An interaction between serotonin receptor signaling and dopamine enhances goal-directed vigor and persistence in mice

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Abstract

The functionally selective 5-HT2C receptor ligand SB242084 can increase motivation and have rapid onset anti– depressant-like effects. We sought to identify the specific behavioral effects of SB242084 treatment and elucidate the mechanism in female and male mice. Using a quantitative behavioral approach, we determined that SB242084 increases the vigor and persistence of goal-directed activity across different types of physical work, particularly when work requirements are demanding. We found this influence of SB242084 on effort, rather than reward to be reflected in striatal DA measured during behavior. Using in vivo fast scan cyclic voltammetry, we found that SB242084 has no effect on reward-related phasic DA release in the NAc. Using in vivo microdialysis to measure tonic changes in extracellular DA, we also found no changes in the NAc. In contrast, SB242084 treatment increases extracellular DA in the dorsomedial striatum, an area that plays a key role in response vigor. These findings have several implications. At the behavioral level, this work shows that the capacity to work in demanding situations can be increased, without a generalized increase in motor activity or reward value. At the circuit level, we identified a pathway restricted potentiation of DA release and showed that this was the reason for the increased response vigor. At the cellular level, we show that a specific serotonin receptor cross talks to the DA system. Together, this information provides promise for the development of treatments for apathy, a serious clinical condition that can afflict patients with psychiatric and neurological disorders.

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Bailey, M. R., Goldman, O., Bello, E. P., Chohan, M. O., Jeong, N., Winiger, V., … Simpson, E. H. (2018). An interaction between serotonin receptor signaling and dopamine enhances goal-directed vigor and persistence in mice. Journal of Neuroscience, 38(9), 2149–2162. https://doi.org/10.1523/JNEUROSCI.2088-17.2018

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