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Eur. j. psychiatry ; 23(4): 225-233, oct.-dic. 2009. tab
Artigo em Inglês | IBECS | ID: ibc-85524

RESUMO

Background and Objectives: TaqI-A polymorphism, related to D2dopamine receptor (DRD2), and event-related P300 potentials have been consideredmarkers of alcohol dependence. The effect of alcohol use variables and TaqI-A on P300 ina single sample have been hardly analysed previously. This study examined changes inP300 parameters after six months of abstinence in alcohol-dependent subjects classifiedby their TaqI-A genotype.Methods: 102 men with alcohol dependence were studied at baseline and at 6 monthsof continued abstinence. P300 was recorded using an auditory paradigm. TaqI-A polymorphismwas genotyped: 34.3% of sample was classified as A1[TaqI-A1/TaqI-A1andTaqI-A1/TaqI-A2] and 65.7% as A2 [TaqI-A2/TaqI-A2]. The association between P300and TaqI-A and the correlation with age and alcohol consumption were considered.Results: The abstinence period was not associated to differences in neither P300 latency(F[1, 99] = 1.154 p = 0.285) nor amplitude (F[1, 99] = 1.453, p = 0.231). A1 subgroup was relatedto a longer latency (F[1, 99] = 5.055 p = 0.027), an early abuse age onset (F[1, 100] =14.552 p < 0.001) and close to be significant to an early dependence age onset (F[1, 100] =3.868 p = 0.052). Other drinking pattern variables were not associated to p300 measures. Familyhistory for alcoholism and TaqI-A were not related (X[1] = 0.327 p = 0.568) and no associationwas found with p300 measures. Current age correlated positively with P300 latency (F[1,99] = 26.082, p < 0,001) and negatively with amplitude (F[1, 99] = 5.297 p = 0.023). P300 amplitudewas not influenced by alcohol use variables nor TaqI-A polymorphism.Conclusions: P300 latency could be a biological marker of vulnerability to alcohol dependencerelated to TaqI-A1 polymorphism, irrespective of alcohol use variables (AU)


Assuntos
Humanos , Alcoolismo/genética , Potenciais Evocados P300 , Predisposição Genética para Doença , Marcadores Genéticos , Polimorfismo Genético , Receptores Dopaminérgicos
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