Presynaptic Ethanol Actions: Potential Roles in Ethanol Seeking

Lovinger, David M.

doi:10.1007/164_2017_76

Cited by 19 publications

(13 citation statements)

References 151 publications

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“…While there have been conflicting reports 29 , it has been suggested that low alcohol concentrations influence the activity of δ-containing GABA A receptors in recombinant receptor systems as well as in slices 9–11,30,31 . However, it is also likely that the well-documented effects of ethanol on presynaptic GABA release 15–17 and/or increases in neurosteroid levels 18–20,32 may indirectly mediate the effects of ethanol on these receptors. Regardless, global deletion of the Gabrd gene was found to be associated with reduced 24 hr alcohol consumption and preference in males and females 12 .…”

Section: Discussionmentioning

confidence: 99%

“…GABA receptors containing the γ2 subunit, which mediate phasic inhibition, respond to high alcohol concentrations; whereas, δ-containing GABA A receptors, which mediate tonic inhibition, have been suggested to respond to low/moderate alcohol concentrations 11–13 . The role of extrasynaptic GABA A Rs in conferring sensitivity to alcohol has been proposed to be due to direct effects on these receptors 14 , but may also be mediated indirectly via changes in presynaptic GABA release 15–17 or ethanol-induced increases in neurosteroids 18–20 that potentiate the effects of GABA on these extrasynaptic receptor subtypes 21 . Whether the δ subunit is necessary for the behavioral effects of alcohol concentrations achieved in an active binge drinking session remains unknown, although the global loss of these receptors has been shown to reduce alcohol intake and alcohol preference 12 .…”

Section: Introductionmentioning

confidence: 99%

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Female-specific decreases in alcohol binge-like drinking resulting from GABAA receptor delta-subunit knockdown in the VTA

Darnieder

Melón

et al. 2019

Sci Rep

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Binge drinking is short-term drinking that achieves blood alcohol levels of 0.08 g/dl or above. It exhibits well-established sex differences in GABAergic inhibitory neurotransmission, including extrasynaptic δ subunit-containing GABA A receptors (δ-GABA A Rs) that mediate tonic inhibition, or synaptic γ2-containing GABA A Rs which underlie fast, synaptic, phasic inhibition have been implicated in sex differences in binge drinking. Ovarian hormones regulate δ-GABA A Rs, further implicating these receptors in potential sex differences. Here, we explored the contribution of extrasynaptic δ-GABA A Rs to male and female binge-like drinking in a critical area of mesolimbic circuitry—the ventral tegmental area (VTA). Quantitative PCR revealed higher Gabrd transcript levels and larger tonic currents in the VTA of females compared to males. In contrast, male and female Gabrg 2 transcript levels and measures of phasic inhibition were equivalent. Intra-VTA infusion of AAV-Cre-GFP in floxed Gabrd mice downregulated δ-GABA A Rs and decreased binge-like drinking in females. There was no significant difference in either male or female mice after GABA A R γ2 subunit reduction in the VTA following AAV-Cre-GFP infusion in floxed Gabrg2 mice. Collectively, these findings suggest sex differences and GABA A R subunit specificity in alcohol intake.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Female-specific decreases in alcohol binge-like drinking resulting from GABAA receptor delta-subunit knockdown in the VTA

Darnieder

Melón

et al. 2019

Sci Rep

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“…20 Acutely, alcohol promotes GABA release and may also reduce GABA degradation, producing sedative and anxiolytic effects. 21 Chronic alcohol use leads to a decrease in the number of GABA A receptors. Clinically, this downregulation manifests as tolerance to alcohol's sedating effects.…”

Section: Modesto-lowe and Colleagues ■ Alcohol's Actionsmentioning

confidence: 99%

“…Clinically, this downregulation manifests as tolerance to alcohol's sedating effects. 21 Alcohol affects the signaling of glutamatergic interaction with the N-methyl-d-aspartate (NMDA) receptor. 22 Glutamate activates this receptor as well as the voltage-gated ion channels, modifying calcium infl ux and increasing neuronal excitability.…”

Section: Modesto-lowe and Colleagues ■ Alcohol's Actionsmentioning

confidence: 99%

Gabapentin for alcohol use disorder: A good option, or cause for concern?

