Giardiasis, which is caused by Giardia lamblia infection, is a relevant cause of morbidity and mortality worldwide. Because no vaccines are currently available to treat giardiasis, chemotherapeutic drugs are the main options for controlling infection. Evidence has shown that the nitro drug nitazoxanide (NTZ) is a commonly prescribed treatment for giardiasis; however, the mechanisms underlying NTZ's antigiardial activity are not well-understood. Herein, we identified the glucose-6-phosphate::6-phosphogluconate dehydrogenase (GlG6PD::6PGL) fused enzyme as a nitazoxanide target, as NTZ behaves as a GlG6PD::6PGL catalytic inhibitor. Furthermore, fluorescence assays suggest alterations in the stability of GlG6PD::6PGL protein, whereas the results indicate a loss of catalytic activity due to conformational and folding changes. Molecular docking and dynamic simulation studies suggest a model of NTZ binding on the active site of the G6PD domain and near the structural NADP(+) binding site. The findings of this study provide a novel mechanistic basis and strategy for the antigiardial activity of the NTZ drug.
Nitazoxanide Inhibits the Bifunctional Enzyme GlG6PD::6PGL of Giardia lamblia: Biochemical and In Silico Characterization of a New Druggable Target.
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作者:MartÃnez-Rosas VÃctor, Hernández-Ochoa Beatriz, Morales-Luna Laura, Ortega-Cuellar Daniel, González-Valdez Abigail, Arreguin-Espinosa Roberto, Rufino-González Yadira, Calderón-Jaimes Ernesto, Castillo-RodrÃguez Rosa Angélica, Wong-Baeza Carlos, Baeza-RamÃrez Isabel, Pérez de la Cruz Verónica, Vidal-Limón Abraham, Gómez-Manzo Saúl
| 期刊: | International Journal of Molecular Sciences | 影响因子: | 4.900 |
| 时间: | 2023 | 起止号: | 2023 Jul 15; 24(14):11516 |
| doi: | 10.3390/ijms241411516 | ||
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