Cyclic Imines in Ugi and Ugi-Type Reactions

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Mohammad Taghi Nazeri, Hassan Farhid, Reza Mohammadian, Ahmad Shaabani*
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引用次数: 31

Abstract

Ugi four-component reactions (U-4CRs) are widely recognized as being highly efficient for the synthesis of pseudopeptides. However, the products of these reactions are not so interesting as drug candidates because they are not conformationally restricted enough for a potent interaction with biological targets. One possible way to overcome this problem is to replace amine and oxo components in the U-4CRs with cyclic imines in so-called Joullié?Ugi three-component reactions (JU-3CRs). This approach provides a robust single-step route to peptide moieties connected to N-heterocyclic motifs that are found as core skeletons in many natural products and pharmaceutical compounds. JU-3CRs also provide much better diastereoselectivity than their four-component analogues. We survey here the redesign of many synthetic routes for the efficient preparation of a wide variety of three-, five-, six-, and seven-membered heterocyclic compounds connected to the peptide backbone. Additionally, in the Ugi reactions based on the cyclic imines, α-acidic isocyanides, or azides can be replaced with normal isocyanides or acids, respectively, leading to the synthesis of N-heterocycles attached to oxazoles or tetrazoles, which are of great pharmaceutical significance. This Review includes all research articles related to Ugi reactions based on the cyclic imines to the year 2020 and will be useful to chemists in designing novel synthetic routes for the synthesis of individual and combinatorial libraries of natural products and drug-like compounds.

Abstract Image

Ugi和Ugi型反应中的环亚胺
Ugi四组分反应(U-4CRs)被广泛认为是合成假肽的高效反应。然而,这些反应的产物并不像候选药物那样令人感兴趣,因为它们的构象限制不够,无法与生物靶点产生有效的相互作用。克服这个问题的一种可能的方法是用所谓的joulli中的环亚胺取代u - 4cr中的胺和氧成分。Ugi三组分反应(ju - 3cr)。这种方法提供了一种强大的单步途径,可以找到与n -杂环基序相连的肽段,这些基序在许多天然产物和药物化合物中被发现为核心骨架。与四组分类似物相比,ju - 3cr也提供了更好的非对映选择性。我们在这里调查了许多合成路线的重新设计,以有效地制备各种与肽主链相连的三、五、六和七元杂环化合物。此外,在以环亚胺为基础的Ugi反应中,α-酸性异氰化物或叠氮化物可以分别被正常异氰化物或酸取代,从而合成与恶唑或四唑相连的n -杂环,这具有重要的药学意义。本综述收录了截至2020年有关环亚胺类Ugi反应的所有研究文章,对化学家设计新的合成路线以合成天然产物和药物样化合物的单个和组合文库具有参考价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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