Influence of stress associated with chronic alcohol exposure on drinking

Becker, Howard C.

doi:10.1016/j.neuropharm.2017.04.028

Cited by 148 publications

(117 citation statements)

References 199 publications

(245 reference statements)

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“…Напротив, относительное количество зрелых Т-лимфоцитов в 1 точке обследова-ния было повышено по отношению к кон-тролю, что может быть обусловлено вклю-чением компенсаторных механизмов при стрессе, поскольку длительное потребление алкоголя и его отмена является мощным стрессором [13,14]. Проведены предварительные экспери-менты по влиянию аскорбата лития на экс-прессию поверхностных рецепторов лим-фоцитов больных алкоголизмом.…”

Section: результаты исследования и их обсуждениеunclassified

Indicators of Red Blood and T-Lymphocytes in Patients With Alcoholism; Protective Potential of Lithium Ascorbate

Vetlugina¹,

Savoshkina²,

Рощина³

et al. 2017

IJAFR (МЖПФИ)

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Проведено исследование состояния красной крови 35 больных алкоголизмом мужчин в динамике тера-пии синдрома отмены и постабстинентного состояния -через 3-4 дня поступления в стационар и на 12-14 день лечения. Выявлено снижение по отношению к контролю (19 практически здоровых мужчин) количе-ства эритроцитов, гематокрита, уровня гемоглобина и его концентрации в эритроците в обеих точках. Ма-кроцитоз (MCV ≥ 100 µm 3 ) выявлен у 29,4 % лиц с алкогольной зависимостью и у 1 человека контрольной группы. Установлена прямая корреляционная зависимость между числом эритроцитов и уровнем суточной толерантности. Ранее в опытах in vitro показано, что аскорбат лития значительно повышает устойчивость эритроцитов к гемолизу, индуцированному этанолом. Предварительные результаты данного исследования свидетельствуют об отсутствии негативного влияния аскорбата лития на экспрессию поверхностных ре-цепторов Т-лимфоцитов в пробах крови больных алкоголизмом. Полученные обнадеживающие результаты являются основанием для дальнейших исследований спектра химически синтезированных органических со-лей лития с целью выявления наиболее перспективных соединений для разработки препаратов, обладающих комбинированным нормотимическим, цитопротекторным, антиоксидантным действием. Mental Health Research Institute, Tomsk National Research Medical Center, Russian Academy of Sciences, Tomsk, e-mail: mental@tnimc.ruHere we present the results of a study of red blood parameters in 35 patients with alcoholism in men. Blood samples were studied in the dynamics of therapy for withdrawal and post-abstinence conditions -after 3-4 days of admission to hospital and on 12-14 days of treatment. Data at both pointes showed a decrease in the number of erythrocytes, hematocrit, hemoglobin level and its concentration in the erythrocyte in comparison with the control (control group19 of practically healthy men). Macrocytosis (MCV≥100 μm3) was detected in 29,4 % of persons with alcohol dependence and only 1 person from the control group. a direct correlation was established between the number of erythrocytes and the level of alcohol daily tolerance. Previously, it was showed that lithium ascorbate significantly increases the resistance of erythrocytes to ethanol-induced hemolysis in vitro. Preliminary results of this study indicate the absence of a negative impact of lithium ascorbate on the expression of surface receptors of T-lymphocytes in blood samples of patients with alcoholism. The received encouraging results are the basis for the further researches of a spectrum of chemically synthesized organic salts of lithium with the purpose of revealing the most perspective compounds for development of the medicines possessing combined normotimic, cytoprotective and antioxidant action.

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Section: результаты исследования и их обсуждениеunclassified

Indicators of Red Blood and T-Lymphocytes in Patients With Alcoholism; Protective Potential of Lithium Ascorbate

Vetlugina¹,

Savoshkina²,

Рощина³

et al. 2017

IJAFR (МЖПФИ)

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“…Despite the clinical importance of understanding the neural substrates responsible for the negative affective state that develops following chronic alcohol exposure and withdrawal, much remains unknown regarding the specific brain regions and circuits that mediate withdrawal-associated increases in anxiety behaviors and alcohol drinking. One preclinical model of AUD that has been extensively validated to address these questions is the chronic intermittent ethanol (CIE) vapor exposure regimen (Becker, 2017;Gilpin et al, 2008;Reynolds and Berridge, n.d.;Vendruscolo and Roberts, 2014). Using this model, which involves daily cycles of ethanol vapor exposure followed by a withdrawal period, rats and mice develop physiological and behavioral signs of ethanol dependence, including marked escalations in ethanol self-administration (Criado and Ehlers, 2013;Finn et al, 2007;O'Dell et al, 2004) and increases in anxiety-like behaviors on assays like the elevated plus-maze (Cagetti et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

Chronic intermittent ethanol exposure selectively increases synaptic excitability in the ventral domain of the rat hippocampus

