Variation at the rat
            <i>Crhr1</i>
            locus and sensitivity to relapse into alcohol seeking induced by environmental stress

Hansson, A C; Cippitelli, Andrea; Sommer, Wolfgang; Fedeli, Amalia; Björk, Karl; Soverchia, Laura; Terasmaa, Anton; Massi, Maurizio; Heilig, Markus; Ciccocioppo, Roberto

doi:10.1073/pnas.0604419103

Cited by 241 publications

(312 citation statements)

References 32 publications

(34 reference statements)

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“…2 [6,23]. As predicted from the allostatic concept of addiction (Box 1) we found upregulated CRH activity in the central amygdala of postdependent animals during acute withdrawal and many weeks thereafter, contributing to increased ethanol intake, anxiety, and ethanol-seeking behavior, all of which can be alleviated by blockade of CRH 1 receptors [6,[23][24][25][26]. In fact, the excessive ethanol consumption appears to be a means to downregulate amygdala CRH 1 receptors [27].…”

Section: Introductionsupporting

confidence: 51%

Targeting brain angiotensin and corticotrophin-releasing hormone systems interaction for the treatment of mood and alcohol use disorders

Sommer

Saavedra

2008

J Mol Med

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The brain renin-angiotensin system (RAS) participates importantly in the regulation of endocrine, autonomic, and behavioral response to stress. Recent data indicate that central action of AT 1 receptor antagonists can reduce anxiety symptoms in experimental animals. Furthermore, central inhibition of RAS activity decreases ethanol intake in an animal model of alcoholism. Pathological anxiety responses and the development of substance dependence are both critically mediated through corticotrophin-releasing hormone (CRH) systems, and the RAS is positioned to interact both with hypothalamic as well as extrahypothalamic CRH systems. The thesis of this paper is that the RAS is part of the neurochemical dysregulation underlying negative affective states, anxiety disorders, and ethanol dependence and that medications targeting the RAS should be considered to augment the treatment of these disorders.

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Section: Introductionsupporting

confidence: 51%

Targeting brain angiotensin and corticotrophin-releasing hormone systems interaction for the treatment of mood and alcohol use disorders

Sommer

Saavedra

2008

J Mol Med

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“…A 15-min electric (1.0 mA current intensity) footshock stress was delivered via the grid floor of the chamber under a variable-interval 40-s schedule (interval range: 10-70 s). We choose 1.0 mA because in a previous study (Hansson et al 2006), we showed that in Wistar rats, the maximum level of responding is obtained at this current intensity. After termination of footshock, the levers were extended into the chambers, and responses were recorded for 30 min.…”

Section: Footshock Stress-induced Reinstatementmentioning

confidence: 99%

Increase of brain endocannabinoid anandamide levels by FAAH inhibition and alcohol abuse behaviours in the rat

et al. 2008

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Rationale A major clinical concern with the use of cannabinoid receptor 1 (CB1) direct agonists is that these compounds increase alcohol drinking and drug abuserelated behaviours. As an alternative approach, CB1-receptor-mediated activity can be facilitated by increasing anandamide levels with the use of hydrolase fatty acid amide hydrolase (FAAH) inhibitors. Objective Using the selective FAAH inhibitor URB597, we investigated whether activation of the endogenous cannabinoid tone increases alcohol abuse liability, as what happens with the CB1 receptor direct agonists.Materials and methods URB597 was tested on alcohol self-administration in Wistar rats and on homecage alcohol drinking in genetically selected Marchigian Sardinian alcohol-preferring (msP) rats. In Wistar rats, URB597 effects on alcohol-induced anxiety and on stress-, yohimbineand cue-induced reinstatement of alcohol seeking were also evaluated. For comparison, the effect of the CB1 receptor antagonist rimonabant on ethanol self-administration was also tested. Results Under our experimental condition, intraperitoneal (IP) administration of URB597 (0.0, 0.3 and 1.0 mg/kg) neither increased voluntary homecage alcohol drinking in msP rats nor facilitated fixed ratio 1 and progressive ratio alcohol self-administration in nonselected Wistars. In the reinstatement tests, the compound did not have effects on cue-, footshock stress-and yohimbine-induced relapse. Conversely, URB597 completely abolished the anxiogenic response measured during withdrawal after an acute IP administration of alcohol (3.0 g/kg). Rimonabant (0.0, 0.3, 1.0 and 3.0 mg/kg) significantly reduced ethanol self-administration. Conclusions Results demonstrate that activation of the endocannabinoid anandamide system by selective inhibition of FAAH does not increase alcohol abuse risks but does reduce anxiety associated to alcohol withdrawal. We thus can speculate that medication based on the use of endocannabinoid system modulators such as URB597 may offer important advantages compared to treatment with direct CB1 receptor activators.

