4.5 Article

The NeuroD6 Subtype of VTA Neurons Contributes to Psychostimulant Sensitization and Behavioral Reinforcement

Journal

ENEURO
Volume 6, Issue 3, Pages -

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/ENEURO.0066-19.2019

Keywords

accumbens; dopamine; mouse genetics; optogenetics; reward; ventral tegmental area

Categories

Funding

  1. Uppsala University
  2. Hjarnfonden
  3. Parkinsonfonden
  4. Research Foundation of Bertil Hallsten
  5. Vetenskapsradet (Medicine Health)
  6. European Research Council
  7. Novo Nordisk Fonden
  8. Strategic Research Programme for Diabetes Research at Karolinska Institutet
  9. National Institutes of Health [DA036612]
  10. Veterans Affairs Grant [BX003759]
  11. Research Foundation of OE Edla Johansson
  12. Research Foundation of Zoologisk Forskning
  13. Research Foundation of Ahlen

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Reward-related behavior is complex and its dysfunction correlated with neuropsychiatric illness. Dopamine (DA) neurons of the ventral tegmental area (VTA) have long been associated with different aspects of reward function, but it remains to be disentangled how distinct VTA DA neurons contribute to the full range of behaviors ascribed to the VTA. Here, a recently identified subtype of VTA neurons molecularly defined by NeuroD6 (NEX1M) was addressed. Among all VTA DA neurons, less than 15% were identified as positive for NeuroD6. In addition to dopaminergic markers, sparse NeuroD6 neurons expressed the vesicular glutamate transporter 2 (Vglut2) gene. To achieve manipulation of NeuroD6 VTA neurons, NeuroD6(NEX)-Cre-driven mouse genetics and optogenetics were implemented. First, expression of vesicular monoamine transporter 2 (VMAT2) was ablated to disrupt dopaminergic function in NeuroD6 VTA neurons. Comparing Vmat2(Cre)(lox/lox;NEX-) conditional knock-out (cKO) mice with littermate controls, it was evident that baseline locomotion, preference for sugar and ethanol, and place preference upon amphetamine-induced and cocaine-induced conditioning were similar between genotypes. However, locomotion upon repeated psychostimulant administration was significantly elevated above control levels in cKO mice. Second, optogenetic activation of NEX-Cre VTA neurons was shown to induce DA release and glutamatergic postsynaptic currents within the nucleus accumbens. Third, optogenetic stimulation of NEX-Cre VTA neurons in vivo induced significant place preference behavior, while stimulation of VTA neurons defined by Calretinin failed to cause a similar response. The results show that NeuroD6 VTA neurons exert distinct regulation over specific aspects of reward-related behavior, findings that contribute to the current understanding of VTA neurocircuitry.

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