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The Journal of Neurophysiology Vol. 83 No. 4 April 2000, pp. 1830-1839
Copyright ©2000 by the American Physiological Society
Traumatic Brain Injury Laboratory, Cara Phelan Centre for Trauma Research and the Department of Anaesthesia, St. Michael's Hospital, University of Toronto, Toronto, Ontario M5B 1W8, Canada
Tian, Guo-Feng and
Andrew J. Baker.
Glycolysis Prevents Anoxia-Induced Synaptic Transmission Damage
in Rat Hippocampal Slices. J. Neurophysiol. 83: 1830-1839, 2000. Prolonged anoxia can cause permanent
damage to synaptic transmission in the mammalian CNS. We tested the
hypothesis that lack of glucose is the major cause of irreversible
anoxic transmission damage, and that anoxic synaptic transmission
damage could be prevented by glycolysis in rat hippocampal slices. The
evoked population spike (PS) was extracellularly recorded in the CA1 pyramidal cell layer after stimulation of the Schaffer collaterals. When the slice was superfused with artificial cerebrospinal fluid (ACSF) containing 4 mM glucose, following 10 min anoxia, the evoked PS
did not recover at all after 60 min reoxygenation. When superfusion ACSF contained 10 mM glucose with or without 0.5 mM
-cyano-4-hydroxycinnate (4-CIN), after 60 min reoxygenation the
evoked PS completely recovered following 10 min anoxia. When
superfusion ACSF contained 20 mM glucose with or without 1 mM sodium
cyanide (NaCN), after 60 min reoxygenation the evoked PS completely
recovered even following 120 min anoxia. In contrast, when superfusion
ACSF contained 4 mM glucose, following 10 min 1 mM NaCN chemical anoxia
alone, without anoxic anoxia, the evoked PS displayed no recovery after 60 min reoxygenation. Moreover, when 16 mM mannitol and 16 sodium L-lactate were added into 4 mM glucose ACSF, following 10 min anoxia the evoked PS failed to recover at all after 60 min
reoxygenation. The results indicate that elevated glucose concentration
powerfully protected the synaptic transmission against anoxic damage,
and the powerful protection is due to anaerobic metabolism of glucose and not a result of the higher osmolality in higher glucose ACSF. We
conclude that lack of glucose is the major cause of anoxia-induced synaptic transmission damage, and that if sufficient glucose is supplied, glycolysis could prevent this damage in vitro.
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