2003
DOI: 10.1038/sj.npp.1300170
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Alcohol Intoxication Increases Allopregnanolone Levels in Female Adolescent Humans

Abstract: Teenage drinking is a cause of growing concern in industrialized countries, where almost 35% of alcohol drinkers are under 16 years old. Increased anxiety, irritability, and depression among adolescents may induce them to seek the anxiolytic and rewarding properties of alcohol. We studied the effects of acute alcohol intoxication (AAI) on the plasma levels of progesterone and allopregnanolone in female adolescents. Blood samples were drawn from female adolescents who arrived at the emergency department. One st… Show more

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Cited by 76 publications
(50 citation statements)
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“…When taken in conjunction with the recent observations that ethanol consumption increased endogenous ALLO concentrations in B6 mice [10] and human adolescents [43,44], and that the inhibition of ALLO biosynthesis attenuated ethanol intake [13], the current findings are consistent with the hypothesis that alterations in endogenous ALLO levels may influence the regulatory processes governing ethanol consumption and reinforcement. The development of pharmacological interventions that manipulate endogenous ALLO concentrations may prove to be a beneficial treatment strategy.…”
Section: Discussionsupporting
confidence: 87%
“…When taken in conjunction with the recent observations that ethanol consumption increased endogenous ALLO concentrations in B6 mice [10] and human adolescents [43,44], and that the inhibition of ALLO biosynthesis attenuated ethanol intake [13], the current findings are consistent with the hypothesis that alterations in endogenous ALLO levels may influence the regulatory processes governing ethanol consumption and reinforcement. The development of pharmacological interventions that manipulate endogenous ALLO concentrations may prove to be a beneficial treatment strategy.…”
Section: Discussionsupporting
confidence: 87%
“…Electrophysiologically, ethanol has been shown to have a direct and indirect effect to potentiate GABA A receptor function, with the indirect effect related to an increase in steroidogenesis (Sanna et al, 2004). This finding is consistent with reports that acute exposure to ethanol by injection or consumption in rodents (Barbaccia et al, 1999;Finn et al, 2004b;Morrow et al, 1999;VanDoren et al, 2000) or consumption in human adolescents (Torres & Ortega, 2003 significantly increased endogenous ALLO levels to pharmacologically active concentrations. The fact that the 5α-reductase inhibitor finasteride (which decreases endogenous ALLO levels) reduced sensitivity to some, but not all, effects of ethanol (e.g., Dazzi et al, 2002;Gabriel et al, 2004;Hirani et al, 2002Hirani et al, , 2005Khisti et al, 2004;Murphy et al, 2006;VanDoren et al, 2000) suggests that there is a complex interaction between ALLO and ethanol in biological systems.…”
Section: Introductionsupporting
confidence: 88%
“…Preliminary clinical evaluations of neurosteroid concentrations in patients afflicted with premenstrual syndrome, major depression, seizure disorders, and alcoholism have indicated an inverse relationship between neurosteroids and symptoms of these disease states, since restoration of neurosteroids to normal levels alleviates adverse symptomology (Griffin et al, 2001). Taken in conjunction with the recent findings that ethanol self-administration led to significantly elevated plasma ALLO levels in male and female adolescents (Torres and Ortega, 2003;Torres and Ortega, 2004) and brain ALLO concentrations in male mice (Finn et al, 2004), it is tempting to speculate that a treatment strategy that involves manipulation of endogenous levels of ALLO and related agonist neurosteroids could yield beneficial outcomes in the management of ethanol's abuse-related effects. The purported involvement of GABAergic neurotransmission in the development of ethanol dependence and withdrawal warrants extensive investigation into GABA-active compounds (Johnson et al, 2005).…”
Section: Discussionsupporting
confidence: 61%