Alcohol during adolescence selectively alters immediate and long-term behavior and neurochemistry.
- Authors
- Maldonado-Devincci, Antoniette M; Badanich, Kimberly A; Kirstein, Cheryl L
- Year
- 2010
- Journal
- Alcohol (Fayetteville, N.Y.)
- PMID
- 20113874
- DOI
- 10.1016/j.alcohol.2009.09.035
- PMCID
- PMC4199380
Alcohol use increases across adolescence and is a concern in the United States. In humans, males and females consume different amounts of alcohol depending on the age of initiation, and the long-term consequences of early ethanol consumption are not readily understood. The purpose of our work was to better understand the immediate and long-term impact of ethanol exposure during adolescence and the effects it can have on behavior and dopaminergic responsivity. We have assessed sex differences in voluntary ethanol consumption during adolescence and adulthood and the influence of binge ethanol exposure during adolescence. We have observed that males are sensitive to passive social influences that mediate voluntary ethanol consumption, and early ethanol exposure induces long-term changes in responsivity to ethanol in adulthood. Exposure to moderate doses of ethanol during adolescence produced alterations in dopamine in the nucleus accumbens septi during adolescence and later in adulthood. Taken together, all of these data indicate that the adolescent brain is sensitive to the impact of early ethanol exposure during this critical developmental period.
The diagram is a schematic of the experimental protocol used in the social interaction experiment.
LLM interpretation
This figure is a schematic diagram illustrating an experimental protocol for a social interaction study. The timeline shows two initial 30-minute social interaction sessions, with a demonstrator being administered water or ethanol between them. This is followed by social interaction (SI) in a CPP box for 30 minutes on postnatal days (PND) 31-34, concluding with a CPP test on PND 35.
As depicted in the figure adolescent male alcohol naΓ―ve observer rats that socially interacted with demonstrators administered the highest dose of ethanol showed an increase in time spent in the chamber paired with social interaction with an alcohol-intoxicated demonstrator after conditioning relative to all other groups. Adolescent alcohol naΓ―ve female observers showed no change in time spent in the chamber paired with social interaction with an alcohol-intoxicated demonstrator, regardless of dose. Data presented are mean +/β SEM difference in seconds spent in the paired chamber at test minus baseline presented as the change in time spent in the chamber paired with social interaction in the adolescent alcohol naive observerβs initially least preferred chamber. * indicates significant difference from all other sex- and dose-matched groups. The bars indicate the type of demonstrator the alcohol naΓ―ve adolescent observer socially interacted with (0.0 (clear bars)- social interaction with a sober peer; 0.5 (light grey) and 1.5 (dark grey)- social interaction with an alcohol-intoxicated peer). Female 0.0 n = 13; Female 0.5 n = 14; Female 1.5 n = 13; Male 0.0 n = 8; Male 0.5 n = 11; Male 1.5 n = 10.
LLM interpretation
This bar chart shows the change in time (Test-Baseline in seconds) spent in a chamber paired with social interaction for adolescent alcohol-naΓ―ve observer rats, categorized by sex (Female, Male) and ethanol dose of the demonstrator (0.0, 0.5, and 1.5). While female observers show minimal change across all doses, male observers show a significant increase in time spent in the paired chamber only in the 1.5 dose group. This specific group is marked with an asterisk (*), indicating a significant difference from all other sex- and dose-matched groups.
As depicted in the figure, animals that were pretreated with ethanol during adolescence and conditioned with ethanol in young adulthood spent more time in the ethanol-paired chamber relative to rats that were pretreated saline and conditioned with ethanol in young adulthood and also those that were pretreated with ethanol during adolescence and conditioned with saline in adulthood. Data presented are mean +/β SEM of the change in time spent in the paired chamber in the initially least preferred chamber (test-baseline). The bars indicate conditioning in young adulthood with saline (clear bars) or ethanol (grey bars). Saline-Saline n = 9; Saline-Ethanol n = 10; Ethanol-Saline n = 9; Ethanol-Ethanol n = 9.
LLM interpretation
This bar chart shows the change in time spent in the least preferred chamber (Test-Baseline) based on adolescent pretreatment (Saline vs. Ethanol) and young adult conditioning (Saline vs. Ethanol). The highest increase in time spent in the paired chamber is observed in the group pretreated with ethanol and conditioned with ethanol. An asterisk (*) denotes statistical significance for the Ethanol-Ethanol group compared to the other conditions.
