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异戊烯化肽、蛋白质和DNA的三唑啉二酮修饰:迈向生物分子的单位点多标记方法

Triazolinedione Modification of Prenylated Peptides, Proteins, and DNA: Toward a Single-Site Multilabeling Approach for Biomolecules.

作者信息

Tack Laure, Manicardi Alex, Leszczynska Grazyna, Dziergowska Agnieszka, Ghielmetti Alyssa, Unal Kamil, Decoene Klaas, Winne Johan, Madder Annemieke

机构信息

Department of Organic and Macromolecular Chemistry, Ghent University, Krijgslaan 281-S4, 9000 Gent, Belgium.

Institute of Organic Chemistry, Lodz University of Technology, Zeromskiego 116, 90-924 Lodz,Poland.

出版信息

ACS Omega. 2025 May 18;10(21):21187-21194. doi: 10.1021/acsomega.4c10125. eCollection 2025 Jun 3.

Abstract

In efforts to shed light on the complexity of biological processes, attaching several or different payloads onto a biomolecular target of interest has become an interesting tool within the field of bioconjugation. Herein, we report on the exploitation of prenylated (bio)-molecules in a 1,2,4-triazole-3,5-(4)-dione-based labeling strategy to develop a two-step single-site multiple labeling methodology that allows the introduction of up to three identical or different property-enhancing moieties. The methodology was first demonstrated on the small molecule targets farnesol and S-geranyl-2-thiouridine to be then applied to multi-(functional) labeling of amino acids and peptides. We further demonstrate the usefulness of this approach to achieve branched lipidation of peptides, a strategy recently receiving more attention for enhanced cellular membrane localization and vaccine development. In addition, proof-of-concept experiments were performed involving single-site multiple labeling of large biomolecules such as farnesylated proteins and geranylated DNA.

摘要

为了阐明生物过程的复杂性,将几种或不同的有效载荷附着到感兴趣的生物分子靶标上已成为生物共轭领域中一种有趣的工具。在此,我们报告了基于1,2,4-三唑-3,5-(4)-二酮的标记策略中异戊烯基化(生物)分子的利用情况,以开发一种两步单位点多重标记方法,该方法允许引入多达三个相同或不同的性质增强基团。该方法首先在小分子靶标法尼醇和S-香叶基-2-硫代尿苷上得到验证,随后应用于氨基酸和肽的多(功能)标记。我们进一步证明了这种方法在实现肽的分支脂化方面的有用性,这是一种最近因增强细胞膜定位和疫苗开发而受到更多关注的策略。此外,还进行了概念验证实验,涉及对法尼醇化蛋白和香叶基化DNA等大型生物分子的单位点多重标记。

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