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酶促肽和蛋白质溴化:BromoTrp 标签。

Enzymatic Peptide and Protein Bromination: The BromoTrp Tag.

机构信息

Organic and Bioorganic Chemistry, Department of Chemistry, Bielefeld University, Universitätsstraße 25, 33615, Bielefeld, Germany.

出版信息

Angew Chem Int Ed Engl. 2024 Jan 25;63(5):e202314961. doi: 10.1002/anie.202314961. Epub 2023 Dec 21.

Abstract

Bio-orthogonal reactions for modification of proteins and unprotected peptides are of high value in chemical biology. The combination of enzymatic halogenation with transition metal-catalyzed cross-coupling provides a feasible approach for the modification of proteins and unprotected peptides. By a semirational protein engineering approach, variants of the tryptophan 6-halogenase Thal were identified that enable efficient bromination of peptides with a C-terminal tryptophan residue. The substrate scope was explored using di-, tri-, and tetrapeptide arrays, leading to the identification of an optimized peptide tag we named BromoTrp tag. This tag was introduced into three model proteins. Preparative scale post-translational bromination was possible with only a single cultivation and purification step using the brominating E. coli coexpression system Brocoli. Palladium-catalyzed Suzuki-Miyaura cross-coupling of the bromoarene was achieved with Pd nanoparticle catalysts at 37 °C, highlighting the rich potential of this strategy for bio-orthogonal functionalization and conjugation.

摘要

生物正交反应在蛋白质和未保护肽的修饰中具有很高的价值。酶卤化与过渡金属催化交叉偶联的结合为蛋白质和未保护肽的修饰提供了一种可行的方法。通过半理性的蛋白质工程方法,鉴定了色氨酸 6-卤代酶 Thal 的变体,这些变体能够有效地对具有 C 末端色氨酸残基的肽进行溴化。使用二肽、三肽和四肽阵列探索了底物范围,确定了一个优化的肽标签,我们将其命名为 BromoTrp 标签。该标签被引入到三个模型蛋白中。使用 Brocoli 共表达系统,仅通过一次培养和纯化步骤即可进行制备规模的翻译后溴化,这突显了该策略在生物正交功能化和缀合方面的丰富潜力。

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