Neural circuitry associated with risk for alcohol use disorders.

paper Cited Public

Authors: Tessner, Kevin D; Hill, Shirley Y
Year: 2010
Journal: Neuropsychology review
PMID: 19685291
DOI: 10.1007/s11065-009-9111-4
PMCID: PMC3580188

Fig. 1

According to Schmahmann and Pandya (1997), the cerebrocerebellar circuit is composed of a feedforward limb that includes the corticopontine and pontocerebellar mossy fiber projections, and a feedback loop that contains the cerebellothalamic and thalamocortical pathways. The corticopontine pathway originates in the Vb layer of cerebral cortex and carries associative, sensory, and motor information from cortical neurons to neurons in the ventral pons. This information is directed to the cerebellum, and then projected to the thalamus through midbrain neurons of the red nucleus. Afferent pathways originating in the thalamus and projecting to the cortex complete the feedback loop

Fig. 2

The extended limbic network consists of the basal forebrain, extended amygdala, and limbic lobe as described by Heimer and Van Hoesen (2006). To aid in visualization, not all structures or established projections are displayed. Regions of the basal forebrain, which includes areas usually referred to as the ventral striatum and nucleus accumbens, receive input from the extended amygdala, limbic lobe, and dopaminergic neurons of the ventral tegmental area. The extended amygdala includes the central and medial nuclei of the amygdala, their extensions to the bed nucleus of the stria terminalis, as well as downstream projections to the ventral striatum and nucleus accumbens. The extended amygdala has abundant associative connections with the hypothalamus as well as greater limbic lobe, including the hippocampus, cingulate and insular cortex, lateral basal cortical amygdala, and OFC

Fig. 3

A schematic representation of the hypothalamic-pituitary-adrenocortical (HPA) system. Cortisol acts on the brain through binding to glucocorticoid receptors (GRs). Binding to these receptors in some regions of the brain, including the hippocampus, cingulate, and frontal cortex triggers a negative feedback system that dampens release of corticotropin-releasing hormone (CRH) and adrenocorticotropic hormone (ACTH), thus modulating HPA activity

Fig. 4

A schematic of the pathways that are of primary relevance to the core features of risk for alcohol dependence, particularly behavioral and affective dysfunction. The pathways are color coded to assist in visualization. The externalizing pathway to alcohol dependence (yellow) is associated with deficits in executive function and in inhibition and may share a common genetic diathesis with ADHD and conduct disorder. The brain regions of the externalizing pathway consist of the cerebellum (Crb), thalamus (Tha), and prefrontal cortex (PFC) which comprise the cerebellothalamocortical feedback system. The internalizing pathway to alcohol dependence (green) is associated with affective dysregulation (i.e. depression and anxiety-related traits), deficient mechanisms of motivation and reward (i.e. impulsivity and dysfunction in decision-making), and autonomic hyperarousal (i.e. harm avoidance and stress reactivity) through overlapping pathways of the HPA system (shown in red). The internalizing pathway includes the amygdala (Amy), orbitofrontal cortex (OFC), and hypothalamus (Hyp) and pituitary (Pit) of the HPA axis, as well as the brain regions of the mesolimbic dopamine pathway (NAc = nucleus accumbens; VTA = ventral tegmental area). The cingulate gyrus (CG) connects these pathways

#	Section	Preview
40	Vulnerable Brain Systems in Individuals at Risk for AUD — Cerebellothalamocortical System	Cerebellar abnormalities are associated with deficits in posture, volitional movements, balance, and…
41	Vulnerable Brain Systems in Individuals at Risk for AUD — Cerebellothalamocortical System	Cerebellar output to ocular muscles via motor neurons in the brainstem control saccadic and smooth…
42	Vulnerable Brain Systems in Individuals at Risk for AUD — Cerebellothalamocortical System	Because deficits in executive function and behavioral control are frequently observed in the…
43	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	The limbic system remains the pre-eminent mechanism of emotion. Heimer and colleagues (Alheid and…
44	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	The broadly defined extended amygdala, which includes the bed nucleus of the stria terminalis and…
45	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	The limbic lobe, on the other hand, is restricted to portions of the cortical mantle on the medial…
46	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	Multiple components of the extended limbic network have been found to be structurally and/or…
47	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	An inverse relationship between grey matter volumes of the OFC and measures of impulsivity has been…
48	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	There appears to be a distinct pattern of anatomical asymmetry, particularly in the OFC, that is…
49	Vulnerable Brain Systems in Individuals at Risk for AUD — The Limbic System	Although the functional and psychopathologic consequences of hemispheric differences remain…
50	Vulnerable Brain Systems in Individuals at Risk for AUD — The HPA System	As noted earlier, individuals at risk for AUD tend to exhibit anomalies in their response to…
51	Vulnerable Brain Systems in Individuals at Risk for AUD — The HPA System	Figure 3 displays a schematic of the HPA system. The system involves regions within the brain…
52	Vulnerable Brain Systems in Individuals at Risk for AUD — The HPA System	The hippocampus plays a role in modulating activity of the HPA axis via a negative feedback system…
53	Vulnerable Brain Systems in Individuals at Risk for AUD — The HPA System	There is an extensive body of literature to support a relationship between neuroendocrine…
54	Possible Neural Diatheses for Alcohol Use Disorders	The emergence of alcohol use disorders, as with other psychiatric disorders that follow a…
55	Possible Neural Diatheses for Alcohol Use Disorders	The preponderance of the data suggests that the externalizing pathway to alcohol dependence may be…
56	Possible Neural Diatheses for Alcohol Use Disorders	The model proposed here encompasses potential neural systems underlying the risk for AUD and serves…
57	Possible Neural Diatheses for Alcohol Use Disorders	The current model provides some indication of the neuroanatomical circuits that may underlie the…
58	Directions for Future Research	Genetic variation may result in differences in the constitution and functioning of neural mechanisms…
59	Directions for Future Research	To date, genetic mechanisms of risk in the offspring of alcoholic parents or families with high…