In both panels, the x-axis denotes Age and the y-axis denotes extracellular DA levels (nM). Both approaches yielded similar age results [quantitative: F(2, 12)=14.01, P < 0.05; conventional: F(3, 279)=17.171, P < 0.05] with late adolescent animals (PND 45) having significantly higher basal DA levels than adults, but with the conventional method (Philpot and Kirstein, 2004), levels obtained in adolescents were higher than those obtained using the quantitative method (Badanich, Adler & Kirstein, 2006). Additionally, the quantitative approach revealed lower basal DA levels for early adolescent (PND 35) rats. For panel A, # = differs from PND 60; ## = differs from PND 45 and PND 60. For panel B, diamonds = differs from PND 45 and PND 60; stars = differs from all other ages. It should be noted the conventional method in panel B shows dialysate DA levels that were not corrected for probe recovery. Figures reproduced with permission from Philpot and Kirstein, 2004 and Badanich et al, 2006).
LLM interpretation
This figure consists of two bar charts (A and B) showing extracellular dopamine (DA) levels (nM) across different postnatal days (PND). Both panels show a peak in DA levels at PND 45 compared to other age groups, with statistical significance indicated by symbols (#, ##, diamonds, and stars). Panel A compares PND 35, 45, and 60 using a "zero net flux" quantitative method, while Panel B compares PND 25, 35, 45, and 60 using a conventional dialysate method.
The amount of DA in the microdialysis perfusate (DAin) is on the x-axis while the difference between DAin and recovered DA (DAout) is on the y-axis (DAin β DAout). The broken horizontal line depicts the point of no net flux of DA between the brain and the microdialysis perfusate. The x-intercept denotes the extracellular DA concentration in the NAcc for ethanol-treated (solid line; n=4) and saline control (broken line n=4) rats. Basal DA was greater for rats pretreated with ethanol during adolescence (6.5 nM DA) than for saline controls (3.6 nM DA); [t(6)= 2.458, P < 0.05]. The slope of the regression line denotes the extraction fraction (Ed), an indirect measure of DA reuptake, for ethanol-treated (87%) and saline control (68%) rats. Each data point denotes mean and SEM. This figure has been reproduced with permission from Badanich et al., 2007.
LLM interpretation
This scatter plot with linear regression lines compares dopamine (DA) kinetics in the NAcc of ethanol-treated (solid line) and saline control (dashed line) rats. The x-axis represents the amount of DA in the perfusate ($\text{DA}_{\text{in}}$), and the y-axis represents the difference between $\text{DA}_{\text{in}}$ and recovered DA ($\text{DA}_{\text{in}} - \text{DA}_{\text{out}}$). The x-intercepts indicate that basal DA was significantly higher for ethanol-treated rats (6.5 nM) compared to saline controls (3.6 nM), with a reported p-value of $P < 0.05$.
| Name | Type |
|---|---|
| 0.5 g/kg group local | cohort |
| 1.5 g/kg group local | cohort |
| Acquisition rate local | phenotype |
| adolescent animals | cohort |
| adolescent drinking | phenotype |
| Adolescent drinking behaviors local | phenotype |
| Adolescent ethanol exposure local | cohort |
| Adolescent female alcohol-preferring P rats local | cohort |
| Adolescent female rats local | cohort |
| Adolescent male alcohol-preferring P rats local | cohort |
| Adolescent male rats local | cohort |
| adolescent observer rats local | cohort |
| Adolescent rat local | cohort |
| adolescent rats | cohort |
| adolescents | cohort |
| Adolescents aged 12β13 local | cohort |
| Adolescents aged 18β20 local | cohort |
| adolescent vulnerability local | phenotype |
| Adult brain functioning local | phenotype |
| Adult female rats local | cohort |
| adulthood | cohort |
| Adult male rats local | cohort |
| adult rats | cohort |
| Adult rodents local | cohort |
| aggression | phenotype |
| alcohol | phenotype |
| alcohol abuse | phenotype |
| Alcohol-free familiar peer local | phenotype |
| alcohol-free peer local | cohort |
| Alcohol-free unfamiliar peer local | phenotype |
| Alcohol-intoxicated familiar peer local | phenotype |
| alcohol-intoxicated peer local | cohort |
| Alcoholβintoxicated peer local | phenotype |
| Alcohol-intoxicated unfamiliar peer local | phenotype |
| alcohol odor local | drug |
| alcohol-related behaviors | phenotype |
| Alcohol seeking | phenotype |
| alcohol self-administration | phenotype |
| Alcohol Use | phenotype |
| Alcohol Use Disorder | phenotype |
| animal models | cohort |
| attention | phenotype |
| Attention to salient stimuli local | phenotype |
| banana odor local | drug |
| Basal dopamine level local | phenotype |
| Behavioral alterations local | phenotype |
| Behavioral change local | phenotype |
| behavioral inhibition | phenotype |
| behavioral sensitization | phenotype |
| binge drinking | phenotype |
| binge drinking episodes | phenotype |
| brain development | phenotype |
| Chamber preference local | phenotype |
| cognition | phenotype |
| conditioned place preference | phenotype |
