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Vol. 63, Issue 4, 896-907, April 2003
-Hydroxybutyric Acid and Diazepam Antagonize a Rapid Increase
in GABAA Receptors
4 Subunit mRNA Abundance
Induced by Ethanol Withdrawal in Cerebellar Granule Cells
Department of Experimental Biology "Bernardo Loddo", University
of Cagliari, Cagliari, Italy (P.F., L.M., F.B., A.M., F.B., G.T., E.S.,
G.B.); CNR Institute of Neuroscience, Section of
Neuropsychopharmacology, Cagliari, Italy (M.C.M., M.P.M., G.B.)
Both benzodiazepines and
-hydroxybutyric acid (GHB) are used to
treat alcohol withdrawal syndrome. The molecular basis for this
therapeutic efficacy was investigated with primary cultures of rat
cerebellar granule cells. Long-term exposure of these cells to ethanol
(100 mM, 5 days) reduced the abundance of mRNAs encoding the
2L and
2S subunits of the GABA type A
receptor (
32 and
23%, respectively) but failed to affect that of
1,
4, or
6 subunit mRNAs.
Subsequent ethanol withdrawal resulted in decreases in the amounts of
1 (
29%),
6 (
27%),
2L
(
64%), and
2S (
76%),subunit mRNAs that were
maximal after 6 to 12 h. In contrast, 3 h after ethanol
withdrawal, the abundance of the
4 subunit mRNA was
increased by 46%. Ethanol withdrawal did not affect neuronal
morphology but reduced cellular metabolic activity. The increase in
4 subunit was confirmed by functional studies showing a
positive action of flumazenil in patch clamp recordings of
GABA-stimulated currents after ethanol withdrawal. Diazepam (10 µM)
or GHB (100 mM) prevented the increase in the amount of the
4 subunit mRNA, the metabolic impairment, and the
positive action of flumazenil induced by ethanol withdrawal but failed
to restore the expression of the
1 and
2
subunits. The antagonism by GHB seems not to be mediated by a direct
action at GABAAR because GHB failed to potentiate the effects of GABA or diazepam on Cl
currents mediated by
GABA type A receptor.
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