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The Journal of Neurophysiology Vol. 86 No. 5 November 2001, pp. 2445-2460
Copyright ©2001 by the American Physiological Society
Departments of Physiology and Anatomy and Center for Neuroscience, University of Wisconsin Medical School, Madison, Wisconsin 53706
Demir, Rezan,
Lewis B. Haberly, and
Meyer
B. Jackson.
Epileptiform Discharges With In-Vivo-Like Features
in Slices of Rat Piriform Cortex With Longitudinal Association
Fibers. J. Neurophysiol. 86: 2445-2460, 2001. Brain slices serve as useful models for the investigation of
epilepsy. However, the preparation of brain slices disrupts circuitry and severs axons, thus complicating efforts to relate epileptiform activity in vitro to seizure activity in vivo. This issue is relevant to studies in transverse slices of the piriform cortex (PC), the preparation of which disrupts extensive rostrocaudal fiber systems. In
these slices, epileptiform discharges propagate slowly and in a
wavelike manner, whereas such discharges in vivo propagate more rapidly
and jump abruptly between layers. The objective of the present study
was to identify fiber systems responsible for these differences. PC
slices were prepared by cutting along three different nearly orthogonal
planes (transverse, parasagittal, and longitudinal), and epileptiform
discharges were imaged with a voltage-sensitive fluorescent dye.
Interictal-like epileptiform activity was enabled by either a
kindling-like induction process or disinhibition with bicuculline. The
pattern of discharge onset was very similar in slices cut in different
planes. As described previously in transverse PC slices, discharges
were initiated in the endopiriform nucleus (En) and adjoining regions
in a two-stage process, starting with low-amplitude "plateau
activity" at one site and leading to an accelerating depolarization
and discharge onset at another nearby site. The similar pattern of
onset in slices of various orientations indicates that the local
circuitry and neuronal properties in and around the En, rather than
long-range fibers, assume dominant roles in the initiation of
epileptiform activity. Subtle variations in the onset site indicate
that interneurons can fine tune the site of discharge onset. In
contrast to the mode of onset, discharge propagation showed striking
variations. In longitudinal slices, where rostrocaudal association
fibers are best preserved, discharge propagation resembled in vivo
seizure activity in the following respects: propagation was as rapid as in vivo and about two to three times faster than in other slices; discharges jumped abruptly between the En and PC; and discharges had
large amplitudes in superficial layers of the PC. Cuts in longitudinal
slices that partially separated the PC from the En eliminated these
unique features. These results help clarify why epileptiform activity
differs between in vitro and in vivo experiments and suggest that
rostrocaudal pyramidal cell association fibers play a major role in the
propagation of discharges in the intact brain. The longitudinal PC
slice, which best preserves these fibers, is ideally suited for the
study their role.
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