Exploring novel inhibitors for Babesia bigemina lactate dehydrogenase: a computational structural biology perspective.

IF 1.8 3区医学 Q2 PARASITOLOGY

Parasitology Research Pub Date : 2025-01-07 DOI:10.1007/s00436-024-08433-5

Safiye Merve Bostancioglu, Ozal Mutlu

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引用次数: 0

Abstract

Babesia bigemina is an apicomplexan parasite responsible for causing "Texas fever" in bovines. Current treatments for bovine babesiosis are hindered by several limitations, including toxicity, insufficient efficacy in eliminating the parasite, and the potential for resistance development. A promising approach to overcome these challenges is the identification of compounds that specifically target essential metabolic pathways unique to the parasite. One such target is lactate dehydrogenase (LDH), a critical enzyme involved in the regulation of anaerobic glycolysis. Notably, Babesia bigemina LDH (BbigLDH) exhibits a five-amino acid insertion in the active site, a feature that differentiates it from the host's LDH. This structural divergence makes apicomplexan LDH an attractive and potentially selective drug target for therapeutic intervention. In this study, a structure-based drug discovery approach was implemented to find novel inhibitor candidates. Potential candidates were identified using a virtual screening workflow. The compounds with favorable docking scores were filtered using the QM-polarized ligand docking and induced fit docking methods. As a result, 20 novel compounds were identified that bind to the active site of BbigLDH but show low affinity to the host LDHs. Molecular dynamics simulations of the complexes (8.8 µs in total) were performed, and binding free energies were calculated. As a result, protein structures containing compounds C9, C16 and C18 maintained their stability throughout 1 µs simulations with low binding free energies and conserved interactions with known catalytic residues. Therefore, these three compounds deserve further investigation to better understand their mode of action and therapeutic potential for babesiosis. The results of this study elucidate the structural features of the BbigLDH enzyme and provide novel LDH binders that may pave the way for further research into the development of parasite-specific LDH inhibitors.

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探索新的巴贝斯虫乳酸脱氢酶抑制剂：计算结构生物学的观点。

双臀巴贝斯虫是一种顶端复合体寄生虫，可引起牛的“德克萨斯热”。目前对牛巴贝斯虫病的治疗受到几个限制的阻碍，包括毒性、消除寄生虫的效力不足以及产生耐药性的可能性。克服这些挑战的一个有希望的方法是鉴定专门针对寄生虫特有的基本代谢途径的化合物。其中一个目标是乳酸脱氢酶（LDH），这是一种参与调节厌氧糖酵解的关键酶。值得注意的是，双双巴贝斯虫LDH （BbigLDH）在活性位点上有一个5个氨基酸的插入，这是它与宿主LDH区别的一个特征。这种结构上的差异使得顶复合体LDH成为治疗干预的一个有吸引力和潜在选择性的药物靶点。在本研究中，采用基于结构的药物发现方法来寻找新的候选抑制剂。潜在的候选人是通过虚拟筛选工作流程确定的。采用qm极化配体对接和诱导拟合对接的方法筛选匹配得分较高的化合物。结果，鉴定出20种与BbigLDH活性位点结合但与宿主ldh亲和力低的新化合物。对配合物进行了分子动力学模拟（共8.8µs），并计算了结合自由能。结果表明，含化合物C9、C16和C18的蛋白质结构在1µs模拟时间内保持稳定，结合自由能低，与已知催化残基的相互作用守恒。因此，这三种化合物值得进一步研究，以更好地了解它们对巴贝斯虫病的作用模式和治疗潜力。本研究的结果阐明了BbigLDH酶的结构特征，并提供了新的LDH结合物，可能为进一步研究寄生虫特异性LDH抑制剂的开发铺平道路。

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

Parasitology Research 医学-寄生虫学

CiteScore

4.10

自引率

5.00%

发文量

346

审稿时长

6 months

期刊介绍： The journal Parasitology Research covers the latest developments in parasitology across a variety of disciplines, including biology, medicine and veterinary medicine. Among many topics discussed are chemotherapy and control of parasitic disease, and the relationship of host and parasite. Other coverage includes: Protozoology, Helminthology, Entomology; Morphology (incl. Pathomorphology, Ultrastructure); Biochemistry, Physiology including Pathophysiology; Parasite-Host-Relationships including Immunology and Host Specificity; life history, ecology and epidemiology; and Diagnosis, Chemotherapy and Control of Parasitic Diseases.