Inhibitory Effect of Gedunin Analogue against the Plasmodium falciparum Dihydrofolate Reductase

V. A. Arazu, C. Nelson, U. O. Henrietta, Ayodele Akinwonmi, A. S. Ochepo, C. Samuel
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Abstract

Objective: Plasmodium parasites are the cause of malaria. Malaria victims get infected upon being bitten by female anopheles mosquito; which transmits the parasite to the victim. The P. falciparum and P. vivax are the most active disease-causing agents of all five malaria-causing species of Plasmodium. The anti-folate drugs which were the first class of clinical antimetabolites act by disrupting metabolic pathways in which the one-carbon moiety supplied by the B9 folate vitamins is a major requirement. Methods: Chemical structures of the anti-folate drugs which served as the experimental control ligands were downloaded from the PubChem database and saved as PDB files while the gedunin modification was achieved using the Marvin-Sketch software. Results: Molecular visualization of the polar interactions with amino acid residues of the Plasmodium falciparum dihydrofolate-reductase showed that all the control ligands interacted with similar residues contrary to the interaction of the gedunin modified ligand in the same binding pocket. Conclusion: Results from the molecular docking study showed that gedunin and its C=O of gedunin might be better antimalarial agents; having exhibited the best binding energies with a score of -9.5 and -9.0 Kcal/mol respectively.
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皂荚素类似物对恶性疟原虫二氢叶酸还原酶的抑制作用
目的:疟原虫是疟疾的病原。疟疾患者被雌性按蚊叮咬后感染疟疾;从而将寄生虫传染给受害者。恶性疟原虫和间日疟原虫是所有五种疟原虫中最活跃的致病因子。抗叶酸药物是一类临床抗代谢药物,通过破坏代谢途径起作用,其中B9叶酸维生素提供的单碳部分是主要需要的。方法:从PubChem数据库中下载作为实验对照配体的抗叶酸药物的化学结构,保存为PDB文件,并使用Marvin-Sketch软件进行皂素修饰。结果:恶性疟原虫二氢叶酸还原酶与氨基酸残基的极性相互作用的分子可视化显示,所有对照配体与相似残基的相互作用与相同结合袋中的皂荚素修饰配体的相互作用相反。结论:分子对接研究结果表明,芍药苷及其C=O可能是较好的抗疟药物;表现出最佳结合能,分别为-9.5和-9.0 Kcal/mol。
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