d -2-羟戊二酸脱氢酶对α-羟基酸的氧化作用。

IF 3.8 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Archives of biochemistry and biophysics Pub Date : 2025-02-22 DOI:10.1016/j.abb.2025.110355

Joanna Afokai Quaye , Bilkis Mehrin Moni , Jessica Eyram Kugblenu , Giovanni Gadda

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引用次数: 0

摘要

α-羟基酸是天然存在的有机分子，具有各种医疗和工业用途。然而，一些α-羟基酸，如d -2-羟基戊二酸酯（D2HG），与癌症和神经代谢疾病如D2HG酸尿有关。对D2HG氧化酶d -2-羟戊二酸脱氢酶（D2HGDH）的研究主要集中在D2HG作为生物传感器的使用和应用。最近一项对细菌中stutzeri假单胞菌和铜绿假单胞菌D2HGDH同源物的基因敲除研究发现，D2HGDH通过驱动l -丝氨酸的生物合成对细菌的生存至关重要。因此，D2HGDH是抗多重耐药铜绿假单胞菌的良好候选治疗靶点。然而，关于D2HGDH的催化机制还没有达成共识，而且一些D2HGDH同源物的结构特性还没有被表征，这是治疗设计的两个关键特征。铜绿假单胞菌D2HGDH是研究最广泛的D2HGDH同源物，它正在成为D2HGDH和活性位点含金属的黄蛋白的典范。在这篇综述中，我们利用AlphaFold 3分析了12个物种中所有已发表的D2HGDH同源物的结构，并强调了所有D2HGDH同源物的完全保守结构和活性位点拓扑结构。此外，进化和功能研究结合酶活性分析表明，原核生物和真核生物的D2HGDH同源物，从两个不同的祖先分化出来，可能有不同的进化，专门从事α-羟基酸催化。此外，本综述确定了所有D2HGDH同源物都是金属和FAD依赖酶，它们在催化过程中使用金属触发的FAD还原。阐明D2HGDH的作用机制，除了将D2HGDH同源物应用于生物传感器外，还可以设计出针对这些酶的抗生素，作为潜在的治疗药物，以对抗铜绿假单胞菌等致病菌。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Oxidation of α-hydroxy acids by D-2-hydroxyglutarate dehydrogenase enzymes

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Oxidation of α-hydroxy acids by D-2-hydroxyglutarate dehydrogenase enzymes

α-Hydroxy acids are naturally occurring organic molecules with various medical and industrial applications. However, some α-hydroxy acids, like D-2-hydroxyglutarate (D2HG), have been implicated in cancers and neurometabolic disorders such as D2HG aciduria. Several studies on the D2HG oxidizing enzyme D-2-hydroxyglutarate dehydrogenase (D2HGDH) from various eukaryotic and prokaryotic sources focus on the use and application of the enzyme as biosensors for detecting D2HG. A recent gene knockout study on the bacterial D2HGDH homologs from Pseudomonas stutzeri and Pseudomonas aeruginosa identified the D2HGDH to be essential for bacterial survival by driving l-serine biosynthesis. Thus, D2HGDH is a good candidate for a therapeutic target against the multidrug-resistant P. aeruginosa. However, there is no consensus on the D2HGDH catalytic mechanism, and several D2HGDH homologs have not been characterized in their structural properties, which are two crucial features for therapeutic design. P. aeruginosa D2HGDH, the most extensively studied D2HGDH homolog, is emerging as a paradigm for D2HGDH and flavoproteins with metal ions in their active site. In this review, we have explored the structures of all published D2HGDH homologs from 12 species using AlphaFold 3 and highlighted the fully conserved structure and active site topologies of all D2HGDH homologs. Additionally, evolutionary and functional studies coupled with analyses of enzymatic activities reveal that prokaryotic and eukaryotic D2HGDH homologs, diverging from two distinct ancestors, may have differentially evolved to specialize in their α-hydroxy acid catalysis. Additionally, this review identifies all D2HGDH homologs as metal and FAD-dependent enzymes that employ a metal-triggered FAD reduction in their catalysis. Elucidation of the D2HGDH mechanism will allow designing antibiotics that target these enzymes as potential therapeutics against pathogenic bacteria like P. aeruginosa in addition to the application of D2HGDH homologs as biosensors.

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来源期刊

Archives of biochemistry and biophysics 生物-生化与分子生物学

CiteScore

7.40

自引率

0.00%

发文量

245

审稿时长

26 days

期刊介绍： Archives of Biochemistry and Biophysics publishes quality original articles and reviews in the developing areas of biochemistry and biophysics. Research Areas Include: • Enzyme and protein structure, function, regulation. Folding, turnover, and post-translational processing • Biological oxidations, free radical reactions, redox signaling, oxygenases, P450 reactions • Signal transduction, receptors, membrane transport, intracellular signals. Cellular and integrated metabolism.