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In this knowledge base

Title	Year	PMID
A KCNJ6 gene polymorphism modulates theta oscillations during reward processing.	2017	27993610

External

Title	Authors	Journal	Year	Link
Exploring Causal Pathways to Sleep Quality in Young Adults Using a Multimodal Data-Driven Causal Discovery Analysis.	Xiao X et al.	—	2025	→
Brain volumes in alcohol use disorder: Do females and males differ? A whole-brain magnetic resonance imaging mega-analysis.	Maggioni E et al.	—	2023	→
Peer victimization and associated alcohol and substance use: Prospective pathways for negative outcomes.	Tretyak V et al.	—	2022	→
Delay discounting and neurocognitive correlates among inner city adolescents with and without family history of substance use disorder.	Rodriguez-Moreno DV et al.	—	2021	→
Parietal P3 and midfrontal theta prospectively predict the development of adolescent alcohol use.	Harper J et al.	—	2021	→
Changes of frontal cortical subregion volumes in alcohol dependent individuals during early abstinence: associations with treatment outcome.	Durazzo TC et al.	—	2020	→
Cigarette smoking history is associated with poorer recovery in multiple neurocognitive domains following treatment for an alcohol use disorder.	Durazzo TC et al.	—	2020	→
Association Between Age and Familial Risk for Alcoholism on Functional Connectivity in Adolescence.	Vaidya JG et al.	—	2019	→
Neurophysiological Correlates and Differential Drug Response in Subjects With a Family History of an Alcohol Use Disorder.	Comstock SM et al.	—	2019	→
Familial Risk for Alcohol Dependence and Brain Morphology: The Role of Cortical Thickness Across the Lifespan.	Hill SY	—	2018	→
P3 Component as a Potential Endophenotype for Control Inhibition in Offspring of Alcoholics.	Domínguez-Centeno I et al.	—	2018	→
A KCNJ6 gene polymorphism modulates theta oscillations during reward processing.	Kamarajan C et al.	—	2017	→
Facial emotion recognition in schizophrenia: An exploratory study on the role of comorbid alcohol and substance use disorders and COMT Val158Met.	Carrà G et al.	—	2017	→
Limitations of lymphoblastoid cell lines for functional analysis of SNPs.	Pathak H et al.	—	2017	→
Nucleus accumbens functional connectivity at age 20 is associated with trajectory of adolescent cannabis use and predicts psychosocial functioning in young adulthood.	Lichenstein SD et al.	—	2017	→
Regional brain volume changes in alcohol-dependent individuals during early abstinence: associations with relapse following treatment.	Durazzo TC et al.	—	2017	→
Volumetric Differences in Cerebellar Lobes in Individuals from Multiplex Alcohol Dependence Families and Controls: Their Relationship to Externalizing and Internalizing Disorders and Working Memory.	Hill SY et al.	—	2016	→
Adolescents' Neural Processing of Risky Decisions: Effects of Sex and Behavioral Disinhibition.	Crowley TJ et al.	—	2015	→
Blunted Heart Rate Response as a Potential Endophenotype of Substance Use Disorders: Evidence from High-Risk Youth.	Evans BE et al.	—	2015	→
Brain activity classifies adolescents with and without a familial history of substance use disorders.	Qiao J et al.	—	2015	→
Facial emotion recognition in alcohol and substance use disorders: A meta-analysis.	Castellano F et al.	—	2015	→
Psychological and Neurobiological Precursors of Alcohol Use Disorders in High Risk Youth.	Hill SY et al.	—	2015	→
Serial longitudinal magnetic resonance imaging data indicate non-linear regional gray matter volume recovery in abstinent alcohol-dependent individuals.	Durazzo TC et al.	—	2015	→
Shared genetic factors influence amygdala volumes and risk for alcoholism.	Dager AD et al.	—	2015	→
Brain proton magnetic resonance spectroscopy of alcohol use disorders.	Meyerhoff DJ	—	2014	→
