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Discriminative aversive learning and amygdala responsivity is enhanced in mice with reduced serotonin transporter activity

João Lima, Trevor Sharp, Amy M. Taylor, David M. Bannerman, View ORCID ProfileStephen B. McHugh
doi: https://doi.org/10.1101/154690
João Lima
aDepartment of Experimental Psychology, University of Oxford, Oxford, 9 South Parks Road, Oxford, UK
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Trevor Sharp
bDepartment of Pharmacology, University of Oxford, Mansfield Road, Oxford, UK
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Amy M. Taylor
aDepartment of Experimental Psychology, University of Oxford, Oxford, 9 South Parks Road, Oxford, UK
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David M. Bannerman
aDepartment of Experimental Psychology, University of Oxford, Oxford, 9 South Parks Road, Oxford, UK
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Stephen B. McHugh
aDepartment of Experimental Psychology, University of Oxford, Oxford, 9 South Parks Road, Oxford, UK
cMedical Research Council Brain Network Dynamics Unit, Mansfield Road, Oxford, UK
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  • ORCID record for Stephen B. McHugh
  • For correspondence: stephen.mchugh@psy.ox.ac.uk;
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Abstract

The serotonin (5-HT) transporter (5-HTT) regulates 5-HT availability at the synapse. Low or null 5-HTT expression results in increased 5-HT availability and has been reported to produce anxious and depressive phenotypes, although this remains highly controversial despite two decades of investigation. Paradoxically, SSRIs, which also increase 5-HT availability, reduce the symptoms of anxiety and depression. An emerging ‘network plasticity’ theory of 5-HT function argues that, rather than influencing mood directly, increasing 5-HT availability enhances learning about emotionally-significant events but evidence supporting this theory is inconclusive. Here, we tested one key prediction of this theory: that increased 5-HT availability enhances aversive learning. In experiment 1, we trained 5-HTT knock-out mice (5-HTTKO), which have increased 5-HT availability, and wild-type mice (WT) on an aversive discrimination learning task in which one auditory cue was paired with an aversive outcome whereas a second auditory cue was not. Simultaneously we recorded neuronal and hemodynamic responses from the amygdala, a brain region necessary for aversive learning. 5-HTTKO mice exhibited superior discrimination learning than WTs, and had stronger theta-frequency neuronal oscillations and larger amygdala hemodynamic responses to the aversive cues, which predicted the extent of learning. In experiment 2, we found that acute SSRI treatment (in naïve non-transgenic mice), given specifically before fear learning sessions, enhanced subsequent fear memory recall. Collectively, our data demonstrate that reducing 5-HTT activity (and thereby increasing 5-HT availability) enhances amygdala responsivity to aversive events and facilitates learning for emotionally-relevant cues. Our findings support the network plasticity theory of 5-HT function.

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Posted June 23, 2017.
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Discriminative aversive learning and amygdala responsivity is enhanced in mice with reduced serotonin transporter activity
João Lima, Trevor Sharp, Amy M. Taylor, David M. Bannerman, Stephen B. McHugh
bioRxiv 154690; doi: https://doi.org/10.1101/154690
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Discriminative aversive learning and amygdala responsivity is enhanced in mice with reduced serotonin transporter activity
João Lima, Trevor Sharp, Amy M. Taylor, David M. Bannerman, Stephen B. McHugh
bioRxiv 154690; doi: https://doi.org/10.1101/154690

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