An Initial, Three-Day-Long Treatment with Alcohol Induces a Long-Lasting Phenomenon of Selective Tolerance in the Activity of the Rat Hypothalamic–Pituitary–Adrenal Axis

Lee, Soon; Rivier, Catherine

doi:10.1523/jneurosci.17-22-08856.1997

Cited by 97 publications

(71 citation statements)

References 62 publications

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“…Also, corticosterone and hypothalamic CRF mRNA are increased during acute withdrawal from long-term cocaine administration (62). Similar decreases in HPA activity have been observed with repeated alcohol administration in a binge model (63)(64)(65). Long-term daily administration of alcohol in a liquid diet showed a decrease in HPA axis activity that persisted up to 3 weeks postabstinence (66).…”

Section: Hormonal and Brain Changes In Excessive Drug-taking Associatmentioning

confidence: 55%

Stress, Dysregulation of Drug Reward Pathways, and the Transition to Drug Dependence

Koob

Kreek²

2007

AJP

783

674

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This review provides a neuroadaptive perspective regarding the role of the hormonal and brain stress systems in drug addiction with a focus on the changes that occur during the transition from limited access to drugs to long-term compulsive use of drugs. A dramatic escalation in drug intake with extended access to drug self-administration is characterized by a dysregulation of brain reward pathways. Hormonal studies using an experimenter-administered cocaine binge model and an escalation self-administration model have revealed large increases in ACTH and corticosterone in rats during an acute binge with attenuation during the chronic binge stage and a reactivation of the hypothalamic-pituitary-adrenal axis during acute withdrawal. The activation of the hypothalamicpituitary-adrenal axis with cocaine appears to depend on feed-forward activation of the mesolimbic dopamine system. At the same time, escalation in drug intake with either extended access or dependence-induction produces an activation of the brain stress system's corticotropin-releasing factor outside of the hypothalamus in the extended amygdala, which is particularly evident during acute withdrawal. A model of the role of different levels of hormonal/brain stress activation in addiction is presented that has heuristic value for understanding individual vulnerability to drug dependence and novel treatments for the disorder.Drug addiction has been conceptualized as a chronic relapsing disorder characterized by compulsive drug-taking behavior with impairment in social and occupational functioning. From a psychiatric perspective, drug addiction has aspects of both impulse control disorders and compulsive disorders (1). Impulse control disorders are characterized by an increasing sense of tension or arousal before the commission of an impulsive act; pleasure, gratification, or relief at the time of commission of the act; and following the act, there may or may not be regret, self-reproach, or guilt (2). In contrast, compulsive disorders are characterized by anxiety and stress before the commission of a compulsive repetitive behavior and relief from the stress by performing the compulsive behavior. As an individual moves from an impulsive disorder to a compulsive disorder, there is a shift from positive reinforcement driving the motivated behavior to negative reinforcement driving the motivated behavior. Drug addiction has been conceptualized as a disorder that progresses from impulsivity to compulsivity in a collapsed cycle of addiction composed of three stages: preoccupation/anticipation, binge/intoxication, and withdrawal/negative affect (3). Different theoretical perspectives ranging from Psychoneuroendocrinology ©2003; Address correspondence and reprint requests to Dr. Koob, Committee on the Neurobiology, of Addictive Disorders, SP30-2400, the Scripps Research, Institute, 10550 North Torrey Pines Rd., La Jolla, CA 92037; gkoob@scripps.edu. All authors report no competing interests. This is publication number 16873-NP from the Scripps Research I...

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Section: Hormonal and Brain Changes In Excessive Drug-taking Associatmentioning

confidence: 55%

Stress, Dysregulation of Drug Reward Pathways, and the Transition to Drug Dependence

Koob

Kreek²

2007

AJP

783

674

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“…Chang et al 1995;) Thiele et al 1996;Lee and Rivier 1997) Suppression Suppression of basal Suppression of PTZSuppression of PTZc-fos expression in induced c-fos in cerebral induced c-fos in cerebral several brain areas, cortex and hippocampus; cortex and hippocampus; no suppression of novel suppression of NMDAsuppression of NMDAenvironment-induced induced c-fos in cerebral induced c-fos in cerebral c-fos expression cortex, but not in cortex, but not in (Ryabinin et al 1997) hippocampus hippocampus (Le et al 1990(Le et al , 1992(Le et al 1990(Le et al , 1992Davidson et al 1995) Davidson et al 1995. Suppression of IL-1β-induced c-fos in the paraventricular nucleus of hypothalamus (Lee and Rivier 1994) Suppression of cocaineinduction of FOS in caudate putamen (Torres 1994) Suppression of stress-, fear conditioning-, and novel context-induced c-fos in hippocampus (Melia et al 1996;Ryabinin et al 1995Ryabinin et al , 1997Ryabinin et al ) et al 1993Hope et al 1994b;Melia et al 1994;Chang et al 1995).…”

