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Group I metabotropic glutamate receptor inhibition selectively blocks a prolonged
Ca2+ elevation associated with age-dependent excitotoxicity. Attuccib, 1,
S., Clodfeltera, 1,G. V., Thibaulta, O., Statona, J., Moronib, F., Landfielda
, P. W. , and Porter a, N. M., a Department of Molecular and Biomedical Pharmacology,
University of Kentucky College of Medicine, Lexington, KY, USA. b Departimento
di Farmacologia, Università di Firenze, Florence, Italy. Neuroscience,
112, (1), 183-194, (2002)
Abstract:
It has been
recognized for some years that a prolonged Ca(2+) elevation that is predictive
of impending cell death develops in cultured neurons following excitotoxic insult.
In addition, neurons exhibit enhanced sensitivity to excitotoxic insult with increasing
age in culture. However, little is known about the processes that selectively
regulate the post-insult Ca(2+) elevation and therefore, it remains unclear whether
it is associated specifically with age-dependent toxicity.Here, we tested the
hypothesis that a group I metabotropic glutamate receptor antagonist selectively
modulates the prolonged Ca(2+) elevation in direct association with its protective
effects against excitotoxicity. Rat hippocampal cultures of two ages (8-9 and
21-28 days in vitro) were exposed to a 5-min glutamate insult (400 microM in younger
and 10 microM in older cultures) sufficient to kill >50% of the neurons, and
were treated with vehicle or the specific group I metabotropic glutamate receptor
antagonist 1-aminoindan-1,5-dicarboxylic acid (AIDA; 1 mM), throughout and following
the insult. Neuronal survival was quantified 24 h after insult. In parallel studies,
neurons of similar age in culture were imaged ratiometrically with a confocal
microscope during and for 60 min after the glutamate insult. A large post-insult
Ca(2+) elevation was present in older but not most younger neurons. The N-methyl-D-aspartate
receptor antagonist, MK-801, blocked the Ca(2+) elevation both during and following
the insult. In contrast, AIDA blocked only the post-insult prolonged Ca(2+) elevation
in older neurons. Moreover, AIDA was neuroprotective in older but not younger
cultures.From these results we suggest that the post-insult Ca(2+) elevation is
regulated differently from the Ca(2+) elevation during glutamate insult and is
modulated by group I metabotropic glutamate receptors. Further, the prolonged
Ca(2+) elevation appears to be directly linked to an age-dependent component of
vulnerability. Copyright © 2002 IBRO.
Link
to Paper
Materials & Methods:
"For confocal imaging
studies, the cell suspension was
diluted with MEM to a final concentration
of V5U105 cells/ml
and 1 ml added to poly-L-lysine-coated (1 mg/ml) glass-bottom
culture dishes (35 mm; MatTek, Ashland, MA, USA) containing 1 ml MEM..."
Microscopic Technique:
Confocal Imaging
Cell Type(s):
GH4, IMR-32
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