| Continued alcohol use in adulthood local | phenotype |
| control animals | cohort |
| control group | cohort |
| Control rat local | cohort |
| control rats | cohort |
| cortex | anatomy |
| decision-making | phenotype |
| Decreased locomotor activity local | phenotype |
| dopamine | drug |
| dopamine expectancy effect local | phenotype |
| Early adolescent rats local | cohort |
| Early adolescent rats (PND 35) local | cohort |
| Early alcohol-seeking behavior local | phenotype |
| early alcohol use | phenotype |
| Early ethanol exposure local | phenotype |
| Early postnatal period local | cohort |
| ethanol 0.5 g/kg | drug |
| Ethanol 1.5 g/kg local | drug |
| ethanol consumption | phenotype |
| Ethanol consumption during adolescence local | phenotype |
| ethanol-naΓ―ve adolescent observer rats local | cohort |
| exploratory behavior | phenotype |
| Female adolescent rats local | cohort |
| female rats | cohort |
| Future drinking patterns local | phenotype |
| glutamate | drug |
| Greater vulnerability to subsequent ethanol exposure local | phenotype |
| high ethanol consumption rates local | phenotype |
| High ethanol consumption rats local | cohort |
| High ethanol dose (1.5 g/kg) local | phenotype |
| high responder to novelty local | phenotype |
| High school students | cohort |
| human | cohort |
| human adolescents | cohort |
| human alcoholics | phenotype |
| impulsivity | phenotype |
| incentive salience | phenotype |
| increased NAcc dopamine levels local | phenotype |
| Increased social interaction local | phenotype |
| Increased voluntary ethanol intake local | phenotype |
| increased vulnerability to ethanol effects local | phenotype |
| Initial exposure to ethanol local | phenotype |
| Intoxicated demonstrator local | phenotype |
| Late adolescent rats local | cohort |
| leftward shift in peak dopamine levels local | phenotype |
| locomotor activity | phenotype |
| Low ethanol dose (0.5 g/kg) local | phenotype |
| low responder to novelty local | phenotype |
| Male adolescent rats local | cohort |
| male rats | cohort |
| mature hormonal cycling local | phenotype |
| Mature hormonal cycling local | phenotype |
| memory | phenotype |
| Mesolimbic dopamine local | drug |
| mesolimbic dopamine system | drug |
| mesolimbic system | anatomy |
| mid adolescence local | phenotype |
| NAcc DA levels local | phenotype |
| Neurochemical reactivity to early life alcohol exposure local | phenotype |
| Neuronal functioning in adulthood local | phenotype |
| Normal brain development local | phenotype |
| novelty preference local | phenotype |
| novelty seeking behaviors local | phenotype |
| nucleus accumbens | anatomy |
| Out-bred female rats local | cohort |
| Outβbred rats local | cohort |
| Passive social influences local | phenotype |
| Passive social modeling behavior local | phenotype |
| Peer interaction | phenotype |
| Perseveration rate local | phenotype |
| persistent behavioral alterations local | phenotype |
| Play behavior | phenotype |
| preadolescence local | phenotype |
| Preadolescent rats local | cohort |
| pre-adolescent rats (PND 25) local | cohort |
| Preference for alcohol local | phenotype |
| Preference for alcohol-associated chamber local | phenotype |
| preference for alcohol odor local | phenotype |
| preference for banana odor local | phenotype |
| Pruning of excitatory synapses local | phenotype |
| puberty | phenotype |
| rats | cohort |
| reproductive maturity local | phenotype |
| Reproductive maturity local | phenotype |
| Responsivity to ethanol local | phenotype |
| reversal learning | phenotype |
| reward | phenotype |
| Rewarding properties of alcohol local | phenotype |
| risk-taking behavior | phenotype |
| rodents | cohort |
| saccharin | drug |
| saline | drug |
| Saline-treated controls local | cohort |
| Sensitivity to alcohol consumption local | phenotype |
| Set-shifting local | phenotype |
| Severe alcohol dependency local | phenotype |
| sex | phenotype |
| sex differences | phenotype |
| sexual maturation | phenotype |
| Sober demonstrator local | phenotype |
| Social contact local | phenotype |
| social facilitation | phenotype |
| Social influences local | phenotype |
| social inhibition | phenotype |
| Social interaction | phenotype |
| Social interaction with alcohol-intoxicated peer local | phenotype |
| Social investigation local | phenotype |
| social isolation | phenotype |
| Social modeling local | phenotype |
| Social play local | phenotype |
| Sprague-Dawley rats | cohort |
| Subsequent ethanol intake in adulthood local | phenotype |
| sucrose | drug |
| Sweetened ethanol local | drug |
| tolerance | phenotype |
| underage drinking | phenotype |
| ventral tegmental area | anatomy |
| voluntary ethanol consumption | phenotype |
| Voluntary ethanol intake local | phenotype |
| Voluntary sweetened ethanol intake local | phenotype |
| water | drug |
| weaning local | phenotype |
| weight gain | phenotype |
| working memory | phenotype |
| Young adulthood (PND 60β69) local | cohort |
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