Ewin

Morgan

Nierre

et al. 2018

Preprint

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Many studies have implicated hippocampal dysregulation in the pathophysiology of alcohol use disorder (AUD). However, over the past twenty years, a growing body of evidence has revealed distinct functional roles of the dorsal (dHC) and ventral (vHC) hippocampal subregions, with the dHC being primarily involved in spatial learning and memory and the vHC regulating anxietyand depressive-like behaviors. Notably, to our knowledge, no rodent studies have examined the effects of chronic ethanol exposure on synaptic transmission along the dorsal/ventral axis. To that end, we examined the effects of the chronic intermittent ethanol vapor exposure (CIE) model of AUD on dHC and vHC synaptic excitability. Adult male Long-Evans rats were exposed to CIE or air for 10 days (12 hrs/day; targeting blood ethanol levels of 175-225 mg%) and recordings were made 24 hours into withdrawal. As expected, this protocol increased anxietylike behaviors on the elevated plus-maze. Extracellular recordings revealed marked CIEassociated increases in synaptic excitation in the CA1 region that were exclusively restricted to the ventral domain of the hippocampus. Western blot analysis of synaptoneurosomal fractions revealed that the expression of two proteins that regulate synaptic strength, GluA2 and SK2, was dysregulated in the vHC, but not the dHC, following CIE. Together, these findings suggest that the ventral CA1 region may be particularly sensitive to the maladaptive effects of chronic ethanol exposure and provide new insight into some of the neural substrates that may contribute to the negative affective state that develops during withdrawal. Keywords: Chronic intermittent ethanol; ventral hippocampus; anxietyAll rights reserved. No reuse allowed without permission.was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.Thecopyright holder for this preprint (which . http://dx.doi.org/10.1101/337097 doi: bioRxiv preprint first posted online Jun. 3, 2018; Highlights-Chronic intermittent ethanol exposure produces robust increases in anxiety-like behavior in male Long Evans rats.-Chronic intermittent ethanol exposure increases synaptic excitability in the ventral, but not the dorsal, domain of the hippocampus.-These changes in excitability are associated with alterations in synaptoneurosomal expression of small conductance calcium-activated potassium channels and the GluA2 AMPA receptor subunit that are also restricted to the ventral hippocampus.All rights reserved. No reuse allowed without permission.was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.

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“…The transition from moderate controlled drinking (<2 drinks per day) to heavy drinking (>5 drinks per day) often involves intermittent bouts of binge consumption of ethanol, culminating in dependence (Becker, 2017). Acute administration of ethanol increases the release of mesolimbic dopamine in VTA projection areas (Di Chiara and Imperato, 1988; Yim et al , 1998; Zapata and Shippenberg, 2006).…”

Section: Introductionmentioning

confidence: 99%

“…Acute administration of ethanol increases the release of mesolimbic dopamine in VTA projection areas (Di Chiara and Imperato, 1988; Yim et al , 1998; Zapata and Shippenberg, 2006). Prolonged excessive alcohol consumption is a potent stressor and produces persistent dysregulation of brain reward systems, including the VTA, as well as stress/anti-stress responsivity (Becker, 2017).…”

Section: Introductionmentioning

confidence: 99%

The CRF-R1 regulation of VTA-GABAergic plasticity is suppressed by CB1 receptor inhibition following chronic exposure to ethanol

Harlan

Becker

Woodward

et al. 2018

Preprint

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Dopamine neurons in the ventral tegmental area (VTA) influence learned behaviors and neuropsychiatric diseases including addiction. The stress peptide corticotrophin-releasing factor (CRF) contributes to relapse to drug and alcohol seeking following withdrawal, although the cellular actions are poorly understood. In this study, we show that presynaptic CRF type 1 receptors (CRF-R1) potentiate GABA release onto mouse VTA dopamine neurons via a PKC-Ca2+ signaling mechanism. In na1ve animals, activation of CRF-R1 by bath application of CRF or ethanol enhanced GABAA inhibitory postsynaptic currents (IPSCs). Following three days of withdrawal from four weekly cycles of chronic intermittent ethanol (CIE) vapor exposure, spontaneous IPSC frequency was enhanced while CRF- and ethanol-potentiation of IPSCs was intact. However, withdrawal for 3 weeks or more was associated with reduced spontaneous IPSC frequency and diminished CRF and ethanol responses. Long-term withdrawal was also accompanied by decreased sensitivity to the CB1 receptor agonist WIN55212 as well as greatly enhanced sensitivity to the CB1 antagonist AM-251. Inclusion of BAPTA in the internal recording solution restored the responsiveness to CRF or ethanol and reduced the potentiating actions of AM251. Together, these data suggest that GABAA inhibition of VTA dopamine neurons is regulated by presynaptic actions of CRF and endocannabinoids and that long-term withdrawal from CIE treatment enhances endocannabinoid mediated inhibition, thereby suppressing CRF facilitation of GABA release. Such findings have implications for understanding the impact of chronic alcohol on stress-related, dopamine-mediated alcohol seeking behaviors.

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Influence of stress associated with chronic alcohol exposure on drinking

Cited by 148 publications

References 199 publications

Indicators of Red Blood and T-Lymphocytes in Patients With Alcoholism; Protective Potential of Lithium Ascorbate

Indicators of Red Blood and T-Lymphocytes in Patients With Alcoholism; Protective Potential of Lithium Ascorbate

Chronic intermittent ethanol exposure selectively increases synaptic excitability in the ventral domain of the rat hippocampus

The CRF-R1 regulation of VTA-GABAergic plasticity is suppressed by CB1 receptor inhibition following chronic exposure to ethanol

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