The cerebellar GABAA alpha6 subunit is differentially modulated by chronic ethanol exposure in normal (R100R) and mutated (Q100Q) sNP rats.
Articolo
Data di Pubblicazione:
2004
Abstract:
Sardinian alcohol non-preferring (sNP) rats carry a point mutation (R100Q) in the
cerebellar expressed GABAA receptor alpha6 subunit gene, leading to a higher
sensitivity to ethanol and diazepam. The role of the alpha6 subunit gene cluster
in the ethanol non-preferring phenotype was here investigated by measuring the
levels of alpha1, alpha6 and gamma2 peptide in the cerebellum of normal (RR) and
mutated (QQ) sNP rats after 2 weeks of chronic ethanol administration. Western
blot analysis revealed that the alpha6 subunit is increased in RR sNP rats after
chronic ethanol exposure (25.44%+/-8.69 versus control), while it remained
unchanged in mutated QQ sNP rats. Interestingly, chronic ethanol administration
decreased alpha1 peptide levels in the cerebellum of both rat lines to a similar
extent (30.99%+/-6.74 and 27.12%+/-9.83 in RR and QQ rats, respectively), while
gamma2 peptide levels remained unchanged. To further correlate the genetic and
biochemical difference of the normal and mutated sNP rats with their aversive
phenotype, we exposed sNP rats to a protocol of acquisition and maintenance of
ethanol drinking. QQ sNP rats drank less ethanol than RR rats during the
acquisition phase, but such difference was lost during the maintenance phase.
These data may contribute to elucidating the mechanisms of alcohol avoidance in
rat lines selected for this behavior when exposed to ethanol solution.
Tipologia CRIS:
01.01 Articolo in rivista
Keywords:
GABAA rec; Ethanol preference; Gene expression
Elenco autori:
Ruiu, Stefania; Marchese, Giorgio; Pani, Luca
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