Diethylmaleate decreased ascorbic acid release induced by cerebral ischemia in cerebral cortex of the anesthetized rat

被引:0
作者
Yang, CS [1 ]
Tsai, PJ [1 ]
Lin, NN [1 ]
Kuo, JS [1 ]
机构
[1] Taichung Vet Gen Hosp, Dept Educ & Res, Taichung 407, Taiwan
来源
CHINESE JOURNAL OF PHYSIOLOGY | 2000年 / 43卷 / 02期
关键词
ascorbic acid; diethylmaleate; L-trans-pyrrolidine-2,4-dicarboxylate; glutamate; glutathione; microdialysis; anesthetized rat; brain cortex;
D O I
暂无
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
The effect of diethylmaleate administration on ascorbic acid release following cerebral ischemia was investigated in anesthetized rat brain cortex. Cerebral ischemia, induced by ligating bilateral common carotid arteries and unilateral middle cerebral artery, significantly increased the extracellular ascorbic acid levels. Diethylmaleate (4 mmoles/kg, i.p.), which has been shown in earlier studies to decrease the ischemia-induced glutamate release, significantly reduced the ischemia-induced ascorbic acid release. The ischemia-induced ascorbic acid release was unaffected by perfusing NMDA receptor antagonist MK 801 (75 mu M) Additionally, elevated extracellular glutamate Levels, achieved by either externally applied glutamate solutions or by perfusing L-trans-pyrrolidine-2,4-dicarboxylate (PDC) (31.4 mM and 15.7 mM) to inhibit the glutamate uptake transporter, also significantly increased the extracellular ascorbic acid levels. These results suggested that ascorbic acid release in cerebral ischemia might be related to the elevated extracellular glutamate levels, which occurs following cerebral ischemia.
引用
收藏
页码:49 / 53
页数:5
相关论文
共 21 条
[1]   ELEVATION OF THE EXTRACELLULAR CONCENTRATIONS OF GLUTAMATE AND ASPARTATE IN RAT HIPPOCAMPUS DURING TRANSIENT CEREBRAL-ISCHEMIA MONITORED BY INTRACEREBRAL MICRODIALYSIS [J].
BENVENISTE, H ;
DREJER, J ;
SCHOUSBOE, A ;
DIEMER, NH .
JOURNAL OF NEUROCHEMISTRY, 1984, 43 (05) :1369-1374
[2]   REGULATION OF EXCITATORY AMINO-ACID RELEASE BY N-METHYL-D-ASPARTATE RECEPTORS IN RAT STRIATUM - INVIVO MICRODIALYSIS STUDIES [J].
BUSTOS, G ;
ABARCA, J ;
FORRAY, MI ;
GYSLING, K ;
BRADBERRY, CW ;
ROTH, RH .
BRAIN RESEARCH, 1992, 585 (1-2) :105-115
[3]   ELECTROCHEMICAL MONITORING OF BRAIN ASCORBIC-ACID CHANGES ASSOCIATED WITH HYPOXIA, SPREADING DEPRESSION, AND SEIZURE ACTIVITY [J].
CAMMACK, J ;
GHASEMZADEH, B ;
ADAMS, RN .
NEUROCHEMICAL RESEARCH, 1992, 17 (01) :23-27
[4]   THE PHARMACOLOGICAL PROFILE OF GLUTAMATE-EVOKED ASCORBIC-ACID EFFLUX MEASURED BY INVIVO ELECTROCHEMISTRY [J].
CAMMACK, J ;
GHASEMZADEH, B ;
ADAMS, RN .
BRAIN RESEARCH, 1991, 565 (01) :17-22
[5]   Physiological release of excitatory amino acids [J].
Fillenz, M .
BEHAVIOURAL BRAIN RESEARCH, 1995, 71 (1-2) :51-67
[6]   GLUTATHIONE AND CYSTEINE DEPLETION IN RATS AND MICE FOLLOWING ACUTE INTOXICATION WITH DIETHYLMALEATE [J].
GERARDMONNIER, D ;
FOUGEAT, S ;
CHAUDIERE, J .
BIOCHEMICAL PHARMACOLOGY, 1992, 43 (03) :451-456
[7]   NMDA RECEPTOR REDOX SITES - ARE THEY TARGETS FOR SELECTIVE NEURONAL PROTECTION [J].
GOZLAN, H ;
BENARI, Y .
TRENDS IN PHARMACOLOGICAL SCIENCES, 1995, 16 (11) :368-374
[8]   L-TRANS-PYRROLIDINE-2,4-DICARBOXYLATE AND CIS-1-AMINOCYCLOBUTANE-1,3-DICARBOXYLATE BEHAVE AS TRANSPORTABLE, COMPETITIVE INHIBITORS OF THE HIGH-AFFINITY GLUTAMATE TRANSPORTERS [J].
GRIFFITHS, R ;
DUNLOP, J ;
GORMAN, A ;
SENIOR, J ;
GRIEVE, A .
BIOCHEMICAL PHARMACOLOGY, 1994, 47 (02) :267-274
[9]   ASCORBIC-ACID IN THE BRAIN [J].
GRUNEWALD, RA .
BRAIN RESEARCH REVIEWS, 1993, 18 (01) :123-133
[10]   INCREASED EXTRACELLULAR LEVELS OF ASCORBATE IN THE STRIATUM AFTER MIDDLE CEREBRAL-ARTERY OCCLUSION IN THE RAT MONITORED BY INTRACEREBRAL MICRODIALYSIS [J].
HILLERED, L ;
PERSSON, L ;
BOLANDER, HG ;
HALLSTROM, A ;
UNGERSTEDT, U .
NEUROSCIENCE LETTERS, 1988, 95 (1-3) :286-290
123