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点击化学法合成三氮唑及其药理学应用的最新进展:综述。

Recent advances in triazole synthesis via click chemistry and their pharmacological applications: A review.

机构信息

School of Pharmacy, National Forensic Sciences University, Gandhinagar, Gujarat, India.

School of Pharmacy, National Forensic Sciences University, Gandhinagar, Gujarat, India.

出版信息

Bioorg Med Chem Lett. 2024 Nov 1;112:129927. doi: 10.1016/j.bmcl.2024.129927. Epub 2024 Aug 15.

DOI:10.1016/j.bmcl.2024.129927
PMID:39153663
Abstract

Click chemistry is a flexible method featuring only the most feasible and efficient chemical reactions. The synthesis of 1,2,3-triazole from azides and terminal acetylenes using copper(I) as a catalyst is an extremely powerful reaction due to the extreme dependability, good selectivity, and biocompatibility of the starting materials. Triazole molecules are more than simple passive linkers; through hydrogen bonding and dipole interactions, they rapidly bind with biological targets. Its applications in drug development are expanding, ranging from target-oriented in situ chemistry and combinatorial mechanisms for lead generation to bioconjugation methods to study proteins and DNA. The click chemistry has frequently been used to speed up drug discovery and optimization processes in the past few years. The click chemistry reaction based on copper-catalyzed azide-alkyne cycloaddition (CuAAC) is a biochemical process with applications in medicinal chemistry and chemical biology. Thus, click reactions are an essential component of the toolkit for medicinal chemistry and help medicinal chemists overcome the barriers in chemical reactions, increase throughput, and improve the standards of compound libraries. The review highlights the recent advancements in the copper-catalyzed azide-alkyne cycloaddition (CuAAC) click chemistry approach for synthesizing biologically important triazole moieties with a greater emphasis on synthesis methodologies and pharmacological applications. Additionally, the triazole-based FDA-approved drugs are also discussed with their mode of action to highlight the importance of the click chemistry approach in synthesizing the bioactive triazole compounds.

摘要

点击化学是一种灵活的方法,仅采用最可行和高效的化学反应。使用铜 (I) 作为催化剂,由叠氮化物和末端炔烃合成 1,2,3-三唑是一种极其强大的反应,因为起始原料具有极高的可靠性、良好的选择性和生物相容性。三唑分子不仅仅是简单的被动连接子;通过氢键和偶极相互作用,它们能够快速与生物靶标结合。其在药物开发中的应用正在不断扩大,从基于靶标的原位化学和组合机制产生先导化合物到用于研究蛋白质和 DNA 的生物缀合方法。在过去的几年中,点击化学经常被用于加速药物发现和优化过程。基于铜催化的叠氮-炔环加成 (CuAAC) 的点击化学反应是一种在药物化学和化学生物学中有应用的生化过程。因此,点击反应是药物化学工具包的重要组成部分,有助于药物化学家克服化学反应中的障碍,提高产量,并提高化合物库的标准。本综述重点介绍了铜催化的叠氮-炔环加成 (CuAAC) 点击化学方法在合成具有重要生物学意义的三唑部分方面的最新进展,重点介绍了合成方法学和药理学应用。此外,还讨论了基于三唑的 FDA 批准药物及其作用模式,以强调点击化学方法在合成生物活性三唑化合物方面的重要性。

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