Ferulic Acid Modulates Dysfunctional Metabolic Pathways and Purinergic Activities, While Stalling Redox Imbalance and Cholinergic Activities in Oxidative Brain Injury

被引:0
|
作者
Veronica F. Salau
Ochuko L. Erukainure
Collins U. Ibeji
Tosin A. Olasehinde
Neil A. Koorbanally
Md. Shahidul Islam
机构
[1] University of KwaZulu-Natal,Department of Biochemistry
[2] Veritas University,Department of Biochemistry
[3] Federal Institute of Industrial Research,Nutrition and Toxicology Division
[4] University of Nigeria,Department of Pure and Industrial Chemistry, Faculty of Physical Sciences
[5] University of Fort Hare,Department of Biochemistry and Microbiology
[6] University of KwaZulu-Natal,School of Chemistry and Physics
来源
Neurotoxicity Research | 2020年 / 37卷
关键词
Antioxidative; Ferulic acid; Iron toxicity; Neurodegenerative disease; Oxidative stress;
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学科分类号
摘要
The neuroprotective activities of phenolics have been demonstrated in several studies, with their antioxidant properties playing an influential role. In this study, the therapeutic effect of ferulic acid was investigated on oxidative stress, purinergic and cholinergic enzymatic activities, and dysregulated metabolic pathways in oxidative brain injury. Ferulic acid significantly elevated the reduced glutathione (GSH) level, superoxide dismutase and catalase activities, and concomitantly depleted malondialdehyde and nitric oxide level. It also inhibited the activities of acetylcholinesterase and butyrylcholinesterase, and increased the activities of ATPase. LC-MS analysis of the metabolites revealed restoration of most depleted metabolites, with concomitant generation of dihydroferulic acid 4-O-glucuronide, diadenosine heptaphosphate, cis-4-decenoic acid, ganglioside GT3 (d18:0/23:0), phosphatidylinositol-3,4,5-trisphosphate, and phosphoribosyl-ATP on treatment with ferulic acid. Pathway analysis of the identified metabolites revealed reactivation of oxidative-inactivated pathways, with concomitant activation of histidine and inositol phosphate metabolic pathways. There was no cytotoxicity on incubation of ferulic acid with HT22 cells. Molecular docking studies revealed a high affinity for acetylcholinesterase, with a binding energy of − 7.4 kcal/mol. In silico simulation analysis predicted permeability of ferulic acid across blood brain barrier (BBB) and an oral LD50 calculated value of 1772 mg/kg, with a toxicity class of 4. These results indicate the antioxidative and protective effects of ferulic acid in oxidative brain injury.
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页码:944 / 955
页数:11
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