Title of article :
Neuroprotective properties of Melissa officinalisafter hypoxic-ischemic injury both in vitro and in vivo
Author/Authors :
Bayat, Mohammad tehran university of medical sciences tums - School of Medicine - Department of Anatomy, تهران, ايران , Azami Tameh, Abolfazl kashan university of medical sciences and health services - Anatomical Sciences Research Center, ايران , Ghahremani, Mohammad Hossein tehran university of medical sciences tums - School of Pharmacy - Department of Toxicology-Pharmacology, تهران, ايران , Akbari, Mohammad tehran university of medical sciences tums - School of Medicine - Department of Anatomy, تهران, ايران , Ejtemaei Mehr, Shahram tehran university of medical sciences tums - School of Medicine - Department of Pharmacology, تهران, ايران , Khanavi, Mahnaz tehran university of medical sciences tums - School of Pharmacy - Department of Pharmacognosy, تهران, ايران , Hassanzadeh, Gholamreza tehran university of medical sciences tums - School of Advanced Medical Technology, School of Medicine - Department of Neuroscience, Department of Anatomy, تهران, ايران
From page :
1
To page :
10
Abstract :
Background: Brain ischemia initiates several metabolic events leading to neuronal death. These events mediate large amount of damage that arises after some neurodegenerative disorders as well as transient brain ischemia. Melissa officinalis is considered as a helpful herbal plant in the prevention of various neurological diseases like Alzheimer that is related with oxidative stress. Methods: We examined the effect of Melissa officinalis on hypoxia induced neuronal death in a cortical neuronal culture system as in vitro model and transient hippocampal ischemia as in vivo model. Transient hippocampal ischemia was induced in male rats by tow vessel-occlusion for 20 min. After reperfusion, the histopathological changes and the levels inflammation, oxidative stress status, and caspase-3 activity in hippocampus were measured. Results: Cytotoxicity assays showed a significant protection of a 10 μg/ml dose of Melissa against hypoxia in cultured neurons which was confirmed by a conventional staining (P 0.05). Melissa treatment decrease caspase3 activity (P 0.05) and TUNEL-positive cells significantly (P 0.01). Melissa oil has also inhibited malon dialdehyde level and attenuated decrease of Antioxidant Capacity in the hippocampus. Pro-inflammatory cytokines TNF-α, IL-1β and HIF-1α mRNA levels were highly increased after ischemia and treatment with Melissa significantly suppressed HIF-1α gene expression (P 0.05). Discussion: Results showed that Melissa officinalis could be considered as a protective agent in various neurological diseases associated with ischemic brain injury.
Keywords :
Melissa officinalis , Ischemia , Cell death , Hippocampus , Neuron
Journal title :
Daru Journal of Pharmaceutical Sciences
Journal title :
Daru Journal of Pharmaceutical Sciences
Record number :
2634716
Link To Document :
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