Low-Serotonin Levels Increase Delayed Reward Discounting in Humans

Previous animal experiments have shown that serotonin is involved in the control of impulsive choice, as characterized by high preference for small immediate rewards over larger delayed rewards. Previous human studies under serotonin manipulation, however, have been either inconclusive on the effect...

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Bibliographic Details
Published inThe Journal of neuroscience Vol. 28; no. 17; pp. 4528 - 4532
Main Authors Schweighofer, Nicolas, Bertin, Mathieu, Shishida, Kazuhiro, Okamoto, Yasumasa, Tanaka, Saori C, Yamawaki, Shigeto, Doya, Kenji
Format Journal Article
LanguageEnglish
Published United States Soc Neuroscience 23.04.2008
Society for Neuroscience
Subjects
Brief Communications
Choice Behavior - physiology
Double-Blind Method
Humans
Male
Reaction Time - physiology
Reward
Serotonin - deficiency
Serotonin - metabolism
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Summary:Previous animal experiments have shown that serotonin is involved in the control of impulsive choice, as characterized by high preference for small immediate rewards over larger delayed rewards. Previous human studies under serotonin manipulation, however, have been either inconclusive on the effect on impulsivity or have shown an effect in the speed of action-reward learning or the optimality of action choice. Here, we manipulated central serotonergic levels of healthy volunteers by dietary tryptophan depletion and loading. Subjects performed a "dynamic" delayed reward choice task that required a continuous update of the reward value estimates to maximize total gain. By using a computational model of delayed reward choice learning, we estimated the parameters governing the subjects' reward choices in low-, normal, and high-serotonin conditions. We found an increase of proportion in small reward choices, together with an increase in the rate of discounting of delayed rewards in the low-serotonin condition compared with the control and high-serotonin conditions. There were no significant differences between conditions in the speed of learning of the estimated delayed reward values or in the variability of reward choice. Therefore, in line with previous animal experiments, our results show that low-serotonin levels steepen delayed reward discounting in humans. The combined results of our previous and current studies suggest that serotonin may adjust the rate of delayed reward discounting via the modulation of specific loops in parallel corticobasal ganglia circuits.
Bibliography:ObjectType-Article-2
SourceType-Scholarly Journals-1
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content type line 23
ISSN:0270-6474
1529-2401
DOI:10.1523/JNEUROSCI.4982-07.2008