通过修饰骨架环化的缓激肽拮抗剂的设计、合成和表征。

S Reissmann, G Greiner, J Jezek, C Amberg, B Müller, L Seyfarth, L F Pineda De Castro, I Paegelow
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引用次数: 0

摘要

为了合成具有最小侧链修饰的非肽激素缓激肽的环拮抗剂,我们进行了主链到主链和主链到侧链的环化。为了探索和比较这种新型环化的不同策略,我们在固相上通过还原烷基化和使用预制构建单元来形成支链肽键。利用苯丙氨酸衍生物N(CH2COOH)Phe和N(CH2CH2NH2)Phe在修饰的酰胺基团之间形成内酰胺桥。偶联剂PyBrop对n -烷基酰胺键的形成效果最好。通过估算n端fmoc基团来监测耦合率。在固体支架上进行环化。在强酸性条件下,n -烷基酰胺键的不稳定性导致了意想不到的困难,用于脱保护和从树脂中去除。我们合成了在位置2和5之间有主链到主链环化,以及在位置0和5之间和2和6之间有主链到侧链环化的肽。一些环类似物相对较高的生物活性支持了缓激肽拮抗剂的受体结合构象,其n端序列有β -转变。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Design, synthesis and characterization of bradykinin antagonists via cyclization of the modified backbone.

With the aim of synthesizing cyclic antagonists of the nonapeptide hormone bradykinin with minimal side chain modification, we performed backbone to backbone and backbone to side chain cyclization. To probe and compare different strategies for this new kind of cyclization, the branched peptide bonds were formed by both reductive alkylation on the solid phase and by using preformed building units. Lactam bridges between the modified amide groups were formed by the use of the phenylalanine derivatives N(CH2COOH)Phe and N(CH2CH2NH2)Phe. The best results in the formation of the N-alkylamide bond were obtained with the coupling reagent PyBrop. The coupling rate was monitored by estimation of the N-terminal Fmoc-group. The cyclization was performed on the solid support. Unexpected difficulties resulted from the instability of the N-alkylamide bond under strong acidic conditions, as used for deprotection and for removal from the resin. We synthesized peptides with backbone to backbone cyclization between positions 2 and 5, as well as backbone to side chain cyclizations between positions 0 and 5, and between 2 and 6. The relatively high biological activities of some of the cyclic analogues support the supposed receptor-bound conformation of bradykinin antagonists with a beta-turn in the N-terminal sequence.

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