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Histidine-Containing Peptide Catalysts Developed by a Facile Library Screening Method

机译:简便的文库筛选方法开发的含有组氨酸的肽催化剂

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摘要

Although peptide catalysts have a high potential for the use as organocatalysts, the optimization of peptide sequences is laborious and time-consuming. To address this issue, a facile screening method for finding efficient aminocatalysts from a peptide library has been developed. In the screening for the Michael addition of a malonate to an enal, a dye-labeled product is immobilized on resin-bound peptides through reductive amination to visualize active catalysts. This procedure allows for the monitoring of the reactivity of entire peptides without modifying the resin beads beforehand. Peptides containing histidine at an appropriate position were identified by this method. A novel function of the histidyl residue, which enhances the binding of a substrate to the catalyst by capturing an iminium intermediate, was indicated.
机译:尽管肽催化剂具有用作有机催化剂的巨大潜力,但是肽序列的优化是费力且费时的。为了解决这个问题,已经开发了用于从肽文库中寻找有效的氨基催化剂的简便筛选方法。在筛选丙二酸酯向烯醛的迈克尔加成反应中,染料标记的产物通过还原胺化固定在树脂结合的肽上,以可视化活性催化剂。该程序允许在不预先修饰树脂珠的情况下监测整个肽的反应性。通过该方法鉴定了在适当位置含有组氨酸的肽。表明了组氨酸残基的新功能,该功能通过捕获亚胺基中间体来增强底物与催化剂的结合。

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