Key Role of Ethanol‐Derived Acetaldehyde in the Motivational Properties Induced by Intragastric Ethanol: A Conditioned Place Preference Study in the Rat

Peana, Alessandra Tiziana; Enrico, Paolo; Assaretti, A.; Pulighe, Elena; Muggironi, Giulia; Nieddu, Maria; Piga, Antonio; Lintas, Alessandra; Diana, Marco

doi:10.1111/j.1530-0277.2007.00574.x

Cited by 73 publications

(119 citation statements)

References 48 publications

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“…Similar research has been completed using the compound D-penicillamine, which acts to sequester ACD into a non-reactive stable adduct but does not alter EtOH metabolism. Studies using D-penicillamine have established that sequestering ACD results in a reduction of alcohol intake and a decrease in alcohol conditioned place preference in rats Font et al, 2006b;Peana et al, 2008). D-penicillamine also reduces alcohol conditioned place preference and alcohol induced motor depression in mice (Font et al, 2005;Font et al, 2006a).…”

Section: Alcohol Acetaldehyde and Acetaldehyde Productsmentioning

confidence: 99%

“…Research has shown that both central and peripheral administration of ACD cause an increase in alcohol consumption in rats (Brown et al, 1979;. Rats will exhibit ACD induced CPP and stimulus preference suggesting that ACD is rewarding (Quertemont & De Witte, 2001;Quintanilla & Tampier, 2003;Smith et al, 1984;Spina et al, 2010); blocking or sequestering the formation of ACD resulting from alcohol exposure produces alterations in the neurobiological and behavioral effects of alcohol (Aragon & Amit, 1992;Diana et al, 2008;Font et al, 2005;Font et al, 2006a;Font et al, 2006b;Kaharanian et al, 2011;Koechling & Amit, 1994;Peana et al, 2008). While it is currently difficult to assert that ACD is absolutely necessary for the neurobiological and behavioral actions of alcohol, data show that ACD is likely to be involved to some extent.…”

Section: Acetaldehyde Is Pharmacologically Active In the Cnsmentioning

confidence: 99%

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What is in that Drink: The Biological Actions of Ethanol, Acetaldehyde, and Salsolinol

Deehan

Brodie

Rodd

2011

Behavioral Neurobiology of Alcohol Addiction

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Alcohol abuse and alcoholism represent substantial problems that affect a large portion of individuals throughout the world. Extensive research continues to be conducted in an effort to identify the biological basis of the reinforcing properties of alcohol in order to develop effective pharmacotherapeutic and behavioral interventions. One theory that has developed within the alcohol field over the past 4 decades postulates that the reinforcing properties of alcohol are due to the action of the metabolites/products of alcohol within the central nervous system (CNS). The most extreme version of this theory suggests that the biologically active metabolites/products of alcohol, created from the breakdown from alcohol, are the ultimate source of the reinforcing properties of alcohol. The contrary theory proposes that the reinforcing properties of alcohol are mediated completely through the interaction of the ethanol molecule with several neurochemical systems within the CNS. While there are scientific findings that offer support for both of these stances, the reinforcing properties of alcohol are most likely generated through a complex series of peripheral and central effects of both alcohol and its metabolites. Nonetheless, the development of a greater understanding for how the metabolites/products of alcohol contribute to the reinforcing properties of alcohol is an important factor in the development of efficacious pharmacotherapies for alcohol abuse and alcoholism. This chapter is intended to provide a historical perspective of the role of acetaldehyde (the first metabolite of alcohol) in alcohol reinforcement as well as review the basic research literature on the effects of acetaldehyde (and acetaldehyde metabolites/products) within the CNS and how these function with regard to alcohol reward.

