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天冬酰胺内肽酶介导的蛋白 C 末端肼解用于生物缀合物的合成。

Asparaginyl Endopeptidase-Mediated Protein C-Terminal Hydrazinolysis for the Synthesis of Bioconjugates.

机构信息

School of Biological Science, Nanyang Technological University, 60 Nanyang Drive, 637551 Singapore.

出版信息

Bioconjug Chem. 2022 Jan 19;33(1):238-247. doi: 10.1021/acs.bioconjchem.1c00551. Epub 2022 Jan 5.

Abstract

Asparaginyl endopeptidases (AEPs) are cysteinyl enzymes naturally catalyzing the hydrolysis and transpeptidation reactions at Asx-Xaa bonds. These reactions go by a common acyl-enzyme thioester intermediate, which is either attacked by water (for a protease-AEP) or by a peptidic amine nucleophile (for a ligase-AEP) to form the respective hydrolysis or aminolysis product. Herein, we show that hydrazine and hydroxylamine, two α-effect nucleophiles, are capable of resolving the thioester intermediate to yield peptide and protein products containing a C-terminal hydrazide and hydroxamic acid functionality, respectively. The hydrazinolysis reaction exhibits very high efficiency and can be completed in minutes at a low enzyme-to-substrate ratio. We further show the utility of the so-formed asparaginyl hydrazide in native chemical ligation and hydrazone conjugation. Using an EGFR-targeting affibody as a model protein, we have showcased our methodology in the preparation of a number of protein ligation or conjugation products, which are decorated with various functional moieties. The Z affibody-doxorubicin conjugate shows high selective binding and cytotoxicity toward the EGFR-positive A431 cells. Our results demonstrate the advantages of AEP-mediated protein hydrazinolysis as a simple and straightforward strategy for the precision manufacturing of protein bioconjugates.

摘要

天冬酰胺内肽酶(AEPs)是一类天然存在的半胱氨酸酶,能够催化 Asx-Xaa 键处的水解和转肽反应。这些反应通过共同的酰基-酶硫酯中间体进行,该中间体可被水分子(用于蛋白酶-AEP)或肽性胺亲核试剂(用于连接酶-AEP)进攻,从而形成相应的水解或氨解产物。在此,我们证明了肼和羟胺这两种 α-效应亲核试剂能够将硫酯中间体分解,分别得到含有 C 末端腙和偕脒酸官能团的肽和蛋白质产物。肼解反应具有很高的效率,在低酶与底物比的情况下,可在数分钟内完成。我们进一步展示了形成的天冬酰肼在天然化学连接和腙键连接中的应用。以一种 EGFR 靶向的亲和体作为模型蛋白,我们在一系列蛋白连接或偶联产物的制备中展示了我们的方法,这些产物都带有各种功能基团。Z 亲和体-阿霉素缀合物对 EGFR 阳性的 A431 细胞表现出高选择性结合和细胞毒性。我们的结果证明了 AEP 介导的蛋白肼解作为一种用于精确制造蛋白生物缀合物的简单直接的策略具有优势。

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