护基的不同方法。将硝基还原为苯胺后,保护基对酸解反应不稳定。展示了骨架保护的两个主要用途,即防止天冬酰胺形成和克服困难的序列,首先是合成具有挑战性的天冬酰胺倾向的测试序列,然后是经典的困难序列ACP(65-74)和23-mer均聚物聚丙氨酸。版权所有(C)2016欧洲肽学会和John Wiley&Sons,Ltd.

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