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Section: Alcohol Acetaldehyde and Acetaldehyde Productsmentioning

confidence: 99%

Section: Acetaldehyde Is Pharmacologically Active In the Cnsmentioning

confidence: 99%

What is in that Drink: The Biological Actions of Ethanol, Acetaldehyde, and Salsolinol

Deehan

Brodie

Rodd

2011

Behavioral Neurobiology of Alcohol Addiction

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“…For that reason, over the last two decades, repeated proposals have suggested that acetaldehyde derived from the ethanol metabolism generated by the activity of this enzyme plays a role in some of the effects observed after ethanol administration (for extensive reviews, see Quertemont et al 2005;Hipólito et al 2007;Deng and Deitrich 2008). In fact, it has been proven that treatment with acetaldehyde-sequestering agents, after ethanol administration, modifies some ethanol-induced behaviors (Font et al 2005(Font et al , 2006aPeana et al 2008Peana et al , 2009Martí-Prats et al 2010;Pautassi et al 2011). Based on these findings, we speculate that the effect of LA on ethanol-stimulated locomotion is due to a reduction in H 2 O 2 levels, and therefore a lower central rate of acetaldehyde formation owing to a decrease in brain catalase-H 2 O 2 system activity.…”

Section: Discussionmentioning

confidence: 96%

Alpha-lipoic acid, a scavenging agent for H2O2, reduces ethanol-stimulated locomotion in mice

Ledesma

Aragón

2011

Psychopharmacology

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Registro de acceso restringido Este recurso no está disponible en acceso abierto por política de la editorial. No obstante, se puede acceder al texto completo desde la Universitat Jaume I o si el usuario cuenta con suscripción. Registre d'accés restringit Aquest recurs no està disponible en accés obert per política de l'editorial. No obstant això, es pot accedir al text complet des de la Universitat Jaume I o si l'usuari compta amb subscripció. Restricted access item This item isn't open access because of publisher's policy. The full--text version is only available from Jaume I University or if the user has a running suscription to the publisher's contents.

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“…Acetaldehyde was also shown to decrease in vivo acetylcholine release in the medial frontal cortex of freely moving rats (Jamal et al 2007b) and to increase in vitro hypothalamic release of β-endorphins (Reddy and Sarkar 1993). In addition, centrally administered or formed acetaldehyde can produce effects similar to ethanol, including increases in locomotion (Arizzi-LaFrance et al 2006;Correa et al 2003) and lever pressing on a low-rate operant schedule , intracranial selfadministration (Brown et al 1979(Brown et al , 1980Rodd-Henricks et al 2002;Rodd et al 2005), and place preference (Smith et al 1984;Peana et al 2008).…”

Section: Discussionmentioning

confidence: 97%

“…These effects appear to include some of the emotional and motivational actions that can support ethanol consumption, such as anxiolysis, motor-energizing properties, and preference for a place previously paired with ethanol (Correa et al 2005;Peana et al 2008).…”

Section: Discussionmentioning

confidence: 97%

Reduction in the anxiolytic effects of ethanol by centrally formed acetaldehyde: the role of catalase inhibitors and acetaldehyde-sequestering agents

et al. 2008

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Thus, when cerebral metabolism of ethanol into acetaldehyde is blocked by catalase inhibitors, or acetaldehyde is inactivated, there is a suppressive effect on the anxiolytic actions of ethanol. These data provide further support for the idea that centrally formed or administered acetaldehyde can contribute to some of the psychopharmacological actions of ethanol, including its anxiolytic properties.

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Key Role of Ethanol‐Derived Acetaldehyde in the Motivational Properties Induced by Intragastric Ethanol: A Conditioned Place Preference Study in the Rat

Cited by 73 publications

References 48 publications

What is in that Drink: The Biological Actions of Ethanol, Acetaldehyde, and Salsolinol

What is in that Drink: The Biological Actions of Ethanol, Acetaldehyde, and Salsolinol

Alpha-lipoic acid, a scavenging agent for H2O2, reduces ethanol-stimulated locomotion in mice

Reduction in the anxiolytic effects of ethanol by centrally formed acetaldehyde: the role of catalase inhibitors and acetaldehyde-sequestering agents

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