Alcoholism Clinical Trial
Official title:
Alcohol Self Administration Laboratory
This is a pilot study in which our intent is to establish an alcohol administration laboratory in which we will be able to test the effect of the anticonvulsant medication zonisamide as compared to placebo on alcohol self administration and on cognitive functioning in non treatment seeking heavy users of alcohol. Our first goal is to establish the safety of zonisamide when used together with alcohol. Our second goal is to test the effect of an acute dose of zonisamide on alcohol consumption and show that it may reduce the consumption of alcohol. To achieve this goal we seek subjects with a history of heavy drinking to be tested on the self-administration procedures described below in two sessions with either zonisamide or placebo. These procedures will involve first, the administration of a challenge dose of ethanol to evaluate the effect of alcohol on performance on neuropsychological tests. This initial challenge will be followed by a period of alcohol self-administration in which the research subject can choose to select either ethanol or another reinforcer, money.
In preclinical studies three novel anticonvulsants have been studied. The administration of
tiagabine did not decrease ethanol consumption in rodents (Schmitt et al., 2002; Rimondini
et al., 2002). In a study with alcohol preferring mice topiramate reduced alcohol
consumption in a two bottle choice prolonged access model of drinking (Gabriel and
Cunningham, 2005). In a study done at our laboratory both topiramate and zonisamide were
found to have similar effects on reducing the consumption of ethanol in Wistar rat (Knapp et
al., 2004). More recently we found that zonisamide administration decreased alcohol
consumption in a limited access model in the C57BL/B6 mouse. These results suggest that
zonisamide might be useful as a medication for the treatment of alcohol dependence.
Topiramate and zonisamide have some structural similarities with a sulfamate or
methane-sulfonamide containing chain respectively attached to cyclic structure. These
structural similarities may explain some of their pharmacological similarities including
blockade of voltage sensitive sodium channels and low potency inhibition of carbonic
anhydrase (Taverna et al., 1999; Dodgson et al., 2000; Schaf et al., 1987; Masudaet al.,
1993). Both topiramate and zonisamide promote weight loss (McElroy et al., 2003; McElroy et
al., 2004; Gadde et al., 2003). This effect may be a result of neuromodulation of the
regulation of alcohol and food shared by these drugs.
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Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Investigator)
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