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在肽骨架上普遍安装(4)-咪唑啉-酰胺生物等排体。

General Installation of (4)-Imidazolone -Amide Bioisosteres Along the Peptide Backbone.

机构信息

Department of Chemistry, Iowa State University, Ames, Iowa 50011, United States.

出版信息

J Am Chem Soc. 2024 May 1;146(17):11648-11656. doi: 10.1021/jacs.3c13825. Epub 2024 Apr 17.

Abstract

Imidazolones represent an important class of heterocycles present in a wide range of pharmaceuticals, metabolites, and bioactive natural products and serve as the active chromophore in green fluorescent protein. Recently, imidazolones have received attention for their ability to act as a nonaromatic amide bond bioisotere which improves pharmacological properties. Herein, we present a tandem amidine installation and cyclization with an adjacent ester to yield (4)-imidazolone products. Using amino acid building blocks, we can access the first examples of α-chiral imidazolones that have been previously inaccessible. Additionally, our method is amenable to on-resin installation which can be seamlessly integrated into existing solid-phase peptide synthesis protocols. Finally, we show that peptide imidazolones are potent -amide bond surrogates that preorganize linear peptides for head-to-tail macrocyclization. This work represents the first general approach to the backbone and side-chain insertion of imidazolone bioisosteres at various positions in linear and cyclic peptides.

摘要

咪唑酮是一类重要的杂环化合物,广泛存在于各种药物、代谢物和生物活性天然产物中,并且是绿色荧光蛋白中活性发色团。最近,由于咪唑酮能够作为非芳香酰胺键生物等排体来改善药理学性质,因此受到了关注。在此,我们提出了一种通过酰胺安装和与相邻酯的环化反应来生成(4)-咪唑酮产物的串联反应。使用氨基酸构建模块,我们可以获得以前无法获得的α-手性咪唑酮的首例实例。此外,我们的方法适用于树脂上的安装,可以无缝集成到现有的固相肽合成方案中。最后,我们表明肽咪唑酮是有效的酰胺键替代物,可以使线性肽预组织成头尾环化的构象。这项工作代表了在线性和环状肽中各种位置插入咪唑酮生物等排体的主链和侧链的第一种通用方法。

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