Section: Inductionmentioning

confidence: 99%

“…These include stress-related areas such as the central nucleus of amygdala, the paraventricular nucleus and several other areas of the hypothalamus, nucleus of solitary tract, the bed nucleus of striatum, and the sensory information processing-associated areas like the Edinger-Westphal nucleus and the paraventricular nucleus of thalamus (Zoeller and Fletcher 1994;Chang et al 1995;Thiele et al 1996;Hitzemann and Hitzemann 1997;Lee and Rivier 1997;Ryabinin et al 1997). Although an increase in c-Fos expression after alcohol intoxication was also observed in the nucleus accumbens and VTA, areas traditionally associated with reward pathways, it was much less robust than in the stress-and sensory processing-associated brain areas (Hitzemann and Hitzemann 1997;Ryabinin et al 1997).…”

Section: Experience-associated Hippocampal Ieg Induction Is Selectivementioning

confidence: 99%

Role of hippocampus in alcohol-induced memory impairment: implications from behavioral and immediate early gene studies

Ryabinin

1998

Psychopharmacology

117

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Acute alcohol intoxication disrupts memory acquisition in humans and laboratory animals. This review summarizes recent behavioral and immediate early gene expression studies addressing the mechanisms of this phenomenon. Most behavioral investigations agree that the amnestic effect of alcohol is due to its preferential detrimental effect on hippocampus-dependent than on hippocampus-independent forms of learning. However, some hippocampal lesion studies contradict these results. Learning in behavioral paradigms is accompanied by induction of c-fos and other immediate early genes in many brain regions of the animal. In contrast, studies on alcohol-mediated changes in expression of this gene confirm selective hippocampal suppression of basal and experience-induced expression of c-fos after acute and repeated administration of alcohol. This hippocampal suppression is in marked contrast with alcohol-mediated induction of c-fos expression in other brain areas. However, the selective suppression of hippocampal gene expression and memory by alcohol is most likely mediated by a number of interacting neurotransmitter systems. Thus, effects of lower doses of alcohol (0.5 g/kg or lower in rats) seem to be preferentially mediated through GABAergic systems. At intermediate doses (0.75-2 g/kg), several other neurotransmitter systems are affected besides GABA. Higher doses lead to none-specific effects, probably involving even more neurotransmitter systems. Elucidation of these neurotransmitter systems will be highly important for developing rational approaches for correction of alcohol-related cognitive disorders.

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“…In other evidence, it has long been known that alcohol stimulates the hypothalamic-pituitaryadrenal (HPA) axis and initially stimulates the autonomic systems by provoking sympathetic arousal followed by depressing such activation (Ehrenreich et al 1997;Lee and Rivier 1997). Dramatic adaptations of the HPA axis akin to tolerance has also been demonstrated with regular and chronic alcohol abuse in animals (Zhou et al 2000;Richardson et al 2008) and in humans (Adinoff et al 1998(Adinoff et al , 2005Wand and Dobs 1991).…”

Section: Chronic Alcohol-related Changes In Emotion Stress and Motivmentioning

confidence: 99%

Modeling Relapse Situations in the Human Laboratory

Sinha

2011

Current Topics in Behavioral Neurosciences

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It is well known that alcoholism is a chronic relapsing illness. While stress significantly impacts alcoholism risk, there is also evidence that increasing levels of alcohol use affect peripheral and central stress and reward pathways thereby setting up a reciprocal relationship among the effects of alcohol consumption of the development, course of and recovery from alcoholism. This chapter reviews our efforts in assessing the integrity of stress pathways in alcoholism by examining whether altered responses of the stress pathways play a role in relapse risk. Using validated human laboratory procedures to model two of the most common situations that contribute to relapse risk, we review how such models in the laboratory can predict subsequent alcohol relapse. Empirical findings from human laboratory and brain imaging studies are reviewed to show that specific stress-related dysregulation accompanies the alcohol craving state in alcohol-dependent individuals, and such dysregulation along with increases in alcohol seeking are predictive of increased alcohol relapse risk. Finally, the significant implications of these findings for the development of novel treatment interventions that target stress processes and alcohol craving to improve alcoholism relapse outcomes are discussed.

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An Initial, Three-Day-Long Treatment with Alcohol Induces a Long-Lasting Phenomenon of Selective Tolerance in the Activity of the Rat Hypothalamic–Pituitary–Adrenal Axis

Cited by 97 publications

References 62 publications

Stress, Dysregulation of Drug Reward Pathways, and the Transition to Drug Dependence

Stress, Dysregulation of Drug Reward Pathways, and the Transition to Drug Dependence

Role of hippocampus in alcohol-induced memory impairment: implications from behavioral and immediate early gene studies

Modeling Relapse Situations in the Human Laboratory

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