PREVENTION OF GLUTAMATE ACCUMULATION AND UPREGULATION OF PHOSPHO-AKT MAY ACCOUNT FOR NEUROPROTECTION AFFORDED BY BERGAMOT ESSENTIAL OIL AGAINST BRAIN INJURY INDUCED BY FOCAL CEREBRAL ISCHEMIA IN RAT

被引:29
作者
Amantea, Diana [1 ,2 ]
Fratto, Vincenzo [3 ]
Maida, Simona [3 ]
Rotiroti, Domenicantonio [3 ]
Ragusa, Salvatore [3 ]
Nappi, Giuseppe [4 ,5 ]
Bagetta, Giacinto [1 ,2 ]
Corasaniti, Maria Tiziona [3 ]
机构
[1] Univ Calabria, UCADH, Dept Pharmacobiol, I-87036 Cosenza, Italy
[2] Univ Calabria, UCADH, Ctr Neuropharmacol Normal & Pathol Neuronal Plast, I-87036 Cosenza, Italy
[3] Magna Graecia Univ Catanzaro, Dept Pharmacobiol Sci, I-88100 Catanzaro, Italy
[4] Univ Roma La Sapienza, Chair Neurol, I-00161 Rome, Italy
[5] IRCCS C Mondino Inst Neurol Fdn, I-27100 Pavia, Italy
来源
ADVANCES IN NEUROPHARMACOLOGY | 2009年 / 85卷
关键词
PROTEIN-KINASE-B; GLYCOGEN-SYNTHASE KINASE-3; TUMOR-SUPPRESSOR PTEN; ARTERY OCCLUSION; NEURONAL SURVIVAL; PHOSPHORYLATION; DEATH; ACTIVATION; MECHANISMS; INHIBITORS;
D O I
10.1016/S0074-7742(09)85027-7
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
The effects of bergamot essential oil (BEO; Citrus bergamia, Risso) on brain damage caused by permanent focal cerebral ischemia in rat were investigated. Administration of BEO (0.1-0.5 ml/kg but not 1 ml/kg, given intraperitoneally I h before occlusion of the middle cerebral artery, MCAo) significantly reduced infarct size after 24 h permanent MCAo. The most effective dose (0.5 ml/kg) resulted in a significant reduction of infarct extension throughout the brain, especially in the medial striatum and the motor cortex as revealed by TTC staining of tissue Slices. Microdialysis experiments show that BEO (0.5 ml/kg) did not a Beet basal amino acid levels, whereas it significantly reduced excitatory amino acid, namely aspartate and glutamate, efflux in the frontoparietal cortex typically observed following MCAo. Western blotting experiments demonstrated that these early effects were associated, 24 h after permanent MCAo, to a significant increase in the phosphorylation and activity of the prosurvival kinase, Akt. Indeed, BEO significantly enhanced the phosphorylation of the deleterious downstream kinase, GSK-3 beta, whose activity is negatively regulated via phosphorylation by Akt.
引用
收藏
页码:389 / 405
页数:17
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