LIPID HYDROPEROXIDE-INDUCED MITOCHONDRIAL DYSFUNCTION FOLLOWING ACUTE ETHANOL INTOXICATION IN RATS - THE CRITICAL ROLE FOR MITOCHONDRIAL REDUCED GLUTATHIONE

被引:62
作者
MASINI, A [1 ]
CECCARELLI, D [1 ]
GALLESI, D [1 ]
GIOVANNINI, F [1 ]
TRENTI, T [1 ]
机构
[1] UNIV MODENA,IST TOSSICOL & FARMACOL CLIN,I-41100 MODENA,ITALY
来源
BIOCHEMICAL PHARMACOLOGY | 1994年 / 47卷 / 02期
关键词
ETHANOL ACUTE INTOXICATION; REDUCED GLUTATHIONE; FATTY ACID HYDROPEROXIDES; MEMBRANE POTENTIAL; PERMEABILITY TRANSITION (RAT LIVER MITOCHONDRIA);
D O I
10.1016/0006-2952(94)90009-4
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
It has been found that acute ethanol (EtOH) intoxication of rats caused depletion of mitochondrial reduced glutathione (GSH) of approximately 40%. A GSH reduction of similar extent was also observed after the administration to rats of buthionine sulphoximine (BSO), a specific inhibitor of GSH synthesis. Combined treatment with BSO plus EtOH further decreased mitochondrial GSH up to 70% in comparison to control. Normal functional efficiency was encountered in BSO-treated mitochondria, as evaluated by membrane potential measurements during a complete cycle of phosphorylation. In contrast a partial loss of coupled functions occurred in mitochondria from EtOH- and BSO plus EtOH-treated rats. The presence in the incubation system of either GSH methyl monoester (GSH-EE), which normalizes GSH levels, or of EGTA, which chelates the available Ca2+ partially restores the mitochondrial phosphorylative efficiency. Following EtOH and BSO plus EtOH intoxication, the presence of fatty-acid-conjugated diene hydroperoxides, such as octadecadienoic acid hydroperoxide (HPODE), was detected in the mitochondrial membrane. Exogenous HPODE, when added to BSO-treated mitochondria, induced, in a concentration-dependent system, membrane potential derangement. The presence of either GSH-EE or EGTA fully prevented a drop in membrane potential. The results obtained suggest that fatty acid hydroperoxides, endogenously formed during EtOH metabolism, brought about non-specific permeability changes in the mitochondrial inner membrane whose extent was strictly dependent on the level of mitochondrial GSH.
引用
收藏
页码:217 / 224
页数:8
相关论文
共 56 条
[1]   GLUTATHIONE MONOETHYL ESTER - PREPARATION, UPTAKE BY TISSUES, AND CONVERSION TO GLUTATHIONE [J].
ANDERSON, ME ;
POWRIE, F ;
PURI, RN ;
MEISTER, A .
ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1985, 239 (02) :538-548
[2]   CONJUGATED DIENE AND TRANS-FATTY-ACIDS IN A CHOLINE-DEVOID DIET HEPATOCARCINOGENIC IN THE RAT [J].
BANNI, S ;
EVANS, RW ;
SALGO, MG ;
CORONGIU, FP ;
LOMBARDI, B .
CARCINOGENESIS, 1990, 11 (11) :2047-2051
[3]   ACUTE ETHANOL INTOXICATION STIMULATES SUPEROXIDE ANION PRODUCTION BY INSITU PERFUSED-RAT-LIVER [J].
BAUTISTA, AP ;
SPITZER, JJ .
HEPATOLOGY, 1992, 15 (05) :892-898
[4]   BIOCHEMICAL-MECHANISM OF GSH DEPLETION INDUCED BY 1,2-DIBROMOETHANE IN ISOLATED RAT-LIVER MITOCHONDRIA - EVIDENCE OF A GSH CONJUGATION PROCESS [J].
BOTTI, B ;
CECCARELLI, D ;
TOMASI, A ;
VANNINI, V ;
MUSCATELLO, U ;
MASINI, A .
BIOCHIMICA ET BIOPHYSICA ACTA, 1989, 992 (03) :327-332
[5]   EFFECTS OF CHRONIC ETHANOL TREATMENT ON MITOCHONDRIAL FUNCTIONS DAMAGE TO COUPLING SITE-1 [J].
CEDERBAUM, AI ;
LIEBER, CS ;
RUBIN, E .
ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1974, 165 (02) :560-569
[6]   HYDROPEROXIDE METABOLISM IN MAMMALIAN ORGANS [J].
CHANCE, B ;
SIES, H ;
BOVERIS, A .
PHYSIOLOGICAL REVIEWS, 1979, 59 (03) :527-605
[7]  
CHANCE B, 1956, ADV ENZYMOL REL S BI, V17, P65
[8]   CARBON-TETRACHLORIDE, BROMOTRICHLOROMETHANE AND ETHANOL ACUTE INTOXICATION - NEW CHEMICAL EVIDENCE FOR LIPID-PEROXIDATION IN RAT-TISSUE MICROSOMES [J].
CORONGIU, FP ;
LAI, M ;
MILIA, A .
BIOCHEMICAL JOURNAL, 1983, 212 (03) :625-631
[9]   KINETIC EVIDENCE FOR A HEART MITOCHONDRIAL PORE ACTIVATED BY CA-2+, INORGANIC-PHOSPHATE AND OXIDATIVE STRESS - A POTENTIAL MECHANISM FOR MITOCHONDRIAL DYSFUNCTION DURING CELLULAR CA-2+ OVERLOAD [J].
CROMPTON, M ;
COSTI, A .
EUROPEAN JOURNAL OF BIOCHEMISTRY, 1988, 178 (02) :489-501
[10]   IMPAIRED UPTAKE OF GLUTATHIONE BY HEPATIC MITOCHONDRIA FROM CHRONIC ETHANOL-FED RATS - TRACER KINETIC-STUDIES INVITRO AND INVIVO AND SUSCEPTIBILITY TO OXIDANT STRESS [J].
FERNANDEZCHECA, JC ;
GARCIARUIZ, C ;
OOKHTENS, M ;
KAPLOWITZ, N .
JOURNAL OF CLINICAL INVESTIGATION, 1991, 87 (02) :397-405
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