Investigating the functional dynamics of glyceraldehyde-3-phosphate dehydrogenase upon ligand binding at the putative allosteric binding sites

IF 3.3 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Biophysical chemistry Pub Date : 2025-02-21 DOI:10.1016/j.bpc.2025.107420

Merve Yuce, Ozge Kurkcuoglu

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Abstract

The glycolytic enzyme glyceraldehyde-3-phosphate dehydrogenase (GAPDH) is an attractive target to combat infection-related diseases as antibiotic resistance poses a global threat. Here, we investigated the functional dynamics of methicillin-resistant S. aureus GAPDH (SaGAPDH) in apo-form and with ligands bound at two distinct potential allosteric binding sites in its tunnel-like region. AutoDock Vina was used for flexible docking with a library of 2447 FDA-approved drugs. After the interaction analysis and chemical fragment clustering, 5 compounds mutual to both sites were selected and subjected to independent 3 × 500 ns-long molecular dynamics (MD) simulations coupled with Molecular Mechanics Generalized Born Surface Area calculations to estimate their binding free energies. The ligand-protein dynamics pointed to either an increase or a decrease in the solvent accessibility of the co-factor NAD⁺ binding site as compared to apo-dynamics without an apparent change in residue fluctuations. Furthermore, dihedral angles of the co-factor binding site residues, particularly R12 and N316 changed upon ligand binding to the tunnel-like region. Residue network models based on the MD trajectories for each system revealed potential allosteric communication pathways linking putative allosteric binding sites to the co-factor binding sites. Favorable interactions between the ligands and the previously suggested hub residues T49-R53, E204 (S-loop) and/or Y180 seemed to affect the solvent accessibility of the binding sites that can either facilitate or prevent NAD⁺ binding. Dynamic coupling of NAD⁺ binding sites through correlated residue fluctuations was consistent in all investigated systems, revealing how cooperativity between the functional sites can be maintained by SaGAPDH. All findings suggested hit compounds and the putative allosteric binding sites to change the NAD⁺ binding site dynamics that should be further evaluated by in vitro studies to assess their antibacterial activities.

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在假定的变构结合位点研究配体结合时甘油醛-3-磷酸脱氢酶的功能动力学

糖酵解酶甘油醛-3-磷酸脱氢酶（GAPDH）是对抗感染相关疾病的一个有吸引力的靶标，因为抗生素耐药性构成了全球威胁。在这里，我们研究了耐甲氧西林金黄色葡萄球菌GAPDH （SaGAPDH）以载虫形式和在其隧道状区域的两个不同的潜在变构结合位点结合的配体的功能动力学。AutoDock Vina用于与2447种fda批准的药物库进行灵活对接。在相互作用分析和化学片段聚类之后，选择了5个与两个位点相互作用的化合物，并进行了独立的3 × 500 ns长的分子动力学（MD）模拟和分子力学广义Born表面积计算，以估计它们的结合自由能。配体-蛋白质动力学表明，与载脂蛋白动力学相比，辅助因子NAD+结合位点的溶剂可及性增加或减少，而残基波动没有明显变化。此外，辅助因子结合位点残基，特别是R12和N316的二面角在配体与隧道状区域结合时发生了变化。基于每个系统MD轨迹的残基网络模型揭示了连接假定的变构结合位点和辅因子结合位点的潜在变构通信途径。配体与先前提出的中心残基T49-R53、E204 （S-loop）和/或Y180之间的良好相互作用似乎影响了结合位点的溶剂亲和性，从而促进或阻止NAD+的结合。在所有被研究的系统中，NAD+结合位点通过相关残基波动的动态耦合是一致的，这揭示了SaGAPDH如何维持功能位点之间的协同性。所有研究结果表明，击中化合物和假定的变构结合位点改变了NAD+结合位点的动力学，需要进一步通过体外研究来评估其抗菌活性。

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来源期刊

Biophysical chemistry 生物-生化与分子生物学

CiteScore

6.10

自引率

10.50%

发文量

121

审稿时长

20 days

期刊介绍： Biophysical Chemistry publishes original work and reviews in the areas of chemistry and physics directly impacting biological phenomena. Quantitative analysis of the properties of biological macromolecules, biologically active molecules, macromolecular assemblies and cell components in terms of kinetics, thermodynamics, spatio-temporal organization, NMR and X-ray structural biology, as well as single-molecule detection represent a major focus of the journal. Theoretical and computational treatments of biomacromolecular systems, macromolecular interactions, regulatory control and systems biology are also of interest to the journal.