Neuroprotection of Tropical Fruit Juice Mixture via the Reduction of iNOS Expression and CRH Level in β-Amyloid-Induced Rats Model of Alzheimer’s Disease

Neuroprotection of Tropical Fruit Juice Mixture via the Reduction of iNOS Expression and CRH Level in β-Amyloid-Induced Rats Model of Alzheimer’s Disease

This study aimed to determine the effects of tropical fruit juice mixture (pomegranate, white guava, and Roselle) on biochemical, behavioral, and histopathological changes of β-amyloid- (Aβ-) induced rats. Formulation 8 (F8) of tropical fruit juice mixture was chosen for this present study due to it...

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Published in:Evidence-based complementary and alternative medicine Vol. 2020; no. 2020; pp. 1 - 11
Main Authors: Shahar, Suzana, Rajab, Nor Fadilah, Sharif, Razinah, Azmi, Norazrina, Ibrahim, Farah Wahida, Rosli, Hanisah, Abdul Malek, Siti Nur Aqilah, Mohd Rosli, Nur Hasnieza, Ahmad Munawar, Munirah, Ooi, Theng Choon, Haron, Hasnah
Format: Journal Article
Language:English
Published: Cairo, Egypt Hindawi Publishing Corporation 2020
Hindawi
Hindawi Limited
Subjects:
Alzheimer's disease
Animal cognition
Animal models
Antioxidants
Experiments
Fruit juices
Fruits
Hippocampus
Ibuprofen
Locomotor activity
Neurodegenerative diseases
Neuropathology
Neuroprotection
Neurotoxicity
Nitric oxide
Nitric-oxide synthase
Nonsteroidal anti-inflammatory drugs
Oxidative stress
Pattern recognition
Phenolic compounds
Polyphenols
Rodents
Superoxide dismutase
Supplements
β-Amyloid
United States > US
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Summary:This study aimed to determine the effects of tropical fruit juice mixture (pomegranate, white guava, and Roselle) on biochemical, behavioral, and histopathological changes of β-amyloid- (Aβ-) induced rats. Formulation 8 (F8) of tropical fruit juice mixture was chosen for this present study due to its high phenolic content and antioxidant capacity. Forty Wistar male rats were divided into five groups: dPBS (sham-operated control), dAβ (Aβ control), JPBS (F8 and PBS), JAβ (F8 and Aβ), and IBFAβ (ibuprofen and Aβ). F8 (5 ml/kg BW), and ibuprofen (10 ml/kg BW) was given orally daily for four weeks before the intracerebroventricular infusion of Aβ for two weeks. Histological analysis and neuronal count of hippocampus tissue in the Cornu Ammonis (CA1) region showed that supplementation with F8 was able to prevent Aβ-induced tissue damage and neuronal shrinkage. However, no significant difference in locomotor activity and novel object recognition (NOR) percentage was detected among different groups at day 7 and day 14 following Aβ infusion. Only effect of time differences (main effect of day) was observed at day 7 as compared to day 14, where reduction in locomotor activity and NOR percentage was observed in all groups, with F (1, 7) = 6.940, p<0.05 and F (1, 7) = 7.152, p<0.05, respectively. Besides, the MDA level of the JAβ group was significantly lower (p<0.01) than that of the dPBS group. However, no significant changes in SOD activity were detected among different groups. Significant reduction in plasma CRH level (p<0.05) and iNOS expression (p<0.01) in the brain was detected in the JAβ group as compared to the dAβ group. Hence, our current findings suggest that the tropical fruit juice mixture (F8) has the potential to protect the rats from Aβ-induced neurotoxicity in brain hippocampus tissue possibly via its antioxidant properties and the suppression of iNOS expression and CRH production.
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Academic Editor: Rocío De la Puerta
ISSN:1741-427X
1741-4288
DOI:10.1155/2020/5126457