2011
DOI: 10.1007/s00213-011-2253-0
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Severity of drinking as a predictor of efficacy of the combination of ondansetron and topiramate in rat models of ethanol consumption and relapse

Abstract: Rationale Alcohol dependence is the third leading cause of preventable death in the USA. While single-agent pharmacotherapies have variable efficacy, medication combinations may produce additive effects by modulating multiple neural pathways. Objectives Here, we examined in animal models of ethanol consumption and relapse the combined effects of ondansetron (a serotonin-3 antagonist) and topiramate (a GABA/ glutamate modulator), two medications with demonstrated efficacy for treating alcohol dependence, hypo… Show more

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Cited by 29 publications
(35 citation statements)
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“…All compounds were dissolved in 0.9% sodium chloride and sterile water. Doses of naltrexone (1 mg/kg) and topiramate (10, 20 g/kg) were chosen based on previous studies demonstrating the ability of these doses to reduce ethanol consumption/reinforcement in male P rats (Lynch et al 2011; Moore et al 2014). …”
Section: Methodsmentioning
confidence: 99%
“…All compounds were dissolved in 0.9% sodium chloride and sterile water. Doses of naltrexone (1 mg/kg) and topiramate (10, 20 g/kg) were chosen based on previous studies demonstrating the ability of these doses to reduce ethanol consumption/reinforcement in male P rats (Lynch et al 2011; Moore et al 2014). …”
Section: Methodsmentioning
confidence: 99%
“…And, GABA A and GABA B receptors mediate some of the rewarding, reinforcing, and motivational effects of alcohol consumption and alcohol binge drinking (Eiler & June, 2007; Nowak, McBride, Lumeng, Li, & Murphy, 1998; Tanchuck, Yoneyama, Ford, Fretwell, & Finn, 2011; also see Agabio & Colombo, 2014). Systemically, the GABA A agonist topiramate (Breslin, Johnson, & Lynch, 2010; Lynch, Bond, Breslin, & Johnson, 2011) and GABA B agonist baclofen (Liang et al, 2006; Maccioni et al, 2012) and GABA B positive modulators GHB (June et al, 1995), CGP7930 (Liang et al, 2006) and GS39783 (Maccioni et al, 2012) all reduced ethanol drinking and/or self-administration by P rats. Similarly, negative modulators of the benzodiazepine-site Ro 15-4513 (McBride, Murphy, Lumeng, & Li, 1988), Ro 19-4603 (June et al, 1996; June, Murphy, Mellor-Burke, Lumeng, & Li, 1994; June, Torres, et al, 1998), Ru 34000 (June, Eggers, et al, 1998), Ro 15-1788 (June et al, 1994; June, Torres, et al, 1998), CGS 8216 and ZK 93426 (June, Devaraju, et al, 1998; June, Zuccarelli, et al, 1998) all reduced ethanol intake and/or self-administration by P rats.…”
Section: Some Neurochemical Neuropharmacological As Well As Neurmentioning
confidence: 99%
“…Topiramate is often used, off-label, as a treatment for alcoholism, and inhibits glutamate release and blocks L-alpha-amino-3-hydroxy-5-methyl-isoxazole-4-propionic acid ionotropic (AMPAR)/ kainate receptors (KAR) as part of a complex pharmacological profile. In rodents, topiramate promotes alcohol intoxication and reduces alcohol drinking and withdrawal, but does not disrupt alcohol place preference (Breslin et al 2010; Cagetti et al 2004; Chen and Holmes 2009; Farook et al 2007; Gremel et al 2006; Hargreaves and McGregor 2007; Knapp et al 2007; Lynch et al 2011; Nguyen et al 2007; Zalewska-Kaszubska et al 2013). Topiramate also reduces craving, withdrawal and drinking in alcoholics (Baltieri et al 2008; Florez et al 2008; Johnson et al 2004; Johnson et al 2003a; Johnson et al 2007; Komanduri 2003; Krupitsky et al 2007b; Miranda et al 2008; Paparrigopoulos et al 2011; Rubio et al 2004; Rustembegovic et al 2002).…”
Section: Glutamate Signaling As a Target For New Alcoholism Treatmentsmentioning
confidence: 99%