Viral-Mediated Knockdown of mGluR7 in the Nucleus Accumbens Mediates Excessive Alcohol Drinking and Increased Ethanol-Elicited Conditioned Place Preference in Rats

Bahí, Amine

doi:10.1038/npp.2012.122

Cited by 28 publications

(34 citation statements)

References 68 publications

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“…Dentro de los modelos animales de refuerzo utilizados para evaluar la preferencia que lleva a un sujeto a consumir encontramos el paradigma de consumo voluntario: sistema de dos botellas, más conocido por su término en inglés "two-bottle choice". Existen diferentes modalidades o variedades dentro de dicho procedimiento pero el objetivo principal del mismo es medir la preferencia del animal por la sustancia de abuso (normalmente alcohol) y su consumo oral frente a otra sustancia no adictiva (como el agua) (Bahi, 2012(Bahi, , 2013a(Bahi, , 2013b. Para medir esta preferencia los animales son expuestos a ambas sustancias durante días, ofreciéndoseles la posibilidad de beber únicamente agua, únicamente alcohol o ambas sustancias al mismo tiempo.…”

Section: Modelos De Consumo Libreunclassified

Modelos animales de adicción a las drogas

et al. 2017

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Resumen Abstract adicciones vol. 29, nº 4 · 2017 revisión Modelos animales de adicción a las drogas Animal Models of Drug AddictionMaría Pilar García Pardo*,**; Concepción Roger Sánchez*; José Enrique de la Rubia Ortí**; María Asunción Aguilar Calpe*. En los últimos años los modelos han incorporado modificaciones metodológicas para incluir el estudio de los procesos de extinción, reinstauración y reconsolidación o para modelar aspectos concretos de la conducta adictiva como puede ser la motivación para consumir la droga, el consumo compulsivo o la búsqueda de la droga bajo situaciones de castigo. Otros modelos interrelacionan diferentes componentes del refuerzo o modelan la motivación voluntaria por consumir (modelos de "two-bottle choice" o "drinking in the dark").En definitiva, las innovaciones en estos modelos contribuyen al avance en el conocimiento científico de los diferentes factores que llevan a tomar una droga y a desarrollar un consumo compulsivo, ofreciendo una vía para identificar futuros tratamientos para la adicción.Palabras clave: Refuerzo; Adicción; Modelos animales; Drogas de abuso.

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Section: Modelos De Consumo Libreunclassified

Modelos animales de adicción a las drogas

et al. 2017

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“…Cells were harvested 72 h later and viruses were concentrated from the supernatant by ultracentrifugation. Vectors were resuspended in PBS-BSA and stored at À80 C until use (Bahi, 2013;Bahi and Dreyer, 2013). The three distinct Drd1a-siRNA sequences were successfully used to knock-down the expression Drd1a mRNA in the NAc (Bahi and Dreyer, 2012) and proteins in the hippocampus (Ortiz et al, 2010).…”

Section: Construction and Validation Of Lv-drd1a-sirnasmentioning

confidence: 99%

Impairment of acquisition of intravenous cocaine self-administration by RNA-interference of dopamine D1-receptors in the nucleus accumbens shell

et al. 2015

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Microdialysis during i.v. drug self-administration (SA) have implicated nucleus accumbens (NAc) shell DA in cocaine and heroin reinforcement. However, this correlative evidence has not been yet substantiated by experimental evidence obtained by studying the effect of selective manipulation of NAc shell DA transmission on cocaine and heroin SA. In order to investigate this issue, DA D1a receptor (D1aR) expression was impaired in the NAc shell and core by locally infusing lentiviral vectors (LV) expressing specific D1aR-siRNAs (LV-siRNAs). Control rats were infused in the same areas with LV expressing GFP. Fifteen days later, rats were trained to acquire i.v. cocaine or heroin self-administration (SA). At the end of behavioral experiments, in order to evaluate the effect of LV-siRNA on D1aR expression, rats were challenged with amphetamine and the brains were processed for immunohistochemical detection of cFos and D1aR. Control rats acquired i.v. cocaine and heroin SA. Infusion of LV-siRNAs in the medial NAc shell reduced D1aR density and the number of c-Fos positive nuclei in the NAc shell, while sparing the core, and prevented the acquisition of cocaine, but not heroin SA. In turn, LV-siRNAs infusion in the core reduced D1aR density and the number of c-Fos positive nuclei in the same area, while sparing the shell, and failed to affect acquisition of cocaine. The differential effect of LV impairment of NAc shell D1aR on cocaine and heroin SA indicates that NAc shell DA acting on D1aR specifically mediates cocaine reinforcement.

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“…The typical two-bottle choice drinking paradigm procedure described previously (Bahi 2013) was used with minor modifications. In brief, the rats were weighed and given access to two-bottles, one containing tap water and the other containing 5% ethanol.…”

Section: Continuous Access To Alcohol In Two-bottle Choice Drinking Pmentioning

confidence: 99%

“…The tubes were centrifuged and the plasma was separated and stored at −20°C. BECs were measured in milligrams per deciliter (BioVision Research Products, CA, USA) as described previously (Bahi 2013). …”

Section: Blood Ethanol Concentrationmentioning

confidence: 99%

Viral-mediated overexpression of the Myelin Transcription Factor 1 (MyT1) in the dentate gyrus attenuates anxiety- and ethanol-related behaviors in rats

Bahí

Dreyer

2017

Psychopharmacology

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Rationale Myelin Transcription Factor 1 (MyT1), a member of the Zinc Finger gene family, plays a fundamental role in the nervous system. Recent research has suggested that this transcription factor is associated with the pathophysiology of psychiatric disorders including addiction, schizophrenia, and depression. However, the role of MyT1 in anxiety-and ethanolrelated behaviors is still unknown. Objectives We evaluated the effects of lentiviral-mediated overexpression of MyT1 in the dentate gyrus (DG) on anxiety-and ethanol-related behaviors in rats. Methods We used the elevated plus maze (EPM) and the open field (OF) tests to assess anxiety-like behavior and a twobottle choice procedure to measure the effects of MyT1 on ethanol intake and preference. Results MyT1 overexpression produced anxiolytic-like effects in the EPM test and decreased the number of fecal boli in the OF test, without affecting locomotor activity in both behavioral tests. Next, we demonstrated that ethanol intake and preference were decreased in the MyT1-overexpressing rats with no effect on saccharin and quinine, used to assess taste discrimination, and no effect on ethanol clearance suggesting specific alterations in the rewarding effects of ethanol.Most importantly, ectopic MyT1 overexpression increased both MyT1 and BDNF mRNA levels in the DG. Using Pearson's correlation, results showed a strong negative relationship between MyT1 mRNA and anxiety parameters and ethanol consumption and a positive correlation between MyT1 and BDNF mRNAs. Conclusion Taken together, MyT1 along with being a key component in anxiety may be a suitable candidate in the search of the molecular underpinnings of alcoholism.

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Viral-Mediated Knockdown of mGluR7 in the Nucleus Accumbens Mediates Excessive Alcohol Drinking and Increased Ethanol-Elicited Conditioned Place Preference in Rats

Cited by 28 publications

References 68 publications

Modelos animales de adicción a las drogas

Modelos animales de adicción a las drogas

Impairment of acquisition of intravenous cocaine self-administration by RNA-interference of dopamine D1-receptors in the nucleus accumbens shell

Viral-mediated overexpression of the Myelin Transcription Factor 1 (MyT1) in the dentate gyrus attenuates anxiety- and ethanol-related behaviors in rats

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