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“…For various endocrine-independent effects of chronic EtOH, more profound effects of CRF 1 receptor manipulations have been described in postdependent animals and in animals that were selectively bred for elevated EtOH preference (54,58,59). CRF 1 receptor antagonists can reduce levels of intake of postdependent animals to the levels observed in nondependent ones (54,58,59).…”

Section: Discussionmentioning

confidence: 99%

“…Given the comorbidity of drug addiction with affective disorders, CRF systems have been suggested as potential common targets for their treatment (50,53). Regarding alcoholism, human and rodent data support a genetically determined relationship between central CRF function and EtOH consumption (54)(55)(56)(57). EtOH-induced longterm neuroadaptations responsible for increased EtOH intake and stress-evoked relapse-like behavior in EtOH-dependent animals withdrawn from EtOH have also been linked to CRF function (54,58,59), and repeated EtOH exposure sensitizes the response to the activating effects of a central CRF administration (40).…”

Section: Deletion Of Ucn 1 Does Not Prevent Psychomotor Sensitizationmentioning

confidence: 99%

Corticotropin-releasing factor-1 receptor involvement in behavioral neuroadaptation to ethanol: A urocortin ₁ -independent mechanism

Pastor

McKinnon

Scibelli

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

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A common expression of neuroadaptations induced by repeated exposure to addictive drugs is a persistent sensitized behavioral response to their stimulant properties. Neuroplasticity underlying drug-induced sensitization has been proposed to explain compulsive drug pursuit and consumption characteristic of addiction. The hypothalamic-pituitary-adrenal (HPA) axis-activating neuropeptide, corticotropin-releasing factor (CRF), may be the keystone in drug-induced neuroadaptation. Corticosterone-activated glucocorticoid receptors (GRs) mediate the development of sensitization to ethanol (EtOH), implicating the HPA axis in this process. EtOHinduced increases in corticosterone require CRF activation of CRF1 receptors. We posited that CRF1 signaling pathways are crucial for EtOH-induced sensitization. We demonstrate that mice lacking CRF1 receptors do not show psychomotor sensitization to EtOH, a phenomenon that was also absent in CRF 1 ؉ 2 receptor doubleknockout mice. Deletion of CRF2 receptors alone did not prevent sensitization. A blunted endocrine response to EtOH was found only in the genotypes showing no sensitization. The CRF1 receptor antagonist CP-154,526 attenuated the acquisition and prevented the expression of EtOH-induced psychomotor sensitization. Because CRF1 receptors are also activated by urocortin-1 (Ucn1), we tested Ucn1 knockout mice for EtOH sensitization and found normal sensitization in this genotype. Finally, we show that the GR antagonist mifepristone does not block the expression of EtOH sensitization. CRF and CRF1 receptors, therefore, are involved in the neurobiological adaptations that underlie the development and expression of psychomotor sensitization to EtOH. A CRF/CRF1-mediated mechanism involving the HPA axis is proposed for acquisition, whereas an extrahypothalamic CRF/CRF1 participation is suggested for expression of sensitization to EtOH.addiction ͉ CP-154,526 ͉ HPA axis ͉ knockout mice ͉ psychomotor sensitization

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Variation at the rat Crhr1 locus and sensitivity to relapse into alcohol seeking induced by environmental stress

Cited by 241 publications

References 32 publications

Targeting brain angiotensin and corticotrophin-releasing hormone systems interaction for the treatment of mood and alcohol use disorders

Targeting brain angiotensin and corticotrophin-releasing hormone systems interaction for the treatment of mood and alcohol use disorders

Increase of brain endocannabinoid anandamide levels by FAAH inhibition and alcohol abuse behaviours in the rat

Corticotropin-releasing factor-1 receptor involvement in behavioral neuroadaptation to ethanol: A urocortin ₁ -independent mechanism

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Variation at the rat Crhr1 locus and sensitivity to relapse into alcohol seeking induced by environmental stress

Cited by 241 publications

References 32 publications

Targeting brain angiotensin and corticotrophin-releasing hormone systems interaction for the treatment of mood and alcohol use disorders

Targeting brain angiotensin and corticotrophin-releasing hormone systems interaction for the treatment of mood and alcohol use disorders

Increase of brain endocannabinoid anandamide levels by FAAH inhibition and alcohol abuse behaviours in the rat

Corticotropin-releasing factor-1 receptor involvement in behavioral neuroadaptation to ethanol: A urocortin 1 -independent mechanism

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Corticotropin-releasing factor-1 receptor involvement in behavioral neuroadaptation to ethanol: A urocortin ₁ -independent mechanism