IspE kinase as an anti-infective target: Role of a hydrophobic pocket in inhibitor binding

IF 4.4 2区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Structure Pub Date : 2024-11-06 DOI:10.1016/j.str.2024.10.009

Rawia Hamid, Danica J. Walsh, Eleonora Diamanti, Diana Aguilar, Antoine Lacour, Mostafa M. Hamed, Anna K.H. Hirsch

引用次数: 0

Abstract

Enzymes of the methylerythritol phosphate (MEP) pathway are potential targets for antimicrobial drug discovery. Here, we focus on 4-diphosphocytidyl-2-C-methyl-D-erythritol (IspE) kinase from the MEP pathway. We use biochemical and structural biology methods to investigate homologs from pathogenic microorganisms; Escherichia coli, Klebsiella pneumoniae, and Acinetobacter baumannii. We determined the X-ray crystal structures of IspE-inhibitor complexes and studied inhibitors’ binding modes targeting the substrate pocket. The experimental results indicate the need for distinct inhibitor strategies due to structural differences among IspE homologs, particularly for A. baumannii IspE, which displays a unique inhibitory profile due to a tighter hydrophobic subpocket in the substrate binding site. This study enhances our understanding of the MEP enzymes and sets the stage for structure-based drug design of selective inhibitors to combat pathogenic microorganisms.

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作为抗感染靶标的 IspE 激酶：疏水袋在抑制剂结合中的作用

磷酸赤藓醇甲酯（MEP）途径的酶是抗菌药物发现的潜在靶标。在这里，我们重点研究 MEP 途径中的 4-二磷酸胞嘧啶-2-C-甲基-D-赤藓醇（IspE）激酶。我们使用生物化学和结构生物学方法研究了病原微生物（大肠埃希菌、肺炎克雷伯氏菌和鲍曼不动杆菌）中的同源物。我们测定了 IspE 抑制剂复合物的 X 射线晶体结构，并研究了抑制剂针对底物口袋的结合模式。实验结果表明，由于 IspE 同源物之间的结构差异，需要采用不同的抑制剂策略，尤其是鲍曼不动杆菌 IspE，它的底物结合位点有一个更紧密的疏水亚口袋，因而显示出独特的抑制作用。这项研究加深了我们对 MEP 酶的了解，并为基于结构的选择性抑制剂药物设计创造了条件，可用于抗击病原微生物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Structure 生物-生化与分子生物学

CiteScore

8.90

自引率

1.80%

发文量

155

审稿时长

3-8 weeks

期刊介绍： Structure aims to publish papers of exceptional interest in the field of structural biology. The journal strives to be essential reading for structural biologists, as well as biologists and biochemists that are interested in macromolecular structure and function. Structure strongly encourages the submission of manuscripts that present structural and molecular insights into biological function and mechanism. Other reports that address fundamental questions in structural biology, such as structure-based examinations of protein evolution, folding, and/or design, will also be considered. We will consider the application of any method, experimental or computational, at high or low resolution, to conduct structural investigations, as long as the method is appropriate for the biological, functional, and mechanistic question(s) being addressed. Likewise, reports describing single-molecule analysis of biological mechanisms are welcome. In general, the editors encourage submission of experimental structural studies that are enriched by an analysis of structure-activity relationships and will not consider studies that solely report structural information unless the structure or analysis is of exceptional and broad interest. Studies reporting only homology models, de novo models, or molecular dynamics simulations are also discouraged unless the models are informed by or validated by novel experimental data; rationalization of a large body of existing experimental evidence and making testable predictions based on a model or simulation is often not considered sufficient.