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基于光点击反应与钯介导的脱烯丙基反应串联的按需连接与释放策略

On-Demand Ligate and Release Strategy Based on Photoclick Reaction in Tandem with Pd-Mediated Deallylation.

作者信息

Loh Boon Shing, Pang Hanqing, Yong Soh Wah, Weng Cheng, Ang Wee Han

机构信息

Department of Chemistry, National University of Singapore, 3 Science Drive 3, Singapore, 117543.

NUS Graduate School of Integrative Sciences and Engineering, National University of Singapore, 28 Medical Drive, Singapore, 117456.

出版信息

Angew Chem Int Ed Engl. 2025 Jul 7;64(28):e202425479. doi: 10.1002/anie.202425479. Epub 2025 May 12.

Abstract

The development of chemoselective tools that can conjugate, modify, and decouple chemical groups from biomacromolecules has enabled the study of biological processes at increasing levels of fidelity. Until recently, these tools can either couple chemical entities to biomacromolecules or decouple them, but not both. A method that can perform these functions in distinct steps on demand would be highly useful. To that end, we devised a new-to-nature strategy by bringing together and modifying two biocompatible transformations. In this new strategy, ligation is accomplished via the photoclick reaction between an allenyl motif with 9,10-phenanthrenequinone which installs an allyl group at the site of conjugation. This allyl group can then be selectively utilized as a handle for phenolic release via Pd-mediated deallylation. As a proof of concept, we demonstrated its utility in the selective labeling and delabeling of model protein scaffolds and cellular matrix. This multifunctional method paves the way for a controllable "ligate and release" strategy that enables on-demand visualization of biological entities but with an in built release mechanism to restore their original state.

摘要

能够将化学基团与生物大分子进行共轭、修饰和解偶联的化学选择性工具的发展,使得人们能够在越来越高的保真度水平上研究生物过程。直到最近,这些工具要么能将化学实体与生物大分子偶联,要么能将它们解偶联,但不能同时做到这两点。一种能够根据需要在不同步骤中执行这些功能的方法将非常有用。为此,我们通过整合和修饰两种生物相容性转化方法,设计了一种全新的策略。在这种新策略中,连接是通过烯丙基基序与9,10-菲醌之间的光点击反应来完成的,该反应在共轭位点安装一个烯丙基。然后,这个烯丙基可以通过钯介导的脱烯丙基反应被选择性地用作酚类释放的手柄。作为概念验证,我们展示了其在模型蛋白支架和细胞基质的选择性标记和去标记中的应用。这种多功能方法为可控的“连接并释放”策略铺平了道路,该策略能够按需可视化生物实体,但具有内置的释放机制以恢复其原始状态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1057/12232882/ab0630cba80d/ANIE-64-e202425479-g002.jpg

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