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Orexin A/Hypocretin-1 selectively promotes motivation for positive reinforcers
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Peer Reviewed
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Author (aut): Borgland, Stephanie L.
Author (aut): Chang, Shao-Ju
Author (aut): Bowers, M. Scott
Author (aut): Thompson, Jennifer L.
Author (aut): Vittoz, Nicole M.
Author (aut): Floresco, Stan B.
Author (aut): Chou, Jonathan
Author (aut): Chen, Billy T.
Author (aut): Bonci, Antonello
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Abstract |
Abstract
Orexin A/hypocretin-1 (oxA/hcrt-1) is known to be a modulator of dopamine-dependent neuronal activity and behaviors. However, the role of this system in driving motivated behaviors remains poorly understood. Here, we show that orexin/hypocretin receptor-1 (ox/hcrt-1R) signaling is important for motivation for highly salient, positive reinforcement. Blockade of ox/hcrt-1R selectively reduced work to self-administer cocaine or high fat food pellets. Moreover, oxA/hcrt-1 strengthened presynaptic glutamatergic inputs to the ventral tegmental area (VTA) only in cocaine or high fat self-administering rats. Finally, oxA/hcrt-1-mediated excitatory synaptic transmission onto VTA neurons was not potentiated following an arousing, aversive stimulus, suggesting that oxA/hcrt-1-mediated glutamatergic synaptic transmission was potentiated selectively with highly salient positive reinforcers. These experiments provide evidence for a selective role of oxA/hcrt-1 signaling in motivation for highly salient reinforcers and may represent a unique opportunity to design novel therapies that selectively reduce excessive drive to consume positive reinforcers of high salience.
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Volume 29, Issue 36
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Physical Description Note
PUBLISHED
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DOI |
DOI
10.1523/JNEUROSCI.6096-08.2009
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0270-6474
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Use and Reproduction |
Use and Reproduction
© 2009. Society for Neuroscience.
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English
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Orexin A/Hypocretin-1 selectively promotes motivation for positive reinforcers
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