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二维等温热滴定技术在阐明.乙酰氨基葡萄糖/乙酰胞壁酸激酶(AmgK)的酶促机制中的应用

Application of 2D-ITC to the Elucidation of the Enzymatic Mechanism of -Acetylmuramic Acid/-Acetylglucosamine Kinase (AmgK) from .

机构信息

Department of Chemistry and Biochemistry, University of Notre Dame, Notre Dame, Indiana 46556, United States.

出版信息

Biochemistry. 2023 Apr 18;62(8):1337-1341. doi: 10.1021/acs.biochem.3c00090. Epub 2023 Mar 27.

DOI:10.1021/acs.biochem.3c00090
PMID:36971350
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11677264/
Abstract

Characterization of the turnover mechanism of bisubstrate enzymes is a tedious task. Molecular tools for studying the enzymatic mechanism are not readily available for all enzymes (e.g., radioactive substrates, substrate-competitive inhibitors, etc.). Wang and Mittermaier recently introduced two-dimensional isothermal titration calorimetry (2D-ITC) for determining the bisubstrate mechanism at high resolution while simultaneously quantifying the kinetic parameters for substrate turnover in a single reporter-free experiment. We demonstrate the utility of 2D-ITC in studying -acetylmuramic acid/-acetylglucosamine kinase (AmgK) from . This enzyme is involved in cytoplasmic cell-wall-recycling events as a step in the peptidoglycan salvage pathway. Furthermore, AmgK phosphorylates -acetylglucosamine and -acetylmuramic acid, linking the recycling events to cell-wall synthesis. We document in a 2D-ITC experiment that AmgK follows an ordered-sequential mechanism, where ATP binds first and ADP is released last. We also show that classical enzyme kinetic methods support the results of 2D-ITC and that 2D-ITC could overcome the shortcomings of these classical methodologies. We provide evidence for inhibition of AmgK by the catalytic product ADP, but not by the phosphorylated sugar product. These results provide a full kinetic characterization of the bacterial kinase AmgK. This work highlights 2D-ITC as a versatile tool for the mechanistic evaluation of bisubstrate enzymes, as an alternative for classical methods.

摘要

双底物酶的周转率机制的特征是一项繁琐的任务。用于研究酶机制的分子工具并非对所有酶都可用(例如,放射性底物、底物竞争性抑制剂等)。Wang 和 Mittermaier 最近引入了二维等温滴定量热法(2D-ITC),用于在单个无报告物实验中同时以高分辨率确定双底物机制并定量测定底物周转率的动力学参数。我们展示了 2D-ITC 在研究. 中的 -乙酰氨基葡萄糖酸/-乙酰葡萄糖胺激酶(AmgK)的应用。该酶作为肽聚糖回收途径中的一步,参与细胞质细胞壁回收事件。此外,AmgK 磷酸化 -乙酰葡萄糖胺和 -乙酰氨基葡萄糖酸,将回收事件与细胞壁合成联系起来。我们在 2D-ITC 实验中记录到 AmgK 遵循有序顺序机制,其中首先结合 ATP,最后释放 ADP。我们还表明,经典的酶动力学方法支持 2D-ITC 的结果,并且 2D-ITC 可以克服这些经典方法的缺点。我们提供了 AmgK 被催化产物 ADP 而不是磷酸化糖产物抑制的证据。这些结果提供了细菌激酶 AmgK 的完整动力学特征。这项工作突出了 2D-ITC 作为双底物酶的机制评估的多功能工具,是经典方法的替代方法。

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