Effects of cigarette smoking history on neurocognitive recovery over 8 months of abstinence in alcohol-dependent individuals.	Durazzo TC et al.	—	2014	→
Interactive effects of chronic cigarette smoking and age on brain volumes in controls and alcohol-dependent individuals in early abstinence.	Durazzo TC et al.	—	2014	→
Maladaptive decision making and substance use outcomes in high-risk individuals: preliminary evidence for the role of 5-HTTLPR variation.	O'Brien JW et al.	—	2014	→
Relationships between reward sensitivity, risk-taking and family history of alcoholism during an interactive competitive fMRI task.	Yarosh HL et al.	—	2014	→
The cerebellum and addiction: insights gained from neuroimaging research.	Moulton EA et al.	—	2014	→
Volumetric differences in the anterior cingulate cortex prospectively predict alcohol-related problems in adolescence.	Cheetham A et al.	—	2014	→
Adolescent brain development, substance use, and psychotherapeutic change.	Wetherill R et al.	—	2013	→
Amygdala Volume in Offspring from Multiplex for Alcohol Dependence Families: The Moderating Influence of Childhood Environment and 5-HTTLPR Variation.	Hill SY et al.	—	2013	→
A risk variant for alcoholism in the NMDA receptor affects amygdala activity during fear conditioning in humans.	Cacciaglia R et al.	—	2013	→
Caudate Volume in Offspring at Ultra High Risk for Alcohol Dependence: COMT Val158Met, DRD2, Externalizing Disorders, and Working Memory.	Hill SY et al.	—	2013	→
Chronic cigarette smoking in alcohol dependence: associations with cortical thickness and N-acetylaspartate levels in the extended brain reward system.	Durazzo TC et al.	—	2013	→
[Cognitive vulnerability to alcohol dependence: related neuroanatomic endophenotypes].	Seigneurie AS et al.	—	2013	→
Family history of alcohol dependence modulates functional neurophysiology in mood/anxiety disorders.	Sjoerds Z et al.	—	2013	→
Loss in connectivity among regions of the brain reward system in alcohol dependence.	Kuceyeski A et al.	—	2013	→
Neural correlates of impulsivity in healthy males and females with family histories of alcoholism.	DeVito EE et al.	—	2013	→
Reduced orbitofrontal cortical thickness in male adolescents with internet addiction.	Hong SB et al.	—	2013	→
Remapping the brain to compensate for impairment in recovering alcoholics.	Chanraud S et al.	—	2013	→
White matter integrity as a link in the association between motivation to abstain and treatment outcome in adolescent substance users.	Chung T et al.	—	2013	→
White matter microstructure, alcohol exposure, and familial risk for alcohol dependence.	Hill SY et al.	—	2013	→
A comprehensive assessment of neurocognition in middle-aged chronic cigarette smokers.	Durazzo TC et al.	—	2012	→
ASTN1 and alcohol dependence: family-based association analysis in multiplex alcohol dependence families.	Hill SY et al.	—	2012	→
Frontal white matter integrity predictors of adult alcohol treatment outcome.	Sorg SF et al.	—	2012	→
Orbitofrontal volumes in early adolescence predict initiation of cannabis use: a 4-year longitudinal and prospective study.	Cheetham A et al.	—	2012	→
Reduced fronto-cerebellar functional connectivity in chronic alcoholic patients.	Rogers BP et al.	—	2012	→
The relationship of appetitive, reproductive and posterior pituitary hormones to alcoholism and craving in humans.	Kenna GA et al.	—	2012	→
Altered fronto-cerebellar connectivity in alcohol-naïve youth with a family history of alcoholism.	Herting MM et al.	—	2011	→
Cerebellum volume in high-risk offspring from multiplex alcohol dependence families: association with allelic variation in GABRA2 and BDNF.	Hill SY et al.	—	2011	→
Cognitive functioning in opioid-dependent patients treated with buprenorphine, methadone, and other psychoactive medications: stability and correlates.	Rapeli P et al.	—	2011	→
Neural plasticity, human genetics, and risk for alcohol dependence.	Hill SY	—	2010	→