Neurobiological signatures associated with alcohol and drug use in the human adolescent brain

Silveri, Marisa M.; Dager, Alecia D.; Cohen‐Gilbert, Julia E.; Sneider, Jennifer T.

doi:10.1016/j.neubiorev.2016.06.042

Cited by 106 publications

(74 citation statements)

References 170 publications

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“…The nature of vulnerability during this period of development highlights the critical role of experience in affecting neurodevelopmental trajectories throughout the lifespan. For example, previous research in animal models and humans have demonstrated that exposure to drugs of abuse during adolescence results in alterations in HPC volume and neurophysiology that has downstream consequences on drug abuse and affective disorders (see Spear, 2016 and Silveri et al, 2016 in the same issue), which may have downstream consequences on HPC-PFC interactions. Characterizing this period of adolescent development, and its sensitivity to drugs of abuse and other environmental insults, is critical to a greater understanding of normative increases in sensation seeking and psychopathology.…”

Section: Discussionmentioning

confidence: 99%

The role of experience in adolescent cognitive development: Integration of executive, memory, and mesolimbic systems

Murty

Calabro

Luna

2016

Neuroscience & Biobehavioral Reviews

116

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Adolescence marks a time of unique neurocognitive development, in which executive functions reach adult levels of maturation. While many core facets of executive function may reach maturation in childhood, these processes continue to be refined and stabilized during adolescence. We propose that this is mediated, in part, by interactions between the hippocampus and pre-frontal cortex. Specifically, we propose that development of this circuit refines adolescents’ ability to extract relevant information from prior experience to support task-relevant behavior. In support of this model, we review evidence for protracted structural and functional development both within and across the hippocampus and prefrontal cortex. We describe emerging research demonstrating the refinement of adolescents’ ability to integrate prior experiences to support goal-oriented behavior, which parallel hippocampal-prefrontal integration. Finally, we speculate that the development of this circuit is mediated by increases in dopaminergic neuromodulation present in adolescence, which may underlie memory processing, plasticity, and circuit integration. This model provides a novel characterization of how memory and executive systems integrate throughout adolescence to support adaptive behavior.

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Section: Discussionmentioning

confidence: 99%

The role of experience in adolescent cognitive development: Integration of executive, memory, and mesolimbic systems

Murty

Calabro

Luna

2016

Neuroscience & Biobehavioral Reviews

116

View full text Add to dashboard Cite

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“…Even the preference for a natural reward—sweet tastes—was found to be greater early in adolescence (11–15 years) than during late adolescence/emerging adulthood (19–25 years) (Desor and Beauchamp, 1987). A multitude of other studies have demonstrated enhanced sensitivity to rewarding stimuli in human adolescents for both decision-making/risk taking behaviors, as well as for cognitive control and learning behaviors, data that have been recently reviewed (see Andersen et al, 2002; and also in this issue: Luciana et al, 2016; Schulz and Sisk, 2016; Silveri et al, 2016; Spear, 2016; Vanderschuren et al, 2016; van Duijvenvoorde et al, 2016). …”

Section: Adolescent Sensitivity To Rewardsmentioning

confidence: 99%

“…Such propensities for alcohol/drug use during adolescence may not only be encouraged by an adolescent reward-sensitive phenotype, but also by (as we shall see) an attenuated sensitivity to aversive stimuli, including the aversive properties of alcohol, nicotine, and illicit drugs. This pattern of increased rewarding but decreased aversive sensitivities may help to promote high levels of alcohol/drug use among susceptible adolescents—elevated use that has the potential to impact normative developmental changes in brain structure and function during this critical period, thus altering neural processes and behaviors occurring within adolescence, as well as into adulthood (see reviews by Silveri et al, 2016 and Spear, 2016). …”

Section: Introductionmentioning

confidence: 99%

Reward-centricity and attenuated aversions: An adolescent phenotype emerging from studies in laboratory animals

