THE EFFECT OF PHOSPHOLIPASES ON THE ACTIVE UPTAKE OF NOREPINEPHRINE BY SYNAPTOSOMES ISOLATED FROM THE CEREBRAL CORTEX OF GUINEA PIG<sup>1</sup>

Kainic acid (KA) is a known potent neuroexcitotoxin, although the biochemical mechanism producing its underlying neurotoxic effect is not quite clear. Histopathological examination of gerbil brains 24 h after systemic injection of KA revealed severe neuronal lesions in different regions of the brain, especially the cerebellar and hippocampal areas. We have detected free radical formation in the brain 1 h after KA administration by using an in vivo spin trapping technique. We have also observed increased lipid peroxidation in the brain after KA-treatment by analyzing thiobarbituric acid reactive substances and conjugated diene formation. Diminished brain specific (Na+, K+)-ATPase activity was also found 2 h after KA injection and persisted to 24 h. It is possible that the free radical reaction is a primary cause of neuronal degeneration after KA administration.

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“…Crude synaptsomes from both control and KA-treated gerbils were used for (Na +, K+)-ATPase assay (Sun, 1974).…”

Section: (Na + K +)-Atpase Activitymentioning

confidence: 99%

The biochemical mechanisms of the excitotoxicity of Kainic acid

Sun

Cheng

et al. 1992

Molecular and Chemical Neuropathology

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“…Many structures such as cell membranes may be present for long periods and undergo progressive and irreversible changes with age (KOHN, 1971). Synaptoso-ma1 membranes may be particularly susceptible to oxidative changes because of their high content of polyunsaturated fatty acids (SUN & SUN, 1972). Studies on subcellular fractions of developing brain showed an increasing trend in lipid peroxidation with the advancing age of the animal (BISHAYEE & BALASUBRAMANIAN, 1971).…”

mentioning

confidence: 99%

“…Studies on subcellular fractions of developing brain showed an increasing trend in lipid peroxidation with the advancing age of the animal (BISHAYEE & BALASUBRAMANIAN, 1971). We have recently shown that lipid peroxidation inhibits membrane-bound synaptosomal (Na' + KC)-ATPase activity (SUN, 1972). Since both ethanol and lipid peroxidation may effect synaptosomal ATPase activity in the brain, it is possible that there may be a significant interaction between these 2 variables which may account for some of the differences in sensitivity to alcohol and other agents in relation to age.…”

mentioning

confidence: 99%

THE EFFECTS OF AGE AND ALCOHOL ON (Na⁺+ K⁺)‐ATPASE ACTIVITY OF WHOLE HOMOGENATE AND SYNAPTOSOMES PREPARED FROM MOUSE AND HUMAN BRAIN

Sun

Samorajski

1975

Journal of Neurochemistry

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Abstract— Whole homogenates of mouse brain and nerve‐ending fractions of mouse and human brain were obtained at various age levels representative of maturity and old age. The mice were 3, 8 and 26–29 months old and the humans ranged in age from 19 to 84 y. Measurements of (Na++ K+)‐ATPase in whole brain homogenate of mouse did not reveal any significant differences in relation to age. However, the ability of ethanol at various concentrations to inhibit membrane‐bound synaptosomal (Na++ K+)‐ATPase was significantly greater in older mice and humans. The data are interpreted as indicating a change in the property of synaptic membranes as a consequence of advancing age.

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“…The active transport of catecholamines depends very much on the structural integrity of synaptosomal membrane (Sun, 1974;Sun & Sun, 1976). Due to the presence of highly unsaturated fatty acids in the synaptosomal membrane (Sun & Sun, 1972) brane structure may be considered as an important aging factor resulting in the formation of age pigment and declining of some membrane dependent enzymic activity (Sun & Samorajski, 1975).…”

Section: Discussionmentioning

confidence: 98%

“…The decrease in catecholamine concentration in brain regions may reflect a decline in enzymic activity for catecholamine synthesis with age or an increase in degradative enzymic activity. Some investigators have demonstrated that brain tyrosine hydroxylase (TH) decreases with age (McGeer & McGeer, 1975;Cote & Kremzner, 1974 , 1974;Cote & Kremzner, 1974). This decreased capacity to synthesize catecholamines, coupled with increasing M A 0 activity could explain the declining motor and mental activities of the aged patients.…”

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confidence: 97%

Aging and in vivo norepinephrine-uptake in mammalian brain

1976

Experimental Aging Research

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In order to examine the cellular effect of aging in the central nervous system, the regional distribution and the dynamic aspects of catecholamine metabolism in the brain were investigated. Results indicated that the endogenous norepinephrine (NE) content is lower in hypothalamus and brain stem of older rats (25 mo. n = 6) than younger rats (12 mo. n = 6). We have also observed in these animals that the age pigments were apparently absent in the brain tissue of young rats but become a very distinct feature for the old rats and that the catecholamine strong vesicles appear to be less dense in the nerve terminals of old as compared with the young ones. 3H-NE was administered intracerebrally to mice of different age groups (4, 8, 12, 21 and 24 months) and the NE-uptake activity was examined by measuring the radioactive NE inside the isolated synaptosomes 5 min after 3H-NE injection. The result indicated that the young group (4 mo) has highest uptake activity. The uptake activity decrease with the older mice and reached the lowest in the age group of 21-24 mo. The decrease in NE-uptake activity may be related to the deterioration of synaptosomal membranes.

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THE EFFECT OF PHOSPHOLIPASES ON THE ACTIVE UPTAKE OF NOREPINEPHRINE BY SYNAPTOSOMES ISOLATED FROM THE CEREBRAL CORTEX OF GUINEA PIG¹

Cited by 21 publications

References 32 publications

The biochemical mechanisms of the excitotoxicity of Kainic acid

The biochemical mechanisms of the excitotoxicity of Kainic acid

THE EFFECTS OF AGE AND ALCOHOL ON (Na⁺+ K⁺)‐ATPASE ACTIVITY OF WHOLE HOMOGENATE AND SYNAPTOSOMES PREPARED FROM MOUSE AND HUMAN BRAIN

Aging and in vivo norepinephrine-uptake in mammalian brain

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THE EFFECT OF PHOSPHOLIPASES ON THE ACTIVE UPTAKE OF NOREPINEPHRINE BY SYNAPTOSOMES ISOLATED FROM THE CEREBRAL CORTEX OF GUINEA PIG1

Cited by 21 publications

References 32 publications

The biochemical mechanisms of the excitotoxicity of Kainic acid

The biochemical mechanisms of the excitotoxicity of Kainic acid

THE EFFECTS OF AGE AND ALCOHOL ON (Na++ K+)‐ATPASE ACTIVITY OF WHOLE HOMOGENATE AND SYNAPTOSOMES PREPARED FROM MOUSE AND HUMAN BRAIN

Aging and in vivo norepinephrine-uptake in mammalian brain

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THE EFFECT OF PHOSPHOLIPASES ON THE ACTIVE UPTAKE OF NOREPINEPHRINE BY SYNAPTOSOMES ISOLATED FROM THE CEREBRAL CORTEX OF GUINEA PIG¹

THE EFFECTS OF AGE AND ALCOHOL ON (Na⁺+ K⁺)‐ATPASE ACTIVITY OF WHOLE HOMOGENATE AND SYNAPTOSOMES PREPARED FROM MOUSE AND HUMAN BRAIN