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首页> 外文期刊>Iranian Journal of Pharmaceutical Research >Novel and efficient method for solid phase synthesis of urea-containing peptides targeting prostate specific membrane antigen (PSMA) in comparison with current methods
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Novel and efficient method for solid phase synthesis of urea-containing peptides targeting prostate specific membrane antigen (PSMA) in comparison with current methods

机译:与目前的方法相比,新型高效固相合成靶向前列腺特异性膜抗原(PSMA)的尿素肽的方法

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摘要

The basic chemical structure of most prostate specific membrane antigen (PSMA) inhibitors which are now in pre-clinical and clinical studies is Glu-Ureido-based peptides. Synthesis of urea-based PSMA inhibitors includes two steps: 1- isocyanate intermediate formation and 2- urea bond formation. In current methods, isocyanate is formed in liquid phase and then reacts with amine existing in liquid phase or bound to solid phase for urea bond formation. In this study, we developed a new facile method for formation of both isocyanate and urea on solid phase under standard peptide coupling conditions. The solid phase-bound isocyanate served as intermediate to form urea bond. To monitor reaction progress qualitative test (Kaiser Test) and On-Bead FT-IR spectroscopy were used. The structure of Glutamate-Urea-Lysine (EUK) was confirmed using LC-Mass and 1H-NMR. This novel method successfully applied to synthesize of another urea-based peptide containing a sequence of Glu-Urea-Lys(OMe)-GABA-Tyr-Tyr-GABA and the bifunctional linker hydrazinonicotinamide (HYNIC) as well.
机译:目前在临床前和临床研究中的大多数前列腺特异性膜抗原(PSMA)抑制剂的基本化学结构是基于Glu-Ureido的肽。脲基PSMA抑制剂的合成包括两个步骤:1-异氰酸酯中间体的形成和2-脲键的形成。在当前方法中,异氰酸酯在液相中形成,然后与液相中存在或与固相结合的胺反应形成脲键。在这项研究中,我们开发了一种在标准肽偶联条件下在固相上同时形成异氰酸酯和尿素的简便方法。固相结合的异氰酸酯用作形成脲键的中间体。为了监测反应进程,使用了定性测试(Kaiser测试)和On-Bead FT-IR光谱。使用LC-Mass和1H-NMR确认了谷氨酸-尿素-赖氨酸(EUK)的结构。该新方法成功地用于合成另一种基于尿素的肽,该肽还包含Glu-Urea-Lys(OMe)-GABA-Tyr-Tyr-GABA序列以及双功能接头肼基烟酰胺(HYNIC)。

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