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The Journal of Neurophysiology Vol. 81 No. 4 April 1999, pp. 1872-1880
Copyright ©1999 by the American Physiological Society
Department of Physiology, Kurume University School of Medicine, 67 Asahi-machi, Kurume 830-0011, Japan
Tanaka, E.,
S. Yamamoto,
H. Inokuchi,
T. Isagai, and
H. Higashi.
Membrane dysfunction induced by in vitro ischemia in rat
hippocampal CA1 pyramidal neurons. Intracellular and
single-electrode voltage-clamp recordings were made to investigate the
process of membrane dysfunction induced by superfusion with oxygen and glucose-deprived (ischemia-simulating) medium in hippocampal CA1 pyramidal neurons of rat tissue slices. To assess correlation between
potential change and membrane dysfunction, the recorded neurons were
stained intracellularly with biocytin. A rapid depolarization was
produced ~6 min after starting superfusion with ischemia-simulating medium. When oxygen and glucose were reintroduced to the bathing medium
immediately after generating the rapid depolarization, the membrane did
not repolarize but depolarized further, the potential reaching 0 mV
~5 min after the reintroduction. In single-electrode voltage-clamp
recording, a corresponding rapid inward current was observed when the
membrane potential was held at 
70 mV. After the reintroduction of
oxygen and glucose, the current induced by ischemia-simulating medium
partially returned to preexposure levels. These results suggest that
the membrane depolarization is involved with the membrane dysfunction.
The morphological aspects of biocytin-stained neurons during ischemic
exposure were not significantly different from control neurons before
the rapid depolarization. On the other hand, small blebs were observed
on the surface of the neuron within 0.5 min of generating the rapid depolarization, and blebs increased in size after 1 min. After 3 min,
neurons became larger and swollen. The long and transverse axes and
area of the cross-sectional cell body were increased significantly 1 and 3 min after the rapid depolarization. When Ca2+-free (0 mM) with Co2+ (2.5 mM)-containing medium including oxygen
and glucose was applied within 1 min after the rapid depolarization,
the membrane potential was restored completely to the preexposure level
in the majority of neurons. In these neurons, the long axis was
lengthened without any blebs being apparent on the membrane surface.
These results suggest that the membrane dysfunction induced by in vitro
ischemia may be due to a Ca2+-dependent process that
commences ~1.5 min after and is completed 3 min after the onset of
the rapid depolarization. Because small blebs occurred immediately
after the rapid depolarization and large blebs appeared 1.5-3 min
after, it is likely that the transformation from small to large blebs
may result in the observed irreversible membrane dysfunction.
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