Physiological Unmasking of New Glutamatergic Pathways in the Dentate Gyrus
of Hippocampal Slices from Kainate-Induced Epileptic Rats.
Peter R. Patrylo, F. Edward Dudek
Department of Anatomy and Neurobiology, Colorado State University, Fort
Collins, CO 80523.
APStracts 4:0246N, 1997.
ABSTRACT
In humans with temporal lobe epilepsy and kainate-treated rats, the mossy
fibers of the dentate granule cells send collateral axons into the inner
molecular layer. Prior investigations on kainate-treated rats demonstrated
that abnormal hilar-evoked events can occasionally be observed in slices with
mossy fiber sprouting when GABAA-mediated inhibition is blocked with
bicuculline. However, these abnormalities were observed infrequently, and it
was unknown whether these rats were epileptic. Wuarin and Dudek (1996)
reported that in slices from kainate-induced epileptic rats (3-13 months after
treatment), hilar stimulation evoked abnormal events in most slices with mossy
fiber sprouting exposed simultaneously to bicuculline and elevated
extracellular potassium concentration [K+]o. Using the same rats,
extracellular recordings were obtained from granule cells in hippocampal
slices to determine whether (1) hilar stimulation could evoke abnormal events
in slices with sprouting in normal artificial cerebrospinal fluid (ACSF), (2)
adding only bicuculline could unmask hilar-evoked abnormalities and glutamate-
receptor antagonists could block these events, and (3) increasing only [K+]o
could unmask these abnormalities. In normal ACSF, hilar stimulation evoked
abnormal field potentials in 27% of slices with sprouting versus controls
without sprouting (i.e., saline-treated or only 2-4 days after kainate
treatment). In bicuculline (10 æM) alone, hilar stimulation triggered
prolonged field potentials in 84% of slices with sprouting, but not in slices
from the two control groups. Addition of the N-methyl-D-aspartate (NMDA)
receptor antagonist, DL-2-amino-5-phosphonopentanoic acid (AP5), either
blocked the bursts or reduced their probability of occurrence. The à-amino-3-
hydroxy-5-methyl-4-isoxazole propionate (AMPA)/kainate receptor antagonist,
6,7,-dinitroquinoxaline-2,3-dione (DNQX), always eliminated the epileptiform
bursts. In kainate-treated rats with sprouting, but not in saline-treated
controls, abnormal hilar-evoked responses were also revealed in 6-9 mM [K+]o.
Additionally, 63% of slices with sprouting generated spontaneous bursts
lasting 1 to 40 s in ACSF containing 9 mm [K+]o; similar bursts were not
observed in controls. These results indicate that: (1) mossy fiber sprouting
is associated with new glutamatergic pathways, and although NMDA receptors are
important for propagation through these circuits, AMPA receptor activation is
crucial, (2) modest elevations of [K+]o, in a range that would have relatively
little effect on granule cells, can unmask these new excitatory circuits and
generate epileptiform bursts, and (3) this new circuitry underlies an
increased electrographic seizure susceptibility when inhibition is depressed
or membrane excitability is increased.
Received 30 January 1997; accepted in final form 9 September 1997.
APS Manuscript Number J94-7.
Article publication pending J. Neurophysiol.
ISSN 1080-4757 Copyright 1997 The American Physiological Society.
Published in APStracts on 7 October 1997