Acute effects of alprazolam on risky decision making in humans |
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| Authors: | Scott?D.?Lane author-information" > author-information__contact u-icon-before" > mailto:scott.d.lane@uth.tmc.edu" title=" scott.d.lane@uth.tmc.edu" itemprop=" email" data-track=" click" data-track-action=" Email author" data-track-label=" " >Email author,Oleg?V.?Tcheremissine,Lori?M.?Lieving,Sylvain?Nouvion,Don?R.?Cherek |
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| Affiliation: | (1) Department of Psychiatry and Behavioral Sciences, UTHSC-Houston, 1300 Moursund St., Houston, TX 77030, USA;(2) Graduate School of Biomedical Sciences, University of Texas Health Science Center-Houston, Houston, TX, USA |
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| Abstract: | Rationale GABA-A receptor ligands, including benzodiapines, may induce disinhibitory effects that increase the probability of risky decision making. To date, few laboratory studies have examined the acute, dose-related effects of benzodiazepines on human risk-taking behavior. Recent data indicate that in the United States alprazolam is the benzodiazepine most frequently misused for recreational purposes. Objectives The present study was designed to demonstrate a dose–response relationship between acute alprazolam administration and human risk taking. Furthermore, this investigation sought to examine: (1) the behavioral mechanisms that may be involved in changes in the probability of risky decision making related to alprazolam administration and (2) risk seeking-related personality variables that may predict drug effects on risk taking. Methods Using a laboratory measure of risk taking designed to address acute drug effects, 16 adults were administered placebo, 0.5, 1.0, and 2.0 mg alprazolam in a within-subject repeated-measures design. The risk-taking task presented subjects with a choice between two response options operationally defined as risky and nonrisky. Data analyses examined subjective effects, response rates, distribution of choices between the risky and nonrisky option, trial-by-trial response probabilities, and personality correlates related to drug effects at the 2.0-mg dose. Results Alprazolam administration produced dose-related changes in subjective effects, response rates, and, most importantly, dose-dependently increased selection of the risky response option. The 2.0-mg dose increased the probability of making consecutive risky responses following a gain on the risky response option. Increases at 2.0 mg were related to a combination of personality scales that included high venturesomeness and novelty seeking and low harm avoidance. Conclusions Alprazolam administration produced increases in human risk taking under laboratory conditions. In union with previous studies, the observed shift in trial-by-trial response probabilities suggests that sensitivity to consequences (e.g., oversensitivity to recent rewards) may be an important mechanism in the psychopharmacology of risky decision making. Additionally, risk-seeking personality traits may be predictive of acute drug effects on risk-taking behavior. |
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| Keywords: | Alprazolam Human Risk taking Decision making Laboratory experiment GABA-A |
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