Neurotherapeutic impact of vanillic acid and ibudilast on the cuprizone model of multiple sclerosis

Multiple sclerosis (MS) affects 2.8 million people worldwide. Although the cause is unknown, various risk factors might be involved. MS involves the immune system attacking the central nervous system’s myelin sheath, leading to neuron damage. This study used a cuprizone (CPZ)-intoxicated mouse model...

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Bibliographic Details
Published in:Frontiers in molecular neuroscience 2025-01, Vol.17
Main Authors: Alderbi, Rasha M., Alam, Mohammad Z., Alghamdi, Badrah S., Alsufiani, Hadeil M., Abd El-Aziz, Gamal S., Omar, Ulfat M., Al-Ghamdi, Maryam A.
Format: Article
Language:English
Subjects:
Acids
anti-inflammatory
Brain research
Central nervous system
Cuprizone
cuprizone model
Demyelination
Disease prevention
FDA approval
ibudilast
Immune system
Inflammation
Lymphocytes
Multiple sclerosis
Myelin
Myelination
Phenolic acids
Risk factors
Vanillic acid
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Summary:Multiple sclerosis (MS) affects 2.8 million people worldwide. Although the cause is unknown, various risk factors might be involved. MS involves the immune system attacking the central nervous system’s myelin sheath, leading to neuron damage. This study used a cuprizone (CPZ)-intoxicated mouse model to simulate MS’s demyelination/remyelination process. It evaluated the molecular, histological, and behavioral effects of vanillic acid (VA), a natural phenolic acid, alone and with Ibudilast (IBD), a clinically tested MS medication. Mice were divided into a control group (regular chow) and a CPZ group (0.3% cuprizone chow for 5 consecutive weeks). During remyelination, the CPZ group was split into four groups: no therapy, 10 mg/kg of IBD, 30 mg/kg of VA, and combined, each treated for 4 weeks. Behavioral, biochemical, molecular, and histopathological tests occurred in the 5 th week (demyelination), 7 th (early remyelination), and 9 th (late remyelination). Cognitive assessments were at weeks 5 and 9. VA enhanced motor, coordination, and cognitive impairments in CPZ-intoxicated mice and improved histopathological, molecular, and biochemical features during early remyelination. IBD improved behavioral abnormalities across all tests, but combined therapy showed no significant difference from single therapies. Further investigations are necessary to understand VA’s mechanisms and potential as an MS treatment.
ISSN:1662-5099
1662-5099
DOI:10.3389/fnmol.2024.1503396