Doremus-Fitzwater

Spear

2016

Neuroscience & Biobehavioral Reviews

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Adolescence is an evolutionarily conserved developmental period, with neural circuits and behaviors contributing to the detection, procurement, and receipt of rewards bearing similarity across species. Studies with laboratory animals suggest that adolescence is typified by a “reward-centric” phenotype—an increased sensitivity to rewards relative to adults. In contrast, adolescent rodents are reportedly less sensitive to the aversive properties of many drugs and naturally aversive stimuli. Alterations within the mesocorticolimbic dopamine and endocannabinoid systems likely contribute to an adolescent reward-sensitive, yet aversion-resistant, phenotype. Although early hypotheses postulated that developmental changes in dopaminergic circuitry would result in a “reward deficiency” syndrome, evidence now suggests the opposite: that adolescents are uniquely poised to seek out hedonic stimuli, experience greater “pleasure” from rewards, and consume rewarding stimuli in excess. Future studies that more clearly define the role of specific brain regions and neurotransmitter systems in the expression of behaviors toward reward- and aversive-related cues and stimuli are necessary to more fully understand an adolescent-proclivity for and vulnerability to rewards and drugs of potential abuse.

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“…Multiple studies, both preclinical (17, 18) and human (19–21) show impaired WM integrity is associated with functional consequences, including impulsivity (19), decision making (22) and relapse (23). Importantly, emerging evidence implicates WM integrity across a range of psychiatric disorders and cognitive processes relevant to addiction (24, 25). Based on (1) modulation of cocaine cue reactivity in animal models via PPAR-γ agonism, and (2) evidence for neuroprotective effects of PPAR-γ agonism, we sought to identify analogous effects of PIO treatment in individuals with CUD.…”

Section: Introductionmentioning

confidence: 99%

PPAR‐gamma agonist pioglitazone modifies craving intensity and brain white matter integrity in patients with primary cocaine use disorder: a double‐blind randomized controlled pilot trial

et al. 2017

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Background and aims Pioglitazone (PIO), a potent agonist of PPAR-gamma, is a promising candidate treatment for cocaine use disorder (CUD). We tested the effects of PIO on targeted mechanisms relevant to CUD: cocaine craving and brain white matter (WM) integrity. Feasibility, medication compliance, and tolerability were evaluated. Design Two-arm double-blind randomized controlled proof-of-concept pilot trial of PIO or placebo (PLC). Setting Single-site outpatient treatment research clinic in Houston, Texas, USA. Participants Thirty treatment-seeking adults with CUD. Mean [standard deviation (SD)] age was 47.8 (7.45), education was 12.7 (1.5), with 19.3 (7.8) years of reported cocaine use. Eighteen of the 30 participants (8=PIO; 10=PLC) completed diffusion tensor imaging (DTI) of WM integrity at pre/post-treatment. Intervention Study medication was dispensed at thrice weekly visits along with once weekly cognitive behavioral therapy for 12 weeks. Measurements Measures of target engagement mechanisms of interest included cocaine craving assessed by the Brief Substance Craving Scale (BSCS), the Obsessive Compulsive Drug Use Scale (OCDUS), a visual analog scale (VAS), and change in WM integrity. Feasibility measures included number completing treatment, medication compliance (riboflavin detection), and tolerability (side effects, serious adverse events). Findings Target engagement change in mechanisms of interest, defined as a ≥ 0.75 Bayesian posterior probability of an interaction existing favoring PIO over PLC, was demonstrated on measures of craving (BSCS, VAS) and WM integrity indexed by fractional anisotropy (FA) values. Outcomes indicated greater decrease in craving and greater increase in FA values in the PIO group. Feasibility was demonstrated by high completion rates among those starting treatment (21/26 = 80%) and medication compliance (≥ 80%). There were no reported serious adverse events for PIO. Conclusions Compared with placebo, patients receiving pioglitazone show a higher likelihood of reduced cocaine craving and improved brain white matter integrity as a function of time in treatment. Pioglitazone shows good feasibility as a treatment for cocaine use disorder.

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Neurobiological signatures associated with alcohol and drug use in the human adolescent brain

Cited by 106 publications

References 170 publications

The role of experience in adolescent cognitive development: Integration of executive, memory, and mesolimbic systems

The role of experience in adolescent cognitive development: Integration of executive, memory, and mesolimbic systems

Reward-centricity and attenuated aversions: An adolescent phenotype emerging from studies in laboratory animals

PPAR‐gamma agonist pioglitazone modifies craving intensity and brain white matter integrity in patients with primary cocaine use disorder: a double‐blind randomized controlled pilot trial

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