Modesto‐Lowe

Barron

Aronow

et al. 2019

CCJM

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P erceptions regarding the use of gabapentin for alcohol use disorder (AUD) have shifted over time. 1-4 Early on, the drug was deemed to be benign and effective. 4-6 But more and more, concerns are being raised about its recreational use to achieve euphoria, 7 and the drug is often misused by vulnerable populations, particularly those with opioid use disorder. 7-9 Given the large number of gabapentin prescriptions written off-label for AUD, it is incumbent on providers to understand how to prescribe it responsibly. 7-9 To that end, this article focuses on the benefi tsand concerns-of this treatment option. We describe the effects of gabapentin on the central nervous system and how it may mitigate alcohol withdrawal and increase the likelihood of abstinence. In addition, we review clinical trials that evaluated potential roles of gabapentin in AUD, discuss the drug's misuse potential, and suggest a framework for its appropriate use in AUD management. ■ ALCOHOL USE DISORDER IS COMMON AND SERIOUS AUD affects about 14% of US adults and represents a signifi cant health burden, 1 often with severe clinical and social implications. It manifests as compulsive drinking and loss of control despite adverse consequences on various life domains. 10 It is generally associated with cravings, tolerance, and withdrawal symptoms upon cessation. Alcohol withdrawal is characterized by tremors, anxiety, sweating, nausea, and tachycardia, and in severe cases, may involve hallucinations, seizures, and delirium tremens. Untreated, alcohol withdrawal can be fatal. 10

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“…For example, loss of endocannabinoid-dependent LTD is observed following exposure to several drugs in addition to ethanol (Mato et al 2005;Xia et al 2006;Adermark et al 2011;Atwood et al 2014a). However, the mechanisms underlying these effects are likely to be different, as cannabinoid drugs down-regulate receptor function, while EtOH may have a more general effect on intraterminal signaling mechanisms involved in presynaptic LTD (Hoffman et al 2003;Mato et al 2005;Lovinger 2017). Given the different primary molecular targets of ethanol and other drugs of abuse, it is likely that compensatory plasticity involving changes in these target molecules would also differ for the different substances.…”

Section: Future Directionsmentioning

confidence: 99%

Synaptic plasticity mechanisms common to learning and alcohol use disorder

Lovinger

Abrahao

2018

Learn. Mem.

Self Cite

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Alcohol use disorders include drinking problems that span a range from binge drinking to alcohol abuse and dependence. Plastic changes in synaptic efficacy, such as long-term depression and long-term potentiation are widely recognized as mechanisms involved in learning and memory, responses to drugs of abuse, and addiction. In this review, we focus on the effects of chronic ethanol (EtOH) exposure on the induction of synaptic plasticity in different brain regions. We also review findings indicating that synaptic plasticity occurs in vivo during EtOH exposure, with a focus on ex vivo electrophysiological indices of plasticity. Evidence for effects of EtOH-induced or altered synaptic plasticity on learning and memory and EtOH-related behaviors is also reviewed. As this review indicates, there is much work needed to provide more information about the molecular, cellular, circuit, and behavioral consequences of EtOH interactions with synaptic plasticity mechanisms.

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Presynaptic Ethanol Actions: Potential Roles in Ethanol Seeking

Cited by 19 publications

References 151 publications

Female-specific decreases in alcohol binge-like drinking resulting from GABAA receptor delta-subunit knockdown in the VTA

Female-specific decreases in alcohol binge-like drinking resulting from GABAA receptor delta-subunit knockdown in the VTA

Gabapentin for alcohol use disorder: A good option, or cause for concern?

Synaptic plasticity mechanisms common to learning and alcohol use disorder

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